TY  - JOUR
T1  - Human P2Y sub(6) Receptor: Molecular Modeling Leads to the Rational Design of a Novel Agonist Based on a Unique Conformational Preference
AN  - 19387457; 7158854
AB  - Combining molecular dynamics (MD) in a hydrated phospholipid (DOPC) bilayer, a Monte Carlo search, and synthesis of locked nucleotide analogues, we discovered that the Southern conformation of the ribose is preferred for ligand recognition by the P2Y sub(6) receptor. 2'-Deoxy-(S)-methanocarbaUDP was found to be a full agonist of the receptor and displayed a 10-fold higher potency than that for the corresponding flexible 2'-deoxyUDP. MD results also suggested a conformational change of the second extracellular loop consequent to agonist binding.
JF  - Journal of Medicinal Chemistry
AU  - Costanzi, S
AU  - Joshi, B V
AU  - Maddileti, S
AU  - Mamedova, L
AU  - Gonzalez-Moa, MJ
AU  - Marquez, V E
AU  - Harden, T K
AU  - Jacobson, KA
AD  - Computational Chemistry Core Laboratory and Molecular Recognition Section, NIDDK, National Institutes of Health, DHHS, Bethesda, Maryland 20892, USA
Y1  - 2005/12/29/
PY  - 2005
DA  - 2005 Dec 29
SP  - 8108
EP  - 8111
VL  - 48
IS  - 26
SN  - 0022-2623, 0022-2623
KW  - Biotechnology and Bioengineering Abstracts
KW  - Molecular modelling
KW  - Ribose
KW  - Purine P2Y receptors
KW  - Nucleotide analogs
KW  - Phospholipids
KW  - Conformation
KW  - W 30915:Pharmaceuticals & Vaccines
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19387457?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Medicinal+Chemistry&rft.atitle=Human+P2Y+sub%286%29+Receptor%3A+Molecular+Modeling+Leads+to+the+Rational+Design+of+a+Novel+Agonist+Based+on+a+Unique+Conformational+Preference&rft.au=Costanzi%2C+S%3BJoshi%2C+B+V%3BMaddileti%2C+S%3BMamedova%2C+L%3BGonzalez-Moa%2C+MJ%3BMarquez%2C+V+E%3BHarden%2C+T+K%3BJacobson%2C+KA&rft.aulast=Costanzi&rft.aufirst=S&rft.date=2005-12-29&rft.volume=48&rft.issue=26&rft.spage=8108&rft.isbn=&rft.btitle=&rft.title=Journal+of+Medicinal+Chemistry&rft.issn=00222623&rft_id=info:doi/10.1021%2Fjm050911p
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Nucleotide analogs; Purine P2Y receptors; Conformation; Ribose; Phospholipids; Molecular modelling
DO  - http://dx.doi.org/10.1021/jm050911p
ER  - 



TY  - JOUR
T1  - Semirational Design of (North)-Methanocarba Nucleosides as Dual Acting A sub(1) and A sub(3) Adenosine Receptor Agonists: Novel Prototypes for Cardioprotection
AN  - 19386734; 7158853
AB  - Ring-constrained adenosine analogues have been designed to act as dual agonists at tissue-protective A sub(1) and A sub(3) adenosine receptors (ARs). 9-Ribosides transformed into the ring-constrained (N)-methanocarba-2-chloro-5'-uronamides consistently lost affinity at A sub(1)/A sub(2A)ARs and gained at A sub(3)AR. Among 9-riboside derivatives, only N super(6)-cyclopentyl and 7-norbornyl moieties were extrapolated for mixed A sub(1)/A sub(3) selectivity and rat/human A sub(3)AR equipotency. Consequently, 2 was balanced in affinity and potency at A sub(1)/A sub(3)ARs as envisioned and dramatically protected in an intact heart model of global ischemia and reperfusion.
JF  - Journal of Medicinal Chemistry
AU  - Jacobson, KA
AU  - Gao, Z-G
AU  - Tchilibon, S
AU  - Duong, H T
AU  - Joshi, B V
AU  - Sonin, D
AU  - Liang, B T
AD  - Molecular Recognition Section, Laboratory of Bioorganic Chemistry, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland 20892, USA
Y1  - 2005/12/29/
PY  - 2005
DA  - 2005 Dec 29
SP  - 8103
EP  - 8107
VL  - 48
IS  - 26
SN  - 0022-2623, 0022-2623
KW  - Biotechnology and Bioengineering Abstracts
KW  - Heart
KW  - Reperfusion
KW  - Adenosine receptors
KW  - nucleosides
KW  - Ischemia
KW  - Models
KW  - W 30915:Pharmaceuticals & Vaccines
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19386734?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Medicinal+Chemistry&rft.atitle=Semirational+Design+of+%28North%29-Methanocarba+Nucleosides+as+Dual+Acting+A+sub%281%29+and+A+sub%283%29+Adenosine+Receptor+Agonists%3A+Novel+Prototypes+for+Cardioprotection&rft.au=Jacobson%2C+KA%3BGao%2C+Z-G%3BTchilibon%2C+S%3BDuong%2C+H+T%3BJoshi%2C+B+V%3BSonin%2C+D%3BLiang%2C+B+T&rft.aulast=Jacobson&rft.aufirst=KA&rft.date=2005-12-29&rft.volume=48&rft.issue=26&rft.spage=8103&rft.isbn=&rft.btitle=&rft.title=Journal+of+Medicinal+Chemistry&rft.issn=00222623&rft_id=info:doi/10.1021%2Fjm050726b
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Adenosine receptors; Ischemia; Reperfusion; Heart; nucleosides; Models
DO  - http://dx.doi.org/10.1021/jm050726b
ER  - 



TY  - JOUR
T1  - Antifungal Flavonoids from Hildegardia barteri
AN  - 19829804; 6674756
AB  - A new isoflavan, (3R)-6,2'-dihydroxy-7-methoxy-4',5'-methylenedioxyisoflavan, hildegardiol (1), and two known flavonoids, 2-hydroxymaackiain (2) and farrerol (3), were isolated from the antifungal root extract of Hildegardia barteri. The pterocarpan 2 was largely responsible for the observed antifungal activity.
JF  - Journal of Natural Products
AU  - Meragelman, T L
AU  - Tucker, K D
AU  - McCloud, T G
AU  - Cardellina, JH II
AU  - Shoemaker, R H
AD  - Screening Technologies Branch, Developmental Therapeutics Program, Division of Cancer Treatment and Diagnosis, and SAIC-Frederick, Inc., National Cancer Institute-Frederick, Frederick, Maryland 21702-1201, USA
Y1  - 2005/12/26/
PY  - 2005
DA  - 2005 Dec 26
SP  - 1790
EP  - 1792
VL  - 68
IS  - 12
SN  - 0163-3864, 0163-3864
KW  - Microbiology Abstracts C: Algology, Mycology & Protozoology; Microbiology Abstracts A: Industrial & Applied Microbiology
KW  - Flavonoids
KW  - Antifungal activity
KW  - Roots
KW  - natural products
KW  - K 03340:Effects of Physical & Chemical Factors
KW  - A 01067:Antifungal & fungicidal
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19829804?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologya&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Natural+Products&rft.atitle=Antifungal+Flavonoids+from+Hildegardia+barteri&rft.au=Meragelman%2C+T+L%3BTucker%2C+K+D%3BMcCloud%2C+T+G%3BCardellina%2C+JH+II%3BShoemaker%2C+R+H&rft.aulast=Meragelman&rft.aufirst=T&rft.date=2005-12-26&rft.volume=68&rft.issue=12&rft.spage=1790&rft.isbn=&rft.btitle=&rft.title=Journal+of+Natural+Products&rft.issn=01633864&rft_id=info:doi/10.1021%2Fnp0503000
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Flavonoids; Antifungal activity; Roots; natural products
DO  - http://dx.doi.org/10.1021/np0503000
ER  - 



TY  - JOUR
T1  - Hormonal contraceptive use, pregnancy and parity, and the risk of cervical intraepithelial neoplasia 3 among oncogenic HPV DNA-positive women with equivocal or mildly abnormal cytology.
AN  - 68731855; 15986443
AB  - Oral contraceptive (OC) use, hormonal contraceptive use and multiparity are potential risk factors for cervical precancer, cervical intraepithelial neoplasia 3 (CIN3), but a limited number of studies have adequately accounted for possible confounding effect of oncogenic human papillomavirus (HPV) infection. To examine the relationships of these factors with CIN3, we conducted an analysis of women (n = 5,060) with minimally abnormal Pap smears who were enrolled in the ASCUS and LSIL Triage Study (ALTS), a clinical trial to evaluate management strategies. Cervical specimens collected at enrollment were tested for HPV DNA using 2 methods. Multivariate logistics regression models were used to assess associations (odds ratio [OR] with 95% confidence intervals [CI]) of the potential risk factors (e.g., OC use and parity) with testing oncogenic HPV positive among controls (<CIN2) (n = 4,114) and with rigorously reviewed cases of CIN3 identified throughout the study (n = 499) among women with oncogenic HPV (n = 3,126). Only former oral contraceptive use (OR = 1.3, 95% CI = 1.0-1.7) was associated marginally with having an oncogenic HPV infection among controls. Restricted to women with oncogenic HPV, current injectable hormonal contraceptive users were at an elevated risk of CIN3 (OR = 1.6, 95% CI = 1.2-2.1) compared to women who never used them. Similarly, restricted to women with HPV16 infection, current users of injectable contraceptives were at a marginally elevated risk of CIN3 (OR = 1.5, 95% CI = 1.0-2.3) compared to women who never used them. Oral contraceptive use, Norplant (implantable hormonal contraceptive) use, a history of pregnancy, age at first pregnancy, lifetime numbers of pregnancies and lifetime numbers of live births were not associated with CIN3. We conclude that only current injectable hormonal contraceptive use slightly elevated the risk (approximately 50%) of CIN3 in this young and low parity population of women with oncogenic HPV and minimally abnormal Pap smears but further confirmation of this relationship is needed.
          Copyright 2005 Wiley-Liss, Inc
JF  - International journal of cancer
AU  - Castle, Philip E
AU  - Walker, Joan L
AU  - Schiffman, Mark
AU  - Wheeler, Cosette M
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, NIH, DHHS, Bethesda, MD 20892, USA. castlep@mail.nih.gov
Y1  - 2005/12/20/
PY  - 2005
DA  - 2005 Dec 20
SP  - 1007
EP  - 1012
VL  - 117
IS  - 6
SN  - 0020-7136, 0020-7136
KW  - Contraceptive Agents, Female
KW  - 0
KW  - Contraceptives, Oral
KW  - DNA, Viral
KW  - Levonorgestrel
KW  - 5W7SIA7YZW
KW  - Index Medicus
KW  - Contraceptives, Oral -- adverse effects
KW  - Prospective Studies
KW  - Logistic Models
KW  - Risk Factors
KW  - Humans
KW  - Injections
KW  - Levonorgestrel -- adverse effects
KW  - Female
KW  - Pregnancy
KW  - Parity
KW  - DNA, Viral -- analysis
KW  - Contraceptive Agents, Female -- adverse effects
KW  - Vaginal Smears
KW  - Papillomaviridae -- genetics
KW  - Contraceptive Agents, Female -- administration & dosage
KW  - Papanicolaou Test
KW  - Cervical Intraepithelial Neoplasia -- etiology
KW  - Cervical Intraepithelial Neoplasia -- epidemiology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68731855?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=International+journal+of+cancer&rft.atitle=Hormonal+contraceptive+use%2C+pregnancy+and+parity%2C+and+the+risk+of+cervical+intraepithelial+neoplasia+3+among+oncogenic+HPV+DNA-positive+women+with+equivocal+or+mildly+abnormal+cytology.&rft.au=Castle%2C+Philip+E%3BWalker%2C+Joan+L%3BSchiffman%2C+Mark%3BWheeler%2C+Cosette+M&rft.aulast=Castle&rft.aufirst=Philip&rft.date=2005-12-20&rft.volume=117&rft.issue=6&rft.spage=1007&rft.isbn=&rft.btitle=&rft.title=International+journal+of+cancer&rft.issn=00207136&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-14
N1  - Date created - 2005-10-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Truncation, Deamidation, and Oxidation of Histone H2B in Cells Cultured with Nickel(II)
AN  - 17070635; 6687654
AB  - Molecular mechanisms of nickel-induced carcinogenesis include interactions of Ni(II) cations with histones. Previously, we demonstrated in vitro and in cells that Ni(II) cleaved off the -SHHKAKGK C-terminal motif of histone H2A. In the present study, Western blotting of histones isolated from rat and human cell lines, cultured for 3-5 days with 0.05-0.5 mM Ni(II), revealed time- and dose-dependent appearance of a new band of histone H2B. This effect was also induced by Co(II), but not by Cu(II), Cd (II), and Zn(II). Mass spectrometry and amino acid sequencing of proteins from the new band allowed for identification of two derivatives of the major variant of histone H2B. The larger protein was histone H2B lacking 16 N-terminal amino acids. The smaller one was histone H2B which, in addition to being shortened at the N-terminus, had nine amino acids deleted from its C-terminus. At both termini, the truncation occurred between lysine and alanine in the two identical -KAVTK- repeats of histone H2B. Also, the truncated H2B proteins had their Q super(22) residues deamidated and M super(59) and M super(62) residues oxidized to sulfoxides, a signature of oxidative stress. The truncation did not concur with apoptosis. Its mechanism involved activation by Ni(II) treatment of specific nuclear proteolytic enzymes belonging to the calpain family. The terminal tails of core histones participate in structuring chromatin and regulating gene expression. Therefore, the observed truncation and other modifications of histone H2B may assist in Ni(II) carcinogenesis through epigenetic mechanisms.
JF  - Chemical Research in Toxicology
AU  - Karaczyn, A A
AU  - Golebiowski, F
AU  - Kasprzak, K S
AD  - Laboratory of Comparative Carcinogenesis, National Cancer Institute at Frederick, Frederick, Maryland 21702, USA
Y1  - 2005/12/19/
PY  - 2005
DA  - 2005 Dec 19
SP  - 1934
EP  - 1942
VL  - 18
IS  - 12
SN  - 0893-228X, 0893-228X
KW  - Biochemistry Abstracts 2: Nucleic Acids; Toxicology Abstracts
KW  - Western blotting
KW  - Molecular modelling
KW  - Apoptosis
KW  - Amino acids
KW  - Alanine
KW  - Chromatin
KW  - C-Terminus
KW  - Lysine
KW  - Mass spectroscopy
KW  - N-Terminus
KW  - Gene expression
KW  - Cations
KW  - Oxidative stress
KW  - epigenetics
KW  - Carcinogenesis
KW  - Oxidation
KW  - Calpain
KW  - Histone H2B
KW  - Histone H2A
KW  - Proteolytic enzymes
KW  - X 24165:Biochemistry
KW  - N 14835:Protein-Nucleic Acids Association
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17070635?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxicologyabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Chemical+Research+in+Toxicology&rft.atitle=Truncation%2C+Deamidation%2C+and+Oxidation+of+Histone+H2B+in+Cells+Cultured+with+Nickel%28II%29&rft.au=Karaczyn%2C+A+A%3BGolebiowski%2C+F%3BKasprzak%2C+K+S&rft.aulast=Karaczyn&rft.aufirst=A&rft.date=2005-12-19&rft.volume=18&rft.issue=12&rft.spage=1934&rft.isbn=&rft.btitle=&rft.title=Chemical+Research+in+Toxicology&rft.issn=0893228X&rft_id=info:doi/10.1021%2Ftx050122a
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-04-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Molecular modelling; Western blotting; Amino acids; Apoptosis; Chromatin; Alanine; C-Terminus; Lysine; Mass spectroscopy; N-Terminus; Gene expression; Cations; epigenetics; Oxidative stress; Oxidation; Carcinogenesis; Calpain; Histone H2B; Histone H2A; Proteolytic enzymes
DO  - http://dx.doi.org/10.1021/tx050122a
ER  - 



TY  - JOUR
T1  - A prospective study of meat and meat mutagens and prostate cancer risk.
AN  - 68900059; 16357191
AB  - High-temperature cooked meat contains heterocyclic amines, including 2-amino-1-methyl-6-phenylimidazo[4,5-b]pyridine (PhIP), and polycyclic aromatic hydrocarbons, such as benzo(a)pyrene (BaP). In rodents, a high intake of PhIP induces prostate tumors. We prospectively investigated the association between meat and meat mutagens, specifically PhIP, and prostate cancer risk in the Prostate, Lung, Colorectal, and Ovarian Cancer Screening Trial. Diet was assessed using a 137-item food frequency questionnaire and a detailed meat-cooking questionnaire linked to a database for BaP and the heterocyclic amines 2-amino-3,8-dimethylimidazo[4,5-b]quinoxaline (MeIQx), 2-amino-3,4,8-trimethylimidazo[4,5-f]quinoxaline (DiMeIQx), and PhIP. During follow-up, we ascertained a total of 1,338 prostate cancer cases among 29,361 men; of these, 868 were incident cases (diagnosed after the first year of follow-up) and 520 were advanced cases (stage III or IV or a Gleason score of > or =7). Total, red, or white meat intake was not associated with prostate cancer risk. More than 10 g/d of very well done meat, compared with no consumption, was associated with a 1.4-fold increased risk of prostate cancer [95% confidence interval (95% CI), 1.05-1.92] and a 1.7-fold increased risk (95% CI, 1.19-2.40) of incident disease. Although there was no association with MeIQx and DiMeIQx, the highest quintile of PhIP was associated with a 1.2-fold increased risk of prostate cancer (95% CI, 1.01-1.48) and a 1.3-fold increased risk of incident disease (95% CI, 1.01-1.61). In conclusion, very well done meat was positively associated with prostate cancer risk. In addition, this study lends epidemiologic support to the animal studies, which have implicated PhIP as a prostate carcinogen.
JF  - Cancer research
AU  - Cross, Amanda J
AU  - Peters, Ulrike
AU  - Kirsh, Victoria A
AU  - Andriole, Gerald L
AU  - Reding, Douglas
AU  - Hayes, Richard B
AU  - Sinha, Rashmi
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, NIH, Department of Health and Human Services, Bethesda, Maryland, USA. crossa@mail.nih.gov
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
SP  - 11779
EP  - 11784
VL  - 65
IS  - 24
SN  - 0008-5472, 0008-5472
KW  - Imidazoles
KW  - 0
KW  - Mutagens
KW  - Quinoxalines
KW  - Benzo(a)pyrene
KW  - 3417WMA06D
KW  - 2-amino-3,8-dimethylimidazo(4,5-f)quinoxaline
KW  - 77500-04-0
KW  - 2-amino-1-methyl-6-phenylimidazo(4,5-b)pyridine
KW  - 909C6UN66T
KW  - 3,4,8-trimethylimidazo(4,5-f)quinoxalin-2-amine
KW  - YRA7G7WU6P
KW  - Index Medicus
KW  - Quinoxalines -- chemistry
KW  - Quinoxalines -- adverse effects
KW  - Prospective Studies
KW  - Risk Factors
KW  - Humans
KW  - Surveys and Questionnaires
KW  - Benzo(a)pyrene -- chemistry
KW  - Aged
KW  - Middle Aged
KW  - Benzo(a)pyrene -- adverse effects
KW  - Male
KW  - Imidazoles -- adverse effects
KW  - Imidazoles -- chemistry
KW  - Prostatic Neoplasms -- etiology
KW  - Meat
KW  - Prostatic Neoplasms -- epidemiology
KW  - Mutagens -- adverse effects
KW  - Cooking
KW  - Diet
KW  - Mutagens -- chemistry
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cancer+research&rft.atitle=A+prospective+study+of+meat+and+meat+mutagens+and+prostate+cancer+risk.&rft.au=Cross%2C+Amanda+J%3BPeters%2C+Ulrike%3BKirsh%2C+Victoria+A%3BAndriole%2C+Gerald+L%3BReding%2C+Douglas%3BHayes%2C+Richard+B%3BSinha%2C+Rashmi&rft.aulast=Cross&rft.aufirst=Amanda&rft.date=2005-12-15&rft.volume=65&rft.issue=24&rft.spage=11779&rft.isbn=&rft.btitle=&rft.title=Cancer+research&rft.issn=00085472&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-23
N1  - Date created - 2005-12-16
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Upregulation of estrogen receptor expression in the uterus of ovariectomized B6C3F1 mice and Ishikawa cells treated with bromoethane.
AN  - 68865104; 15922381
AB  - In a 2-year NTP bioassay, Bromoethane (BE) was found to induce endometrial neoplasms in the uterus of B6C3F1 mice [; ]. In women, hormonal influences, such as "unopposed" estrogenic stimulus, have been implicated as important etiologic factors in uterine cancer. BE, however, does not affect the serum concentrations of sex hormones in female B6C3F1 mice [] and the mechanism of BE-induced uterine carcinogenesis still remains unclear. In the present study, we examined the estrogenic effects of BE on the uterus of ovariectomized B6C3F1 mice and on Ishikawa cells. Groups of 6 mice were given daily s.c. injections of 0, 100, 500 or 1000 mg BE/kg for 3 consecutive days. Mice treated with 17beta-estradiol served as positive controls. Mice were necropsied 24 h after the final injection, and uteri were weighed and examined histologically and immunohistochemically along with the vagina. Changes observed in the estrogen-treated mice included increased uterine weights, edema and inflammation of the endometrium, increased epithelial layers of the uterine and vaginal lumens and keratinization of the vaginal epithelium. In the BE-treated mice, no such changes occurred; however, immunohistochemical staining of the uterus revealed a significant increase in immunoexpression of the estrogen receptor alpha (ERalpha) in the two higher dose groups. Analysis of mRNA also showed slightly increased uterine ERalpha expression in these groups. Upregulated expression of ERalpha was confirmed in BE-treated Ishikawa cells, in which Western blotting analyses identified an intense signal at approximately 66 kDa, which is consistent with ERalpha. These data suggest that upregulated expression of ERalpha may be important in the induction of endometrial neoplasms in BE-treated mice.
JF  - Toxicology and applied pharmacology
AU  - Aoyama, Hiroaki
AU  - Couse, John F
AU  - Hewitt, Sylvia C
AU  - Haseman, Joseph K
AU  - He, Hong
AU  - Zheng, Xiaolin
AU  - Majstoravich, Sonja
AU  - Korach, Kenneth S
AU  - Dixon, D
AD  - Laboratory of Experimental Pathology, National Institute of Environmental Health Sciences, P.O. Box 12233, MD C2-09, Research Triangle Park, NC 27709, USA.
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
SP  - 226
EP  - 235
VL  - 209
IS  - 3
SN  - 0041-008X, 0041-008X
KW  - Estrogen Receptor alpha
KW  - 0
KW  - Hydrocarbons, Brominated
KW  - Proliferating Cell Nuclear Antigen
KW  - Estradiol
KW  - 4TI98Z838E
KW  - Hypoxanthine Phosphoribosyltransferase
KW  - EC 2.4.2.8
KW  - Ribonucleases
KW  - EC 3.1.-
KW  - bromoethane
KW  - LI8384T9PH
KW  - Index Medicus
KW  - Animals
KW  - Endometritis -- chemically induced
KW  - Ribonucleases -- antagonists & inhibitors
KW  - Dose-Response Relationship, Drug
KW  - Estradiol -- pharmacology
KW  - Hypoxanthine Phosphoribosyltransferase -- metabolism
KW  - Proliferating Cell Nuclear Antigen -- analysis
KW  - Mice
KW  - Cell Line, Tumor
KW  - Ribonucleases -- metabolism
KW  - Mice, Inbred Strains
KW  - Blotting, Western
KW  - Endometrium -- drug effects
KW  - Up-Regulation -- drug effects
KW  - Endometrium -- chemistry
KW  - Injections, Subcutaneous
KW  - Endometrium -- pathology
KW  - Immunochemistry -- methods
KW  - Endometritis -- pathology
KW  - Female
KW  - Organ Size -- drug effects
KW  - Uterus -- metabolism
KW  - Estrogen Receptor alpha -- biosynthesis
KW  - Hydrocarbons, Brominated -- administration & dosage
KW  - Ovariectomy
KW  - Uterus -- drug effects
KW  - Hydrocarbons, Brominated -- toxicity
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68865104?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Toxicology+and+applied+pharmacology&rft.atitle=Upregulation+of+estrogen+receptor+expression+in+the+uterus+of+ovariectomized+B6C3F1+mice+and+Ishikawa+cells+treated+with+bromoethane.&rft.au=Aoyama%2C+Hiroaki%3BCouse%2C+John+F%3BHewitt%2C+Sylvia+C%3BHaseman%2C+Joseph+K%3BHe%2C+Hong%3BZheng%2C+Xiaolin%3BMajstoravich%2C+Sonja%3BKorach%2C+Kenneth+S%3BDixon%2C+D&rft.aulast=Aoyama&rft.aufirst=Hiroaki&rft.date=2005-12-15&rft.volume=209&rft.issue=3&rft.spage=226&rft.isbn=&rft.btitle=&rft.title=Toxicology+and+applied+pharmacology&rft.issn=0041008X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-17
N1  - Date created - 2005-12-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Prednisolone pharmacokinetics in the presence and absence of ritonavir after oral prednisone administration to healthy volunteers.
AN  - 68796678; 16284534
AB  - Corticosteroid therapy has been associated with bone toxicities (eg, osteonecrosis) and Cushing syndrome in HIV-infected patients; this may be partially attributable to a pharmacokinetic drug interaction between HIV protease inhibitors and corticosteroids. The purpose of this study was to characterize the influence of low-dose ritonavir on prednisolone pharmacokinetics in healthy subjects. Ten HIV-seronegative volunteers were given single oral doses of prednisone, 20 mg, before (baseline) and after receiving ritonavir, 200 mg, twice daily for 4 and 14 days. After each prednisone dose, serial blood samples were collected and prednisolone concentrations were determined; pharmacokinetic parameter values were compared between the groups. Geometric mean ratios (GMRs, 90% confidence interval [CI]) of the prednisolone area under the plasma concentration versus time curve (AUC0-infinity) after 4 and 14 days of ritonavir versus baseline were 1.41 (90% CI: 1.08 to 1.74) and 1.30 (90% CI: 1.09 to 1.49), respectively (P = 0.002 and P = 0.004, respectively). GMRs of prednisolone apparent oral clearance (Cl/F) were 0.71 (09% CI: 0.57 to 0.93) and 0.77 (90% CI: 0.67 to 0.92) after 4 and 14 days of ritonavir versus baseline, respectively (P = 0.0004 and P = 0.0003, respectively). Ritonavir significantly increased the systemic exposure of prednisolone in healthy subjects. Results from this investigation suggest that corticosteroid exposure is likely elevated in HIV-infected patients receiving protease inhibitors.
JF  - Journal of acquired immune deficiency syndromes (1999)
AU  - Penzak, Scott R
AU  - Formentini, Elizabeth
AU  - Alfaro, Raul M
AU  - Long, Michael
AU  - Natarajan, Ven
AU  - Kovacs, Joseph
AD  - Warren G. Magnuson Clinical Center, Pharmacy Department, National Institutes of Health, Bethesda, MD 20892, USA. Spenzak@mail.cc.nih.gov
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
SP  - 573
EP  - 580
VL  - 40
IS  - 5
SN  - 1525-4135, 1525-4135
KW  - Glucocorticoids
KW  - 0
KW  - HIV Protease Inhibitors
KW  - Prednisolone
KW  - 9PHQ9Y1OLM
KW  - Ritonavir
KW  - O3J8G9O825
KW  - Index Medicus
KW  - AIDS/HIV
KW  - Drug Interactions
KW  - Area Under Curve
KW  - Humans
KW  - Adult
KW  - HIV Seronegativity
KW  - Male
KW  - Female
KW  - Prednisolone -- pharmacokinetics
KW  - Glucocorticoids -- pharmacokinetics
KW  - Ritonavir -- pharmacokinetics
KW  - Ritonavir -- pharmacology
KW  - Glucocorticoids -- administration & dosage
KW  - Ritonavir -- administration & dosage
KW  - HIV Protease Inhibitors -- pharmacology
KW  - HIV Protease Inhibitors -- pharmacokinetics
KW  - Prednisolone -- administration & dosage
KW  - HIV Protease Inhibitors -- administration & dosage
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68796678?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+acquired+immune+deficiency+syndromes+%281999%29&rft.atitle=Prednisolone+pharmacokinetics+in+the+presence+and+absence+of+ritonavir+after+oral+prednisone+administration+to+healthy+volunteers.&rft.au=Penzak%2C+Scott+R%3BFormentini%2C+Elizabeth%3BAlfaro%2C+Raul+M%3BLong%2C+Michael%3BNatarajan%2C+Ven%3BKovacs%2C+Joseph&rft.aulast=Penzak&rft.aufirst=Scott&rft.date=2005-12-15&rft.volume=40&rft.issue=5&rft.spage=573&rft.isbn=&rft.btitle=&rft.title=Journal+of+acquired+immune+deficiency+syndromes+%281999%29&rft.issn=15254135&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-23
N1  - Date created - 2005-11-14
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Uptake and Trafficking of Exogenous Sterol in Saccharomyces Cerevisiae
T2  - 2005 Biochemical Society Focused Meeting on Non-Vesicular Intracellular Traffic
AN  - 39824813; 4040165
JF  - 2005 Biochemical Society Focused Meeting on Non-Vesicular Intracellular Traffic
AU  - Prinz, Will
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Sterols
KW  - Saccharomyces cerevisiae
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+consulting+and+clinical+psychology&rft.atitle=A+new+tool+to+assess+treatment+fidelity+and+evaluation+of+treatment+fidelity+across+10+years+of+health+behavior+research&rft.au=Borrelli%2C+Belinda%3BSepinwall%2C+Deborah%3BErnst%2C+Denise%3BBellg%2C+Albert+J%3BCzajkowski%2C+Susan%3BBreger%2C+Rosemary%3BDeFrancesco%2C+Carol%3BLevesque%2C+Chantal%3BSharp%2C+Daryl+L%3BOgedegbe%2C+Gbenga%3BResnick%2C+Barbara%3BOrwig%2C+Denise&rft.aulast=Borrelli&rft.aufirst=Belinda&rft.date=2005-10-01&rft.volume=73&rft.issue=5&rft.spage=852&rft.isbn=&rft.btitle=&rft.title=Journal+of+consulting+and+clinical+psychology&rft.issn=0022006X&rft_id=info:doi/10.1037%2F0022-006X.73.5.852
L2  - http://www.biochemistry.org/meetings/programme.cfm?Meeting_No=SA053
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Amazing Versatility of Proteins - Structural Polymorphism and Evolution
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39823201; 4060133
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Gronenborn, A M
AU  - Byeon, I L
AU  - Louis, J M
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Gene polymorphism
KW  - Evolution
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39823201?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=The+Amazing+Versatility+of+Proteins+-+Structural+Polymorphism+and+Evolution&rft.au=Gronenborn%2C+A+M%3BByeon%2C+I+L%3BLouis%2C+J+M&rft.aulast=Gronenborn&rft.aufirst=A&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Direct Effects of Ionizing Radiation on Supercoiled Plasmid DNA
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39808881; 4060927
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Kempner, E S
AU  - Anchordoquy, T
AU  - Molina, M
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Ionizing radiation
KW  - Plasmids
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39808881?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Direct+Effects+of+Ionizing+Radiation+on+Supercoiled+Plasmid+DNA&rft.au=Kempner%2C+E+S%3BAnchordoquy%2C+T%3BMolina%2C+M&rft.aulast=Kempner&rft.aufirst=E&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Solution Structure of the Phosphoryl Transfer Complex Between the Cytoplasmic A Domain and B Domain of the Mannitol Transporter II: Mannitol of the E. Coli Phosphotransferase System
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39808578; 4058040
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Suh, J
AU  - Cai, M
AU  - Williams Jr, D
AU  - Clore, M
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Mannitol
KW  - Phosphotransferase
KW  - Escherichia coli
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39808578?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Solution+Structure+of+the+Phosphoryl+Transfer+Complex+Between+the+Cytoplasmic+A+Domain+and+B+Domain+of+the+Mannitol+Transporter+II%3A+Mannitol+of+the+E.+Coli+Phosphotransferase+System&rft.au=Suh%2C+J%3BCai%2C+M%3BWilliams+Jr%2C+D%3BClore%2C+M&rft.aulast=Suh&rft.aufirst=J&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Continued Importance of Medicinal Plants and International Collaboration in the Discovery of Novel Drug Leads
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39806338; 4064226
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Cragg, G M
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Medicinal plants
KW  - Drug discovery
KW  - Lead
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39806338?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Continued+Importance+of+Medicinal+Plants+and+International+Collaboration+in+the+Discovery+of+Novel+Drug+Leads&rft.au=Cragg%2C+G+M&rft.aulast=Cragg&rft.aufirst=G&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Visualizing Structural Dynamics in Proteins withPicosecond Time-Resolved Laue Crystallography
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39784870; 4064466
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Anfinrud, P
AU  - Schotte, F
AU  - Hummer, G
AU  - Wulff, M
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Crystallography
KW  - Structural dynamics
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39784870?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Visualizing+Structural+Dynamics+in+Proteins+withPicosecond+Time-Resolved+Laue+Crystallography&rft.au=Anfinrud%2C+P%3BSchotte%2C+F%3BHummer%2C+G%3BWulff%2C+M&rft.aulast=Anfinrud&rft.aufirst=P&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Chromatographic Chiral Recognition on Immobilized Cellular Membrane-based Stationary Phase: The Enantioselective Binding of Noncompetitive Inhibitors to Neuronal Nicotinic Acetylcholine Receptors
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39780037; 4059238
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Wainer, I W
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Acetylcholine receptors (nicotinic)
KW  - Stationary phase
KW  - Neurotransmitters
KW  - Inhibitors
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39780037?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Chromatographic+Chiral+Recognition+on+Immobilized+Cellular+Membrane-based+Stationary+Phase%3A+The+Enantioselective+Binding+of+Noncompetitive+Inhibitors+to+Neuronal+Nicotinic+Acetylcholine+Receptors&rft.au=Tarran%2C+Robert%3BButton%2C+Brian%3BPicher%2C+Maryse%3BParadiso%2C+Anthony+M%3BRibeiro%2C+Carla+M%3BLazarowski%2C+Eduardo+R%3BZhang%2C+Liqun%3BCollins%2C+Peter+L%3BPickles%2C+Raymond+J%3BFredberg%2C+Jeffrey+J%3BBoucher%2C+Richard+C&rft.aulast=Tarran&rft.aufirst=Robert&rft.date=2005-10-01&rft.volume=280&rft.issue=42&rft.spage=35751&rft.isbn=&rft.btitle=&rft.title=Journal+of+Biological+Chemistry&rft.issn=00219258&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - NIH Dietary Supplements Methods and Reference Materials Program
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39777812; 4058646
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Betz, J M
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Dietary supplements
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39777812?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=NIH+Dietary+Supplements+Methods+and+Reference+Materials+Program&rft.au=Betz%2C+J+M&rft.aulast=Betz&rft.aufirst=J&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Recent Developments with Anti-HIV Cyclotides and Other Naturally Occurring Cyclized Peptides"
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39775900; 4060136
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Gustafson, K
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Peptides
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39775900?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Recent+Developments+with+Anti-HIV+Cyclotides+and+Other+Naturally+Occurring+Cyclized+Peptides%22&rft.au=Gustafson%2C+K&rft.aulast=Gustafson&rft.aufirst=K&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Comparison of an Open Tubular Column Containing Immobilized P-glycoprotein with Caco-2 Cell Monolayers for the Identification of Pgp Substrates
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39773250; 4059052
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Wainer, I W
AU  - Moaddel, R
AU  - Bullock, P
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - P-Glycoprotein
KW  - Monomolecular films
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - HIV-1 Integrase Inhibitor Development Based on Model of Full-Length HIV-1 Integrase Complexed with Viral DNA
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39772741; 4059646
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Nicklaus, M C
AU  - Karki, R G
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Integrase
KW  - Models
KW  - Inhibitors
KW  - Human immunodeficiency virus 1
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - New Molecular Target Modulating Metabolites from Marine Sponges and Bryozoans
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39769995; 4063612
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Gustafson, K
AU  - Oku, N
AU  - Milanowski, D
AU  - McMahon, J
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Porifera
KW  - Metabolites
KW  - Marine invertebrates
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Chemotherapeutic Potentiation of Targeted a-Particle Therapy
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39764645; 4067400
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Brechbiel, M
AU  - Milenic, D
AU  - Garmestani, K
AU  - Abdulla, A
AU  - Overstreet, T
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Potentiation
KW  - Therapy
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39764645?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Value of Natural Products as Leads to Drug Candidates
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39762796; 4058002
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Newman, D J
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Drugs
KW  - Natural products
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39762796?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Value+of+Natural+Products+as+Leads+to+Drug+Candidates&rft.au=Newman%2C+D+J&rft.aulast=Newman&rft.aufirst=D&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Structure, Dynamics and Function of Water in Hydrophobic Confinement
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39757041; 4065375
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Hummer, G
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Structure-function relationships
KW  - Hydrophobicity
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39757041?accountid=14244
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L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Marine Natural Products in Current Screening Approaches at the National Cancer Institute
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39754226; 4063037
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Cardellina, J H
AU  - Scudiero, D A
AU  - McCloud, T G
AU  - Shoemaker, R H
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Cancer
KW  - Natural products
KW  - Screening
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39754226?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Marine+Natural+Products+in+Current+Screening+Approaches+at+the+National+Cancer+Institute&rft.au=Cardellina%2C+J+H%3BScudiero%2C+D+A%3BMcCloud%2C+T+G%3BShoemaker%2C+R+H&rft.aulast=Cardellina&rft.aufirst=J&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Examining Reaction Processes in Macromolecular Systems
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39746039; 4065634
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Woodcock, H L
AU  - Hodoscek, M
AU  - Brooks, B R
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Macromolecules
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39746039?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Examining+Reaction+Processes+in+Macromolecular+Systems&rft.au=Woodcock%2C+H+L%3BHodoscek%2C+M%3BBrooks%2C+B+R&rft.aulast=Woodcock&rft.aufirst=H&rft.date=2005-12-15&rft.volume=&rft.issue=19&rft.spage=6862&rft.isbn=&rft.btitle=&rft.title=Journal+of+Bacteriology&rft.issn=00219193&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Fish are Contaminated with Mercury and PCBs: Collaborating with the Hmong Community in Milwaukee to Communicate the Risks and Benefits of Local Fish Consumption
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39721561; 4058648
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Petering, D H
AU  - Kiatousaysy, L
AU  - McAvoy, P
AU  - Rostenkowski, A
AU  - Weber, D
AU  - Gallun, T
AU  - Dellinger, J
AU  - Driscoll, M
AU  - Percy, S
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - USA, Wisconsin, Milwaukee
KW  - Pisces
KW  - Heavy metals
KW  - Mercury
KW  - PCB
KW  - Polychlorinated biphenyls
KW  - Fish consumption
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39721561?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Fish+are+Contaminated+with+Mercury+and+PCBs%3A+Collaborating+with+the+Hmong+Community+in+Milwaukee+to+Communicate+the+Risks+and+Benefits+of+Local+Fish+Consumption&rft.au=Petering%2C+D+H%3BKiatousaysy%2C+L%3BMcAvoy%2C+P%3BRostenkowski%2C+A%3BWeber%2C+D%3BGallun%2C+T%3BDellinger%2C+J%3BDriscoll%2C+M%3BPercy%2C+S&rft.aulast=Petering&rft.aufirst=D&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Weak Alignment Offers New Opportunities in NMR Structure Determination
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39720494; 4059971
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Bax, A
AU  - Grishaev, A
AU  - Bryce, D
AU  - Jaroniec, C
AU  - Wu, J.
AU  - Baber, J
AU  - Ulmer, T
AU  - Delaglio, F
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - N.M.R.
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39720494?accountid=14244
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L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Role and Value of Natural Products
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39719901; 4057895
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Newman, D J
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Natural products
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39719901?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Bacteriology&rft.atitle=Role+of+RcsF+in+Signaling+to+the+Rcs+Phosphorelay+Pathway+in+Escherichia+coli&rft.au=Majdalani%2C+Nadim%3BHeck%2C+Michael%3BStout%2C+Valerie%3BGottesman%2C+Susan&rft.aulast=Majdalani&rft.aufirst=Nadim&rft.date=2005-10-01&rft.volume=187&rft.issue=19&rft.spage=6770&rft.isbn=&rft.btitle=&rft.title=Journal+of+Bacteriology&rft.issn=00219193&rft_id=info:doi/
L2  - http://www.pacifichem.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Mechanism of Sonodynamic Therapy of Cancer Cells
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39711926; 4059452
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Miyoshi, N
AU  - Sostaric, J Z
AU  - Tuziuti, T
AU  - Kyuichi, Y
AU  - Iida, Y
AU  - Peter, R
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Cancer
KW  - Therapy
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39711926?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.atitle=Mechanism+of+Sonodynamic+Therapy+of+Cancer+Cells&rft.au=Miyoshi%2C+N%3BSostaric%2C+J+Z%3BTuziuti%2C+T%3BKyuichi%2C+Y%3BIida%2C+Y%3BPeter%2C+R&rft.aulast=Miyoshi&rft.aufirst=N&rft.date=2005-12-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+International+Chemical+Congress+of+Pacific+Basin+Societies+%28PACIFICHEM+2005%29&rft.issn=&rft_id=info:doi/
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Marine Natural Products: Inhibitors in Infectious Diseases
T2  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AN  - 39708302; 4063044
JF  - 2005 International Chemical Congress of Pacific Basin Societies (PACIFICHEM 2005)
AU  - Bewley, C
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
KW  - Infectious diseases
KW  - Natural products
KW  - Inhibitors
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39708302?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Progress and New Directions in Genetics of Tuberculosis: An NHLBI Working Group Report
AN  - 199606419; 16192449
AB  - Tuberculosis (TB), along with AIDS and malaria, is one of the three major killers among infectious diseases. New approaches to preventing, diagnosing, and curing TB are needed, which depend on a better understanding of Mycobacterium tuberculosis and the host. The National Heart, Lung, and Blood Institute convened a working group to develop recommendations for future TB research, including genetic aspects of the disease. The following areas were identified: (1) animal model research to improve understanding of persistence, reactivation, and granulomatous reactions; (2) preclinical studies aimed at shortening treatment of TB; (3) new resources for manipulating and characterizing the M. tuberculosis genome, proteome chips for more specific diagnoses, and studies of genes that appear to be essential but whose functions are not known; (4) prospective studies associated with clinical trials in populations with or at risk of TB to advance development of diagnostics and prognostics; (5) new quantitative and bioinformatic approaches to study the interaction between M. tuberculosis and the infected host and how this influences the infection process; (6) molecular characterization of M. tuberculosis genome diversity and phylogenetic analysis; (7) coordinated studies of human genome scans; (8) genetic epidemiology studies; (9) activities to foster knowledge dissemination, education, and training; and (10) coordination between the National Institutes of Health, the Gates Foundation, the Global Alliance for Tuberculosis Drug Development, and other organizations.
JF  - American Journal of Respiratory and Critical Care Medicine
AU  - Smith, Issar
AU  - Nathan, Carl
AU  - Peavy, Hannah H
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
SP  - 1491
EP  - 6
CY  - New York
PB  - American Thoracic Society
VL  - 172
IS  - 12
SN  - 1073449X
KW  - Medical Sciences--Respiratory Diseases
KW  - Animals
KW  - Tuberculosis -- therapy
KW  - Humans
KW  - Tuberculosis -- physiopathology
KW  - Biomedical Research -- trends
KW  - Tuberculosis -- genetics
KW  - Mycobacterium tuberculosis -- genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/199606419?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ahealthcompleteshell&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=American+Journal+of+Respiratory+and+Critical+Care+Medicine&rft.atitle=Progress+and+New+Directions+in+Genetics+of+Tuberculosis%3A+An+NHLBI+Working+Group+Report&rft.au=Smith%2C+Issar%3BNathan%2C+Carl%3BPeavy%2C+Hannah+H&rft.aulast=Smith&rft.aufirst=Issar&rft.date=2005-12-15&rft.volume=172&rft.issue=12&rft.spage=1491&rft.isbn=&rft.btitle=&rft.title=American+Journal+of+Respiratory+and+Critical+Care+Medicine&rft.issn=1073449X&rft_id=info:doi/
LA  - English
DB  - ProQuest Central
N1  - Copyright - Copyright American Thoracic Society Dec 15, 2005
N1  - Last updated - 2017-01-07
ER  - 



TY  - JOUR
T1  - Biological, cellular, and molecular characteristics of an inducible transgenic skin tumor model: a review
AN  - 19742040; 6687887
AB  - The genetically initiated Tg.AC transgenic mouse carries a transgene consisting of an oncogenic v-Ha-ras coding region flanked 5' by a mouse xi -globin promoter and 3' by an SV-40 polyadenylation sequence. Located on chromosome 11, the transgene is transcriptionally silent until activated by chemical carcinogens, UV light, or full-thickness wounding. Expression of the transgene is an early event that drives cellular proliferation resulting in clonal expansion and tumor formation, the unique characteristics now associated with the Tg.AC mouse. This ras-dependent phenotype has resulted in the widespread interest and use of the Tg.AC mouse in experimental skin carcinogenesis and as an alternative carcinogenesis assay. This review examines the general biology of the tumorigenic responses observed in Tg.AC mice, the genetic interactions of the ras transgene, and explores the cellular and molecular regulation of xi -globin promoted transgene expression. As a prototype alternative model to the current long-term rodent bioassays, the Tg.AC has generated a healthy discussion on the future of transgenic bioassays, and opened the doors for subsequent models for toxicity testing. The further exploration and elucidation of the molecular controls of transgene expression will enhance the usefulness of this mouse and enable a better understanding of the Tg. AC's discriminate response to chemical carcinogens.
JF  - Oncogene
AU  - Humble, M C
AU  - Trempus, C S
AU  - Spalding, J W
AU  - Cannon, R E
AU  - Tennant, R W
AD  - National Center for Toxicogenomics, National Institute of Environmental Health Sciences, PO Box 12233, MD F1-05, 111 Alexander Drive, Research Triangle Park, NC 27709, USA
Y1  - 2005/12/15/
PY  - 2005
DA  - 2005 Dec 15
SP  - 8217
EP  - 8228
VL  - 24
IS  - 56
SN  - 0950-9232, 0950-9232
KW  - Genetics Abstracts; Biotechnology and Bioengineering Abstracts; Oncogenes & Growth Factors Abstracts
KW  - Ras protein
KW  - chromosome 11
KW  - Molecular modelling
KW  - Skin
KW  - Animal models
KW  - Skin cancer
KW  - Transcription
KW  - Polyadenylation
KW  - Carcinogens
KW  - Tumors
KW  - Transgenic mice
KW  - Promoters
KW  - Globins
KW  - U.V. radiation
KW  - Ha-Ras protein
KW  - Reviews
KW  - Carcinogenesis
KW  - Exploration
KW  - Toxicity testing
KW  - Wounding
KW  - W 30925:Genetic Engineering
KW  - B 26130:Ras and Ras related oncogenes (Rho/Rac/Ral)
KW  - G 07870:Mammals
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19742040?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Oncogene&rft.atitle=Biological%2C+cellular%2C+and+molecular+characteristics+of+an+inducible+transgenic+skin+tumor+model%3A+a+review&rft.au=Humble%2C+M+C%3BTrempus%2C+C+S%3BSpalding%2C+J+W%3BCannon%2C+R+E%3BTennant%2C+R+W&rft.aulast=Humble&rft.aufirst=M&rft.date=2005-12-15&rft.volume=24&rft.issue=56&rft.spage=8217&rft.isbn=&rft.btitle=&rft.title=Oncogene&rft.issn=09509232&rft_id=info:doi/10.1038%2Fsj.onc.1209000
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-01-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Ras protein; Molecular modelling; chromosome 11; Skin; Animal models; Transcription; Skin cancer; Polyadenylation; Tumors; Carcinogens; Transgenic mice; Globins; Promoters; U.V. radiation; Reviews; Ha-Ras protein; Carcinogenesis; Exploration; Toxicity testing; Wounding
DO  - http://dx.doi.org/10.1038/sj.onc.1209000
ER  - 



TY  - JOUR
T1  - Cardiovascular phenotyping of fetal mice by noninvasive high-frequency ultrasound facilitates recovery of ENU-induced mutations causing congenital cardiac and extracardiac defects.
AN  - 68896708; 16174781
AB  - As part of a large-scale noninvasive fetal ultrasound screen to recover ethylnitrosourea (ENU)-induced mutations causing congenital heart defects in mice, we established a high-throughput ultrasound scanning strategy for interrogating fetal mice in utero utilizing three orthogonal imaging planes defined by the fetus' vertebral column and body axes, structures readily seen by ultrasound. This contrasts with the difficulty of acquiring clinical ultrasound imaging planes which are defined by the fetal heart. By use of the three orthogonal imaging planes for two-dimensional (2D) imaging together with color flow, spectral Doppler, and M-mode imaging, all of the major elements of the heart can be evaluated. In this manner, 10,091 ENU-mutagenized mouse fetuses were ultrasound scanned between embryonic days 12.5 and 19.5, with 324 fetuses found to die prenatally and 425 exhibiting cardiovascular defects. Further analysis by necropsy and histology showed heart defects that included conotruncal anomalies, obstructive lesions, and shunt lesions as well as other complex heart diseases. Ultrasound imaging also identified craniofacial/head defects and body wall closure defects, which necropsy revealed as encephalocele, holoprosencephaly, omphalocele, or gastroschisis. Genome scanning mapped one ENU-induced mutation associated with persistence truncus arteriosus and holoprosencephaly to mouse chromosome 2, while another mutation associated with cardiac defects and omphalocele was mapped to mouse chromosome 17. These studies show the efficacy of this novel ultrasound scanning strategy for noninvasive ultrasound phenotyping to facilitate the recovery of ENU-induced mutations causing congenital heart defects and other extracardiac anomalies.
JF  - Physiological genomics
AU  - Shen, Yuan
AU  - Leatherbury, L
AU  - Rosenthal, J
AU  - Yu, Qing
AU  - Pappas, M A
AU  - Wessels, A
AU  - Lucas, J
AU  - Siegfried, B
AU  - Chatterjee, B
AU  - Svenson, Karen
AU  - Lo, C W
AD  - Laboratory of Developmental Biology, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, Maryland 20892-8019, USA.
Y1  - 2005/12/14/
PY  - 2005
DA  - 2005 Dec 14
SP  - 23
EP  - 36
VL  - 24
IS  - 1
KW  - Ethylnitrosourea
KW  - P8M1T4190R
KW  - Index Medicus
KW  - Animals
KW  - Mice
KW  - Female
KW  - Pregnancy
KW  - Fetus -- radiation effects
KW  - Cardiovascular Physiological Phenomena
KW  - Ultrasonography, Prenatal
KW  - Heart Defects, Congenital -- diagnostic imaging
KW  - Ethylnitrosourea -- toxicity
KW  - Abnormalities, Multiple -- embryology
KW  - Heart Defects, Congenital -- embryology
KW  - Abnormalities, Multiple -- diagnostic imaging
KW  - Mutation
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68896708?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Physiological+genomics&rft.atitle=Cardiovascular+phenotyping+of+fetal+mice+by+noninvasive+high-frequency+ultrasound+facilitates+recovery+of+ENU-induced+mutations+causing+congenital+cardiac+and+extracardiac+defects.&rft.au=Shen%2C+Yuan%3BLeatherbury%2C+L%3BRosenthal%2C+J%3BYu%2C+Qing%3BPappas%2C+M+A%3BWessels%2C+A%3BLucas%2C+J%3BSiegfried%2C+B%3BChatterjee%2C+B%3BSvenson%2C+Karen%3BLo%2C+C+W&rft.aulast=Shen&rft.aufirst=Yuan&rft.date=2005-12-14&rft.volume=24&rft.issue=1&rft.spage=23&rft.isbn=&rft.btitle=&rft.title=Physiological+genomics&rft.issn=1531-2267&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-02
N1  - Date created - 2005-12-15
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Role of Telomeres in Cancer and Aging: A Matter of Bad Ends
T2  - 2005 Conference on Genes and Cancer
AN  - 39782539; 4055496
JF  - 2005 Conference on Genes and Cancer
AU  - Blasco, Maria
Y1  - 2005/12/12/
PY  - 2005
DA  - 2005 Dec 12
KW  - Aging
KW  - Cancer
KW  - Telomeres
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39782539?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Conference+on+Genes+and+Cancer&rft.atitle=Role+of+Telomeres+in+Cancer+and+Aging%3A+A+Matter+of+Bad+Ends&rft.au=Blasco%2C+Maria&rft.aulast=Blasco&rft.aufirst=Maria&rft.date=2005-12-12&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Conference+on+Genes+and+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://science.cancerresearchuk.org/genes_and_cancer/2005/programme?version =3
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The TGF-b System in Breast Cancer: A Double-Edged Sword
T2  - 2005 Conference on Genes and Cancer
AN  - 39730389; 4055489
JF  - 2005 Conference on Genes and Cancer
AU  - Wakefield, Lalage
Y1  - 2005/12/12/
PY  - 2005
DA  - 2005 Dec 12
KW  - Breast cancer
KW  - Transforming growth factor-^b
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39730389?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Conference+on+Genes+and+Cancer&rft.atitle=The+TGF-b+System+in+Breast+Cancer%3A+A+Double-Edged+Sword&rft.au=Wakefield%2C+Lalage&rft.aulast=Wakefield&rft.aufirst=Lalage&rft.date=2005-12-12&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Conference+on+Genes+and+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://science.cancerresearchuk.org/genes_and_cancer/2005/programme?version =3
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Development of cancer chemopreventive drugs based on mechanistic approaches.
AN  - 68827011; 16083917
AB  - One of the most important medical practices of the 21st century is the chemoprevention of cancer. Much progress has been made in this new emerging field, but much work remains before widespread use and practice of cancer prevention becomes commonplace. Cancer chemoprevention includes the concepts of inhibition, reversal, and retardation of the cancer process. The process of carcinogenesis requires 20-40 years to reach invasive cancer. This process follows multiple, diverse, and complex pathways in a stochastic process, called clonal evolution. Many of these pathways appear amenable to inhibition, reversal, or retardation at various points. It is urgent that we identify key pathways in the evolution of the cancer cell, which can be exploited to prevent this carcinogenesis process. Basic researchers are identifying many genetic lesions and epigenetic processes associated with the progression of precancer to invasive disease. These precancer lesions are also called intraepithelial neoplasia (IEN). Many of these early precancerous lesions favor cell division over quiescence and protect cells against apoptosis when signals are present. Many oncogenes, which are active during early development, are reactivated in adulthood by aberrant gene promoting errors. Normal regulatory genes can become mutated, making them insensitive to normal regulatory signals. Tumor suppressor genes are deleted or mutated rendering them inactive. These are several of a wide range of defects in cellular machinery, which can lead to evolution of the cancer phenotype. Errors may not have to appear in a defined order for cells to progress along the cancer pathway. To conquer this diverse disease, it is necessary to attack multiple key pathways at once for a predetermined period of time. Agent combination prevention strategies are, therefore, essential to decrease cancer morbidity. Each cancer type, organ location, or individual genetic background may require a custom combination of prevention strategies to be successful.
JF  - Mutation research
AU  - Steele, Vernon E
AU  - Kelloff, Gary J
AD  - National Cancer Institute, EPN 2108, MSC 7322, 9000 Rockville Pike, National Institutes of Health, Bethesda, MD 20892-7322, USA. vs1y@nih.gov
Y1  - 2005/12/11/
PY  - 2005
DA  - 2005 Dec 11
SP  - 16
EP  - 23
VL  - 591
IS  - 1-2
SN  - 0027-5107, 0027-5107
KW  - Anticarcinogenic Agents
KW  - 0
KW  - Index Medicus
KW  - Humans
KW  - Anticarcinogenic Agents -- therapeutic use
KW  - Neoplasms -- prevention & control
KW  - Mutation
KW  - Neoplasms -- genetics
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Mutation+research&rft.atitle=Development+of+cancer+chemopreventive+drugs+based+on+mechanistic+approaches.&rft.au=Steele%2C+Vernon+E%3BKelloff%2C+Gary+J&rft.aulast=Steele&rft.aufirst=Vernon&rft.date=2005-12-11&rft.volume=591&rft.issue=1-2&rft.spage=16&rft.isbn=&rft.btitle=&rft.title=Mutation+research&rft.issn=00275107&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-09-15
N1  - Date created - 2005-11-23
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Translating Evidence-Based Practices into Health Policy: A Tool to Reduce Cancer Health Disparities
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39933087; 4084997
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Cooper, Leslie C
AU  - McCrae, Tarsha
AU  - Wingrove, Barbara K
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Cancer
KW  - Policies
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39933087?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.atitle=Translating+Evidence-Based+Practices+into+Health+Policy%3A+A+Tool+to+Reduce+Cancer+Health+Disparities&rft.au=Cooper%2C+Leslie+C%3BMcCrae%2C+Tarsha%3BWingrove%2C+Barbara+K&rft.aulast=Cooper&rft.aufirst=Leslie&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.issn=&rft_id=info:doi/
L2  - http://apha.confex.com/apha/133am/techprogram/meeting.htm
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Tobacco Dependence and Psychiatric Comorbidity: Possible Mechanisms of Association
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39922692; 4085209
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Riley, William
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Tobacco
KW  - Morbidity
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39922692?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.atitle=Tobacco+Dependence+and+Psychiatric+Comorbidity%3A+Possible+Mechanisms+of+Association&rft.au=Riley%2C+William&rft.aulast=Riley&rft.aufirst=William&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.issn=&rft_id=info:doi/
L2  - http://apha.confex.com/apha/133am/techprogram/meeting.htm
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Education Level and Drinking Behavior Among Racial/Ethnic Groups: Results from the 20012002 National Epidemiologic Survey on Alcohol and Related Conditions (NESARC)
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39920939; 4085275
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Yoon, Young-Hee
AU  - Yi, Hsiao-ye
AU  - Chen, Chiung M
AU  - Breslow, Rosalind
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Alcohols
KW  - Ethnic groups
KW  - Education
KW  - Drinking behavior
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39920939?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.atitle=Education+Level+and+Drinking+Behavior+Among+Racial%2FEthnic+Groups%3A+Results+from+the+20012002+National+Epidemiologic+Survey+on+Alcohol+and+Related+Conditions+%28NESARC%29&rft.au=Yoon%2C+Young-Hee%3BYi%2C+Hsiao-ye%3BChen%2C+Chiung+M%3BBreslow%2C+Rosalind&rft.aulast=Yoon&rft.aufirst=Young-Hee&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.issn=&rft_id=info:doi/
L2  - http://apha.confex.com/apha/133am/techprogram/meeting.htm
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - More Research will not Solve Health Disparities; Using Health Policy to Sustain Evidence-Based Practices
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39867618; 4084998
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Wingrove, Barbara K
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Policies
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39867618?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.atitle=More+Research+will+not+Solve+Health+Disparities%3B+Using+Health+Policy+to+Sustain+Evidence-Based+Practices&rft.au=Wingrove%2C+Barbara+K&rft.aulast=Wingrove&rft.aufirst=Barbara&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.issn=&rft_id=info:doi/
L2  - http://apha.confex.com/apha/133am/techprogram/meeting.htm
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Fruit and Vegetable Consumption Among African American Adult Males: Correlates of Awareness and Consumption
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39852048; 4086733
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Robinson, JaMuir M
AU  - Massett, Holly
AU  - DiSogra, Lorelei
AU  - Moser, Richard P
AU  - Maibach, Edward
AU  - Weber, Deanne
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Africa
KW  - Ethnic groups
KW  - Vegetables
KW  - Fruits
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Promoting the Body and Soul Program: Lessons Learned from the Nationwide Dissemination of a Health Promotion Program for African American Churches
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39851922; 4088585
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Williams, Alexis M
AU  - DiSogra, Lorelei
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Africa
KW  - Health promotion
KW  - Ethnic groups
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Associations Between Craving for Tobacco Cigarettes and Illicit Drugs
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39850588; 4085208
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Heishman, Stephen J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Tobacco
KW  - Drug addiction
KW  - Cigarettes
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Community Environmnetal forum Theater: Tox and Risk Take the Stage
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39849469; 4086242 DE:
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Sullivan, john
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39849469?accountid=14244
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TY  - CPAPER
T1  - Effects of the Checkpoints Program on Parent-Imposed Driving Limits and Crash Outcomes Among Novice Teen Drivers at 6-Months Post-Licensure
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39842823; 4087776 DE:
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Simons-Morton, Bruce G
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39842823?accountid=14244
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Development of the Adaptations Index for Women with Pelvic Floor Disorders: The Value of the Patients Voice
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39842613; 4088642
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Wren, Patricia A
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Adaptations
KW  - Pelvis
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Public Health in Public Housing: Improving Health, Changing Lives Results of a Strategic Planning Workshop to Address CVD and Asthma in Public Housing Settings
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39841833; 4088475
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Simon, Lenee N
AU  - Fulwood, Robinson
AU  - Morosco, Gregory J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Housing
KW  - Respiratory diseases
KW  - Asthma
KW  - Public health
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Evidence Base for Cancer Screening Promotion: How Good a Fit for Public Health Practice?
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39833430; 4086007
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Breen, Nancy
AU  - Meissner, Helen
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Public health
KW  - Cancer
KW  - Screening
KW  - U 7000:Multidisciplinary
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.atitle=Evidence+Base+for+Cancer+Screening+Promotion%3A+How+Good+a+Fit+for+Public+Health+Practice%3F&rft.au=Breen%2C+Nancy%3BMeissner%2C+Helen&rft.aulast=Breen&rft.aufirst=Nancy&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.issn=&rft_id=info:doi/
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TY  - CPAPER
T1  - A Dynamic Panel Study of the Linkages Between Smoking Behavior and Health Expenditures
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39828536; 4085326
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Shaw, James W
AU  - Horrace, William C
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Smoking
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39828536?accountid=14244
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TY  - CPAPER
T1  - Drinking Patterns of Recovering Alcoholics: Results from the 20012002 National Epidemiologic Survey on Alcohol and Related Conditions (NESARC)
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39828092; 4085235
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Chen, Chiung M
AU  - Yi, Hsiao-ye
AU  - Hilton, Michael E
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Alcohols
KW  - Ethanol
KW  - Alcoholics
KW  - Drinking
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Software for Survival Analysis of Studies Nested within Cohorts to Estimate Relative, Absolute, and Attributable Risks
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39827192; 4086582
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Katki, Hormuzd
AU  - Mark, Steven D
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Computer programs
KW  - Software
KW  - Survival
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Vesicular Trafficking And Signal Relay During Chemotaxis
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39824367; 4033803
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Kriebel, P W
AU  - Barr, V A
AU  - Mihaylov, V A
AU  - Parent, C A
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Chemotaxis
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - New Look at Patterns of Tobacco and Alcohol Comorbidities in the U.S. Population
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39821741; 4085206
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Chiapella, Page
AU  - Fertig, Joanne
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - USA
KW  - Alcohols
KW  - Tobacco
KW  - Morbidity
KW  - U 7000:Multidisciplinary
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Glia&rft.atitle=Interactive+role+of+the+toll-like+receptor+4+and+reactive+oxygen+species+in+LPS-induced+microglia+activation.&rft.au=Qin%2C+Liya%3BLi%2C+Guorong%3BQian%2C+Xun%3BLiu%2C+Yuxin%3BWu%2C+Xuefei%3BLiu%2C+Bin%3BHong%2C+Jau-Shyong%3BBlock%2C+Michelle+L&rft.aulast=Qin&rft.aufirst=Liya&rft.date=2005-10-01&rft.volume=52&rft.issue=1&rft.spage=78&rft.isbn=&rft.btitle=&rft.title=Glia&rft.issn=08941491&rft_id=info:doi/
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TY  - CPAPER
T1  - Poverty, Perceived Discrimination, and Parenting Stress in African American mothers of Young Children
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39821163; 4088302
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Siefert, Kristine
AU  - Finlayson, Tracy L
AU  - Ismail, Amid
AU  - Delva, Jorge
AU  - Williams, David R
AU  - Amaya, Ashley
AU  - Lepkowski, James
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Africa
KW  - Children
KW  - Stress
KW  - Discrimination
KW  - Ethnic groups
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Cigarette Smoking Among Low-Income African American Women: A Hidden, Neglected, and Growing Public Health Problem
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39820661; 4085417
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Delva, Jorge
AU  - Tellez, Marisol
AU  - Finlayson, Tracy L
AU  - Gretebeck, Kimberlee
AU  - Siefert, Kristine
AU  - Williams, David R
AU  - Ismail, Amid
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Africa
KW  - Public health
KW  - Socio-economic aspects
KW  - Ethnic groups
KW  - Cigarette smoking
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39820661?accountid=14244
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TY  - CPAPER
T1  - NIDCR: Addressing Oral Health Disparities through Research
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39820229; 4086116 DE:
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Nowjack-Raymer, Ruth
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39820229?accountid=14244
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TY  - CPAPER
T1  - Neuroglia Specific Expression of a FRET-based Calcium Indicator in Transgenic Mice
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39819514; 4033516
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Atkin, S D
AU  - Holtzclaw, L A
AU  - Pickel, J M
AU  - Russell, J T
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Mice
KW  - Calcium
KW  - Transgenic mice
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39819514?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Changes in Chromatin Structure and Mobility in Living Cells at Sites of DNA Double-strand Breaks
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39818552; 4033320
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Kruhlak, M J
AU  - Celeste, A
AU  - Fernandez-Capetillo, O
AU  - Dellaire,
AU  - Muller, G W
AU  - McNally, J G
AU  - Bazett-Jones, D P
AU  - Nussenzweig, A
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Mobility
KW  - Chromatin
KW  - DNA damage
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39818552?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Changes+in+Chromatin+Structure+and+Mobility+in+Living+Cells+at+Sites+of+DNA+Double-strand+Breaks&rft.au=Kruhlak%2C+M+J%3BCeleste%2C+A%3BFernandez-Capetillo%2C+O%3BDellaire%2C%3BMuller%2C+G+W%3BMcNally%2C+J+G%3BBazett-Jones%2C+D+P%3BNussenzweig%2C+A&rft.aulast=Kruhlak&rft.aufirst=M&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - An Unexpected Role of Bcl-2 Family Members in Mitochondrial Morphogenesis
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39818238; 4032445
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Youle, R J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Morphogenesis
KW  - Bcl-2 protein
KW  - Mitochondria
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39818238?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Diet, Activity, and Smoking: What do Data from Various Studies Reveal Regarding Their Relation?
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39817239; 4085207
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Augustson, Erik M
AU  - Wanke, Kay L
AU  - Bergen, Andrew W
AU  - Lanza, Elaine
AU  - Caporaso, Neil E
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Smoking
KW  - Diets
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39817239?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Hemoglobin Genotype-dependent Erythrocyte Membrane Potential Correlates to Innate Protection Against Severe Malaria
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39816027; 4033579
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Tokumasu, F
AU  - Dvorak, J A
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Malaria
KW  - Membrane potential
KW  - Hemoglobin
KW  - Erythrocytes
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39816027?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Modeling the Relationship Between Healthy People 2010 Upstream (Risk Factors and Screening) and Downstream (Mortality) Goals for Cancer
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39815446; 4086564
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Feuer, Eric J
AU  - Cronin, Kathleen
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Mortality
KW  - Cancer
KW  - Risk factors
KW  - Screening
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39815446?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Lessons Learned: Environmental Health Information Outreach to Native Americans
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39813844; 4086281
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Love, Cynthia
AU  - Dutcher, Gale
AU  - Arnesen, Stacey J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Ethnic groups
KW  - Environmental health
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39813844?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Plasma Membrane ABCG1 Mediates Cellular Cholesterol Efflux to Lipoproteins
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39812018; 4034682
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Neufeld, E B
AU  - O'Brien, K
AU  - Demosky, S J
AU  - Stonik, J A
AU  - Sabol, S L
AU  - Malide, D
AU  - Combs, C A
AU  - Remaley, A T
AU  - Santamaina-Fojo, S
AU  - Brewer, H B
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Cholesterol
KW  - Plasma membranes
KW  - Lipoproteins
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39812018?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Characterization of DetaD Endocytosis and Recycling
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39811741; 4034633
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Palardy, G
AU  - Goswami, M
AU  - Chitnis, A
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Protein turnover
KW  - Recycling
KW  - Endocytosis
KW  - Waste management
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39811741?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - What Do Alcohol, Tobacco, Other Drugs, Physical Inactivity, and Mental Health Disorders Have in Common?
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39806038; 4085205
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Backinger, Cathy L
AU  - Chiapella, Page
AU  - Augustson, Erik M
AU  - Heishman, Stephen J
AU  - Riley, William
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Physical activity
KW  - Alcohols
KW  - Tobacco
KW  - Drugs
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39806038?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Level and Concentration of Alcohol Consumption by Beverage Type and Demographic Characteristics: Results from the 20012002 NESARC
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39774878; 4085239
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Yi, Hsiao-ye
AU  - Chen, Chiung M
AU  - Hilton, Michael E
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Alcohols
KW  - Ethanol
KW  - Demography
KW  - Beverages
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Taking a Systems Approach to Tobacco Research: Modeling Dynamic Processes for a Complex World
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39773539; 4085324
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Leischow, Scott J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Tobacco
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39773539?accountid=14244
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TY  - CPAPER
T1  - Multi-Morbid DSM-IV Axis I Psychological and Axis II Personality Disorders and Their Association with Substance Use Disorders and Hazardous Drinking: Results from the National Epidemiologic Survey on Alcohol and Related Conditions (NESARC)
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39768732; 4085237
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Falk, Daniel E
AU  - Yi, Hsiao-ye
AU  - Breslow, Rosalind
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Psychology
KW  - Alcohols
KW  - Personality
KW  - Drinking
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39768732?accountid=14244
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TY  - CPAPER
T1  - Question of Whether DSM-IV Alcohol Dependence is a Categorical or a Continuous Variable
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39768696; 4085236
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Yahr, Harold T
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Alcohols
KW  - Drug dependence
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39768696?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Interactions between HIV-1 and HIV-2 Gag Polyproteins in vivo
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39765071; 4035164
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Boyko, V P
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Polyproteins
KW  - Human immunodeficiency virus 2
KW  - Human immunodeficiency virus 1
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39765071?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Findings from the National Cancer Institute and Vietnamese American Medical Association Pap Test Barriers Survey for Health Care Providers
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39765038; 4087930
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Solomon, Felicia M
AU  - DeJoice, Rhonda W
AU  - Nguyen, Si V
AU  - Kwon, Harry T
AU  - Berlin, Nina
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Health care
KW  - Cancer
KW  - Barriers
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39765038?accountid=14244
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TY  - CPAPER
T1  - Disparities in the Consequences of Drug Use Among Minority Populations: Need for Culture-Specific Interventions
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39764894; 4085611
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Jones, Dionne
AU  - Fernandez, M Isabel
AU  - Harrison, Murelle G
AU  - McCoy, Clyde B
AU  - Devieux, Jessy G
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Drug abuse
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39764894?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Structural Mechanism for Sterol Sensing and Transport by OSBP-related Proteins
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39764795; 4033929
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Im, Y.
AU  - Raychaudhuri, S
AU  - Prinz, W A
AU  - Hurley, J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Sterols
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Oral Cancer Knowledge, Attitudes, and Behaviors of At-Risk African American Men in Washington, D.C
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39760676; 4088377
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Boehm, Karina
AU  - Daum, Mary
AU  - Bobbin, Marilyn
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - USA, Washington
KW  - Africa
KW  - Ethnic groups
KW  - Cancer
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39760676?accountid=14244
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ER  - 



TY  - CPAPER
T1  - National Cancer Institute's Cancer Information Service Research Program: Integrating Health Communication Research into Service
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39759349; 4088442
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Vanderpool, Robin Cline
AU  - Squiers, Linda Brafford
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Cancer
KW  - Communication
KW  - Research programs
KW  - Information services
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39759349?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Thread-to-Grain Transition of Mitochondria Induced by Cytomegalovirus-Encoded vMIA is Independent of Pro-Apoptotic Bcl-2 Family Member, Bax
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39756524; 4033519
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Norris, K L
AU  - Karbowski, M
AU  - Dlouhy, B
AU  - Youle, R J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Bax protein
KW  - Bcl-2 protein
KW  - Mitochondria
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39756524?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Chromogranin A Deficiency in Transgenic Mice Leads to Aberrant Chromaffin Granule Biogenesis
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39755746; 4033498
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Kim, T
AU  - Zhang, C
AU  - Sun, Z
AU  - Wu, H.
AU  - Loh, Y P
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Chromaffin granules
KW  - Biogenesis
KW  - Mice
KW  - Chromogranins
KW  - Evolution
KW  - Transgenic mice
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39755746?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - MAD1 Haplo-insufficiency and Tumor Development in Mice
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39755181; 4033379
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Iwanaga, Y
AU  - Miyazato, A
AU  - Chi, Y
AU  - Haller, K
AU  - Ward, J M
AU  - Jeang, K
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Mice
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39755181?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Patient Recruitment to a Phase III Complementary and Alternative Medicine Clinical Trial: Overcoming Challenges
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39753698; 4088092
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Cotler, Alyssa
AU  - Arciniega, Jacqueline
AU  - Doner, Lynne
AU  - Lange, Amy
AU  - Liu, Irene
AU  - Nahin, Richard
AU  - Tisch, Jennifer
AU  - Lamas, Gervasio
AU  - Lambe, Lindsay
AU  - Clapp-Channing, Nancy
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Clinical trials
KW  - Recruitment
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Ezrin is Activated by PKC and Contributes to Metastatic Phenotype of Osteosarcoma Cells
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39752698; 4032573
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Ren, L
AU  - Hong, S
AU  - Cassavaugh, J
AU  - Khanna, C
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Ezrin
KW  - Osteosarcoma cells
KW  - Phenotypes
KW  - Metastases
KW  - Protein kinase C
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39752698?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Ezrin+is+Activated+by+PKC+and+Contributes+to+Metastatic+Phenotype+of+Osteosarcoma+Cells&rft.au=Ren%2C+L%3BHong%2C+S%3BCassavaugh%2C+J%3BKhanna%2C+C&rft.aulast=Ren&rft.aufirst=L&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Perturbation of the Endocytic Pathway Affects Expression and Translocation of Salmonella-effector Proteins in Cultured Epithelial Cells
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39744792; 4033598
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Fuentes, P
AU  - Drecktrah, D
AU  - Knodler, L A
AU  - Steele-Mortimer, O
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Translocation
KW  - Fish culture
KW  - Epithelial cells
KW  - Salmonidae
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39744792?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Perturbation+of+the+Endocytic+Pathway+Affects+Expression+and+Translocation+of+Salmonella-effector+Proteins+in+Cultured+Epithelial+Cells&rft.au=Fuentes%2C+P%3BDrecktrah%2C+D%3BKnodler%2C+L+A%3BSteele-Mortimer%2C+O&rft.aulast=Fuentes&rft.aufirst=P&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Development of a Polarized Epithelial Cell Model to Study the Role of Akt/PKB in Salmonella Enterica Interactions with the Intestinal Epithelium
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39744709; 4033597
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Ireland, R
AU  - Steele-Mortimer, O
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Intestine
KW  - Cell culture
KW  - Epithelium
KW  - AKT protein
KW  - Epithelial cells
KW  - Salmonella enterica
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39744709?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Development+of+a+Polarized+Epithelial+Cell+Model+to+Study+the+Role+of+Akt%2FPKB+in+Salmonella+Enterica+Interactions+with+the+Intestinal+Epithelium&rft.au=Ireland%2C+R%3BSteele-Mortimer%2C+O&rft.aulast=Ireland&rft.aufirst=R&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=03768716&rft_id=info:doi/10.1016%2Fj.drugalcdep.2005.03.009
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - K-165: An Organelle Motor in the Squid Giant Axon
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39741974; 4034277
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - DeGiorgis, J A
AU  - Gallant, P E
AU  - Reese, T S
AU  - Galbraith, J A
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Organelles
KW  - Neurons
KW  - Giant axons
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39741974?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=K-165%3A+An+Organelle+Motor+in+the+Squid+Giant+Axon&rft.au=DeGiorgis%2C+J+A%3BGallant%2C+P+E%3BReese%2C+T+S%3BGalbraith%2C+J+A&rft.aulast=DeGiorgis&rft.aufirst=J&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Fibroblast Growth Factor (FGF) Signaling Regulates the Expression and the Activity of Matrix Metalloproteases (MMPs) during Mouse Submandibular Gland (SMG) Branching Morphogenesis
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39738747; 4034884
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Rebustini, I T
AU  - Hoffman, M P
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Fibroblast growth factor
KW  - Morphogenesis
KW  - Glands
KW  - Signal transduction
KW  - Submandibular gland
KW  - Matrix metalloproteinase
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39738747?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Fibroblast+Growth+Factor+%28FGF%29+Signaling+Regulates+the+Expression+and+the+Activity+of+Matrix+Metalloproteases+%28MMPs%29+during+Mouse+Submandibular+Gland+%28SMG%29+Branching+Morphogenesis&rft.au=Rebustini%2C+I+T%3BHoffman%2C+M+P&rft.aulast=Rebustini&rft.aufirst=I&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Curing of Yeast [PSI@@u+@] Prion by Guanidine Inactivation of Hsp104 Does Not Require Cell Division
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39736717; 4034737
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Wu, Y.
AU  - Greene, L E
AU  - Masison, D C
AU  - Eisenberg, E
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Curing
KW  - Cell division
KW  - Prion protein
KW  - Guanidine
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39736717?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Curing+of+Yeast+%5BPSI%40%40u%2B%40%5D+Prion+by+Guanidine+Inactivation+of+Hsp104+Does+Not+Require+Cell+Division&rft.au=Wu%2C+Y.%3BGreene%2C+L+E%3BMasison%2C+D+C%3BEisenberg%2C+E&rft.aulast=Wu&rft.aufirst=Y.&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Differential Expression of Cdh23 Isoforms in the Cochlea and Retina of Wild Type and Waltzer Mice
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39735260; 4034899
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Lagziel, A
AU  - Ahmed, Z M
AU  - Peters, L M
AU  - Friedman, T B
AU  - Morell, R J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Mice
KW  - Cochlea
KW  - Retina
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39735260?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Differential+Expression+of+Cdh23+Isoforms+in+the+Cochlea+and+Retina+of+Wild+Type+and+Waltzer+Mice&rft.au=Lagziel%2C+A%3BAhmed%2C+Z+M%3BPeters%2C+L+M%3BFriedman%2C+T+B%3BMorell%2C+R+J&rft.aulast=Lagziel&rft.aufirst=A&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Conditional Ablation of Nonmuscle Myosin II-B in the Mouse Heart
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39733297; 4032757
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Singh, A K
AU  - Wei, Q
AU  - Takeda, K
AU  - Zerfas, P
AU  - Birdsall, C
AU  - Sidenko, S
AU  - Adelstein, R S
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Myosin
KW  - Ablation
KW  - Heart
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39733297?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Conditional+Ablation+of+Nonmuscle+Myosin+II-B+in+the+Mouse+Heart&rft.au=Singh%2C+A+K%3BWei%2C+Q%3BTakeda%2C+K%3BZerfas%2C+P%3BBirdsall%2C+C%3BSidenko%2C+S%3BAdelstein%2C+R+S&rft.aulast=Singh&rft.aufirst=A&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Role of GlUT1 in HTLV Infection
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39733146; 4033753
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Lisinski, I M
AU  - Takenouchi, N
AU  - Kazunori, F
AU  - Yao, K
AU  - Ruscetti, F W
AU  - Jones, K
AU  - Cushman, S W
AU  - Jacobsen, S
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Infection
KW  - Human T-lymphotropic virus
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39733146?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=The+Role+of+GlUT1+in+HTLV+Infection&rft.au=Lisinski%2C+I+M%3BTakenouchi%2C+N%3BKazunori%2C+F%3BYao%2C+K%3BRuscetti%2C+F+W%3BJones%2C+K%3BCushman%2C+S+W%3BJacobsen%2C+S&rft.aulast=Lisinski&rft.aufirst=I&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Six1 Promotes Rhabdomyosarcoma Metastasis through Ezrin
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39732291; 4033855
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Yu, Y.
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Ezrin
KW  - Metastases
KW  - Rhabdomyosarcoma
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39732291?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Six1+Promotes+Rhabdomyosarcoma+Metastasis+through+Ezrin&rft.au=Yu%2C+Y.&rft.aulast=Yu&rft.aufirst=Y.&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Examination of Endothelial Lumenization Processes in vivo Using Zebrafish Danio rerio
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39732155; 4033835
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Kamei, M
AU  - Bayless, K J
AU  - Davis, G E
AU  - Weinstein, B M
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Freshwater fish
KW  - Danio rerio
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39732155?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Examination+of+Endothelial+Lumenization+Processes+in+vivo+Using+Zebrafish+Danio+rerio&rft.au=Kamei%2C+M%3BBayless%2C+K+J%3BDavis%2C+G+E%3BWeinstein%2C+B+M&rft.aulast=Kamei&rft.aufirst=M&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Targeted Disruption of N-RAP Gene Function by RNA Interference: A Role for N-RAP in Myofibril Organization
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39727805; 4034257
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Dhume, A
AU  - Horowits, R
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - RNA-mediated interference
KW  - Myofibrils
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39727805?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Targeted+Disruption+of+N-RAP+Gene+Function+by+RNA+Interference%3A+A+Role+for+N-RAP+in+Myofibril+Organization&rft.au=Dhume%2C+A%3BHorowits%2C+R&rft.aulast=Dhume&rft.aufirst=A&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Centrosome and Golgi Complex Reorganization during Myogenesis Can Proceed without a Coherent, Dynamic Microtubule Network
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39727518; 4033718
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Zaal, K J M
AU  - Reid, E
AU  - Gundersen, G G
AU  - Zhang, T
AU  - Ralston, E
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Microtubules
KW  - Golgi apparatus
KW  - Myogenesis
KW  - Centrosomes
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39727518?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Centrosome+and+Golgi+Complex+Reorganization+during+Myogenesis+Can+Proceed+without+a+Coherent%2C+Dynamic+Microtubule+Network&rft.au=Zaal%2C+K+J+M%3BReid%2C+E%3BGundersen%2C+G+G%3BZhang%2C+T%3BRalston%2C+E&rft.aulast=Zaal&rft.aufirst=K+J&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Transcription Factor Sp3 and DNA Methylation Regulate the Nonmuscle Myosin Heavy Chain II-C Promoter
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39726235; 4032759
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Chung, M
AU  - Adelstein, R S
AU  - Kawamoto, S
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - DNA methylation
KW  - Promoters
KW  - Myosin
KW  - Transcription factors
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39726235?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Transcription+Factor+Sp3+and+DNA+Methylation+Regulate+the+Nonmuscle+Myosin+Heavy+Chain+II-C+Promoter&rft.au=Chung%2C+M%3BAdelstein%2C+R+S%3BKawamoto%2C+S&rft.aulast=Chung&rft.aufirst=M&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Reduction of ss-Integrin Expression and Cell Attachments in Nonmucle Myosin II-B Null Mouse Embryonic Fibroblasts
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39726194; 4032755
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Kim, K
AU  - Adelstein, R S
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Myosin
KW  - Embryo fibroblasts
KW  - Embryos
KW  - Fibroblasts
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39726194?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Reduction+of+ss-Integrin+Expression+and+Cell+Attachments+in+Nonmucle+Myosin+II-B+Null+Mouse+Embryonic+Fibroblasts&rft.au=Kim%2C+K%3BAdelstein%2C+R+S&rft.aulast=Kim&rft.aufirst=K&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Cellular Regulation of the Hematopoietic Stem Cell Niche
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39726156; 4033097
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Gillette, J M
AU  - Lippincott-Schwartz, J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Stem cells
KW  - Niches
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39726156?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Cellular+Regulation+of+the+Hematopoietic+Stem+Cell+Niche&rft.au=Gillette%2C+J+M%3BLippincott-Schwartz%2C+J&rft.aulast=Gillette&rft.aufirst=J&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Identification of a Novel Monoclonal Antibody to a Cell Surface Antigen that Isolates Neuronal Stem Cells From Murine and Pig Adult Skeletal Muscle and Murine Embryo
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39724401; 4034658
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Winitsky, S O
AU  - Gopal, T V
AU  - Hassanzadeh, S
AU  - Kassahun, Y A
AU  - Epstein, N D
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Stem cells
KW  - Skeletal muscle
KW  - Embryos
KW  - Monoclonal antibodies
KW  - Antigens
KW  - Cell surface
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39724401?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Identification+of+a+Novel+Monoclonal+Antibody+to+a+Cell+Surface+Antigen+that+Isolates+Neuronal+Stem+Cells+From+Murine+and+Pig+Adult+Skeletal+Muscle+and+Murine+Embryo&rft.au=Winitsky%2C+S+O%3BGopal%2C+T+V%3BHassanzadeh%2C+S%3BKassahun%2C+Y+A%3BEpstein%2C+N+D&rft.aulast=Winitsky&rft.aufirst=S&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Differential Sub-cellular Localization of NGEP, a Prostate Specific Protein in Two Prostate Cancer Cell Lines.
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39724094; 4033191
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Das, S
AU  - Nagata, S
AU  - Bera, T
AU  - Pastan, I
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Tumor cell lines
KW  - Prostate cancer
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39724094?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Differential+Sub-cellular+Localization+of+NGEP%2C+a+Prostate+Specific+Protein+in+Two+Prostate+Cancer+Cell+Lines.&rft.au=Das%2C+S%3BNagata%2C+S%3BBera%2C+T%3BPastan%2C+I&rft.aulast=Das&rft.aufirst=S&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Elucidating the Structural Role of Dnm1 in Mitochondrial Fission
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39723804; 4034508
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Mears, J A
AU  - Ingerman, E
AU  - Marino, M
AU  - Nunnari, J
AU  - Hinshaw, J E
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Mitochondria
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39723804?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Elucidating+the+Structural+Role+of+Dnm1+in+Mitochondrial+Fission&rft.au=Mears%2C+J+A%3BIngerman%2C+E%3BMarino%2C+M%3BNunnari%2C+J%3BHinshaw%2C+J+E&rft.aulast=Mears&rft.aufirst=J&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A Truncated Leishmania K39 Kinesin Protein Binds Along Cortical Microtubules in an ATP-Dependant Manner and Accumulates at the Tip of the Cell
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39722001; 4034276
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Gerald, N J
AU  - Dwyer, D M
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Microtubules
KW  - Kinesin
KW  - Leishmania
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39722001?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=A+Truncated+Leishmania+K39+Kinesin+Protein+Binds+Along+Cortical+Microtubules+in+an+ATP-Dependant+Manner+and+Accumulates+at+the+Tip+of+the+Cell&rft.au=Gerald%2C+N+J%3BDwyer%2C+D+M&rft.aulast=Gerald&rft.aufirst=N&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Probing Arf Guanine Nucleotide Exchange Factor (GEF) Specificity with Chimeric Proteins
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39718071; 4033262
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Cohen, L A
AU  - Donaldson, J G
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Nucleotides
KW  - Specificity
KW  - Guanine nucleotide exchange factor
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39718071?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Probing+Arf+Guanine+Nucleotide+Exchange+Factor+%28GEF%29+Specificity+with+Chimeric+Proteins&rft.au=Cohen%2C+L+A%3BDonaldson%2C+J+G&rft.aulast=Cohen&rft.aufirst=L&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Calcium Signaling Protein Complexes in Oligodendrocyte Precursor (OP Cell) Membranes Isolated from Rat Cortices
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39715200; 4034154
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Weerth, S H
AU  - Hauser, J
AU  - Russell, J T
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Oligodendrocytes
KW  - Calcium signalling
KW  - Cell membranes
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39715200?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Calcium+Signaling+Protein+Complexes+in+Oligodendrocyte+Precursor+%28OP+Cell%29+Membranes+Isolated+from+Rat+Cortices&rft.au=Weerth%2C+S+H%3BHauser%2C+J%3BRussell%2C+J+T&rft.aulast=Weerth&rft.aufirst=S&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Nitric Oxide Activates Peroxisome Proliferator-Activated Receptor Gamma through a p38 MAPK Signaling Pathway
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39712448; 4034577
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Ptasinska, A
AU  - Wang, S
AU  - Zhang, J
AU  - Danner, R L
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Peroxisome proliferator-activated receptors
KW  - MAP kinase
KW  - Signal transduction
KW  - Nitric oxide
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39712448?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Nitric+Oxide+Activates+Peroxisome+Proliferator-Activated+Receptor+Gamma+through+a+p38+MAPK+Signaling+Pathway&rft.au=Ptasinska%2C+A%3BWang%2C+S%3BZhang%2C+J%3BDanner%2C+R+L&rft.aulast=Ptasinska&rft.aufirst=A&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Rab11a is Required for Canalicular Biogenesis in WIF-B9 Hepatic Cells
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39712379; 4034557
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Wakabayashi, Y
AU  - Dutt, P
AU  - Lippincott-Schwartz, J
AU  - Arias, I M
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Biogenesis
KW  - Liver
KW  - Evolution
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39712379?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Rab11a+is+Required+for+Canalicular+Biogenesis+in+WIF-B9+Hepatic+Cells&rft.au=Wakabayashi%2C+Y%3BDutt%2C+P%3BLippincott-Schwartz%2C+J%3BArias%2C+I+M&rft.aulast=Wakabayashi&rft.aufirst=Y&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Racial/Ethnic Variation in Colorectal Cancer Diagnosis: Should Screening Guidelines Consider Race/Ethnicity?
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39711388; 4085000
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Shavers, Vickie L
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Ethnic groups
KW  - Colorectal cancer
KW  - Races
KW  - Screening
KW  - Subpopulations
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39711388?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.atitle=Racial%2FEthnic+Variation+in+Colorectal+Cancer+Diagnosis%3A+Should+Screening+Guidelines+Consider+Race%2FEthnicity%3F&rft.au=Shavers%2C+Vickie+L&rft.aulast=Shavers&rft.aufirst=Vickie&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=133rd+Annual+Meeting+and+Exposition+of+the+American+Public+Health+Association&rft.issn=&rft_id=info:doi/
L2  - http://apha.confex.com/apha/133am/techprogram/meeting.htm
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Metabolism of Tasidotin (ILX-651) by Cancer Cells: Mechanisms of Activation and Resistance
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39710995; 4033936
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Bai, R
AU  - Edler, M C
AU  - Copeland, T D
AU  - Schmid, S
AU  - Arthaud, L E
AU  - Hamel, E
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Metabolism
KW  - Cancer
KW  - U 7000:Multidisciplinary
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L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Gonadotropin Receptor-Mediated Activation of G Protein-Activated Inwardly Rectifying K@@u+@ (GIRK) Channels in Hypothalamic GnRH Neurons.
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39710919; 4033515
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Hu, L.
AU  - Krsmanovic, L Z
AU  - Catt, K J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Potassium channels (inwardly-rectifying)
KW  - Pituitary (anterior)
KW  - Potassium
KW  - Channels
KW  - Neurons
KW  - Hypothalamus
KW  - Gonadotropin-releasing hormone
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The szy-20 (bs52) Mutation is a Suppressor of zyg-1 and Defines a Novel Regulator of the Cell Cycle
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39710413; 4033389
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Song, M
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Mutation
KW  - Suppressors
KW  - Cell cycle
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39710413?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=The+szy-20+%28bs52%29+Mutation+is+a+Suppressor+of+zyg-1+and+Defines+a+Novel+Regulator+of+the+Cell+Cycle&rft.au=Song%2C+M&rft.aulast=Song&rft.aufirst=M&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Cyclin Dependent Kinase 5 Activator p39 Binds Myosin Essential Light Chain
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39708509; 4032764
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Tripathi, B K
AU  - Ledee, D R
AU  - Zelenka, P S
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Myosin
KW  - Light chains
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39708509?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=The+Cyclin+Dependent+Kinase+5+Activator+p39+Binds+Myosin+Essential+Light+Chain&rft.au=Tripathi%2C+B+K%3BLedee%2C+D+R%3BZelenka%2C+P+S&rft.aulast=Tripathi&rft.aufirst=B&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Increased Expression of the Inserted Myosin II-C Isoform in Tumor Cell Lines
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39708424; 4032760
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Jana, S S
AU  - Adelstein, R S
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Myosin
KW  - Tumor cell lines
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39708424?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Increased+Expression+of+the+Inserted+Myosin+II-C+Isoform+in+Tumor+Cell+Lines&rft.au=Jana%2C+S+S%3BAdelstein%2C+R+S&rft.aulast=Jana&rft.aufirst=S&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Intracellular Dynamics of Drosophila Myosin-V
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39705120; 4032686
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Toth, J
AU  - Sellers, J R
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Drosophila
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39705120?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Intracellular+Dynamics+of+Drosophila+Myosin-V&rft.au=Toth%2C+J%3BSellers%2C+J+R&rft.aulast=Toth&rft.aufirst=J&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Tobacco and Alcohol Use Among Homosexual and Bisexual Adults in California
T2  - 133rd Annual Meeting and Exposition of the American Public Health Association
AN  - 39705017; 4085420
JF  - 133rd Annual Meeting and Exposition of the American Public Health Association
AU  - Grauman, Alyssa R
AU  - Lawrence, Deirdre M
AU  - Allen, Nathaniel
AU  - Davis, William
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - USA, California
KW  - Alcohols
KW  - Homosexuality
KW  - Tobacco
KW  - Bisexual
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39705017?accountid=14244
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L2  - http://apha.confex.com/apha/133am/techprogram/meeting.htm
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Monitoring the ER Luminal and the Cytosolic Face of the ERAD Substrate CD3delta
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39695995; 4033288 DE:
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Lorenz, H
AU  - Lippincott-Schwartz, J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39695995?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Monitoring+the+ER+Luminal+and+the+Cytosolic+Face+of+the+ERAD+Substrate+CD3delta&rft.au=Lorenz%2C+H%3BLippincott-Schwartz%2C+J&rft.aulast=Lorenz&rft.aufirst=H&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Avian Malaria Parasite Plasmodium gallinaceum Modifies the Surface Topography of Infected Erythrocytes
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39693376; 4033580
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Arie, T
AU  - Dorward, D W
AU  - Dvorak, J A
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Parasites
KW  - Malaria
KW  - Erythrocytes
KW  - Topography
KW  - Surface topography
KW  - Plasmodium gallinaceum
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39693376?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=The+Avian+Malaria+Parasite+Plasmodium+gallinaceum+Modifies+the+Surface+Topography+of+Infected+Erythrocytes&rft.au=Arie%2C+T%3BDorward%2C+D+W%3BDvorak%2C+J+A&rft.aulast=Arie&rft.aufirst=T&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Src-kinase Expression Inhibits Compensatory Endocytosis During Early Sea Urchin Development
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39689323; 4033263
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Covian-Nares, J F
AU  - Vogel, S S
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Endocytosis
KW  - Echinoidea
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39689323?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Src-kinase+Expression+Inhibits+Compensatory+Endocytosis+During+Early+Sea+Urchin+Development&rft.au=Covian-Nares%2C+J+F%3BVogel%2C+S+S&rft.aulast=Covian-Nares&rft.aufirst=J&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Folding of Nascent SecM within the Ribosome Exit Tunnel is Required for Translation Arrest
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39688961; 4033166
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Woolhead, C A
AU  - Johnson, A E
AU  - Bernstein, H D
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Translation
KW  - Tunnels
KW  - Ribosomes
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39688961?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Folding+of+Nascent+SecM+within+the+Ribosome+Exit+Tunnel+is+Required+for+Translation+Arrest&rft.au=Woolhead%2C+C+A%3BJohnson%2C+A+E%3BBernstein%2C+H+D&rft.aulast=Woolhead&rft.aufirst=C&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A Rap-GEF/Rap GTPase Signaling Controls Stem Cell Niche Formation through Regulating Adherens Junctions in the Drosophila Testis
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39687447; 4034851
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Hou, S X
AU  - Wang, H
AU  - Singh, S
AU  - Zheng, Z
AU  - Oh, S.
AU  - Chen, X
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Adherens junctions
KW  - Stem cells
KW  - Guanosinetriphosphatase
KW  - Signal transduction
KW  - Niches
KW  - Testes
KW  - Drosophila
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39687447?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=A+Rap-GEF%2FRap+GTPase+Signaling+Controls+Stem+Cell+Niche+Formation+through+Regulating+Adherens+Junctions+in+the+Drosophila+Testis&rft.au=Hou%2C+S+X%3BWang%2C+H%3BSingh%2C+S%3BZheng%2C+Z%3BOh%2C+S.%3BChen%2C+X&rft.aulast=Hou&rft.aufirst=S&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Phosphatases and Kinases Regulate AP2 Binding and Release from Plasma Membrane
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39683854; 4034995
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Yim, Y
AU  - Scarselletta, S
AU  - Eisenberg, E
AU  - Greene, L E
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Plasma membranes
KW  - Phosphatase
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39683854?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Phosphatases+and+Kinases+Regulate+AP2+Binding+and+Release+from+Plasma+Membrane&rft.au=Yim%2C+Y%3BScarselletta%2C+S%3BEisenberg%2C+E%3BGreene%2C+L+E&rft.aulast=Yim&rft.aufirst=Y&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Syntabulin-Mediated Anterograde Transport of Mitochondria Along Neuronal Processes
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39682783; 4033541
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Cai, Q
AU  - Sheng, Z
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Anterograde transport
KW  - Mitochondria
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Mammary Stem Cell Niche Modulates the Repertoire of Testicular Stem Cells
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39681415; 4034854
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Boulanger, C A
AU  - Mack, D L
AU  - Booth, B W
AU  - Smith, G H
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Stem cells
KW  - Niches
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39681415?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=The+Mammary+Stem+Cell+Niche+Modulates+the+Repertoire+of+Testicular+Stem+Cells&rft.au=Boulanger%2C+C+A%3BMack%2C+D+L%3BBooth%2C+B+W%3BSmith%2C+G+H&rft.aulast=Boulanger&rft.aufirst=C&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The SPG3A Hereditary Spastic Paraplegia Protein Atlastin-1 is Enriched in Axonal Growth Cones
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39680851; 4034742
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Zhu, P
AU  - Tao-Cheng, S J H
AU  - Smith, C L
AU  - Stadler, J
AU  - Yang, S M
AU  - Blackstone, C
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Growth cones
KW  - Spastic paraplegia
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39680851?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=The+SPG3A+Hereditary+Spastic+Paraplegia+Protein+Atlastin-1+is+Enriched+in+Axonal+Growth+Cones&rft.au=Zhu%2C+P%3BTao-Cheng%2C+S+J+H%3BSmith%2C+C+L%3BStadler%2C+J%3BYang%2C+S+M%3BBlackstone%2C+C&rft.aulast=Zhu&rft.aufirst=P&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Displacement of the Bromodomain Protein Brd4 from Chromosomes is Required for the Recovery from Anti-Microtubule Drug Induced Mitotic Arrest
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39680360; 4035054
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Nishiyama, A
AU  - Ozato, K
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Drugs
KW  - Chromosomes
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39680360?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Displacement+of+the+Bromodomain+Protein+Brd4+from+Chromosomes+is+Required+for+the+Recovery+from+Anti-Microtubule+Drug+Induced+Mitotic+Arrest&rft.au=Nishiyama%2C+A%3BOzato%2C+K&rft.aulast=Nishiyama&rft.aufirst=A&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Drosophila Myosin V
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39679090; 4034615
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Hong, A
AU  - Toth, J
AU  - Sellers, J R
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Myosin
KW  - Drosophila
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39679090?accountid=14244
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L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Agrin-induced Formation of Filopodia Depends on GAG Chains and Cdc42
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39678178; 4034396
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Lin, L
AU  - McCroskery, S
AU  - Ross, J M
AU  - Daniels, M P
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Pseudopodia
KW  - Cdc42 protein
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39678178?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Agrin-induced+Formation+of+Filopodia+Depends+on+GAG+Chains+and+Cdc42&rft.au=Lin%2C+L%3BMcCroskery%2C+S%3BRoss%2C+J+M%3BDaniels%2C+M+P&rft.aulast=Lin&rft.aufirst=L&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Over Expression of Human ClpP Reduces AIF Levels and Inhibits Cisplatin-Induced Apoptosis in Huh4 Cells.
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39674273; 4032496
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Zhang, Y
AU  - Barr, V
AU  - Maurizi1, M. R.
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Apoptosis-inducing factor
KW  - Apoptosis
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39674273?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Over+Expression+of+Human+ClpP+Reduces+AIF+Levels+and+Inhibits+Cisplatin-Induced+Apoptosis+in+Huh4+Cells.&rft.au=Zhang%2C+Y%3BBarr%2C+V%3BMaurizi1%2C+M.+R.&rft.aulast=Zhang&rft.aufirst=Y&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Activated AKT Regulates Nf-?B Activation, P53 Inhibition and Cell Survival in HTLV-1-transformed Cells
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39674142; 4032454
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Jeong, S
AU  - Pise-Masison, C A
AU  - Radonovich, M F
AU  - Park, H
AU  - Brady, J N
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - AKT protein
KW  - Cell survival
KW  - P53 protein
KW  - Human T-lymphotropic virus
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39674142?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Activated+AKT+Regulates+Nf-%3FB+Activation%2C+P53+Inhibition+and+Cell+Survival+in+HTLV-1-transformed+Cells&rft.au=Jeong%2C+S%3BPise-Masison%2C+C+A%3BRadonovich%2C+M+F%3BPark%2C+H%3BBrady%2C+J+N&rft.aulast=Jeong&rft.aufirst=S&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Actin Rockets Guide Membrane Protrusion and Position Primed Integrins to Direct Pathfinding
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39673028; 4032846
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Galbraith, C G
AU  - Yamada, K M
AU  - Galbraith, J A
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Membranes
KW  - Integrins
KW  - Actin
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39673028?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Actin+Rockets+Guide+Membrane+Protrusion+and+Position+Primed+Integrins+to+Direct+Pathfinding&rft.au=Galbraith%2C+C+G%3BYamada%2C+K+M%3BGalbraith%2C+J+A&rft.aulast=Galbraith&rft.aufirst=C&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Dissecting the Role of Rho-Mediated Signaling in Contractile Ring Formation
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39668551; 4032541
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Kamijo, K
AU  - Ohara, N
AU  - Abe, M
AU  - Uchimura, T
AU  - Hosoya, H
AU  - Lee, J
AU  - Miki, T
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Signal transduction
KW  - Contractility
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39668551?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Dissecting+the+Role+of+Rho-Mediated+Signaling+in+Contractile+Ring+Formation&rft.au=Kamijo%2C+K%3BOhara%2C+N%3BAbe%2C+M%3BUchimura%2C+T%3BHosoya%2C+H%3BLee%2C+J%3BMiki%2C+T&rft.aulast=Kamijo&rft.aufirst=K&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Peroxisomal Membrane Protein, Pex16p, is Involved in the Formation Peroxisomes at the Endoplasmic Reticulum
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39637007; 4033186
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Kim, P K
AU  - Mullen, R T
AU  - Lippincott-Schwartz, J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Peroxisomal membrane protein
KW  - Peroxisomes
KW  - Endoplasmic reticulum
KW  - Membranes
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39637007?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=The+Peroxisomal+Membrane+Protein%2C+Pex16p%2C+is+Involved+in+the+Formation+Peroxisomes+at+the+Endoplasmic+Reticulum&rft.au=Kim%2C+P+K%3BMullen%2C+R+T%3BLippincott-Schwartz%2C+J&rft.aulast=Kim&rft.aufirst=P&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Transmembrane Domain of the PC3: A Key Motif for Targeting to the Regulated Secretory Pathway
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39636956; 4033177
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Lou, H
AU  - Smith, A M
AU  - Coates, L C
AU  - Birch, N P
AU  - Loh, Y P
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Transmembrane domains
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39636956?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=The+Transmembrane+Domain+of+the+PC3%3A+A+Key+Motif+for+Targeting+to+the+Regulated+Secretory+Pathway&rft.au=Lou%2C+H%3BSmith%2C+A+M%3BCoates%2C+L+C%3BBirch%2C+N+P%3BLoh%2C+Y+P&rft.aulast=Lou&rft.aufirst=H&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Bcl-XL Enhances the Effect of GM-CSF in the in Vitro Development of the Monocyte/Macrophage Lineage
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39636385; 4033406
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Antignani, A
AU  - Youle, R J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Granulocyte-macrophage colony-stimulating factor
KW  - Macrophages
KW  - Bcl-x protein
KW  - Monocytes
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39636385?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.atitle=Bcl-XL+Enhances+the+Effect+of+GM-CSF+in+the+in+Vitro+Development+of+the+Monocyte%2FMacrophage+Lineage&rft.au=Antignani%2C+A%3BYoule%2C+R+J&rft.aulast=Antignani&rft.aufirst=A&rft.date=2005-12-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Annual+Meeting+of+the+American+Society+for+Cell+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Activities of Dolastatin 15 Peptide Analogs as Inhibitors of Tubulin Assembly and Vinblastine Binding
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39634706; 4032769
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Edler, M C
AU  - Bai, R
AU  - Hamel, E
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Vinblastine
KW  - Peptides
KW  - Analogs
KW  - Inhibitors
KW  - Tubulin
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39634706?accountid=14244
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L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Induction of Macroautophagy by Proteasome Inhibition in Living Cells
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39633683; 4034675
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Hailey, D W
AU  - Whiteman, E L
AU  - Lorenz, H
AU  - Lippincott-Schwartz, J
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Proteasomes
KW  - U 7000:Multidisciplinary
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L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Differential Sulfation Pattern of Chondroitin Regulates Axonal Guidance
T2  - 45th Annual Meeting of the American Society for Cell Biology
AN  - 39632645; 4034877
JF  - 45th Annual Meeting of the American Society for Cell Biology
AU  - Katagiri, Y
AU  - Wang, H
AU  - Geller, H M
Y1  - 2005/12/10/
PY  - 2005
DA  - 2005 Dec 10
KW  - Axon guidance
KW  - U 7000:Multidisciplinary
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L2  - http://www.ascb.org/meetings/am2005/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Neuroscience. Synaptic membranes bend to the will of a neurotoxin.
AN  - 68892494; 16339436
JF  - Science (New York, N.Y.)
AU  - Zimmerberg, Joshua
AU  - Chernomordik, Leonid V
AD  - Laboratory of Cellular and Molecular Biophysics, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, MD 20892-1855, USA. joshz@helix.nih.gov
Y1  - 2005/12/09/
PY  - 2005
DA  - 2005 Dec 09
SP  - 1626
EP  - 1627
VL  - 310
IS  - 5754
KW  - Fatty Acids
KW  - 0
KW  - Lipid Bilayers
KW  - Lysophospholipids
KW  - Membrane Lipids
KW  - Micelles
KW  - Neurotoxins
KW  - Neurotransmitter Agents
KW  - Phospholipases A
KW  - EC 3.1.1.32
KW  - Index Medicus
KW  - Animals
KW  - Neurotoxins -- metabolism
KW  - Membrane Lipids -- metabolism
KW  - Exocytosis
KW  - Mice
KW  - Neuromuscular Junction -- physiology
KW  - Neurotoxins -- toxicity
KW  - Hydrolysis
KW  - Neuromuscular Junction -- drug effects
KW  - Neurotransmitter Agents -- metabolism
KW  - Membrane Lipids -- analysis
KW  - Membrane Fusion
KW  - Synaptic Vesicles -- physiology
KW  - Phospholipases A -- toxicity
KW  - Synaptic Membranes -- chemistry
KW  - Lysophospholipids -- metabolism
KW  - Synaptic Membranes -- physiology
KW  - Phospholipases A -- metabolism
KW  - Fatty Acids -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-19
N1  - Date created - 2005-12-12
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment On:
Science. 2005 Dec 9;310(5754):1678-80 [16339444]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Multifunctional roles of the conserved Arg residues in the second region of homology of p97/valosin-containing protein.
AN  - 68859656; 16216872
AB  - The 97-kDa molecular chaperone valosin-containing protein (VCP) belongs to a highly conserved AAA family and forms a hexameric structure that is essential for its biological functions. The AAA domain contains highly conserved motifs, the Walker A, Walker B, and the second region of homology (SRH). Although Walker A and B motifs mediate ATP binding and hydrolysis, respectively, the function of the SRH in VCP is not clear. We examined the significance of the SRH in VCP, especially the conserved Arg(359) and Arg(362) in the first AAA domain, D1 and Arg(635) and Arg(638) in the second AAA domain, D2. We show that Arg(359) and Arg(362) in D1 are critical for maintaining the hexameric structure and the ability to bind the polyubiquitin chains. Although the rest of the tested SRH mutants retain the hexameric structure, all of them exhibit severely reduced ATPase activity. Tryptophan fluorescence analysis showed that all of the tested mutants can bind to ATP or ADP. Thus, the reduced ATPase activity likely results from the hampered communications among protomers during hydrolysis. Moreover, when the ATPase-defective mutant R635A or R638A is mixed with the Walker A mutant of D2, the ATPase activity is partially restored, suggesting that Arg(635) and Arg(638) can stimulate the ATPase activity of the neighboring protomer. Interestingly, mutation of Arg(359) and Arg(362) uncouples the inhibitory effect of p47, a VCP co-factor, on the ATPase activity of VCP. Therefore, the Arg residues allow D1 to take on a specific conformation that is required for substrate binding and co-factor communications. Taken together, these results demonstrate that the conserved Arg residues in the SRH of both D1 and D2 play critical roles in communicating the conformational changes required for ATP hydrolysis, and SRH in D1 also contributes to substrate binding and co-factor communications.
JF  - The Journal of biological chemistry
AU  - Wang, Qing
AU  - Song, Changcheng
AU  - Irizarry, Lauren
AU  - Dai, Renming
AU  - Zhang, Xiaodong
AU  - Li, Chou-Chi H
AD  - Laboratory of Cancer Prevention, National Cancer Institute at Frederick, National Institutes of Health, Frederick, Maryland 21702, USA. qwang@ncifcrf.gov
Y1  - 2005/12/09/
PY  - 2005
DA  - 2005 Dec 09
SP  - 40515
EP  - 40523
VL  - 280
IS  - 49
SN  - 0021-9258, 0021-9258
KW  - Cell Cycle Proteins
KW  - 0
KW  - Recombinant Fusion Proteins
KW  - Polyubiquitin
KW  - 120904-94-1
KW  - Tryptophan
KW  - 8DUH1N11BX
KW  - Adenosine Triphosphate
KW  - 8L70Q75FXE
KW  - Arginine
KW  - 94ZLA3W45F
KW  - Adenosine Triphosphatases
KW  - EC 3.6.1.-
KW  - CDC48 protein
KW  - Index Medicus
KW  - Mutagenesis, Site-Directed
KW  - Polyubiquitin -- metabolism
KW  - Spectrometry, Fluorescence
KW  - Adenosine Triphosphate -- metabolism
KW  - Molecular Sequence Data
KW  - Adenosine Triphosphatases -- metabolism
KW  - Amino Acid Sequence
KW  - Tryptophan -- chemistry
KW  - Hydrolysis
KW  - Adenosine Triphosphatases -- genetics
KW  - Structure-Activity Relationship
KW  - Protein Conformation
KW  - Cell Cycle Proteins -- physiology
KW  - Cell Cycle Proteins -- chemistry
KW  - Conserved Sequence
KW  - Cell Cycle Proteins -- genetics
KW  - Arginine -- genetics
KW  - Arginine -- chemistry
KW  - Arginine -- physiology
KW  - Sequence Homology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-06
N1  - Date created - 2005-12-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Induction of apoptosis in human leukemia cells by black tea and its polyphenol theaflavin.
AN  - 68734903; 16253767
AB  - Treatment of human leukemic cell lines HL-60 and K-562 with extracts of green and black tea and their polyphenols epigallocatechin gallate and theaflavins, respectively, showed a dose dependent inhibition of growth as a result of cytotoxicity and suppression of cell proliferation. Based on the IC50 values obtained from cytotoxicity data it was clearly evident that black tea was as efficient as green tea. Analysis of polyphenol contents of tea extracts revealed that not only epigallocatechin gallate, which is a predominant polyphenol of green tea, but also theaflavin that is abundantly present in black tea affords significant chemotherapeutic action by imparting cytotoxicity to human leukemic cells. Electrophoretic analysis of fragmented DNA from treated cells displayed characteristic ladder pattern. Flow cytometric analysis revealed the dose dependent increase in sub-G1 peak. These criteria confirmed that cytotoxic activity of green and black tea was due to induction of apoptosis. Such induction was found to be mediated through activation of caspases 3 and 8, particularly caspase 3 and by altering apoptosis related genes as evident by down-regulation of Bcl-2 and up-regulation of Bax proteins.
JF  - Cancer letters
AU  - Kundu, Trina
AU  - Dey, Subhabrata
AU  - Roy, Madhumita
AU  - Siddiqi, M
AU  - Bhattacharya, R K
AD  - Department of Environmental Carcinogenesis and Toxicology, Chittaranjan National Cancer Institute, 37 S.P. Mukherjee Road, Kolkata 700 026, India.
Y1  - 2005/12/08/
PY  - 2005
DA  - 2005 Dec 08
SP  - 111
EP  - 121
VL  - 230
IS  - 1
SN  - 0304-3835, 0304-3835
KW  - Antioxidants
KW  - 0
KW  - Biflavonoids
KW  - Flavonoids
KW  - Phenols
KW  - Polyphenols
KW  - Tea
KW  - bcl-2-Associated X Protein
KW  - theaflavin
KW  - 1IA46M0D13
KW  - Catechin
KW  - 8R1V1STN48
KW  - CASP3 protein, human
KW  - EC 3.4.22.-
KW  - CASP8 protein, human
KW  - Caspase 3
KW  - Caspase 8
KW  - Caspases
KW  - Index Medicus
KW  - Phenols -- pharmacology
KW  - HL-60 Cells
KW  - Humans
KW  - Caspases -- metabolism
KW  - Phenols -- analysis
KW  - Flavonoids -- analysis
KW  - Genes, bcl-2
KW  - Down-Regulation
KW  - Flow Cytometry
KW  - Caspases -- drug effects
KW  - Flavonoids -- pharmacology
KW  - Antioxidants -- pharmacology
KW  - Apoptosis -- drug effects
KW  - Biflavonoids -- pharmacology
KW  - Tea -- chemistry
KW  - Catechin -- pharmacology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-23
N1  - Date created - 2005-10-28
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Diphenylmethyl selenocyanate inhibits DMBA-croton oil induced two-stage mouse skin carcinogenesis by inducing apoptosis and inhibiting cutaneous cell proliferation.
AN  - 68733085; 16253765
AB  - Numerous epidemiological and experimental studies have showed the inverse relationship between dietary selenium intake and different types of cancer. Continuous efforts are going on to develop suitable organoselenium compounds, which can be used as cancer chemopreventive agents for human. In the present study, a synthetic organoselenium compound diphenylmethyl selenocyanate was evaluated for its ability to arrest cell proliferation and to induce apoptosis against 7,12-dimethylbenz[a]anthracene-croton oil induced two-stage mouse skin carcinogenesis model. Reduction in the incidence and number of papilloma, the preneoplastic lesion, was considered to be the mean of assessment. Significant decrease in the level of cell proliferation (p<0.01) and significant enhancement in the level of apoptosis (p<0.01) were found. Caspase-3, which contribute a part in the process of cellular apoptosis to prevent further cellular differentiation was also elevated significantly (P<0.01) during the treatment with the Se compound. These observations seem to be correlated with the significant reduction in the corresponding number of skin papilloma formation after 12 weeks of experiment. Thus the compound, diphenylmethyl selenocyanate may be considered for further research to establish it as an effective cancer chemopreventive agent.
JF  - Cancer letters
AU  - Das, Rajat Kumar
AU  - Hossain, S K Ugir
AU  - Bhattacharya, Sudin
AD  - Department of Cancer Chemoprevention, Chittaranjan National Cancer Institute, 37, S.P. Mukherjee Road, Kolkata 700 026, India.
Y1  - 2005/12/08/
PY  - 2005
DA  - 2005 Dec 08
SP  - 90
EP  - 101
VL  - 230
IS  - 1
SN  - 0304-3835, 0304-3835
KW  - Carcinogens
KW  - 0
KW  - Dermatologic Agents
KW  - Organoselenium Compounds
KW  - diphenylmethyl selenocyanate
KW  - 9,10-Dimethyl-1,2-benzanthracene
KW  - 57-97-6
KW  - Croton Oil
KW  - 8001-28-3
KW  - CASP3 protein, human
KW  - EC 3.4.22.-
KW  - Casp3 protein, mouse
KW  - Caspase 3
KW  - Caspases
KW  - Index Medicus
KW  - Cell Proliferation -- drug effects
KW  - Animals
KW  - Caspases -- analysis
KW  - Apoptosis -- drug effects
KW  - Caspases -- biosynthesis
KW  - Mice
KW  - Chemoprevention
KW  - Female
KW  - Skin Neoplasms -- physiopathology
KW  - Organoselenium Compounds -- pharmacology
KW  - Croton Oil -- toxicity
KW  - Papilloma -- prevention & control
KW  - 9,10-Dimethyl-1,2-benzanthracene -- toxicity
KW  - Skin Neoplasms -- chemically induced
KW  - Carcinogens -- toxicity
KW  - Papilloma -- physiopathology
KW  - Skin Neoplasms -- prevention & control
KW  - Papilloma -- chemically induced
KW  - Dermatologic Agents -- toxicity
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-23
N1  - Date created - 2005-10-28
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Adjuvant chemotherapy for stage III colon cancer: implications of race/ethnicity, age, and differentiation.
AN  - 68879390; 16333005
AB  - A 1990 National Institutes of Health Consensus Conference recommended that patients with stage III colon cancer receive adjuvant chemotherapy because survival was improved in clinical trials in patients who received a 5-fluorouracil-based regimen.
          To determine whether adjuvant chemotherapy is used in the community as a standard of practice that improves outcome and whether it failed to benefit any specific sets of patients. Prospective data from 85 934 patients with stage III colon cancer from 560 hospital cancer registries were entered into the National Cancer Data Base between 1990 and 2002 and included standard clinical, pathological, and first course of treatment variables.
          Prevalence of adjuvant chemotherapy usage and 5-year survival in patients treated in US hospitals. Adjuvant chemotherapy use increased from 39% in 1991 to 64% in 2002 but was lower in black, female, and elderly patients. It improved 5-year survival from almost 8% in 1991 to more than 16% in 1997 compared with surgery alone. Adjuvant chemotherapy increases survival in elderly patients as much as it does in younger patients. However, the benefit of adjuvant chemotherapy in blacks and those with high-grade cancers is not as great. Adjuvant chemotherapy use has increased from 1990 to 2002 for patients with stage III colon cancer with an associated increase in 5-year survival of 16%. The benefit of adjuvant chemotherapy seems to be lower in black patients and high-grade cancers. Women have the same benefit but are less often treated. Elderly patients have the same benefit as younger patients but are less frequently treated. New options for adjuvant therapy in 2004-2005 may further improve the outcome of patients with stage III colon cancer.
JF  - JAMA
AU  - Jessup, J Milburn
AU  - Stewart, Andrew
AU  - Greene, Frederick L
AU  - Minsky, Bruce D
AD  - Department of Oncology, Georgetown University Medical Center, Washington, DC, USA. jessupj@mail.nih.gov
Y1  - 2005/12/07/
PY  - 2005
DA  - 2005 Dec 07
SP  - 2703
EP  - 2711
VL  - 294
IS  - 21
KW  - Adjuvants, Immunologic
KW  - 0
KW  - Antimetabolites, Antineoplastic
KW  - Levamisole
KW  - 2880D3468G
KW  - Fluorouracil
KW  - U3P01618RT
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - United States
KW  - Age Factors
KW  - Sex Factors
KW  - Neoplasm Staging
KW  - Humans
KW  - Prognosis
KW  - Aged
KW  - European Continental Ancestry Group -- statistics & numerical data
KW  - African Continental Ancestry Group -- statistics & numerical data
KW  - Drug Utilization
KW  - Fluorouracil -- therapeutic use
KW  - Aged, 80 and over
KW  - Middle Aged
KW  - Antimetabolites, Antineoplastic -- therapeutic use
KW  - Male
KW  - Adjuvants, Immunologic -- therapeutic use
KW  - Female
KW  - Survival Analysis
KW  - Proportional Hazards Models
KW  - Levamisole -- therapeutic use
KW  - Chemotherapy, Adjuvant -- utilization
KW  - Colonic Neoplasms -- mortality
KW  - Colonic Neoplasms -- drug therapy
KW  - Colonic Neoplasms -- ethnology
KW  - Colonic Neoplasms -- pathology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-09
N1  - Date created - 2005-12-07
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment In:
JAMA. 2005 Dec 7;294(21):2758-60 [16333012]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Toll-like receptor 4 in butylated hydroxytoluene-induced mouse pulmonary inflammation and tumorigenesis.
AN  - 68874081; 16333033
AB  - Because chronic pulmonary diseases predispose to lung neoplasia, the identification of the molecular mechanisms involved could provide novel preventive, diagnostic, and therapeutic strategies. Toll-like receptors (TLRs) transduce exogenous and endogenous signals into the production of inflammatory cytokines to coordinate adaptive immune responses. To determine the role of Tlr4 in chronic lung inflammation, we compared lung permeability, leukocyte infiltration, and nuclear factor kappa B (NFkappaB) and activator protein 1 (AP-1) DNA binding in butylated hydroxytoluene (BHT)-treated (four weekly injections of 125-200 mg/kg each) inbred mouse strains with functional Tlr4 (OuJ and BALB) and mutated Tlr4 (HeJ and BALB(Lps-d)). We also measured primary tumor formation in these mice after single-carcinogen injection (3-methylcholanthrene; 10 microg/kg), followed by BHT treatment (six weekly injections of 125-200 mg/kg each). Mice with functional Tlr4 had reduced lung permeability, leukocyte inflammation, and primary tumor formation (BALB(Lps-d), mean = 22.3 tumors/mouse, versus BALB, mean = 13.9 tumors/mouse, difference = 8.4 tumors/mouse, 95% confidence interval = 4.6 to 12.1 tumors/mouse; P = .025) compared with mice with mutated Tlr4. NFkappaB DNA binding activity was higher in OuJ than in HeJ mice; however, AP-1 activity was elevated in HeJ mice. To our knowledge, this is the first model to demonstrate a modulatory role for Tlr4 in chronic lung inflammation and tumorigenesis.
JF  - Journal of the National Cancer Institute
AU  - Bauer, Alison K
AU  - Dixon, Darlene
AU  - DeGraff, Laura M
AU  - Cho, Hye-Youn
AU  - Walker, Christopher R
AU  - Malkinson, Alvin M
AU  - Kleeberger, Steven R
AD  - Laboratory of Respiratory Biology, National Institute of Environmental Health Sciences, National Institutes of Health, Research Triangle Park, NC 27709, USA. bauer1@niehs.nih.gov
Y1  - 2005/12/07/
PY  - 2005
DA  - 2005 Dec 07
SP  - 1778
EP  - 1781
VL  - 97
IS  - 23
KW  - NF-kappa B
KW  - 0
KW  - Tlr4 protein, mouse
KW  - Toll-Like Receptor 4
KW  - Transcription Factor AP-1
KW  - Butylated Hydroxytoluene
KW  - 1P9D0Z171K
KW  - Index Medicus
KW  - Mice, Inbred Strains
KW  - Animals
KW  - Transcription Factor AP-1 -- metabolism
KW  - Disease Models, Animal
KW  - Mice
KW  - Mutation
KW  - NF-kappa B -- metabolism
KW  - Pneumonia -- chemically induced
KW  - Toll-Like Receptor 4 -- genetics
KW  - Toll-Like Receptor 4 -- metabolism
KW  - Lung Neoplasms -- chemically induced
KW  - Pneumonia -- metabolism
KW  - Lung Neoplasms -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-15
N1  - Date created - 2005-12-07
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Mutational analysis of the Arf1*GTP/Arf GAP interface reveals an Arf1 mutant that selectively affects the Arf GAP ASAP1.
AN  - 68876671; 16332543
AB  - Arf1 is a GTP binding protein that functions at a number of cellular sites to control membrane traffic and actin remodeling. Arf1 is regulated by site-specific GTPase-activating proteins (GAPs). The combined results of crystallographic and biochemical studies have led to the proposal that Arf1 GAPs differ in the specific interface formed with Arf1. To test this hypothesis, we have used mutagenesis to examine the interaction of three Arf GAPs (ASAP1, AGAP1, and ArfGAP1) with switch 1, switch 2, and alpha helix3 of Arf1. The GAPs were similar in being affected by mutations in switch 1 and 2. However, effects of a mutation within alpha helix3 and specific mutations within switch 1 and 2 differed among the GAPs. The largest differences were observed with a change of isoleucine 46 to aspartate ([I46D]Arf1), which reduced ASAP1-induced catalysis by approximately 10,000-fold but had a 3-fold effect on AGAP1. The reduction was due to an isolated effect on the catalytic rate, k(cat). In vivo [I46D]Arf1 had no detectable effect on the Golgi apparatus but, instead, functioned as a constitutively active mutant in the cell periphery, affecting the localization of ASAP1 and paxillin. Based on our results, we conclude that the contribution of specific residues within switch 1 of Arf to binding and achieving a transition state toward GTP hydrolysis differs among Arf GAPs.
JF  - Current biology : CB
AU  - Luo, Ruibai
AU  - Jacques, Kerry
AU  - Ahvazi, Bijan
AU  - Stauffer, Stacey
AU  - Premont, Richard T
AU  - Randazzo, Paul A
AD  - Laboratory of Cellular Oncology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/12/06/
PY  - 2005
DA  - 2005 Dec 06
SP  - 2164
EP  - 2169
VL  - 15
IS  - 23
SN  - 0960-9822, 0960-9822
KW  - AGAP1 protein, human
KW  - 0
KW  - ASAP1 protein, human
KW  - Adaptor Proteins, Signal Transducing
KW  - GTPase-Activating Proteins
KW  - Guanosine Triphosphate
KW  - 86-01-1
KW  - ADP-Ribosylation Factor 1
KW  - EC 3.6.5.2
KW  - ADP-Ribosylation Factors
KW  - Index Medicus
KW  - Animals
KW  - Humans
KW  - DNA Mutational Analysis
KW  - Mutation -- genetics
KW  - Mice
KW  - Golgi Apparatus -- metabolism
KW  - Fluorescent Antibody Technique
KW  - NIH 3T3 Cells
KW  - Guanosine Triphosphate -- metabolism
KW  - Catalysis
KW  - Adaptor Proteins, Signal Transducing -- metabolism
KW  - GTPase-Activating Proteins -- metabolism
KW  - Models, Molecular
KW  - ADP-Ribosylation Factors -- metabolism
KW  - ADP-Ribosylation Factor 1 -- metabolism
KW  - ADP-Ribosylation Factor 1 -- genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68876671?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Current+biology+%3A+CB&rft.atitle=Mutational+analysis+of+the+Arf1*GTP%2FArf+GAP+interface+reveals+an+Arf1+mutant+that+selectively+affects+the+Arf+GAP+ASAP1.&rft.au=Luo%2C+Ruibai%3BJacques%2C+Kerry%3BAhvazi%2C+Bijan%3BStauffer%2C+Stacey%3BPremont%2C+Richard+T%3BRandazzo%2C+Paul+A&rft.aulast=Luo&rft.aufirst=Ruibai&rft.date=2005-12-06&rft.volume=15&rft.issue=23&rft.spage=2164&rft.isbn=&rft.btitle=&rft.title=Current+biology+%3A+CB&rft.issn=09609822&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-07-12
N1  - Date created - 2005-12-07
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - The "Binding Site Barrier" and other Factors that Limit Antibody Penetration into Tumors
T2  - 16th Annual International Antibody Engineering Conference (Antibody Engineering)
AN  - 39828293; 4041305
JF  - 16th Annual International Antibody Engineering Conference (Antibody Engineering)
AU  - Weinstein, John N
Y1  - 2005/12/05/
PY  - 2005
DA  - 2005 Dec 05
KW  - Barriers
KW  - Antibodies
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39828293?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=16th+Annual+International+Antibody+Engineering+Conference+%28Antibody+Engineering%29&rft.atitle=The+%22Binding+Site+Barrier%22+and+other+Factors+that+Limit+Antibody+Penetration+into+Tumors&rft.au=Weinstein%2C+John+N&rft.aulast=Weinstein&rft.aufirst=John&rft.date=2005-12-05&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=16th+Annual+International+Antibody+Engineering+Conference+%28Antibody+Engineering%29&rft.issn=&rft_id=info:doi/
L2  - http://www.ibclifesciences.com/antibodyeng
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Integrating Hypothesis-Driven and "Omic" Approaches to Cancer Biology, Biomarkers, and Therapeutics
T2  - 16th Annual International Antibody Engineering Conference (Antibody Engineering)
AN  - 39752940; 4041290
JF  - 16th Annual International Antibody Engineering Conference (Antibody Engineering)
AU  - Weinstein, John N
Y1  - 2005/12/05/
PY  - 2005
DA  - 2005 Dec 05
KW  - Bioindicators
KW  - Biomarkers
KW  - Cancer
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39752940?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=16th+Annual+International+Antibody+Engineering+Conference+%28Antibody+Engineering%29&rft.atitle=Integrating+Hypothesis-Driven+and+%22Omic%22+Approaches+to+Cancer+Biology%2C+Biomarkers%2C+and+Therapeutics&rft.au=Weinstein%2C+John+N&rft.aulast=Weinstein&rft.aufirst=John&rft.date=2005-12-05&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=16th+Annual+International+Antibody+Engineering+Conference+%28Antibody+Engineering%29&rft.issn=&rft_id=info:doi/
L2  - http://www.ibclifesciences.com/antibodyeng
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Error-prone translesion synthesis by human DNA polymerase eta on DNA-containing deoxyadenosine adducts of 7,8-dihydroxy-9,10-epoxy-7,8,9,10-tetrahydrobenzo[a]pyrene.
AN  - 68839904; 16188888
AB  - When human DNA polymerase eta (pol eta) encounters N6-deoxyadenosine adducts formed by trans epoxide ring opening of the 7,8-dihydroxy-9,10-epoxy-7,8,9,10-tetrahydrobenzo[a]pyrene (BaP DE) isomer with (+)-7R,8S,9S,10R configuration ((+)-BaP DE-2), misincorporation of A or G and incorporation of the correct T are equally likely to occur. On the other hand, the enzyme exhibits a 3-fold preference for correct T incorporation opposite adducts formed by trans ring opening of the (-)-(7S,8R,9R,10S)-DE-2 enantiomer. Adducts at dA formed by cis ring opening of these two BaP DE-2 isomers exhibit a 2-3-fold preference for A over T incorporation, with G intermediate between the two. Extension one nucleotide beyond these adducts is generally weaker than incorporation across from them, but among mismatches the (adducted A*) x A mispair is the most favored for extension. Because mutations can only occur if mispairs are extended, this observation is consistent with the occurrence of A x T to T x A transversions as common mutations in animal cells treated with BaP DE-2 isomers. Adducts with S absolute configuration at the point of attachment of the hydrocarbon to the base inhibit incorporation and extension by pol eta to a lesser extent than their R counterparts. Template-primers containing each of the four isomeric dA adducts derived from BaP DE-2 and two adducts derived from 9,10-epoxy-7,8,9,10-tetrahydrobenzo-[a]pyrene in which the 7- and 8-hydroxyl groups of the DEs are replaced with hydrogens exhibit reduced electrophoretic mobilities relative to the unadducted oligonucleotides. This effect is largely independent of DNA sequence. Decreased mobility correlates with an increased rate of incorporation by pol eta, suggesting a systematic relationship between the overall DNA structure and efficiency of the enzyme.
JF  - The Journal of biological chemistry
AU  - Chiapperino, Dominic
AU  - Cai, Mangmang
AU  - Sayer, Jane M
AU  - Yagi, Haruhiko
AU  - Kroth, Heiko
AU  - Masutani, Chikahide
AU  - Hanaoka, Fumio
AU  - Jerina, Donald M
AU  - Cheh, Albert M
AD  - Laboratory of Bioorganic Chemistry, NIDDK, National Institutes of Health, DHHS, Bethesda, Maryland 20892, USA.
Y1  - 2005/12/02/
PY  - 2005
DA  - 2005 Dec 02
SP  - 39684
EP  - 39692
VL  - 280
IS  - 48
SN  - 0021-9258, 0021-9258
KW  - DNA Adducts
KW  - 0
KW  - DNA Primers
KW  - Deoxyadenosines
KW  - Hydrocarbons
KW  - Oligonucleotides
KW  - 7,8-Dihydro-7,8-dihydroxybenzo(a)pyrene 9,10-oxide
KW  - 55097-80-8
KW  - Hydrogen
KW  - 7YNJ3PO35Z
KW  - DNA
KW  - 9007-49-2
KW  - DNA-Directed DNA Polymerase
KW  - EC 2.7.7.7
KW  - Rad30 protein
KW  - Index Medicus
KW  - Hydrocarbons -- chemistry
KW  - Oligonucleotides -- chemistry
KW  - Hydrogen -- chemistry
KW  - Electrophoresis, Polyacrylamide Gel
KW  - Kinetics
KW  - Humans
KW  - Models, Chemical
KW  - Sequence Analysis, DNA
KW  - Nucleic Acid Conformation
KW  - Mutation
KW  - DNA Primers -- chemistry
KW  - DNA-Directed DNA Polymerase -- physiology
KW  - DNA Repair
KW  - Base Pair Mismatch
KW  - DNA -- chemistry
KW  - Deoxyadenosines -- chemistry
KW  - 7,8-Dihydro-7,8-dihydroxybenzo(a)pyrene 9,10-oxide -- chemistry
KW  - DNA-Directed DNA Polymerase -- chemistry
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2005-11-28
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Reactive oxygen species and p38 phosphorylation regulate the protective effect of Delta9-tetrahydrocannabinol in the apoptotic response to NMDA.
AN  - 68554545; 16098661
AB  - NMDA causes oxidative stress in neurons, and produces cell death involving elements of both necrosis and apoptosis. To examine the neuroprotective mechanism of Delta9-tetrahydrocannabinol (THC) in NMDA-induced death of AF5 cells, we measured reactive oxygen species (ROS) formation after exposure to NMDA. ROS generation was increased by NMDA, and NMDA-induced ROS generation was significantly decreased by THC. Western blotting revealed an increase in phosphorylated p38 MAPK after NMDA treatment, which was also blocked by pretreatment with THC. The time course of ROS generation and activation of MAPK signaling pathways were similar. SB203580, a p38 inhibitor, partially blocked glutamate excitotoxicity in AF5 cells. The present data suggest that THC protects against NMDA-induced apoptosis in AF5 cells by blocking ROS generation and inhibiting the activation of p38-MAPK.
JF  - Neuroscience letters
AU  - Chen, Jia
AU  - Errico, Stacie L
AU  - Freed, William J
AD  - Development and Plasticity Section, Cellular Neurobiology Research Branch, Intramural Research Program, National Institute on Drug Abuse, National Institutes of Health, Baltimore, MD 21224, USA. jchen@intra.nida.nih.gov
Y1  - 2005/12/02/
PY  - 2005
DA  - 2005 Dec 02
SP  - 99
EP  - 103
VL  - 389
IS  - 2
SN  - 0304-3940, 0304-3940
KW  - Enzyme Inhibitors
KW  - 0
KW  - Neuroprotective Agents
KW  - Neurotoxins
KW  - Reactive Oxygen Species
KW  - N-Methylaspartate
KW  - 6384-92-5
KW  - Dronabinol
KW  - 7J8897W37S
KW  - p38 Mitogen-Activated Protein Kinases
KW  - EC 2.7.11.24
KW  - Index Medicus
KW  - Animals
KW  - MAP Kinase Signaling System -- drug effects
KW  - Neurodegenerative Diseases -- physiopathology
KW  - MAP Kinase Signaling System -- physiology
KW  - Dose-Response Relationship, Drug
KW  - Enzyme Activation -- physiology
KW  - Phosphorylation -- drug effects
KW  - Neuroprotective Agents -- pharmacology
KW  - Oxidative Stress -- physiology
KW  - Cell Survival -- drug effects
KW  - Neurodegenerative Diseases -- metabolism
KW  - Oxidative Stress -- drug effects
KW  - Enzyme Activation -- drug effects
KW  - Enzyme Inhibitors -- pharmacology
KW  - Cell Line, Transformed
KW  - Cell Survival -- physiology
KW  - Reactive Oxygen Species -- metabolism
KW  - p38 Mitogen-Activated Protein Kinases -- antagonists & inhibitors
KW  - Dronabinol -- pharmacology
KW  - Apoptosis -- physiology
KW  - Apoptosis -- drug effects
KW  - N-Methylaspartate -- toxicity
KW  - N-Methylaspartate -- antagonists & inhibitors
KW  - Neurotoxins -- toxicity
KW  - p38 Mitogen-Activated Protein Kinases -- metabolism
KW  - Neurotoxins -- antagonists & inhibitors
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-24
N1  - Date created - 2005-09-06
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Am J Physiol Heart Circ Physiol. 2003 Aug;285(2):H822-32 [12714335]
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J Neurochem. 2003 Feb;84(3):566-75 [12558976]
J Cell Physiol. 2002 Jul;192(1):1-15 [12115731]
Exp Neurol. 2002 Jun;175(2):318-37 [12061863]
J Neurochem. 2002 Feb;80(3):448-56 [11905991]
Neurochem Res. 2001 May;26(5):525-32 [11513480]
J Neurochem. 2001 May;77(3):957-60 [11331425]
J Neurosci. 2000 Aug 1;20(15):5715-23 [10908611]
Mol Pharmacol. 2000 Oct;58(4):814-20 [10999952]
J Physiol. 2001 Feb 15;531(Pt 1):147-63 [11179399]
Trends Pharmacol Sci. 1999 Nov;20(11):441-4 [10542441]
Neuroreport. 2003 Oct 6;14(14):1815-9 [14534426]
Exp Cell Res. 2003 Nov 15;291(1):251-66 [14597424]
Neurosci Lett. 1986 May 15;66(2):193-8 [3014386]
Brain Res Mol Brain Res. 2005 Apr 4;134(2):215-25 [15836919]
Anesth Analg. 2005 Apr;100(4):929-36 [15781500]
Rev Pneumol Clin. 2005 Feb;61(1 Pt 1):16-21 [15772575]
Mol Cell Neurosci. 2005 Jan;28(1):189-94 [15607953]
Annu Rev Physiol. 1998;60:619-42 [9558479]
J Biol Chem. 1997 Jul 25;272(30):18518-21 [9228012]
Neuron. 1995 Feb;14(2):303-15 [7857640]
FEBS Lett. 1995 May 8;364(2):229-33 [7750577]
J Biol Chem. 1986 Oct 25;261(30):14201-8 [2876985]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Distinct Protein Classes Including Novel Merozoite Surface Antigens in Raft-like Membranes of Plasmodium falciparum
AN  - 20254325; 7143458
AB  - Glycosylphosphatidylinositol (GPI)-anchored proteins coat the surface of extracellular Plasmodium falciparum merozoites, of which several are highly validated candidates for inclusion in a blood-stage malaria vaccine. Here we determined the proteome of gradient-purified detergent-resistant membranes of mature blood-stage parasites and found that these membranes are greatly enriched in GPI-anchored proteins and their putative interacting partners. Also prominent in detergent-resistant membranes are apical organelle (rhoptry), multimembrane-spanning, and proteins destined for export into the host erythrocyte cytosol. Four new GPI-anchored proteins were identified, and a number of other novel proteins that are predicted to localize to the merozoite surface and/or apical organelles were detected. Three of the putative surface proteins possessed six-cysteine (Cys sub(6)) motifs, a distinct fold found in adhesive surface proteins expressed in other life stages. All three Cys sub(6) proteins, termed Pf12, Pf38, and Pf41, were validated as merozoite surface antigens recognized strongly by antibodies present in naturally infected individuals. In addition to the merozoite surface, Pf38 was particularly prominent in the secretory apical organelles. A different cysteine-rich putative GPI-anchored protein, Pf92, was also localized to the merozoite surface. This insight into merozoite surfaces provides new opportunities for understanding both erythrocyte invasion and anti-parasite immunity.
JF  - Journal of Biological Chemistry
AU  - Sanders, Paul R
AU  - Gilson, Paul R
AU  - Cantin, Greg T
AU  - Greenbaum, Doron C
AU  - Nebl, Thomas
AU  - Carucci, Daniel J
AU  - McConville, Malcolm J
AU  - Schofield, Louis
AU  - Hodder, Anthony N
AU  - Yates, John RIII
AU  - Crabb, Brendan S
AD  - The Walter and Eliza Hall Institute of Medical Research, Parkville, VIC 3050 Australia, The Co-operative Research Centre for Vaccine Technology, Australia and the Department of Medical Biology, The University of Melbourne, VIC 3010 Australia, the Department of Cell Biology, The Scripps Research Institute, La, Jolla, California 92037, The Foundation for the National Institutes of Health, Bethesda, Maryland 20814, and the Department of Biochemistry and Molecular Biology, The University of Melbourne, VIC 3050 Australia
Y1  - 2005/12/02/
PY  - 2005
DA  - 2005 Dec 02
SP  - 40169
EP  - 40176
PB  - American Society for Biochemistry and Molecular Biology, 9650 Rockville Pike Bethesda MD 20814-3996 USA, [mailto:asbmb@asbmb.faseb.org]
VL  - 280
IS  - 48
SN  - 0021-9258, 0021-9258
KW  - ASFA 3: Aquatic Pollution & Environmental Quality; Biotechnology and Bioengineering Abstracts; Microbiology Abstracts C: Algology, Mycology & Protozoology
KW  - Parasites
KW  - Human diseases
KW  - Erythrocytes
KW  - Disease control
KW  - Malaria
KW  - Antigens
KW  - Protein folding
KW  - Glycosylphosphatidylinositol
KW  - Adhesives
KW  - Protein transport
KW  - Developmental stages
KW  - Plasmodium falciparum
KW  - Immunity
KW  - Antibodies
KW  - surface antigens
KW  - Cytosol
KW  - Merozoites
KW  - Vaccines
KW  - Organelles
KW  - K 03330:Biochemistry
KW  - W 30915:Pharmaceuticals & Vaccines
KW  - Q5 08524:Public health, medicines, dangerous organisms
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20254325?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aasfaaquaticpollution&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Biological+Chemistry&rft.atitle=Distinct+Protein+Classes+Including+Novel+Merozoite+Surface+Antigens+in+Raft-like+Membranes+of+Plasmodium+falciparum&rft.au=Sanders%2C+Paul+R%3BGilson%2C+Paul+R%3BCantin%2C+Greg+T%3BGreenbaum%2C+Doron+C%3BNebl%2C+Thomas%3BCarucci%2C+Daniel+J%3BMcConville%2C+Malcolm+J%3BSchofield%2C+Louis%3BHodder%2C+Anthony+N%3BYates%2C+John+RIII%3BCrabb%2C+Brendan+S&rft.aulast=Sanders&rft.aufirst=Paul&rft.date=2005-12-02&rft.volume=280&rft.issue=48&rft.spage=40169&rft.isbn=&rft.btitle=&rft.title=Journal+of+Biological+Chemistry&rft.issn=00219258&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2016-05-27
N1  - SubjectsTermNotLitGenreText - Parasites; Human diseases; Antigens; Erythrocytes; Disease control; Malaria; Immunity; Vaccines; Protein transport; Developmental stages; Antibodies; Protein folding; surface antigens; Cytosol; Merozoites; Glycosylphosphatidylinositol; Organelles; Adhesives; Plasmodium falciparum
ER  - 



TY  - JOUR
T1  - Conservation and variation of gene regulation in embryonic stem cells assessed by comparative genomics
AN  - 864949249; 13857308
AB  - We have examined the gene structure and regulatory regions of octamer-binding transcription factor 3/4 (Oct 3/4), sex determining region Y box 2 (Sox2), signal transducer and activator of transcription 3 (Stat3), embryonal stem cell-specific gene 1 (ESG), nanog homeobox (Nanog), and several other genes highly expressed in embryonic stem (ES) cells across different species. Our analysis showed that ES cell-expressed Ras (ERAS) was orthologous to a human pseudogene Harvey Ras (HRASP) and that the promoter and other regulatory sequences were highly divergent. No ortholog of (ES) cell-derived homeobox containing gene (Ehox) could be identified in human, and the closest paralogs PEPP gene subfamily 1 (PEPP1), PEPP2, and extraembryonic, spermatogenesis, homeobox 1 (Esx1) were not expressed by ES cells and shared little homology. The Sox2 promoter was the most conserved across species and the Oct3/4 promoter region showed significant homology particularly in the distal enhancer active in ES cells. Analysis suggested common and divergent pathways of regulation. Conserved Oct3/4 and Sox2 co-binding domains were identified in most ES expressed genes, highlighting the importance of this transcriptional pathway. Conserved fibroblast growth factor response element sites were identified in regulatory regions, suggesting a potential parallel pathway for regulation by FGFs. A central role of Stat3 activation in self-renewal and in a regulatory feedback loop was suggested by the identification of the conserved binding sites in most pathways. Although most pathways were evolutionarily conserved, promoters and genomic structure of the leukemia inhibitory factor (LIF) pathway components were divergent, likely explaining the differential requirement of LIF for human and rodent cells. Our analysis further suggested that the Nanog regulatory pathway was relatively independent of the LIF/Oct pathway and may interact with the Nodal/transforming growth factor-b pathway. These results provide a framework for examining the current reported differences between rodent and human ES cells and define targets for future perturbation studies.
JF  - Cell Biochemistry and Biophysics
AU  - Zhan, Ming
AU  - Miura, Takumi
AU  - Xu, Xiangru
AU  - Rao, Mahendra S
AD  - Stem Cell Section, Laboratory of Neurosciences, National Institute on Aging, NIH, 21224, Baltimore, MD
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 379
EP  - 405
PB  - Humana Press Inc., 999 Riverview Dr., Ste. 208 Totowa NJ 07512 USA
VL  - 43
IS  - 3
SN  - 1085-9195, 1085-9195
KW  - Genetics Abstracts; Biochemistry Abstracts 2: Nucleic Acids; Biotechnology and Bioengineering Abstracts
KW  - Ras protein
KW  - Pseudogenes
KW  - Stat3 protein
KW  - Leukemia inhibitory factor
KW  - Regulatory sequences
KW  - Homeobox
KW  - Spermatogenesis
KW  - Promoters
KW  - Enhancers
KW  - Stem cells
KW  - Homology
KW  - Embryo cells
KW  - Gene regulation
KW  - Transcription factors
KW  - Fibroblast growth factor
KW  - Transforming growth factor- beta
KW  - Conservation
KW  - Transforming growth factor-b
KW  - Feedback
KW  - genomics
KW  - Oct-4 protein
KW  - Evolution
KW  - Sex
KW  - N 14835:Protein-Nucleic Acids Association
KW  - G 07730:Development & Cell Cycle
KW  - W 30965:Miscellaneous, Reviews
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/864949249?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cell+Biochemistry+and+Biophysics&rft.atitle=Conservation+and+variation+of+gene+regulation+in+embryonic+stem+cells+assessed+by+comparative+genomics&rft.au=Zhan%2C+Ming%3BMiura%2C+Takumi%3BXu%2C+Xiangru%3BRao%2C+Mahendra+S&rft.aulast=Zhan&rft.aufirst=Ming&rft.date=2005-12-01&rft.volume=43&rft.issue=3&rft.spage=379&rft.isbn=&rft.btitle=&rft.title=Cell+Biochemistry+and+Biophysics&rft.issn=10859195&rft_id=info:doi/10.1385%2FCBB%3A43%3A3%3A379
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2011-05-01
N1  - Last updated - 2012-03-29
N1  - SubjectsTermNotLitGenreText - Ras protein; Pseudogenes; Leukemia inhibitory factor; Stat3 protein; Regulatory sequences; Homeobox; Spermatogenesis; Enhancers; Promoters; Stem cells; Embryo cells; Homology; Transcription factors; Gene regulation; Transforming growth factor- beta; Fibroblast growth factor; Transforming growth factor-b; Conservation; Feedback; genomics; Oct-4 protein; Evolution; Sex
DO  - http://dx.doi.org/10.1385/CBB:43:3:379
ER  - 



TY  - JOUR
T1  - Automatic Priming of Semantically Related Words Reduces Activity in the Fusiform Gyrus
AN  - 85632733; 200609750
AB  - We used rapid, event-related fMRI to identify the neural systems underlying object semantics. During scanning, subjects silently read rapidly presented word pairs (150 msec, SOA = 250 msec) that were either unrelated in meaning (ankle-carrot), semantically related (fork-cup), or identical (crow-crow). Activity in the left posterior region of the fusiform gyrus & left inferior frontal cortex was modulated by word-pair relationship. Semantically related pairs yielded less activity than unrelated pairs, but greater activity than identical pairs, mirroring the pattern of behavioral facilitation as measured by word reading times. These findings provide strong support for the involvement of these areas in the automatic processing of object meaning. In addition, words referring to animate objects produced greater activity in the lateral region of the fusiform gyri, right superior temporal sulcus, & medial region of the occipital lobe relative to manmade, manipulable objects, whereas words referring to manmade, manipulable objects produced greater activity in the left ventral premotor, left anterior cingulate, & bilateral parietal cortices relative to animate objects. These findings are consistent with the dissociation between these areas based on sensory- & motor-related object properties, providing further evidence that conceptual object knowledge is housed, in part, in the same neural systems that subserve perception & action. 3 Tables, 3 Figures, 1 Appendix, 98 References. Adapted from the source document
JF  - Journal of Cognitive Neuroscience
AU  - Wheatley, Thalia
AU  - Weisberg, Jill
AU  - Beauchamp, Michael S
AU  - Martin, Alex
AD  - Laboratory Brain & Cognition, National Instit Mental Health, National Instits Health, Bethesda MD wheatley@nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1871
EP  - 1885
VL  - 17
IS  - 12
SN  - 0898-929X, 0898-929X
KW  - Animacy and Inanimacy (03100)
KW  - Cerebral Dominance (11500)
KW  - Priming (67670)
KW  - Meaning (52200)
KW  - Semantic Categories (76580)
KW  - Semantic Processing (76760)
KW  - Neuroimaging Techniques (57245)
KW  - Reading Rate (71250)
KW  - article
KW  - 4018: psycholinguistics; neurolinguistics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/85632733?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Allba&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Cognitive+Neuroscience&rft.atitle=Automatic+Priming+of+Semantically+Related+Words+Reduces+Activity+in+the+Fusiform+Gyrus&rft.au=Wheatley%2C+Thalia%3BWeisberg%2C+Jill%3BBeauchamp%2C+Michael+S%3BMartin%2C+Alex&rft.aulast=Wheatley&rft.aufirst=Thalia&rft.date=2005-12-01&rft.volume=17&rft.issue=12&rft.spage=1871&rft.isbn=&rft.btitle=&rft.title=Journal+of+Cognitive+Neuroscience&rft.issn=0898929X&rft_id=info:doi/
LA  - English
DB  - Linguistics and Language Behavior Abstracts (LLBA)
N1  - Date revised - 2006-09-01
N1  - Last updated - 2016-09-27
N1  - CODEN - JCONEO
N1  - SubjectsTermNotLitGenreText - Neuroimaging Techniques (57245); Priming (67670); Semantic Processing (76760); Semantic Categories (76580); Cerebral Dominance (11500); Meaning (52200); Reading Rate (71250); Animacy and Inanimacy (03100)
ER  - 



TY  - JOUR
T1  - Validity of a modified Parkinson's disease screening questionnaire in India: effects of literacy of participants and medical training of screeners and implications for screening efforts in developing countries.
AN  - 85396222; pmid-16078206
AB  - The prevalence of Parkinson's disease (PD) is low among Indians, except in the Parsis. Data for Indians come from studies using different screening tools and criteria to detect PD. An epidemiological study in India, which has nearly a billion people, more than 18 spoken languages, and varying levels of literacy, requires development and validation of a screening tool for PD. The objectives of this study are to (1) validate a modified version of a widely used screening questionnaire for PD to suit the needs of the Indian population; (2) compare the use of a nonmedical assistant (NMA) with the use of a medical person during screening; and (3) compare the effect of literacy of participants on the validity of the screening tool. The validity of the questionnaire was tested on 125 participants from a home for the elderly. NMAs of similar background and medical personnel administered the modified screening questionnaire. A movement disorder neurologist blind to the responses on the questionnaire, examined participants independently and diagnosed if participants had PD. The questionnaire was validated in the movement disorders clinic, on known PD patients and their family members without PD. In the movement disorders clinic, sensitivity and specificity of the questionnaire were 100% and 89%, respectively. Fifty-seven participants were included for analysis. The questionnaire had a higher sensitivity when NMAs (75%) rather than the medical personnel (61%) administered it, and its specificity was higher with the medical personnel (61%) than with NMAs (55% and 25%). The questionnaire had a higher specificity in literates than illiterates, whereas sensitivity varied considerably. The modified questionnaire translated in a local Indian language had reasonable sensitivity and can be used to screen individuals for PD in epidemiological studies in India. This questionnaire can be administered by NMAs to screen PD and this strategy would reduce manpower costs. Literacy may influence epidemiological estimates when screening PD.
JF  - Movement disorders : official journal of the Movement Disorder Society
AU  - Sarangmath, Nagaraja
AU  - Rattihalli, Rohini
AU  - Ragothaman, Mona
AU  - Gopalkrishna, Gururaj
AU  - Doddaballapur, Subbakrishna
AU  - Louis, Elan D
AU  - Muthane, Uday B
AD  - Department of Neurology, National Institute of Mental Health and Neurosciences, Bangalore, India.
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1550
EP  - 1556
VL  - 20
IS  - 12
SN  - 0885-3185, 0885-3185
KW  - Index Medicus
KW  - National Library of Medicine
KW  - Aged
KW  - Aged, 80 and over
KW  - *Developing Countries: statistics & numerical data
KW  - *Educational Status
KW  - Female
KW  - Humans
KW  - India: epidemiology
KW  - India: ethnology
KW  - Interviews as Topic: methods
KW  - Male
KW  - *Mass Screening
KW  - Movement Disorders: diagnosis
KW  - *Parkinson Disease: diagnosis
KW  - Parkinson Disease: epidemiology
KW  - *Professional Role
KW  - *Questionnaires
KW  - Reproducibility of Results
KW  - Sensitivity and Specificity
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/85396222?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acomdisdome&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Movement+disorders+%3A+official+journal+of+the+Movement+Disorder+Society&rft.atitle=Validity+of+a+modified+Parkinson%27s+disease+screening+questionnaire+in+India%3A+effects+of+literacy+of+participants+and+medical+training+of+screeners+and+implications+for+screening+efforts+in+developing+countries.&rft.au=Sarangmath%2C+Nagaraja%3BRattihalli%2C+Rohini%3BRagothaman%2C+Mona%3BGopalkrishna%2C+Gururaj%3BDoddaballapur%2C+Subbakrishna%3BLouis%2C+Elan+D%3BMuthane%2C+Uday+B&rft.aulast=Sarangmath&rft.aufirst=Nagaraja&rft.date=2005-12-01&rft.volume=20&rft.issue=12&rft.spage=1550&rft.isbn=&rft.btitle=&rft.title=Movement+disorders+%3A+official+journal+of+the+Movement+Disorder+Society&rft.issn=08853185&rft_id=info:doi/
LA  - English (eng)
DB  - ComDisDome
N1  - Date revised - 2011-12-15
N1  - Last updated - 2012-07-13
ER  - 



TY  - JOUR
T1  - Neural correlates of script event knowledge: a neuropsychological study following prefrontal injury.
AN  - 85395373; pmid-16350660
AB  - Scripts sequentially link information about daily activities and event knowledge. Patients have difficulty sequencing script events following lesions of the prefrontal cortex while showing intact access to selective aspects of script knowledge. It has been suggested that the sequencing impairment is due to a deficit in an inhibitory gating mechanisms that usually enables selection of an item from competing alternatives. If this is the case, then an inhibitory task should reveal script processing impairments on a script categorization task that is not normally associated with poor performance following prefrontal damage. To test this hypothesis, we administered a simple untimed classification task and a modified Go/NoGo task in which subjects classified events from social and non-social activities (e.g., read the menu, order the food) and related semantic items (e.g., menu, order) in terms of whether they belonged to a target activity. Participants were patients with lesions of the prefrontal cortex and matched controls. The results showed that damage to the right orbitofrontal cortex was associated with social item classification errors in the simple untimed classification task. In addition, the damage to the right prefrontal cortex was associated with increased response times to respond correctly to Go trials in the modified Go/NoGo task. The data demonstrate that damage to the right orbitofrontal cortex results in impairment in the accessibility of script and semantic representations of social activities. This impairment is exacerbated by an inefficient inhibitory gating mechanism.
JF  - Cortex; a journal devoted to the study of the nervous system and behavior
AU  - Wood, Jacqueline N
AU  - Tierney, Michael
AU  - Bidwell, Laura A
AU  - Grafman, Jordan
AD  - Cognitive Neuroscience Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD 20892-1440, USA.
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 796
EP  - 804
VL  - 41
IS  - 6
SN  - 0010-9452, 0010-9452
KW  - Index Medicus
KW  - National Library of Medicine
KW  - Adult
KW  - Aged
KW  - Female
KW  - *Functional Laterality: physiology
KW  - Humans
KW  - Magnetic Resonance Imaging
KW  - Male
KW  - *Mental Processes: physiology
KW  - Middle Aged
KW  - *Neuropsychological Tests
KW  - *Prefrontal Cortex: pathology
KW  - Prefrontal Cortex: radiography
KW  - Psychomotor Performance: physiology
KW  - Reaction Time: physiology
KW  - Social Behavior
KW  - Stroke: pathology
KW  - *Stroke: psychology
KW  - Stroke: radiography
KW  - Tomography, X-Ray Computed
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/85395373?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acomdisdome&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cortex%3B+a+journal+devoted+to+the+study+of+the+nervous+system+and+behavior&rft.atitle=Neural+correlates+of+script+event+knowledge%3A+a+neuropsychological+study+following+prefrontal+injury.&rft.au=Wood%2C+Jacqueline+N%3BTierney%2C+Michael%3BBidwell%2C+Laura+A%3BGrafman%2C+Jordan&rft.aulast=Wood&rft.aufirst=Jacqueline&rft.date=2005-12-01&rft.volume=41&rft.issue=6&rft.spage=796&rft.isbn=&rft.btitle=&rft.title=Cortex%3B+a+journal+devoted+to+the+study+of+the+nervous+system+and+behavior&rft.issn=00109452&rft_id=info:doi/
LA  - English (eng)
DB  - ComDisDome
N1  - Date revised - 2011-12-15
N1  - Last updated - 2012-07-13
ER  - 



TY  - JOUR
T1  - Taiwanese cases of SCA2 are derived from a single founder.
AN  - 85391554; pmid-16078202
AB  - We have assessed the haplotypes at the ATXN2 locus in Taiwanese controls and in individuals with SCA2 ataxia with both ataxic and parkinsonian features. Our intention was to determine whether a different ataxin 2 haplotypes predisposed to the two phenotypes. In fact, our analysis showed that all SCA2 mutations carriers had the same ataxin 2 haplotype: haplotype B, which accounts for only 15% of control haplotypes, implying that there is a common founder for all Taiwanese SCA2 patients.
JF  - Movement disorders : official journal of the Movement Disorder Society
AU  - Momeni, Parastoo
AU  - Lu, Chin-Song
AU  - Chou, Yah-Huei Wu
AU  - Chang, Hsiu-Chen
AU  - Chen, Rou-Shayn
AU  - Chen, Chiung-Chu
AU  - Hsu, Jin-Tian
AU  - Singleton, Andrew
AU  - Hardy, John
AD  - Laboratory of Neurogenetics, National Institute on Aging, National Institutes of Health, Bethesda, Maryland 20952, USA. momeni@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1633
EP  - 1636
VL  - 20
IS  - 12
SN  - 0885-3185, 0885-3185
KW  - Index Medicus
KW  - National Library of Medicine
KW  - Adult
KW  - Aged
KW  - *Ataxia: genetics
KW  - DNA Mutational Analysis
KW  - Female
KW  - Gene Frequency
KW  - Genetic Predisposition to Disease
KW  - Haplotypes
KW  - Humans
KW  - Male
KW  - Middle Aged
KW  - *Nerve Tissue Proteins: genetics
KW  - Parkinson Disease: genetics
KW  - *Polymorphism, Single Nucleotide: genetics
KW  - Taiwan: ethnology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/85391554?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acomdisdome&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Movement+disorders+%3A+official+journal+of+the+Movement+Disorder+Society&rft.atitle=Taiwanese+cases+of+SCA2+are+derived+from+a+single+founder.&rft.au=Momeni%2C+Parastoo%3BLu%2C+Chin-Song%3BChou%2C+Yah-Huei+Wu%3BChang%2C+Hsiu-Chen%3BChen%2C+Rou-Shayn%3BChen%2C+Chiung-Chu%3BHsu%2C+Jin-Tian%3BSingleton%2C+Andrew%3BHardy%2C+John&rft.aulast=Momeni&rft.aufirst=Parastoo&rft.date=2005-12-01&rft.volume=20&rft.issue=12&rft.spage=1633&rft.isbn=&rft.btitle=&rft.title=Movement+disorders+%3A+official+journal+of+the+Movement+Disorder+Society&rft.issn=08853185&rft_id=info:doi/
LA  - English (eng)
DB  - ComDisDome
N1  - Date revised - 2011-12-15
N1  - Last updated - 2012-07-13
ER  - 



TY  - JOUR
T1  - Normal tissue radiosensitivity: prediction on deterministic or stochastic basis?
AN  - 70180125; 17102816
AB  - For the same standardized physical radiation dose there is considerable variation, among different patients, of the magnitude of early and late normal tissue reactions. Technical and clinical factors account for about one third only of these variations. Genetic or epigenetic differences between patients account for the greater proportion of interpatient radiosensitivity differences. Attempts have been made to correlate differences in the tissue radiosensitivity with the in vitro radiosensitivity of fibroblasts or lymphocytes as well as with other biological cellular processes related to cell death (mainly DNA repair and chromosomal aberrations). Apart from some genetic diseases such as ataxia telangiectasia, there were positive results in some studies that could not be reproduced in others. It is now realized that for normal tissue radiation-induced morbidity (a) cell kill is not the only factor, (b) interaction with a large number of gene products, such as IL-2, IL-6, TGF-beta, is involved, and (c) radiosensitivity differences can reflect genetic differences. Polymorphism in a wide range of genes can now be demonstrated and analyzed as a source of variations in the radiation response. cDNA microarray procedures can also allow simultaneous measurement, in the same sample, of thousands of genes and thus avoiding basing the investigation on a restricted number of genes. Preliminary results could show retrospectively a correlation between late normal tissue reactions and expression of certain genes. Using cDNA microarray before radiotherapy to predict the occurrence of serious late reactions is still under consideration. Theoretically, an efficient predictor procedure may serve in (a) detection of hypersensitive patients before submitting them to highly toxic radiotherapy regimes such as whole body irradiation, (b) detection of hypersensitive patients in clinical situations where radiotherapy can be effectively replaced by other modalities, and (c) selection of patients for elaborate radiotherapy techniques involving dose escalation to high levels.
JF  - Journal of the Egyptian National Cancer Institute
AU  - Awwad, Hassan K
AD  - The Department of Radiotherapy, National Cancer Institute, Cairo University.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 221
EP  - 230
VL  - 17
IS  - 4
SN  - 1110-0362, 1110-0362
KW  - Index Medicus
KW  - Polymorphism, Genetic
KW  - Dose Fractionation
KW  - Humans
KW  - Dose-Response Relationship, Radiation
KW  - Radiation Tolerance -- genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/70180125?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=American+Journal+of+Respiratory+and+Critical+Care+Medicine&rft.atitle=Diminished+Lipoxin+Biosynthesis+in+Severe+Asthma&rft.au=Levy%2C+Bruce+D%3BBonnans%2C+Caroline%3BSilverman%2C+Eric+S%3BPalmer%2C+Lyle+J%3Bet+al&rft.aulast=Levy&rft.aufirst=Bruce&rft.date=2005-10-01&rft.volume=172&rft.issue=7&rft.spage=824&rft.isbn=&rft.btitle=&rft.title=American+Journal+of+Respiratory+and+Critical+Care+Medicine&rft.issn=1073449X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2007-06-06
N1  - Date created - 2006-11-14
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Abatement by naringenin of doxorubicin-induced cardiac toxicity in rats.
AN  - 70178993; 17102822
AB  - Doxorubicin is one of the most active cytotoxic agents in current use. It has proven efficacy in various malignancies either alone or combined with other cytocidal agents. The clinical usefulness of the anthracycline drug has been precluded by cardiac toxicity. Many therapeutic interventions have been attempted to improve the therapeutic benefits of the drug. Few, however, have been efficacious in this setting.
          We have addressed in the current study the possible protective effects of naringenin, a flavonoid known to have anti-oxidant properties, on doxorubicin-induced cardiac toxicity in male Swiss albino rats. Forty male Swiss albino rats were used in this study. Naringenin (25 mg/kg body weight) was administered daily by gavage for 7 consecutive days before a cumulative single dose of doxorubicin (15 mg/kg body weight, ip).
          Doxorubicin induced marked biochemical alterations characteristic of cardiac toxicity including, elevated activities of serum total lactate dehydrogenase (LDH) and creatine phosphokinase (CPK), enhanced lipid peroxidation measured as malondialdehyde (MDA). The anthracycline drug has also reduced the cardiac enzymatic activities of superoxide dismutase (SOD), glutathione-S-transferase (GST) and catalase (CAT). Besides, it reduced significantly the reduced glutathione (GSH) level, but it increased the total NO content in heart tissue. Prior administration of naringenin ahead of doxorubicin challenge ameliorated all these biochemical markers. Taken together, one could conclude that naringenin has a protective role in the abatement of doxorubicin-induced cardiac toxicity that resides, at least in part, on its anti-radical effects and regulatory role on NO production.
JF  - Journal of the Egyptian National Cancer Institute
AU  - Arafa, Hossam M
AU  - Abd-Ellah, Mohamed F
AU  - Hafez, Hafez F
AD  - The Department of Pharmacology and Toxicology, Faculty of Pharmacy, Al-Azhar University, National Cancer Institute, Cairo University.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 291
EP  - 300
VL  - 17
IS  - 4
SN  - 1110-0362, 1110-0362
KW  - Antibiotics, Antineoplastic
KW  - 0
KW  - Antioxidants
KW  - Flavanones
KW  - Nitric Oxide
KW  - 31C4KY9ESH
KW  - Doxorubicin
KW  - 80168379AG
KW  - L-Lactate Dehydrogenase
KW  - EC 1.1.1.27
KW  - Catalase
KW  - EC 1.11.1.6
KW  - Superoxide Dismutase
KW  - EC 1.15.1.1
KW  - Glutathione Transferase
KW  - EC 2.5.1.18
KW  - Creatine Kinase
KW  - EC 2.7.3.2
KW  - naringenin
KW  - HN5425SBF2
KW  - Index Medicus
KW  - Animals
KW  - Creatine Kinase -- drug effects
KW  - L-Lactate Dehydrogenase -- drug effects
KW  - Glutathione Transferase -- metabolism
KW  - Lipid Peroxidation -- drug effects
KW  - Superoxide Dismutase -- metabolism
KW  - Nitric Oxide -- metabolism
KW  - Superoxide Dismutase -- drug effects
KW  - Rats
KW  - Catalase -- metabolism
KW  - Creatine Kinase -- blood
KW  - L-Lactate Dehydrogenase -- blood
KW  - Catalase -- drug effects
KW  - Glutathione Transferase -- drug effects
KW  - Male
KW  - Doxorubicin -- adverse effects
KW  - Flavanones -- therapeutic use
KW  - Heart Diseases -- chemically induced
KW  - Antioxidants -- therapeutic use
KW  - Heart Diseases -- prevention & control
KW  - Antibiotics, Antineoplastic -- adverse effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2007-06-06
N1  - Date created - 2006-11-14
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Evaluation of neurotoxic potential by use of in vitro systems.
AN  - 70170689; 16863434
AB  - In vitro systems have been proposed, but not yet demonstrated, as a method to assess the neurotoxicity of compounds in an efficient and rapid manner. Although such tests are desired both for pharmaceuticals and environmental agents, such a battery has yet to be developed that is based on known processes of nervous system dysfunction. In this review article, characteristics and potential limitations associated with in vitro methods are discussed. Many of these features have been identified from a larger body of work examining the neurotoxicity of environmental agents and the mechanisms underlying activity of known neurotoxicants. These issues include relevant drug concentrations, factors that limit or alter drug accessibility to the nervous system, and the need for assays to reflect biologically meaningful end points. This commentary briefly surveys in vitro systems of increasing biological complexity currently available for toxicity testing, from single cell types to systems that preserve some aspects of tissue structure and function. A small number of studies to evaluate drugs for cytotoxicity and biological responses in vitro are presented as representative of the current state of the field and to provide a reference and direction for additional development of methods to assess a compound's potential for neurotoxicity.
JF  - Expert opinion on drug metabolism & toxicology
AU  - Harry, Gaylia Jean
AU  - Tiffany-Castiglioni, Evelyn
AD  - National Institutes of Health, Laboratory of Neurobiology, National Institute of Environmental Health Sciences, Department of Health and Human Services, Research Triangle Park, NC 27709, USA. harry@niehs.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 701
EP  - 713
VL  - 1
IS  - 4
SN  - 1742-5255, 1742-5255
KW  - Index Medicus
KW  - Animals
KW  - Animal Testing Alternatives
KW  - Cell Survival -- drug effects
KW  - Neurites -- drug effects
KW  - Humans
KW  - Learning -- drug effects
KW  - Neurites -- physiology
KW  - Organ Culture Techniques
KW  - Cell Line
KW  - Blood-Brain Barrier
KW  - Nervous System -- drug effects
KW  - Toxicity Tests -- methods
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-08-16
N1  - Date created - 2006-07-25
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Role of loss of heterozygosity on chromosomes 8 and 9 in the development and progression of cancer bladder.
AN  - 70168569; 17102820
AB  - Loss of heterozygosity (LOH) in tumor samples is believed to be a marker for the absence of a functional tumor suppressor gene. Non-random chromosome deletion and LOH at specific chromosomal regions are identified in a number of common human cancers including carcinoma of the bladder, which is considered the most predominant cancer in Egypt due to the prevalence of schistosomiasis.
          The main objective of the present study is to clarify the role of chromosomes 8 and 9 in the establishment and/or progression of schistosomiasis-related bladder cancer through detection of LOH of 8 microsatellite markers on both chromosomes. It also aims to compare the LOH pattern of the tested markers between schistosomiasis- associated and non schistosomiasis-associated bladder cancer. To achieve this purpose, DNA was extracted from the tumor specimens and the corresponding peripheral blood samples of 42 primary bladder cancer patients (schistosomal and non schistosomal). Twenty nine of these were diagnosed as squamous cell type (SCC), 11 were transitional (TCC), and 2 were adenocarcinoma (with different stages and grades). LOH at chromosomes 8 and 9 was evaluated for 8 highly polymorphic microsatellite markers distributed at different regions of both chromosomes using the dinucleotide repeat-PCR technique.
          The overall percentage of LOH in chromosome 8 was 74% in at least one marker. The highest incidence of LOH was recorded for D8S84 (41%) followed by 37% for D8S87, 29% for D8S85, and 25% for D8S88. Deletions at chromosome 8 were shown to be associated with high grade of the tumor and LOH at D8S85 was associated with metastatic lymph nodes. The overall percentage of LOH in chromosome 9 was 54% and its highest incidence was for D9S126 (36%), followed by 26%, 21%, 19% for D9S166, D9S128 and D9S180, respectively. Fifty nine percent (59%) of the cases with LOH at 9q were diagnosed as squamous cell type (SCC), whereas 9% only were transitional cell type (TCC). No significant association was recorded between the presence of schistosomiasis and LOH detected in all markers used in this study. Our data indicate that more than one tumor suppressor gene on chromosomes 8 and 9 are involved in high grades of bladder carcinogenesis, one at 8p12 and another at 8q21.1 regions. Also, a region at 8q23-quarter may harbor tumor suppressor gene that involved in metastasis of bladder cancer. Our study also revealed that 9p21 (p16INK4) region is involved in both types of the tumor (SCC & TCC). PTCH located at 9q22.3, as well as the TSC gene at 9q34 are involved in squamous cell carcinoma rather than transitional carcinoma. Region 9q12-13 is considered to be a critical region of urothelial tumor suppressor genes. Finally, the present study shows no line of demarcation between schistosomiasis-associate and non schistosomiasis-associated bladder cancer in terms of LOH of the tested microsatellite markers on chromosome 8 and 9. This suggests that data obtained from schistosoma-associated bladder cancer can be extrapolated to bladder cancer induced by a schistosomiasis independent mechanism.
JF  - Journal of the Egyptian National Cancer Institute
AU  - Abdel Wahab, Abdel Hady A
AU  - Abo-Zeid, Hamdy I
AU  - El-Husseini, Motawa I
AU  - Ismail, Mohsein
AU  - El-Khor, Akmal M
AD  - The Department of Biochemistry & Molecular Biology Unit, NCI, Cairo University.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 260
EP  - 269
VL  - 17
IS  - 4
SN  - 1110-0362, 1110-0362
KW  - DNA, Neoplasm
KW  - 0
KW  - Index Medicus
KW  - Polymerase Chain Reaction
KW  - Microsatellite Repeats
KW  - Humans
KW  - Disease Progression
KW  - DNA, Neoplasm -- analysis
KW  - Loss of Heterozygosity
KW  - Schistosomiasis haematobia -- complications
KW  - Urinary Bladder Neoplasms -- genetics
KW  - Chromosomes, Human, Pair 8 -- genetics
KW  - Urinary Bladder Neoplasms -- microbiology
KW  - Chromosomes, Human, Pair 9 -- genetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2007-06-06
N1  - Date created - 2006-11-14
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Weight of evidence: a review of concept and methods.
AN  - 70146526; 16506981
AB  - "Weight of evidence" (WOE) is a common term in the published scientific and policy-making literature, most often seen in the context of risk assessment (RA). Its definition, however, is unclear. A systematic review of the scientific literature was undertaken to characterize the concept. For the years 1994 through 2004, PubMed was searched for publications in which "weight of evidence" appeared in the abstract and/or title. Of the 276 papers that met these criteria, 92 were selected for review: 71 papers published in 2003 and 2004 (WOE appeared in abstract/title) and 21 from 1994 through 2002 (WOE appeared in title). WOE has three characteristic uses in this literature: (1) metaphorical, where WOE refers to a collection of studies or to an unspecified methodological approach; (2) methodological, where WOE points to established interpretative methodologies (e.g., systematic narrative review, meta-analysis, causal criteria, and/or quality criteria for toxicological studies) or where WOE means that "all" rather than some subset of the evidence is examined, or rarely, where WOE points to methods using quantitative weights for evidence; and (3) theoretical, where WOE serves as a label for a conceptual framework. Several problems are identified: the frequent lack of definition of the term "weight of evidence," multiple uses of the term and a lack of consensus about its meaning, and the many different kinds of weights, both qualitative and quantitative, which can be used in RA. A practical recommendation emerges: the WOE concept and its associated methods should be fully described when used. A research agenda should examine the advantages of quantitative versus qualitative weighting schemes, how best to improve existing methods, and how best to combine those methods (e.g., epidemiology's causal criteria with toxicology's quality criteria).
JF  - Risk analysis : an official publication of the Society for Risk Analysis
AU  - Weed, Douglas L
AD  - National Cancer Institute, Rockville, MD 20852, USA. dw102i@nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1545
EP  - 1557
VL  - 25
IS  - 6
SN  - 0272-4332, 0272-4332
KW  - Index Medicus
KW  - Public Health
KW  - Epidemiology
KW  - Humans
KW  - Meta-Analysis as Topic
KW  - Toxicology
KW  - Risk Assessment
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-04-20
N1  - Date created - 2006-03-01
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment In:
Risk Anal. 2006 Jun;26(3):573-5; author reply 577 [16834614]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - A slow disengagement from platinum-based chemotherapy for patients with advanced non-small cell lung cancer.
AN  - 70112277; 16434876
JF  - Cancer biology & therapy
AU  - Ballas, Marc S
AU  - Dennis, Phillip A
AD  - Medical Oncology Branch, Center for Cancer Research, National Cancer Institute, Bethesda, Maryland 20889, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1316
EP  - 1317
VL  - 4
IS  - 12
SN  - 1538-4047, 1538-4047
KW  - irinotecan
KW  - 0H43101T0J
KW  - Platinum
KW  - 49DFR088MY
KW  - Paclitaxel
KW  - P88XT4IS4D
KW  - Camptothecin
KW  - XT3Z54Z28A
KW  - Index Medicus
KW  - Paclitaxel -- administration & dosage
KW  - Drug Administration Schedule
KW  - Diarrhea -- chemically induced
KW  - Paclitaxel -- adverse effects
KW  - Survival Rate
KW  - Humans
KW  - Camptothecin -- analogs & derivatives
KW  - Neutropenia -- chemically induced
KW  - Maximum Tolerated Dose
KW  - Camptothecin -- adverse effects
KW  - Time Factors
KW  - Camptothecin -- administration & dosage
KW  - Carcinoma, Non-Small-Cell Lung -- mortality
KW  - Platinum -- therapeutic use
KW  - Lung Neoplasms -- drug therapy
KW  - Lung Neoplasms -- mortality
KW  - Antineoplastic Combined Chemotherapy Protocols -- adverse effects
KW  - Antineoplastic Combined Chemotherapy Protocols -- therapeutic use
KW  - Carcinoma, Non-Small-Cell Lung -- drug therapy
KW  - Lung Neoplasms -- pathology
KW  - Carcinoma, Non-Small-Cell Lung -- pathology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-22
N1  - Date created - 2006-02-07
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment On:
Cancer Biol Ther. 2005 Dec;4(12):1311-5 [16258263]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Imatinib synergizes with donor lymphocyte infusions to achieve rapid molecular remission of CML relapsing after allogeneic stem cell transplantation.
AN  - 69062281; 16205732
AB  - Donor lymphocyte infusions (DLI) have been the mainstay of treatment for chronic myeloid leukemia (CML) relapsing after allogeneic stem cell transplantation (allo-SCT). Imatinib mesylate (IM) is also effective in these patients. However, advanced phase relapse (APRel) responds poorly with either treatment. To test the possibility that combinations of DLI and IM might be more effective, 37 patients with CML relapsing after allo-SCT between August 1994 and May 2004 were studied. Ten had molecular relapse (MRel), 14 hematological relapse (HRel) and 13 APRel. Thirteen received DLI, 9 IM and 11 DLI+IM. Four patients received DLI+IM but not concurrently. Thirty (81%) patients responded (actuarial survival and current leukemia-free survival of 80.6 +/- 6.7% and 69.1 +/- 7.7%). Of 30 patients, 26 are in molecular remission (MR), median follow-up of 1,226 days (range 249-3257) since relapse. Ten of 11 patients (including four with APRel) treated with DLI+IM achieved MR in 3 months and all are alive in MR. In contrast, only two of 22 treated with either modality (1/13 DLI and 1/9 IM) achieved MR at 3 months, 15 are alive, 11 in MR. Four patients receiving nonconcurrent DLI+IM are also alive in MR. In conclusion, DLI appears to synergize with IM to induce rapid and durable MR.
JF  - Bone marrow transplantation
AU  - Savani, B N
AU  - Montero, A
AU  - Kurlander, R
AU  - Childs, R
AU  - Hensel, N
AU  - Barrett, A J
AD  - Stem Cell Allogeneic Transplantation Section, Hematology Branch, NHLBI, National Institutes of Health, Building 10, Hatfield CRC, 10 Center Drive MSC 1202, Bethesda, MD 20892-1202, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1009
EP  - 1015
VL  - 36
IS  - 11
SN  - 0268-3369, 0268-3369
KW  - Benzamides
KW  - 0
KW  - Piperazines
KW  - Pyrimidines
KW  - Imatinib Mesylate
KW  - 8A1O1M485B
KW  - Index Medicus
KW  - Humans
KW  - Adult
KW  - Retrospective Studies
KW  - Aged
KW  - Remission Induction -- methods
KW  - Middle Aged
KW  - Transplantation, Homologous
KW  - Drug Synergism
KW  - Adolescent
KW  - Recurrence
KW  - Male
KW  - Female
KW  - Survival Analysis
KW  - Lymphocyte Transfusion
KW  - Leukemia, Myelogenous, Chronic, BCR-ABL Positive -- mortality
KW  - Hematopoietic Stem Cell Transplantation
KW  - Leukemia, Myelogenous, Chronic, BCR-ABL Positive -- therapy
KW  - Pyrimidines -- administration & dosage
KW  - Piperazines -- administration & dosage
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-04-03
N1  - Date created - 2006-01-04
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Evaluation of fluorenhymustine as a rationally designed novel anticancer agent.
AN  - 69061070; 16404347
AB  - To develop a rationally designed new nitrogen mustard namely Fluorenhymustine (compound 2), where N,N'-bis(2chloro-ethyl)amino group, the established anticancer functionality, is attached to the 2-ethyl fluorenone hydantoin moiety.
          Starting from fluorenone hydantoin, a 3-step synthetic procedure was followed to obtain the title compound. 4-(4-Nitrobenzyl)pyridine was used to assess its chemical alkylating activity. Murine tumors (Ehrlich ascites carcinoma (EAC) and Sarcoma-180 (S-180)) were used to assess its in vivo activity. Its cytotoxicity was determined in vitro in MCF-7 human breast tumor cell line, toxicity - in vivo in normal and EAC bearing mice. 3H-Thymidine and 3H-Uridine were employed to study its inhibitory effect on DNA and RNA synthesis respectively in S-180 tumor cells in vitro. Alkylating activity of fluorenmustine exceeded that of N-di(2-chloroethyl)amine used as a standard alkylating compound. It has displayed an excellent and reproducible antitumor activity in vivo against EAC and S-180 comparable to that of 5-fluorouracil judging by the increase in median survival times of treated animals. It also significantly increased the life span of mice bearing advanced tumors for 6 days before the drug challenge. However in vitro screening in MCF-7 did not reveal any significant cytotoxicity. The compound did not adversely affect hematopoiesis at its optimum dose. Drug-induced hepatotoxicity and nephrotoxicity were also not detected. It inhibited the synthesis of DNA and RNA in S-180 tumor cells at 8 microM concentration.
          Results indicated promising chemotherapeutic potential of Fluorenhymustine.
JF  - Experimental oncology
AU  - Samanta, S
AU  - Pain, A
AU  - Ghosh, M
AU  - Dutta, S
AU  - Sanyal, U
AD  - Department of Anticancer Drug Development, Chittaranjan National Cancer Institute, Calcutta 700026, India.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 279
EP  - 285
VL  - 27
IS  - 4
SN  - 1812-9269, 1812-9269
KW  - Antineoplastic Agents, Alkylating
KW  - 0
KW  - Nitrogen Mustard Compounds
KW  - fluorenhymustine
KW  - Index Medicus
KW  - Drug Screening Assays, Antitumor
KW  - Animals
KW  - Dose-Response Relationship, Drug
KW  - Humans
KW  - Mice
KW  - Cell Line, Tumor
KW  - Drug Evaluation, Preclinical
KW  - Antineoplastic Agents, Alkylating -- chemical synthesis
KW  - Antineoplastic Agents, Alkylating -- pharmacology
KW  - Nitrogen Mustard Compounds -- chemical synthesis
KW  - Neoplasms, Experimental -- drug therapy
KW  - Nitrogen Mustard Compounds -- pharmacology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-02
N1  - Date created - 2006-01-11
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - [Social aspects and cancer: information dedicated to cancer patients and relatives].
TT  - Démarches sociales et cancer Information à l'usage des personnes malades et de leurs proches.
AN  - 69054045; 16396756
AB  - In response to the evolution of the information-seeking behaviour of patients and concerns from health professionals regarding cancer patient information, the French National Federation of Comprehensive Cancer Centres (FNCLCC) introduced, in 1998, an information and education program dedicated to patients and relatives, the SOR SAVOIR PATIENT program (SSP). The methodology of this program adheres to established quality criteria regarding the elaboration of patient information. Cancer patient information, developed in this program, is based on clinical practice guidelines produced by the FNCLCC and the twenty French regional cancer centres, the National League against Cancer, The National Cancer Institute, the French Hospital Federation, the National Oncology Federation of Regional and University Hospitals, the French Oncology Federation of General Hospitals, many learned societies, as well as an active participation of patients, former patients and caregivers. The information and dialogue handbook SOR SAVOIR PATIENT Social aspects & cancer partly published in this edition of the Bulletin du cancer, provides specific information regarding patient social rights and benefits extracted from the texts of laws currently in force in France. It also relies on the handbook A "Prévoir Demain, La réinsertion des patients traités pour cancers A", realised in partnership with the FNCLCC, the Coloplast foundation for quality of life and the National League against Cancer. This document is available from the FNCLCC (101, rue de Tolbiac, 75013 Paris, Tel. (0033) 1 44 23 04 68, www.fnclcc.fr). The handbook A "Social aspects & cancer A" was worked out and published in 2004. Information may change with new legal regulations. It is therefore strongly advised to refer to the texts of laws in force to check for possible amendments. This article aims to help patients and relatives to be better aware of their social rights, to locate the different social and administrative services concerned (CAF, Cotorep, etc.) and to turn to the right person and the appropriate agency in the event of social difficulties during and after the disease. This document is designed to offer health professionals a validated information digest of all resources available in order to better communicate with the patient on social aspects of cancer.
JF  - Bulletin du cancer
AU  - FNCLCC
AU  - French regional cancer centres
AU  - National League against Cancer
AU  - National Cancer Institute
AU  - French Hospital Federation
AU  - National Oncology Federation of Regional and University Hospitals
AU  - French Oncology Federation of General Hospitals
AD  - FNCLCC ; French regional cancer centres ; National League against Cancer ; National Cancer Institute ; French Hospital Federation ; National Oncology Federation of Regional and University Hospitals ; French Oncology Federation of General Hospitals
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1093
EP  - 1113
VL  - 92
IS  - 12
KW  - Index Medicus
KW  - France
KW  - Humans
KW  - Program Development
KW  - Home Care Services -- organization & administration
KW  - Guidelines as Topic
KW  - Occupational Diseases -- therapy
KW  - Patient Education as Topic
KW  - Family
KW  - Neoplasms -- therapy
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LA  - fre
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-19
N1  - Date created - 2006-01-06
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - A pilot study to evaluate the vascular endothelial growth factor receptor tyrosine kinase inhibitor AZD2171 and chemotherapy in locally advanced and inflammatory breast cancer.
AN  - 69047013; 16381631
JF  - Clinical breast cancer
AU  - Denduluri, Neelima
AU  - Tan, Antoinette R
AU  - Walshe, Janice
AU  - Berman, Arlene
AU  - Yang, Sherry X
AU  - Chow, Catherine K
AU  - Swain, Sandra M
AD  - Breast Cancer Section, Medical Oncology Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 460
EP  - 463
VL  - 6
IS  - 5
SN  - 1526-8209, 1526-8209
KW  - Enzyme Inhibitors
KW  - 0
KW  - Quinazolines
KW  - Receptors, Vascular Endothelial Growth Factor
KW  - EC 2.7.10.1
KW  - cediranib
KW  - NQU9IPY4K9
KW  - Index Medicus
KW  - Randomized Controlled Trials as Topic
KW  - Clinical Trials, Phase II as Topic
KW  - Humans
KW  - Inflammation -- drug therapy
KW  - Pilot Projects
KW  - Female
KW  - Breast Neoplasms -- drug therapy
KW  - Enzyme Inhibitors -- adverse effects
KW  - Receptors, Vascular Endothelial Growth Factor -- antagonists & inhibitors
KW  - Enzyme Inhibitors -- therapeutic use
KW  - Quinazolines -- therapeutic use
KW  - Breast Neoplasms -- etiology
KW  - Quinazolines -- adverse effects
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+breast+cancer&rft.atitle=A+pilot+study+to+evaluate+the+vascular+endothelial+growth+factor+receptor+tyrosine+kinase+inhibitor+AZD2171+and+chemotherapy+in+locally+advanced+and+inflammatory+breast+cancer.&rft.au=Denduluri%2C+Neelima%3BTan%2C+Antoinette+R%3BWalshe%2C+Janice%3BBerman%2C+Arlene%3BYang%2C+Sherry+X%3BChow%2C+Catherine+K%3BSwain%2C+Sandra+M&rft.aulast=Denduluri&rft.aufirst=Neelima&rft.date=2005-12-01&rft.volume=6&rft.issue=5&rft.spage=460&rft.isbn=&rft.btitle=&rft.title=Clinical+breast+cancer&rft.issn=15268209&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-26
N1  - Date created - 2005-12-29
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Concepts and clinical trials of dose-dense chemotherapy for breast cancer .
AN  - 69043758; 16381623
AB  - This article will review the strategy of dose-dense administration of chemotherapy for breast cancer. Increased dose density is achieved by reducing the interval between each dose of chemotherapy. The cumulative drug dose remains constant, but the same amount of drug is administered over a shorter period. Mathematical models of tumor growth have provided the basis for the clinical application of dose-dense chemotherapy. The Norton-Simon model suggests that increasing the dose density of chemotherapy will increase efficacy by minimizing the opportunity for regrowth of tumor cells between cycles of chemotherapy. Intergroup trial 9741, coordinated by the Cancer and Leukemia Group B (CALGB), tested the 2 hypotheses that dose-dense and sequential administration of chemotherapy regimens incorporating doxorubicin, cyclophosphamide, and paclitaxel would improve disease-free survival and overall survival. A statistically significant 4-year disease-free survival advantage was detected for the 2 dose-dense regimens compared with the regimens administered every 3 weeks. The mathematical concepts and previous clinical trials of dose density that contributed to the design of CALGB 9741 will be reviewed. The strengths and limitations of CALGB 9741 will then be discussed before the presentation of future directions of research and recommendations for clinical practice today.
JF  - Clinical breast cancer
AU  - Orzano, Jennifer A
AU  - Swain, Sandra M
AD  - Cancer Therapeutics Branch, Center for Cancer Research, National Cancer Institute, Department of Health & Human Services, Bethesda, MD, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 402
EP  - 411
VL  - 6
IS  - 5
SN  - 1526-8209, 1526-8209
KW  - Taxoids
KW  - 0
KW  - Index Medicus
KW  - Humans
KW  - Clinical Trials as Topic
KW  - Models, Biological
KW  - Female
KW  - Mathematics
KW  - Breast Neoplasms -- drug therapy
KW  - Breast Neoplasms -- pathology
KW  - Dose-Response Relationship, Drug
KW  - Antineoplastic Combined Chemotherapy Protocols -- administration & dosage
KW  - Taxoids -- toxicity
KW  - Taxoids -- therapeutic use
KW  - Antineoplastic Combined Chemotherapy Protocols -- therapeutic use
KW  - Taxoids -- pharmacology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-26
N1  - Date created - 2005-12-29
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Local distribution and toxicity of prolonged hippocampal infusion of muscimol.
AN  - 69043209; 16381190
AB  - The activity of gamma-aminobutyric acid (GABA), the principal inhibitory neurotransmitter, is reduced in the hippocampus in patients with complex partial seizures from mesial temporal sclerosis. To provide preliminary safety and distribution data on using convection-enhanced delivery of agents to treat complex partial seizures and to test the efficacy and safety of regional selective neuronal suppression, the authors infused muscimol, a GABA-A receptor agonist, directly into the hippocampus of nonhuman primates using an integrated catheter electrode.
          Ten rhesus monkeys were divided into three groups: 1) use of catheter electrode alone (four monkeys); 2) infusion of escalating concentrations of muscimol followed by vehicle (three monkeys); and 3) infusion of vehicle and subsequent muscimol mixed with muscimol tracer (three monkeys). Infusions were begun 5 days after catheter electrode placement and continued for 5.6 days before switching to the other agent. Head magnetic resonance (MR) images and electroencephalography recordings were obtained before and during the infusions. Brain histological studies and quantitative autoradiography were performed. Neurological function was normal in controls and when muscimol concentrations were 0.125 mM or less, whereas higher concentrations (0.5 and 1 mM) produced reversible apathy and somnolence. Fluid distribution was demonstrated on MR images and muscimol distribution was demonstrated on autoradiographs throughout the hippocampus and adjacent white matter. Targeted modulation of neuronal activity is a reasonable research strategy for the investigation and treatment of medically intractable epilepsy.
JF  - Journal of neurosurgery
AU  - Heiss, John D
AU  - Walbridge, Stuart
AU  - Morrison, Paul
AU  - Hampton, Robert R
AU  - Sato, Susumu
AU  - Vortmeyer, Alexander
AU  - Butman, John A
AU  - O'Malley, James
AU  - Vidwan, Param
AU  - Dedrick, Robert L
AU  - Oldfield, Edward H
AD  - Surgical Neurology Branch, Electroencephalography Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892-1414, USA. heissj@ninds.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1035
EP  - 1045
VL  - 103
IS  - 6
SN  - 0022-3085, 0022-3085
KW  - GABA Agonists
KW  - 0
KW  - Muscimol
KW  - 2763-96-4
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Osmolar Concentration
KW  - Magnetic Resonance Imaging
KW  - Animals
KW  - Drug Administration Schedule
KW  - Dose-Response Relationship, Drug
KW  - Brain -- pathology
KW  - Electroencephalography
KW  - Macaca mulatta
KW  - Drug Delivery Systems -- adverse effects
KW  - Tissue Distribution
KW  - Autoradiography
KW  - Male
KW  - Female
KW  - Muscimol -- administration & dosage
KW  - Hippocampus -- physiology
KW  - GABA Agonists -- pharmacokinetics
KW  - GABA Agonists -- administration & dosage
KW  - Hippocampus -- metabolism
KW  - Muscimol -- poisoning
KW  - Muscimol -- pharmacokinetics
KW  - GABA Agonists -- poisoning
KW  - Hippocampus -- drug effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-10
N1  - Date created - 2005-12-29
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Comparison of ramosetron and granisetron for the prevention of acute and delayed emesis in Cisplatin-based chemotherapy: a randomized controlled trial.
AN  - 69039624; 16319109
AB  - A clinical study of ramosetron was carried out to evaluate its efficacy in preventing both acute and delayed emesis in cisplatin-based chemotherapy by using a double-blind method with granisetron as the comparative drug.
          Cisplatin at a dose of > or =70 mg/m(2) was administered as a single intravenous (i.v.) infusion over 4 h. Patients were randomly assigned to receive either ramosetron (0.3 mg i.v. bolus 30 min before cisplatin on Day 1 and a 0.1 mg tablet in the morning for Days 2 to 5 after completion of chemotherapy; n = 36) or granisetron (3 mg i.v. infusion 30 min before cisplatin on Day 1 and a 1 mg tablet in the morning for Days 2 to 5 after completion of chemotherapy; n = 37). The observation period started with the initiation of chemotherapy (0 h) and continued for 24 h after completion of the chemotherapy for acute emesis, and on Days 2 to 5 for delayed nausea and vomiting.
          A total of 73 patients were eligible for evaluation, with 36 patients in the ramosetron group and 37 in the granisetron group. The efficacy of both drugs was analyzed in terms of the degree of achievement in each day of treatment. Ramosetron was as effective as granisetron in preventing nausea and vomiting (both acute and delayed emesis). The two drugs had a similar safety profile and adverse events were generally mild and transient. Ramosetron is effective and safe for the control of acute and delayed emesis induced by cisplatin.
JF  - Japanese journal of clinical oncology
AU  - Cheirsilpa, Arkom
AU  - Sinthusake, Tanadej
AU  - Songsakkaesorn, Apinya
AU  - Visawaprasit, Somchit
AU  - Chulaka, Kemachit
AU  - Changkuingdee, Nunchaporn
AD  - Division of Medical Oncology, National Cancer Institute, 268/1 Rama 6th Road, Rajthevi, Bangkok 10400, Thailand. silpa@health.moph.go.th
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 695
EP  - 699
VL  - 35
IS  - 12
SN  - 0368-2811, 0368-2811
KW  - Antiemetics
KW  - 0
KW  - Benzimidazoles
KW  - ramosetron
KW  - 7ZRO0SC54Y
KW  - Cisplatin
KW  - Q20Q21Q62J
KW  - Granisetron
KW  - WZG3J2MCOL
KW  - Index Medicus
KW  - Dizziness -- chemically induced
KW  - Neoplasms -- drug therapy
KW  - Drug Administration Schedule
KW  - Double-Blind Method
KW  - Endpoint Determination
KW  - Humans
KW  - Aged
KW  - Antineoplastic Combined Chemotherapy Protocols -- adverse effects
KW  - Headache -- chemically induced
KW  - Aged, 80 and over
KW  - Adult
KW  - Middle Aged
KW  - Antineoplastic Combined Chemotherapy Protocols -- therapeutic use
KW  - Male
KW  - Female
KW  - Granisetron -- adverse effects
KW  - Antiemetics -- therapeutic use
KW  - Granisetron -- therapeutic use
KW  - Nausea -- prevention & control
KW  - Benzimidazoles -- adverse effects
KW  - Vomiting, Anticipatory -- prevention & control
KW  - Benzimidazoles -- therapeutic use
KW  - Cisplatin -- adverse effects
KW  - Antiemetics -- adverse effects
KW  - Cisplatin -- administration & dosage
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-03
N1  - Date created - 2005-12-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Reproductive outcomes in men with prenatal exposure to diethylstilbestrol.
AN  - 68904275; 16359959
AB  - To examine prenatal diethylstilbestrol (DES) exposure in relation to male reproductive outcomes.
          Prospective observational study. Participants were identified through record review, clinical trial participation, or an obstetrics clinic.
          A total of 1,085 DES-exposed and 1,047 unexposed men. Participants were exposed prenatally to DES through the mother's obstetrics care or clinical trial participation.
          Infertility; never fathering a pregnancy or live birth; number of pregnancies or live births fathered. We found little evidence that prenatal DES exposure affects the likelihood of never fathering a pregnancy or live birth, or influences the mean number of fathered pregnancies or live births. Our data suggest that DES-exposed men are slightly more likely to experience infertility (relative risk [RR] = 1.3, 95% confidence interval [CI] = 1.0-1.6). The DES dose and gestational timing did not influence infertility or the number of pregnancies or live births fathered, but results were inconsistent for dose effects on the likelihood of never fathering a pregnancy or a live birth.
          Prenatal DES exposure may be associated with a slightly increased risk of having an infertility experience, but does not increase the likelihood of never fathering a pregnancy or a live birth, or the number of pregnancies or live births fathered.
JF  - Fertility and sterility
AU  - Perez, Kimberly M
AU  - Titus-Ernstoff, Linda
AU  - Hatch, Elizabeth E
AU  - Troisi, Rebecca
AU  - Wactawski-Wende, Jean
AU  - Palmer, Julie R
AU  - Noller, Kenneth
AU  - Hoover, Robert N
AU  - National Cancer Institute's DES Follow-up Study Group
AD  - Department of Social and Preventive Medicine, University of Buffalo, State of New York, Buffalo, New York, USA. ; National Cancer Institute's DES Follow-up Study Group
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1649
EP  - 1656
VL  - 84
IS  - 6
KW  - Estrogens, Non-Steroidal
KW  - 0
KW  - Diethylstilbestrol
KW  - 731DCA35BT
KW  - Index Medicus
KW  - Prospective Studies
KW  - Humans
KW  - Adult
KW  - Surveys and Questionnaires
KW  - Interviews as Topic
KW  - Middle Aged
KW  - Follow-Up Studies
KW  - Adolescent
KW  - Male
KW  - Female
KW  - Pregnancy
KW  - Age Distribution
KW  - Diethylstilbestrol -- adverse effects
KW  - Pregnancy Outcome -- epidemiology
KW  - Prenatal Exposure Delayed Effects -- epidemiology
KW  - Infertility, Male -- chemically induced
KW  - Estrogens, Non-Steroidal -- administration & dosage
KW  - Diethylstilbestrol -- administration & dosage
KW  - Infertility, Male -- epidemiology
KW  - Estrogens, Non-Steroidal -- adverse effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-08
N1  - Date created - 2005-12-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Science and society: the Long Island Breast Cancer Study Project.
AN  - 68885594; 16341086
AB  - In the early 1990s, breast cancer advocates petitioned the United States Congress to investigate the high rates of breast cancer on Long Island in the state of New York. The resulting law led to the Long Island Breast Cancer Study Project (LIBCSP)--more than ten research projects designed to study the possible causes of this increased incidence of cancer. This project reported that there was no evidence that environmental exposures were responsible. Controversial from its start, the LIBCSP has had an important role in efforts to understand the reasons for the high rates of breast cancer in some regions of the United States.
JF  - Nature reviews. Cancer
AU  - Winn, Deborah M
AD  - Clinical and Genetic Epidemiology Research Branch, Division of Cancer Control and Population Sciences, Executive Plaza North, Room 5134, MSC 7393, 6130 Executive Boulevard, Bethesda, Maryland 20892-7393, USA. winnde@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 986
EP  - 994
VL  - 5
IS  - 12
SN  - 1474-175X, 1474-175X
KW  - Index Medicus
KW  - Risk Factors
KW  - Humans
KW  - Cohort Studies
KW  - New York -- epidemiology
KW  - Cluster Analysis
KW  - Female
KW  - Breast Neoplasms -- mortality
KW  - Environmental Exposure
KW  - Breast Neoplasms -- etiology
KW  - Breast Neoplasms -- epidemiology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-16
N1  - Date created - 2005-12-12
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Secondary ion mass spectroscopy demonstrates retention of beryllium in chronic beryllium disease granulomas.
AN  - 68885496; 16340702
AB  - We hypothesized that beryllium (Be) might persist in lung granulomas in patients with chronic beryllium disease (CBD).
          A total of 33 Be-exposed ceramics workers underwent transbronchial biopsy. They were classified based on histopathology and Be-lymphocyte proliferation test as CBD or other categories. Lung tissue sections were analyzed using secondary ion mass spectroscopy. Be was detected in the lungs of all Be-exposed groups. Be levels were increased within the granulomas of patients with CBD compared with the Be levels outside granulomas. Notably, Be was detectable in the lungs of CBD patients who had ceased exposure to Be an average of 9 years previously.
          Be was detected in the lungs of all Be-exposed subjects, with the highest levels of persistent Be inside CBD lung granulomas. Be antigen persistence may help explain the chronicity of this granulomatous disorder.
JF  - Journal of occupational and environmental medicine
AU  - Sawyer, Richard T
AU  - Abraham, Jerrold L
AU  - Daniloff, Elaine
AU  - Newman, Lee S
AD  - Division of Environmental and Occupational Health Sciences, Robert Hollis Laboratory of Environmental and Occupational Health Sciences, Department of Medicine, National Jewish Medical and Research Center, Denver, Colorado, USA. sawyerr@niaid.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1218
EP  - 1226
VL  - 47
IS  - 12
SN  - 1076-2752, 1076-2752
KW  - Beryllium
KW  - OW5102UV6N
KW  - Index Medicus
KW  - Occupational Exposure
KW  - Humans
KW  - Adult
KW  - Aged
KW  - Middle Aged
KW  - Chronic Disease
KW  - Biopsy
KW  - Male
KW  - Female
KW  - Berylliosis
KW  - Spectrometry, Mass, Secondary Ion -- methods
KW  - Granuloma, Respiratory Tract
KW  - Beryllium -- analysis
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-14
N1  - Date created - 2005-12-12
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - A pilot study of an investigational testosterone transdermal patch system in young women with spontaneous premature ovarian failure.
AN  - 68873895; 16174721
AB  - Evidence suggests that young women with spontaneous premature ovarian failure (sPOF) have significantly lower androgen levels than age-matched regularly menstruating women.
          The objective of the study was to evaluate an investigational testosterone transdermal patch (TTP) designed to deliver the normal ovarian production rate of testosterone. This was an open-label study (2-month baseline period followed by 2-month treatment period).
          Nine women with sPOF and a history of regular bleeding patterns on standard estrogen/progestogen cyclic treatment participated in the study. One subject with abnormal baseline levels was excluded. Four consecutive 28-d cycles of transdermal estradiol (E2; 0.1 mg/d) and sequential oral medroxyprogesterone acetate (MPA; 10 mg/d for the last 12 d of each cycle). During cycles 3 and 4, an investigational TTP (nominal delivery 150 microg/d) was applied twice weekly to the abdomen.
          Steady-state pharmacokinetic profiles of free and total testosterone and scheduled vaginal bleeding patterns were studied. The mean (95% confidence interval) of the time-average free testosterone levels during TTP treatment was 7.5 (4.9-9.9) pg/ml; 26.0 (17.2-34.6) pmol/liter (with E2), and 6.9 (4.9-8.8) pg/ml; 23.9 (17.2-30.5) pmol/liter (with E2 and MPA). The confidence intervals of the means include the upper limit of normal for premenopausal women, i.e. 6.8 pg/ml (23.5 pmol/liter), although the mean values are slightly above this.
          The addition of TTP to cyclic E2/MPA therapy in women with sPOF produced mean free testosterone levels that approximate the upper limit of normal. A 3-yr study to assess safety and effectiveness in this population is in progress.
JF  - The Journal of clinical endocrinology and metabolism
AU  - Kalantaridou, Sophia N
AU  - Calis, Karim A
AU  - Mazer, Norman A
AU  - Godoy, Heidy
AU  - Nelson, Lawrence M
AD  - Developmental Endocrinology Branch, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 6549
EP  - 6552
VL  - 90
IS  - 12
SN  - 0021-972X, 0021-972X
KW  - Androgens
KW  - 0
KW  - Hormones
KW  - Testosterone
KW  - 3XMK78S47O
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Administration, Cutaneous
KW  - Humans
KW  - Adult
KW  - Hormones -- blood
KW  - Pilot Projects
KW  - Menstrual Cycle -- drug effects
KW  - Female
KW  - Androgens -- therapeutic use
KW  - Testosterone -- therapeutic use
KW  - Testosterone -- administration & dosage
KW  - Primary Ovarian Insufficiency -- physiopathology
KW  - Primary Ovarian Insufficiency -- blood
KW  - Androgens -- adverse effects
KW  - Testosterone -- adverse effects
KW  - Primary Ovarian Insufficiency -- drug therapy
KW  - Androgens -- administration & dosage
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-10
N1  - Date created - 2005-12-06
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Research opportunities on alcohol and liver damage.
AN  - 68868252; 16317668
JF  - Hepatology (Baltimore, Md.)
AU  - Zakhari, Samir
AU  - Hoofnagle, Jay H
AD  - Division of Metabolism and Health Effects NIAAA, National Institutes of Health Bethesda, MD, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1243
VL  - 42
IS  - 6
SN  - 0270-9139, 0270-9139
KW  - Ethanol
KW  - 3K9958V90M
KW  - Index Medicus
KW  - United States
KW  - Animals
KW  - Humans
KW  - National Institute of Mental Health (U.S.)
KW  - Research
KW  - Liver -- drug effects
KW  - Ethanol -- toxicity
KW  - Ethanol -- metabolism
KW  - Liver Diseases, Alcoholic -- etiology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Hepatology+%28Baltimore%2C+Md.%29&rft.atitle=Research+opportunities+on+alcohol+and+liver+damage.&rft.au=Zakhari%2C+Samir%3BHoofnagle%2C+Jay+H&rft.aulast=Zakhari&rft.aufirst=Samir&rft.date=2005-12-01&rft.volume=42&rft.issue=6&rft.spage=1243&rft.isbn=&rft.btitle=&rft.title=Hepatology+%28Baltimore%2C+Md.%29&rft.issn=02709139&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-22
N1  - Date created - 2005-12-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Hepatitis C virus load and survival among injection drug users in the United States.
AN  - 68867246; 16317675
AB  - Persons chronically infected with hepatitis C virus (HCV), some of whom may be coinfected with HIV and human T-lymphotropic virus type II (HTLV-II), are at high risk for end-stage liver disease (ESLD). We evaluated whether ESLD death was associated with premorbid HCV RNA level or specific HCV protein antibodies among persons with or without HIV/HTLV-II coinfection in a cohort of 6,570 injection drug users who enrolled in 9 US cities between 1987 and 1991. We compared 84 ESLD descendents and 305 randomly selected cohort participants with detectable HCV RNA, stratified by sex, race, HIV, and HTLV-II strata. Relative hazard (RH) of ESLD death was derived from the proportional hazard model. Risk of ESLD death was unrelated to the intensity of antibodies against the HCV c-22(p), c-33(p), c-100(p), and NS5 proteins, individually or combined, but it increased with HCV RNA level (RH(adj) = 2.26 per log(10) IU/mL, 95% CI: 1.45-5.92). The association between HCV RNA level and ESLD death remained significant after adjustment for alcohol consumption (RH(adj) = 2.57 per log(10) IU/mL, 95% CI: 1.50-8.10). Deaths from AIDS (n = 45) and other causes (n = 43) were unrelated to HCV RNA (RH(adj)= 1.14 and 1.29 per log(10) IU/mL, respectively). HIV infection was not associated with ESLD risk in multivariate analyses adjusted for HCV RNA. Men had an increased risk of ESLD death in unadjusted analyses (RH = 1.92, 95% CI: 1.15-3.56) but not in multivariate analysis (RH(adj) = 0.98, 95% CI: 0.48-2.88). Non-black patients were at increased risk for ESLD death (RH(adj)= 2.76, 95% CI: 1.49-10.09). In conclusion, HCV RNA level is a predictor of ESLD death among persons with chronic HCV infection.
JF  - Hepatology (Baltimore, Md.)
AU  - Hisada, Michie
AU  - Chatterjee, Nilanjan
AU  - Kalaylioglu, Zeynep
AU  - Battjes, Robert J
AU  - Goedert, James J
AD  - Viral Epidemiology Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, Rockville, MD 20852, USA. hisadam@exchange.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1446
EP  - 1452
VL  - 42
IS  - 6
SN  - 0270-9139, 0270-9139
KW  - RNA, Viral
KW  - 0
KW  - Index Medicus
KW  - HIV Infections -- virology
KW  - Humans
KW  - Adult
KW  - Aged
KW  - Middle Aged
KW  - Male
KW  - Female
KW  - RNA, Viral -- blood
KW  - Viral Load
KW  - Substance Abuse, Intravenous -- virology
KW  - Hepacivirus -- isolation & purification
KW  - Hepatitis C, Chronic -- virology
KW  - Substance Abuse, Intravenous -- mortality
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-22
N1  - Date created - 2005-12-05
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment In:
Hepatology. 2005 Dec;42(6):1261-3 [16317702]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Topiramate in chronic lumbar radicular pain.
AN  - 68863905; 16326371
AB  - Chronic lumbar radicular pain is the most common neuropathic pain syndrome. This was a double-blind, randomized, 2-period crossover trial of topiramate (50 to 400 mg) and diphenhydramine (6.25 to 50 mg) as active placebo to assess the efficacy of topiramate. Each period consisted of a 4-week escalation, a 2-week maintenance at the highest tolerated dose, and a 2-week taper. Main outcome was the mean daily leg pain score on a 0 to 10 scale during the maintenance period. Global pain relief was assessed on a 6-level category scale. In the 29 of 42 patients who completed the study, topiramate reduced leg pain by a mean of 19% (P = .065). Global pain relief scores were significantly better on topiramate (P < .005). Mean doses were topiramate 200 mg and diphenhydramine 40 mg. We concluded that topiramate treatment might reduce chronic sciatica in some patients but causes frequent side effects and dropouts. We would not recommend topiramate unless studies of alternative regimens showed a better therapeutic ratio. The anticonvulsant topiramate might reduce chronic lumbar nerve root pain through effects such as blockade of voltage-gated sodium channels and AMPA/kainite glutamate receptors, modulation of voltage-gated calcium channels, and gamma-aminobutyric acid agonist-like effects.
JF  - The journal of pain : official journal of the American Pain Society
AU  - Khoromi, Suzan
AU  - Patsalides, Athos
AU  - Parada, Suzan
AU  - Salehi, Vesta
AU  - Meegan, Jennifer M
AU  - Max, Mitchell B
AD  - Pain and Neurosensory Mechanisms Branch, National Institute of Dental and Craniofacial Research, Bethesda, MD 20892-1302, USA. khoromisu@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 829
EP  - 836
VL  - 6
IS  - 12
SN  - 1526-5900, 1526-5900
KW  - Analgesics
KW  - 0
KW  - Anticonvulsants
KW  - Ion Channels
KW  - Placebos
KW  - Receptors, Glutamate
KW  - topiramate
KW  - 0H73WJJ391
KW  - Fructose
KW  - 30237-26-4
KW  - Diphenhydramine
KW  - 8GTS82S83M
KW  - Index Medicus
KW  - Drug Administration Schedule
KW  - Double-Blind Method
KW  - Dose-Response Relationship, Drug
KW  - Receptors, Glutamate -- drug effects
KW  - Humans
KW  - Ion Channels -- drug effects
KW  - Anticonvulsants -- adverse effects
KW  - Aged
KW  - Anticonvulsants -- administration & dosage
KW  - Analgesics -- adverse effects
KW  - Patient Compliance -- statistics & numerical data
KW  - Diphenhydramine -- pharmacology
KW  - Adult
KW  - Treatment Outcome
KW  - Cross-Over Studies
KW  - Middle Aged
KW  - Chronic Disease
KW  - Analgesics -- administration & dosage
KW  - Male
KW  - Female
KW  - Low Back Pain -- drug therapy
KW  - Fructose -- analogs & derivatives
KW  - Intervertebral Disc Displacement -- physiopathology
KW  - Radiculopathy -- physiopathology
KW  - Fructose -- adverse effects
KW  - Low Back Pain -- physiopathology
KW  - Low Back Pain -- etiology
KW  - Fructose -- administration & dosage
KW  - Radiculopathy -- drug therapy
KW  - Intervertebral Disc Displacement -- drug therapy
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-24
N1  - Date created - 2005-12-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Gateway vectors for the production of combinatorially-tagged His6-MBP fusion proteins in the cytoplasm and periplasm of Escherichia coli.
AN  - 68860336; 16322578
AB  - Many proteins that accumulate in the form of insoluble aggregates when they are overproduced in Escherichia coli can be rendered soluble by fusing them to E. coli maltose binding protein (MBP), and this will often enable them to fold in to their biologically active conformations. Yet, although it is an excellent solubility enhancer, MBP is not a particularly good affinity tag for protein purification. To compensate for this shortcoming, we have engineered and successfully tested Gateway destination vectors for the production of dual His6MBP-tagged fusion proteins in the cytoplasm and periplasm of E. coli. The MBP moiety improves the yield and solubility of its fusion partners while the hexahistidine tag (His-tag) serves to facilitate their purification. The availability of a vector that targets His6MBP fusion proteins to the periplasm expands the utility of this dual tagging approach to include proteins that contain disulfide bonds or are toxic in the bacterial cytoplasm.
JF  - Protein science : a publication of the Protein Society
AU  - Nallamsetty, Sreedevi
AU  - Austin, Brian P
AU  - Penrose, Kerri J
AU  - Waugh, David S
AD  - National Cancer Institute at Frederick, P.O. Box B, Frederick, MD 21702, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 2964
EP  - 2971
VL  - 14
IS  - 12
SN  - 0961-8368, 0961-8368
KW  - Carrier Proteins
KW  - 0
KW  - His-His-His-His-His-His
KW  - Maltose-Binding Proteins
KW  - Oligopeptides
KW  - Recombinant Fusion Proteins
KW  - Histidine
KW  - 4QD397987E
KW  - Ribonucleases
KW  - EC 3.1.-
KW  - Index Medicus
KW  - Recombinant Fusion Proteins -- metabolism
KW  - Base Sequence
KW  - Solubility
KW  - Ribonucleases -- isolation & purification
KW  - Ribonucleases -- genetics
KW  - Recombinant Fusion Proteins -- isolation & purification
KW  - Recombinant Fusion Proteins -- genetics
KW  - Molecular Sequence Data
KW  - Gene Expression
KW  - Ribonucleases -- chemistry
KW  - Amino Acid Sequence
KW  - Genetic Vectors -- genetics
KW  - Ribonucleases -- metabolism
KW  - Escherichia coli -- metabolism
KW  - Carrier Proteins -- metabolism
KW  - Cytoplasm -- metabolism
KW  - Histidine -- genetics
KW  - Escherichia coli -- cytology
KW  - Carrier Proteins -- genetics
KW  - Periplasm -- metabolism
KW  - Oligopeptides -- genetics
KW  - Oligopeptides -- metabolism
KW  - Escherichia coli -- genetics
KW  - Histidine -- metabolism
KW  - Carrier Proteins -- isolation & purification
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2005-12-02
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Eur J Biochem. 2000 Jan;267(2):566-72 [10632727]
Trends Biotechnol. 2005 Jun;23(6):316-20 [15922084]
Structure. 2000 Sep 15;8(9):R177-85 [10986469]
Protein Eng. 2001 Apr;14(4):297-305 [11391022]
Toxicon. 2001 Oct;39(10):1595-600 [11478968]
J Mol Biol. 2001 Sep 7;312(1):79-93 [11545587]
Protein Sci. 2002 Feb;11(2):313-21 [11790841]
Protein Eng. 2001 Dec;14(12):993-1000 [11809930]
Acta Crystallogr D Biol Crystallogr. 2002 Mar;58(Pt 3):398-406 [11856824]
Cancer Lett. 2005 Jul 28;225(2):225-36 [15978327]
Methods Mol Biol. 2007;363:1-19 [17272834]
Eur J Biochem. 2002 Apr;269(7):1854-65 [11952787]
Protein Sci. 2002 Jul;11(7):1714-9 [12070324]
Methods Mol Biol. 2003;205:99-117 [12491882]
FEBS Lett. 2003 Feb 27;537(1-3):53-7 [12606030]
J Struct Funct Genomics. 2002;2(2):83-92 [12836665]
Biochemistry. 2003 Nov 18;42(45):13202-11 [14609331]
Protein Expr Purif. 2003 Dec;32(2):194-201 [14965764]
Curr Opin Struct Biol. 2004 Oct;14(5):577-83 [15465318]
Protein Expr Purif. 2004 Nov;38(1):108-15 [15477088]
J Bacteriol. 1967 Dec;94(6):1934-45 [4294595]
Gene. 1983 Nov;25(2-3):167-78 [6363212]
Protein Eng. 1995 Mar;8(3):261-73 [7479688]
Protein Expr Purif. 1997 Aug;10(3):309-19 [9268677]
Protein Sci. 1999 Aug;8(8):1668-74 [10452611]
Mol Biotechnol. 2000 May;15(1):51-63 [10911622]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Tumor regression and autoimmunity in patients treated with cytotoxic T lymphocyte-associated antigen 4 blockade and interleukin 2: a phase I/II study.
AN  - 68852939; 16283570
AB  - Cytotoxic T lymphocyte-associated antigen (CTLA)-4 can inhibit T-cell responses and is involved in tolerance against self antigens. We previously reported autoimmune manifestations and objective cancer regressions in patients with metastatic melanoma treated with CTLA-4 blockade. The possibility of activating tumor-reactive T cells while removing inhibitory activity with CTLA-4 blockade has stimulated interest in using anti-CTLA-4 antibodies in combination with other cancer immunotherapies to improve clinical outcomes. In this study, we assessed the antitumor activity and autoimmune toxicity of CTLA-4 blockade in combination with an immune-activating stimulus, interleukin (IL)-2, in patients with metastatic melanoma.
          Thirty-six patients received anti-CTLA-4 antibody every 3 weeks. Three patients per cohort received doses of .1, .3, 1.0, and 2.0 mg/kg. Twenty-four patients received 3.0 mg/kg. All patients received IL-2 therapy (720,000 IU/kg every 8 hours to a maximum of 15 doses). Eight patients (22%) experienced objective tumor responses (three complete and five partial), including metastases in the lungs, lymph nodes, mediastinum, and subcutaneous tissues. Six of the eight patients have ongoing objective responses at 11 to 19 months. Five patients (14%) developed grade III/IV autoimmune toxicities secondary to anti-CTLA-4 administration, including four patients with enterocolitis and one with arthritis and uveitis.
          There is not evidence to support a synergistic effect of CTLA-4 blockade plus IL-2 administration, because the 22% objective response rate is that expected from the sum of these two agents administered alone. Durable cancer regressions were seen in patients treated with this combination.
JF  - Annals of surgical oncology
AU  - Maker, Ajay V
AU  - Phan, Giao Q
AU  - Attia, Peter
AU  - Yang, James C
AU  - Sherry, Richard M
AU  - Topalian, Suzanne L
AU  - Kammula, Udai S
AU  - Royal, Richard E
AU  - Haworth, Leah R
AU  - Levy, Catherine
AU  - Kleiner, David
AU  - Mavroukakis, Sharon A
AU  - Yellin, Michael
AU  - Rosenberg, Steven A
AD  - Surgery Branch, National Cancer Institute, National Institutes of Health, CRC Room 3-3940, 10 Center Drive, MSC 1201, Bethesda, MD 20814, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1005
EP  - 1016
VL  - 12
IS  - 12
SN  - 1068-9265, 1068-9265
KW  - Antibodies, Monoclonal
KW  - 0
KW  - Antigens, CD
KW  - Antigens, Differentiation
KW  - CTLA-4 Antigen
KW  - CTLA4 protein, human
KW  - Immunosuppressive Agents
KW  - Interleukin-2
KW  - ipilimumab
KW  - 6T8C155666
KW  - Index Medicus
KW  - Drug Therapy, Combination
KW  - Humans
KW  - Adult
KW  - Tomography, X-Ray Computed
KW  - Autoimmunity
KW  - Middle Aged
KW  - Flow Cytometry
KW  - Male
KW  - Female
KW  - Melanoma -- diagnostic imaging
KW  - Skin Neoplasms -- immunology
KW  - Melanoma -- secondary
KW  - Antigens, Differentiation -- therapeutic use
KW  - Melanoma -- immunology
KW  - Skin Neoplasms -- secondary
KW  - Antibodies, Monoclonal -- therapeutic use
KW  - Immunotherapy -- methods
KW  - Skin Neoplasms -- drug therapy
KW  - Antibodies, Monoclonal -- pharmacokinetics
KW  - Interleukin-2 -- therapeutic use
KW  - Melanoma -- drug therapy
KW  - Skin Neoplasms -- diagnostic imaging
KW  - Immunosuppressive Agents -- therapeutic use
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-09
N1  - Date created - 2005-12-05
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
J Immunother. 2001 Jul-Aug;24(4):287-93 [11565830]
Nat Immunol. 2002 Jul;3(7):611-8 [12087419]
Annu Rev Immunol. 1996;14:233-58 [8717514]
J Exp Med. 1996 Jun 1;183(6):2541-50 [8676075]
J Exp Med. 1996 Jun 1;183(6):2533-40 [8676074]
Science. 1996 Mar 22;271(5256):1734-6 [8596936]
Science. 1995 Nov 10;270(5238):985-8 [7481803]
J Immunol. 1993 Oct 1;151(7):3489-99 [8397258]
J Immunol. 1992 Jul 15;149(2):380-8 [1320641]
J Exp Med. 1991 Sep 1;174(3):561-9 [1714933]
Science. 1990 Jun 15;248(4961):1349-56 [2113314]
Proc Natl Acad Sci U S A. 2003 Jul 8;100(14):8372-7 [12826605]
J Immunol. 1996 Aug 15;157(4):1333-6 [8759711]
J Neuroimmunol. 1997 Mar;73(1-2):57-62 [9058759]
Immunity. 1997 Oct;7(4):445-50 [9354465]
J Exp Med. 1998 Feb 2;187(3):427-32 [9449722]
Ann Surg. 1998 Sep;228(3):307-19 [9742914]
J Exp Med. 2000 Jul 17;192(2):303-10 [10899917]
J Exp Med. 2000 Jul 17;192(2):295-302 [10899916]
Cancer Res. 2000 May 1;60(9):2444-8 [10811122]
J Clin Oncol. 1999 Jul;17(7):2105-16 [10561265]
J Clin Oncol. 2005 Sep 1;23(25):6043-53 [16087944]
Eur J Immunol. 2004 Dec;34(12):3485-96 [15484187]
J Exp Med. 1999 Aug 2;190(3):355-66 [10430624]
J Immunol. 1999 May 15;162(10):5813-20 [10229815]
Comment In:
Ann Surg Oncol. 2005 Dec;12(12):957-9 [16244797]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Tenofovir disoproxil fumarate and an optimized background regimen of antiretroviral agents as salvage therapy for pediatric HIV infection.
AN  - 68848556; 16291735
AB  - Highly active antiretroviral therapy has altered the course of HIV infection among children, but new antiretroviral agents are needed for treatment-experienced children with drug-resistant virus. Tenofovir disoproxil fumarate (DF) is a promising agent for use in pediatric salvage therapy, because of its tolerability, efficacy, and resistance profile. We designed this study to provide preliminary pediatric safety and dosing information on tenofovir DF, while also providing potentially efficacious salvage therapy for heavily treatment-experienced, HIV-infected children.
          Tenofovir DF, alone and in combination with optimized background antiretroviral regimens, was studied among 18 HIV-infected children (age range: 8.3-16.2 years) who had progressive disease with > or = 2 prior antiretroviral regimens, in a single-center, open-label trial. Tenofovir DF monotherapy for 6 days was followed by the addition of individualized antiretroviral regimens. Subjects were monitored with HIV RNA reverse transcription-polymerase chain reaction, flow cytometry, and routine laboratory studies; monitoring for bone toxicity included measurement of lumbar spine bone mineral density (BMD) with dual-energy x-ray absorptiometry. Subjects were monitored through 48 weeks.
          Two subjects developed grade 3 elevated hepatic transaminase levels during monotherapy and were removed from the study. The remaining 16 subjects had a median of 4 antiretroviral agents (range: 3-5 agents) added to tenofovir DF. HIV plasma RNA levels decreased from a median pretreatment level of 5.4 log10 copies per mL (range: 4.1-5.9 log10 copies per mL) to 4.21 log10 copies per mL at week 48 (n = 15), with 6 subjects having 6% decrease in BMD for 5 of 15 subjects evaluated at week 48, necessitating the discontinuation of tenofovir DF therapy for 2; all 5 subjects experienced >2 log10 copies per mL decreases in HIV plasma RNA levels.
          Tenofovir DF-containing, individualized, highly active antiretroviral therapy regimens were well tolerated and effective among heavily treatment-experienced, HIV-infected children. Loss of BMD may limit tenofovir DF use among prepubertal patients.
JF  - Pediatrics
AU  - Hazra, Rohan
AU  - Gafni, Rachel I
AU  - Maldarelli, Frank
AU  - Balis, Frank M
AU  - Tullio, Antonella N
AU  - DeCarlo, Ellen
AU  - Worrell, Carol J
AU  - Steinberg, Seth M
AU  - Flaherty, John
AU  - Yale, Kitty
AU  - Kearney, Brian P
AU  - Zeichner, Steven L
AD  - HIV and AIDS Malignancy Branch, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - e846
EP  - e854
VL  - 116
IS  - 6
KW  - Anti-HIV Agents
KW  - 0
KW  - Organophosphonates
KW  - Tenofovir
KW  - 99YXE507IL
KW  - Adenine
KW  - JAC85A2161
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Viral Load
KW  - Drug Resistance, Viral
KW  - Humans
KW  - Salvage Therapy
KW  - Antiretroviral Therapy, Highly Active
KW  - Child
KW  - CD4 Lymphocyte Count
KW  - Adolescent
KW  - Male
KW  - Female
KW  - Child, Preschool
KW  - Adenine -- therapeutic use
KW  - Organophosphonates -- therapeutic use
KW  - Anti-HIV Agents -- therapeutic use
KW  - HIV Infections -- drug therapy
KW  - Adenine -- analogs & derivatives
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-22
N1  - Date created - 2005-12-02
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Hematopoietic stem cell gene therapy: dead or alive?
AN  - 68847047; 16216357
AB  - Despite some reports of toxicity in recent clinical trials, many scientists believe that the use of gene therapy in the treatment of congenital genetic defects and acquired disorders has too much potential to abandon. Hematopoietic stem cells (HSCs) have been primary targets for gene therapy owing to their capacity for differentiation and self-renewal, whereby multiple cell lineages can potentially be corrected for the lifetime of an individual. These efforts represent a long-term investment towards broadening physicians' treatment options for patients whose diseases, in particular certain immunodeficiencies, are fatal and where no other therapy is available. We review the recent progress and clinical triumphs as well as the reported toxicity related to insertional mutagenesis. We also discuss the current risk-to-benefit estimates and future strategies to reduce the risks and allow full realization of clinical potential. Scientists are continually revising protocols: going both from "bench to bedside" and, as strikingly demonstrated by HSC gene therapy, from "bedside to bench."
JF  - Trends in biotechnology
AU  - Ferguson, Cole
AU  - Larochelle, Andre
AU  - Dunbar, Cynthia E
AD  - Molecular Hematopoiesis Section, Hematology Branch, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, MD, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 589
EP  - 597
VL  - 23
IS  - 12
SN  - 0167-7799, 0167-7799
KW  - Index Medicus
KW  - Animals
KW  - Severe Combined Immunodeficiency -- therapy
KW  - Gene Transfer Techniques
KW  - Humans
KW  - Clinical Trials as Topic
KW  - Disease Models, Animal
KW  - Forecasting
KW  - Severe Combined Immunodeficiency -- genetics
KW  - Mutagenesis, Insertional
KW  - Hematopoietic Stem Cells
KW  - Genetic Therapy -- methods
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-18
N1  - Date created - 2005-11-29
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Can experimental paradigms and animal models be used to discover clinically effective medications for alcoholism?
AN  - 68843169; 16318951
AB  - Evaluating medications in animal laboratory paradigms can reveal whether the compound is effective in an established alcoholism model, at clinically relevant doses and exposure conditions, when administered orally (or transdermally) and without serious limiting side effects. Positive outcomes constitute a possible discovery for relevance to alcoholism and, under favorable marketing conditions, encourage further development. Medication testing using animal models of alcoholism might also guide clinical testing by discriminating clinically effective from clinically ineffective compounds. This ability rests on whether there are tests or, more reasonably, batteries of tests having this discriminative ability. The present paper examines this possibility. Effects of naltrexone and acamprosate in animal paradigms which model behavioral aspects of alcoholism are reviewed and compared with the effects of compounds which have limited effects in alcoholics. It is not clear at present whether any single paradigm or combination of paradigms differentiates clinically effective from clinically limited compounds. Steps are suggested to improve the use of preclinical laboratory tests to predict which compounds are likely to be effective medications for reducing drinking and sustaining abstinence in human alcoholics.
JF  - Addiction biology
AU  - Egli, Mark
AD  - Division of Neuroscience and Behavior, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Department of Health and Human Services Bethesda, MD 20892-9304, USA. megli@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 309
EP  - 319
VL  - 10
IS  - 4
SN  - 1355-6215, 1355-6215
KW  - Alcohol Deterrents
KW  - 0
KW  - Taurine
KW  - 1EQV5MLY3D
KW  - Naltrexone
KW  - 5S6W795CQM
KW  - acamprosate
KW  - N4K14YGM3J
KW  - Index Medicus
KW  - Taurine -- analogs & derivatives
KW  - Naltrexone -- administration & dosage
KW  - Animals
KW  - Taurine -- toxicity
KW  - Humans
KW  - Clinical Trials as Topic
KW  - Taurine -- administration & dosage
KW  - Rodentia
KW  - Drug Evaluation, Preclinical
KW  - Naltrexone -- toxicity
KW  - Alcoholism -- rehabilitation
KW  - Disease Models, Animal
KW  - Alcohol Deterrents -- administration & dosage
KW  - Alcohol Deterrents -- toxicity
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-04-03
N1  - Date created - 2005-12-01
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Molecularly targeted therapy for pediatric brain tumors.
AN  - 68839572; 16195796
AB  - Treatment of pediatric brain tumors remains a challenge because of the toxicity associated with conventional treatment and the relative resistance of tumors at the time of recurrence. The traditional approach of administering cytotoxic agents at the maximum tolerated dose is being supplanted by the development of molecularly targeted agents aimed at critical cellular changes that are responsible for the growth and spread of cancer cells. These agents theoretically should be more specific for tumor cells and less toxic to normal cells. While the idea of targeted therapy has generated much excitement in the oncology community, the degree of benefit to patients with central nervous system (CNS) tumors remains unclear. Numerous challenges remain in the development of these agents, including identification of meaningful targets, delivery of agents in sufficient quantity at the target site, and determination of any biologic response to these agents. This article discusses the rationale behind several of these agents and their use in pediatric patients with brain tumors.
JF  - Journal of neuro-oncology
AU  - K E, Warren
AD  - National Cancer Institute, Neuro-Oncology Branch, Bloch Bldg, 82, Rm 224, 9030 Old Georgetown Road, Bethesda, Maryland 20892-8200, USA. warrenk@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 335
EP  - 343
VL  - 75
IS  - 3
SN  - 0167-594X, 0167-594X
KW  - Antineoplastic Agents
KW  - 0
KW  - Enzyme Inhibitors
KW  - Platelet-Derived Growth Factor
KW  - Receptor, Epidermal Growth Factor
KW  - EC 2.7.10.1
KW  - Index Medicus
KW  - Receptor, Epidermal Growth Factor -- drug effects
KW  - Humans
KW  - Platelet-Derived Growth Factor -- drug effects
KW  - Receptor, Epidermal Growth Factor -- physiology
KW  - Child
KW  - Platelet-Derived Growth Factor -- physiology
KW  - Enzyme Inhibitors -- therapeutic use
KW  - Brain Neoplasms -- drug therapy
KW  - Brain Neoplasms -- genetics
KW  - Enzyme Inhibitors -- pharmacology
KW  - Brain Neoplasms -- physiopathology
KW  - Antineoplastic Agents -- therapeutic use
KW  - Antineoplastic Agents -- pharmacology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-28
N1  - Date created - 2005-11-29
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Endogenous PACAP acts as a stress response peptide to protect cerebellar neurons from ethanol or oxidative insult.
AN  - 68831645; 16009465
AB  - The rodent cerebellum is richly supplied with PACAPergic innervation. Exogenous pituitary adenylate cyclase-activating polypeptide (PACAP) increases cerebellar granule cell survival and differentiation in culture, and enhances the number of neuroblasts in the molecular and internal granule cell layers (IGL) when injected postnatally into the cerebellum in vivo. Here, we have investigated the role of endogenous PACAP during cerebellar development by comparing the morphology of normal and PACAP-deficient mouse cerebellum, and the response of cerebellar granule cells from normal and PACAP-deficient mice subjected to neurotoxic insult in culture. There was no difference in cerebellar volume or granule cell number, in 11-day-old wild type versus PACAP-deficient mice. Cultured cerebellar neurons from PACAP-deficient and wild type mice also showed no apparent differences in survival and differentiation either under depolarizing conditions, or non-depolarizing conditions in the presence or absence of either dibutyryl cAMP or 100 nM PACAP. However, cultured cerebellar neurons from PACAP-deficient mice were significantly more sensitive than wild type neurons to ethanol- or hydrogen peroxide-induced toxicity. Differential ethanol toxicity was reversed by addition of 100 nM exogenous PACAP, suggesting that endogenous PACAP has neuroprotective activity in the context of cellular insult or stress. The neuroprotective action of PACAP was mimicked by dibutryl cAMP, indicating that it occurred via activation of adenylate cyclase. These results indicate that PACAP might act to protect the brain from paraphysiological insult, including exposure to toxins or hypoxia.
JF  - Peptides
AU  - Vaudry, David
AU  - Hamelink, Carol
AU  - Damadzic, Ruslan
AU  - Eskay, Robert L
AU  - Gonzalez, Bruno
AU  - Eiden, Lee E
AD  - Section on Molecular Neuroscience, Laboratory of Cellular and Molecular Regulation, National Institute of Mental Health, 49 Convent Drive, Rm. 5A68, MSC 4090, 9000 Rockville Pike, Bethesda, MD 20892-4483, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 2518
EP  - 2524
VL  - 26
IS  - 12
SN  - 0196-9781, 0196-9781
KW  - Anti-Infective Agents, Local
KW  - 0
KW  - Pituitary Adenylate Cyclase-Activating Polypeptide
KW  - Ethanol
KW  - 3K9958V90M
KW  - Hydrogen Peroxide
KW  - BBX060AN9V
KW  - Index Medicus
KW  - Animals
KW  - Cells, Cultured
KW  - Mice
KW  - Mice, Knockout
KW  - Hydrogen Peroxide -- toxicity
KW  - Cerebellum -- cytology
KW  - Neurons -- metabolism
KW  - Pituitary Adenylate Cyclase-Activating Polypeptide -- pharmacology
KW  - Cerebellum -- growth & development
KW  - Neurons -- cytology
KW  - Oxidative Stress -- drug effects
KW  - Ethanol -- toxicity
KW  - Anti-Infective Agents, Local -- toxicity
KW  - Pituitary Adenylate Cyclase-Activating Polypeptide -- metabolism
KW  - Pituitary Adenylate Cyclase-Activating Polypeptide -- deficiency
KW  - Cerebellum -- metabolism
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Peptides&rft.atitle=Endogenous+PACAP+acts+as+a+stress+response+peptide+to+protect+cerebellar+neurons+from+ethanol+or+oxidative+insult.&rft.au=Vaudry%2C+David%3BHamelink%2C+Carol%3BDamadzic%2C+Ruslan%3BEskay%2C+Robert+L%3BGonzalez%2C+Bruno%3BEiden%2C+Lee+E&rft.aulast=Vaudry&rft.aufirst=David&rft.date=2005-12-01&rft.volume=26&rft.issue=12&rft.spage=2518&rft.isbn=&rft.btitle=&rft.title=Peptides&rft.issn=01969781&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-28
N1  - Date created - 2005-11-25
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Novel molecular targeted therapy for esophageal cancer.
AN  - 68825908; 16299785
AB  - Esophageal cancers are highly lethal neoplasms which are generally refractory to conventional multidisciplinary interventions. Recent elucidation of the mechanisms of esophageal carcinogenesis, as well as preclinical studies utilizing chromatin remodeling agents and inhibitors of oncogene signaling in conjunction with conventional chemotherapeutic agents provide new opportunities for the development of potentially efficacious molecular targeted therapies for these malignancies.
          (c) 2005 Wiley-Liss, Inc.
JF  - Journal of surgical oncology
AU  - Schrump, David S
AU  - Nguyen, Dao M
AD  - Thoracic Oncology Section, Surgery Branch, National Cancer Institute, Bldg. 10, Rm. 4-3490, 10 Center Drive MSC 1201, Bethesda, MD 20892, USA. David_Schrump@nih.gov
Y1  - 2005/12/01/
PY  - 2005
DA  - 2005 Dec 01
SP  - 257
EP  - 261
VL  - 92
IS  - 3
SN  - 0022-4790, 0022-4790
KW  - Depsipeptides
KW  - 0
KW  - Glycoproteins
KW  - Histone Deacetylase Inhibitors
KW  - tissue-factor-pathway inhibitor 2
KW  - Protein Kinase C
KW  - EC 2.7.11.13
KW  - Mitogen-Activated Protein Kinases
KW  - EC 2.7.11.24
KW  - Paclitaxel
KW  - P88XT4IS4D
KW  - Index Medicus
KW  - Animals
KW  - Drug Screening Assays, Antitumor
KW  - Apoptosis
KW  - Genes, Tumor Suppressor
KW  - Humans
KW  - Clinical Trials as Topic
KW  - Paclitaxel -- pharmacology
KW  - Adenocarcinoma -- genetics
KW  - Mitogen-Activated Protein Kinases -- physiology
KW  - Adenocarcinoma -- pathology
KW  - Gene Expression Regulation, Neoplastic
KW  - Barrett Esophagus -- pathology
KW  - DNA Methylation
KW  - Glycoproteins -- metabolism
KW  - Barrett Esophagus -- genetics
KW  - Depsipeptides -- pharmacology
KW  - Protein Kinase C -- physiology
KW  - Signal Transduction
KW  - Cell Transformation, Neoplastic
KW  - Esophageal Neoplasms -- prevention & control
KW  - Esophageal Neoplasms -- metabolism
KW  - Esophageal Neoplasms -- genetics
KW  - Esophageal Neoplasms -- pathology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-23
N1  - Date created - 2005-11-24
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Prevalence, correlates, co-morbidity, and comparative disability of DSM-IV generalized anxiety disorder in the USA: results from the National Epidemiologic Survey on Alcohol and Related Conditions.
AN  - 68824459; 16202187
AB  - This study addressed the prevalences, correlates, co-morbidity and disability of DSM-IV generalized anxiety disorder (GAD) and other psychiatric disorders in a large national survey of the general population, the National Institute on Alcohol Abuse and Alcoholism's (NIAAA) National Epidemiologic Survey on Alcohol and Related Conditions (NESARC). The study presents nationally representative data, for the first time, on prevalence, correlates, co-morbidity, and comparative disability of DSM-IV GAD.
          Data are taken from a large (n=43093) representative sample of the adult USA population.R: Prevalences of 12-month and lifetime GAD were 2.1% and 4.1%. Being female, middle-aged, widowed/separated/divorced, and low income increased risk, while being Asian, Hispanic, or Black decreased risk. GAD was highly co-morbid with substance use, and other anxiety, mood, and personality disorders. Co-morbidity in GAD was not substantially greater than for most other Axis I and II disorders. Disability and impairment in pure GAD were equivalent to pure mood disorders, but significantly greater than in pure substance use, and other anxiety and personality disorders. Individuals co-morbid for GAD and each mood disorder were more disabled than those with pure forms of GAD or each mood disorder. When co-morbid with GAD, nicotine dependence and other anxiety and personality disorders were not associated with increased disability over that associated with pure GAD, but GAD did show increased disability over that due to each of these disorders in pure form.Conclusions. Associations between GAD and Axis I and II disorders were strong and significant, with variation among specific disorders. Results strongly support GAD as an independent disorder with significant impairment and disability.
JF  - Psychological medicine
AU  - Grant, Bridget F
AU  - Hasin, Deborah S
AU  - Stinson, Frederick S
AU  - Dawson, Deborah A
AU  - June Ruan, W
AU  - Goldstein, Risë B
AU  - Smith, Sharon M
AU  - Saha, Tulshi D
AU  - Huang, Boji
AD  - Laboratory of Epidemiology and Biometry, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Bethesda, MD 20892-9304, USA. bgrant@willco.niaaa.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1747
EP  - 1759
VL  - 35
IS  - 12
SN  - 0033-2917, 0033-2917
KW  - Index Medicus
KW  - United States
KW  - Severity of Illness Index
KW  - Humans
KW  - Adult
KW  - Middle Aged
KW  - Adolescent
KW  - Sex Distribution
KW  - Male
KW  - Female
KW  - Comorbidity
KW  - Prevalence
KW  - Alcoholism -- epidemiology
KW  - Anxiety Disorders -- psychology
KW  - Alcoholism -- diagnosis
KW  - Anxiety Disorders -- diagnosis
KW  - Disability Evaluation
KW  - Anxiety Disorders -- epidemiology
KW  - Diagnostic and Statistical Manual of Mental Disorders
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-10
N1  - Date created - 2005-11-22
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Childhood exposure to environmental tobacco smoke and chronic respiratory symptoms in non-smoking adults: the Singapore Chinese Health Study.
AN  - 68819506; 16131525
AB  - Childhood exposure to environmental tobacco smoke has been extensively associated with childhood respiratory illness; fewer studies have addressed the effects on adults.
          Childhood environmental tobacco smoke exposure in relation to chronic cough, phlegm, and asthma diagnosis was studied in never smokers from a cohort of Singaporeans of Chinese ethnicity aged 45-74 years at enrollment from 1993 to 1998. From 1999 to 2004 subjects were interviewed regarding environmental tobacco smoke exposure before and after the age of 18 and the presence and duration of current symptoms of chronic cough and phlegm production and asthma diagnosis. Among 35,000 never smokers, fewer had smoking mothers (19%) than fathers (48%). Although few subjects currently lived (20%) or worked (4%) with smokers, 65% reported living with a daily smoker before the age of 18 years. Living with a smoker before the age of 18 increased the odds of chronic dry cough (149 cases, odds ratio 2.1, 95% CI 1.4 to 3.3) and, to a lesser extent, phlegm, after adjustment for age, sex, dialect group, and current and past exposure to smokers at home and at work after the age of 18. Associations strengthened with higher numbers of smokers in childhood. There was no association with asthma or chronic bronchitis. There was evidence to suggest a stronger association among subjects with a lower adult intake of fibre which has previously been found to be protective for respiratory symptoms.
          In this large study of non-smokers, living with a smoker in childhood was associated with chronic dry cough and phlegm in adulthood, independent of later exposures to environmental tobacco smoke.
JF  - Thorax
AU  - David, G L
AU  - Koh, W-P
AU  - Lee, H-P
AU  - Yu, M C
AU  - London, S J
AD  - Epidemiology Branch, National Institute of Environmental Health Sciences, NIH, Department of Health and Human Services, P O Box 12233, Mail Drop A3-05, Research Triangle Park, NC 27709, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1052
EP  - 1058
VL  - 60
IS  - 12
SN  - 0040-6376, 0040-6376
KW  - Tobacco Smoke Pollution
KW  - 0
KW  - Index Medicus
KW  - Humans
KW  - Infant, Newborn
KW  - Aged
KW  - Child
KW  - Child, Preschool
KW  - Cough -- etiology
KW  - Infant
KW  - Singapore -- epidemiology
KW  - Adult
KW  - Cough -- ethnology
KW  - Middle Aged
KW  - Chronic Disease
KW  - Adolescent
KW  - China -- ethnology
KW  - Male
KW  - Female
KW  - Tobacco Smoke Pollution -- statistics & numerical data
KW  - Respiratory Tract Diseases -- etiology
KW  - Respiratory Tract Diseases -- ethnology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-19
N1  - Date created - 2005-11-21
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Am J Respir Crit Care Med. 1997 Nov;156(5):1447-52 [9372659]
J Asthma. 1997;34(1):67-76 [9033442]
Am J Respir Crit Care Med. 1998 Sep;158(3):802-6 [9731008]
Am J Respir Crit Care Med. 1998 Nov;158(5 Pt 1):1493-8 [9817698]
Am J Respir Crit Care Med. 1999 Apr;159(4 Pt 1):1257-66 [10194174]
Thorax. 1999 Apr;54(4):357-66 [10092699]
JAMA. 2005 Sep 28;294(12):1505-10 [16189363]
QJM. 1999 Sep;92(9):527-30 [10627873]
Environ Health Perspect. 2001 Aug;109 Suppl 4:573-8 [11544166]
Chest. 2001 Sep;120(3):711-7 [11555497]
Nutr Cancer. 2001;39(2):187-95 [11759279]
J Epidemiol Community Health. 2002 Mar;56(3):167-70 [11854334]
Am J Clin Nutr. 2002 Mar;75(3):492-8 [11864854]
Epidemiology. 2002 May;13(3):268-76 [11964927]
Scand J Work Environ Health. 2002;28 Suppl 2:52-70 [12058803]
Am J Respir Crit Care Med. 2003 Jan 1;167(1):45-9 [12502475]
Am J Respir Crit Care Med. 2003 Mar 15;167(6):911-6 [12623860]
Cancer Epidemiol Biomarkers Prev. 2003 Sep;12(9):890-8 [14504200]
N Engl J Med. 2003 Oct 9;349(15):1414-22 [14534334]
Diabetes Care. 2004 Mar;27(3):752-7 [14988297]
Thorax. 2004 Apr;59(4):274-6 [15047943]
Thorax. 2004 Apr;59(4):295-302 [15047948]
J Allergy Clin Immunol. 2004 May;113(5):845-52 [15131565]
Am J Respir Crit Care Med. 2004 Aug 1;170(3):279-87 [15117740]
Am Rev Respir Dis. 1978 Dec;118(6 Pt 2):1-120 [742764]
Am Rev Respir Dis. 1986 Jun;133(6):1171-80 [3717766]
Singapore Med J. 1988 Apr;29(2):119-24 [3399913]
Singapore Med J. 1988 Jun;29(3):233-9 [3187574]
Am Rev Respir Dis. 1988 Aug;138(2):296-9 [3195829]
Int J Epidemiol. 1993 Oct;22(5):809-17 [8282459]
BMJ. 1994 Jul 9;309(6947):90-3 [8038673]
Am J Respir Crit Care Med. 1994 Nov;150(5 Pt 1):1222-8 [7952544]
Eur J Clin Nutr. 1994 Jul;48(7):522-4 [7956995]
J AOAC Int. 1995 Jan-Feb;78(1):22-36 [7703724]
JAMA. 1996 Apr 24;275(16):1233-40 [8601954]
BMJ. 1996 May 11;312(7040):1195-9 [8634562]
Lancet. 1998 Aug 8;352(9126):453 [9708758]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Incidence of haematopoietic malignancies in US radiologic technologists.
AN  - 68819095; 16299095
AB  - There are limited data on risks of haematopoietic malignancies associated with protracted low-to-moderate dose radiation.
          To contribute the first incidence risk estimates for haematopoietic malignancies in relation to work history, procedures, practices, and protective measures in a large population of mostly female medical radiation workers. The investigators followed up 71,894 (77.9% female) US radiologic technologists, first certified during 1926-80, from completion of a baseline questionnaire (1983-89) to return of a second questionnaire (1994-98), diagnosis of a first cancer, death, or 31 August 1998 (731,306 person-years), whichever occurred first. Cox proportional hazards regression was used to compute risks.
          Relative risks (RR) for leukaemias other than chronic lymphocytic leukaemia (non-CLL, 41 cases) were increased among technologists working five or more years before 1950 (RR = 6.6, 95% CI 1.0 to 41.9, based on seven cases) or holding patients 50 or more times for x ray examination (RR = 2.6, 95% CI 1.3 to 5.4). Risks of non-CLL leukaemias were not significantly related to the number of years subjects worked in more recent periods, the year or age first worked, the total years worked, specific procedures or equipment used, or personal radiotherapy. Working as a radiologic technologist was not significantly linked with risk of multiple myeloma (28 cases), non-Hodgkin's lymphoma (118 cases), Hodgkin's lymphoma (31 cases), or chronic lymphocytic leukaemia (23 cases). Similar to results for single acute dose and fractionated high dose radiation exposures, there was increased risk for non-CLL leukaemias decades after initial protracted radiation exposure that likely cumulated to low-to-moderate doses.
JF  - Occupational and environmental medicine
AU  - Linet, M S
AU  - Freedman, D M
AU  - Mohan, A K
AU  - Doody, M M
AU  - Ron, E
AU  - Mabuchi, K
AU  - Alexander, B H
AU  - Sigurdson, A
AU  - Hauptmann, M
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, Department of Health and Human Services, Bethesda, MD 20892, USA. linetm@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 861
EP  - 867
VL  - 62
IS  - 12
KW  - Index Medicus
KW  - Occupational Exposure
KW  - Radiation Dosage
KW  - Age Factors
KW  - Sex Factors
KW  - Humans
KW  - Risk Assessment
KW  - Lymphoma -- mortality
KW  - Lymphoma -- epidemiology
KW  - Leukemia -- mortality
KW  - Leukemia -- epidemiology
KW  - Multiple Myeloma -- epidemiology
KW  - Adult
KW  - Cohort Studies
KW  - Incidence
KW  - Middle Aged
KW  - United States -- epidemiology
KW  - Time Factors
KW  - Multiple Myeloma -- mortality
KW  - Female
KW  - Male
KW  - Proportional Hazards Models
KW  - Personnel, Hospital
KW  - Neoplasms, Radiation-Induced -- epidemiology
KW  - Technology, Radiologic -- manpower
KW  - Neoplasms, Radiation-Induced -- mortality
KW  - Hematologic Neoplasms -- epidemiology
KW  - Hematologic Neoplasms -- mortality
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2005-11-21
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
J Radiol Prot. 2000 Dec;20(4):353-9 [11140709]
Nucleonics. 1949 Dec;5(6):63-6 [15394470]
Health Phys. 2002 Apr;82(4):455-66 [11906134]
Int J Cancer. 2003 Jan 10;103(2):259-67 [12455042]
Semin Ultrasound CT MR. 2002 Oct;23(5):428-42 [12509113]
Am J Epidemiol. 1975 Mar;101(3):199-210 [1115059]
Radiology. 1978 Mar;126(3):677-9 [628739]
Br J Radiol. 1981 Mar;54(639):187-94 [7470779]
JAMA. 1990 Aug 1;264(5):601-4 [2366300]
Br J Radiol. 1991 May;64(761):455-60 [2036572]
Cancer. 1992 Jan 15;69(2):586-98 [1728391]
Radiat Res. 1995 Apr;142(1):1-11 [7899552]
Radiat Res. 1995 May;142(2):117-32 [7724726]
Radiat Res. 1995 Nov;144(2):160-9 [7480642]
Am J Epidemiol. 1997 Jan 1;145(1):72-80 [8982025]
J Radiol Prot. 1999 Mar;19(1):3-26 [10321692]
J Epidemiol. 1999 Apr;9(2):61-72 [10337078]
Radiat Res. 1999 Sep;152(3):280-92 [10453089]
Radiology. 1953 Feb;60(2):186-91 [13112398]
Am J Roentgenol Radium Ther Nucl Med. 1957 Dec;78(6):988-92 [13478785]
Science. 1963 Dec 13;142(3598):1492-4 [14077037]
Br J Radiol. 2001 Jun;74(882):507-19 [11459730]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Epidural fentanyl speeds the onset of sensory and motor blocks during epidural ropivacaine anesthesia.
AN  - 68816252; 16301269
AB  - In this study we examined the onset times of sensory and motor block during epidural ropivacaine anesthesia with and without the addition of fentanyl to the epidural solution. Forty-five young male patients undergoing knee arthroscopic surgery were randomly allocated into 3 groups of 15 patients each: epidural fentanyl (EF; epidural administration of 15 mL of 1% ropivacaine plus 100 mug fentanyl followed by IV injection of 2 mL of normal saline); IV fentanyl (IF; epidural administration of 15 mL of 1% ropivacaine plus 2 mL of normal saline followed by IV injection of 100 mug fentanyl); and control (C; epidural administration of 15 mL of 1% ropivacaine plus 2 mL of normal saline followed by IV injection of 2 mL of normal saline). The sensory and motor blocks were assessed by pinprick and modified Bromage scale, respectively. The hemodynamic changes, postepidural shivering, and side effects of epidural fentanyl were also recorded. There was no difference in the distribution of age, weight, and height among the 3 groups. The onset time of sensory block to the T10 dermatome was significantly more rapid in the EF group (13.0 +/- 3.0 min) than in the IF group (16.2 +/- 3.5 min, P < 0.05) or C group (17.7 +/- 3.6 min, P < 0.05). The onset times of motor block up to Bromage scale 1 and 2 were significantly more rapid in the EF group (11.9 +/- 4.6 and 24.4 +/- 5.9 min) than in the IF group (16.9 +/- 4.7 and 30.8 +/- 5.6 min, P < 0.05) or C group (18.3 +/- 4.9 and 32.7 +/- 5.7 min, P < 0.05). There was no difference in the incidence of shivering among the three groups. Pruritus was observed in three patients of the EF group and one patient of the IF group. No nausea, vomiting, respiratory depression, urinary retention, or hypotension was observed in any patient. We conclude that epidural administration of the mixture of 100 mug fentanyl and 1% ropivacaine solution accelerated the onset of sensory and motor blocks during epidural ropivacaine anesthesia without significant fentanyl-related side effects.
JF  - Anesthesia and analgesia
AU  - Cherng, Chen-Hwan
AU  - Yang, Chih-Ping
AU  - Wong, Chih-Shung
AD  - Department of Anesthesiology, Tri-Service General Hospital, No. 325, Sec. 2, Cheng-Gung Road, Nei-Hu, 114, Taipei, Taiwan. cherng1018@yahoo.com.tw
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1834
EP  - 1837
VL  - 101
IS  - 6
SN  - 0003-2999, 0003-2999
KW  - Amides
KW  - 0
KW  - Analgesics, Opioid
KW  - Anesthetics, Local
KW  - ropivacaine
KW  - 7IO5LYA57N
KW  - Fentanyl
KW  - UF599785JZ
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Prospective Studies
KW  - Arthroscopy
KW  - Double-Blind Method
KW  - Humans
KW  - Adult
KW  - Drug Synergism
KW  - Sensation
KW  - Knee -- surgery
KW  - Amides -- pharmacology
KW  - Anesthetics, Local -- pharmacology
KW  - Analgesics, Opioid -- pharmacology
KW  - Fentanyl -- pharmacology
KW  - Anesthesia, Epidural -- methods
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-20
N1  - Date created - 2005-11-22
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Brain hyperthermia as physiological and pathological phenomena.
AN  - 68807323; 15890410
AB  - Although brain metabolism consumes high amounts of energy and is accompanied by intense heat production, brain temperature is usually considered a stable, tightly "regulated" homeostatic parameter. Current research, however, revealed relatively large and rapid brain temperature fluctuations (3-4 degrees C) in animals during various normal, physiological, and behavioral activities at stable ambient temperatures. This review discusses these data and demonstrates that physiological brain hyperthermia has an intra-brain origin, resulting from enhanced neural metabolism and increased intra-brain heat production. Therefore, brain temperature is an important physiological parameter that both reflects alterations in metabolic neural activity and affects various neural functions. This work also shows that brain hyperthermia may be induced by various drugs of abuse that cause metabolic brain activation and impair heat dissipation. While individual drugs (i.e., heroin, cocaine, methamphetamine, MDMA) have specific, dose-dependent effects on brain and body temperatures, these effects are strongly modulated by an individual's activity state and environmental conditions, and change dramatically during the development of drug self-administration. Thus, brain thermorecording may provide new information on the central effects of various addictive drugs, drug-activity-environment interactions in mediating drugs' adverse effects, and alterations in metabolic neural activity associated with the development of drug-seeking and drug-taking behavior. While ambient temperatures and impairment of heat dissipation may also affect brain temperature, these environmental conditions strongly potentiate thermal effects of psychomotor stimulant drugs, resulting in pathological brain overheating. Since hyperthermia exacerbates drug-induced toxicity and is destructive to neural cells and brain functions, use of these drugs under activated conditions that restrict heat loss may pose a significant health risk, resulting in both acute life-threatening complications and chronic destructive CNS changes.
JF  - Brain research. Brain research reviews
AU  - Kiyatkin, Eugene A
AD  - Cellular Neurobiology Branch, National Institute on Drug Abuse-Intramural Research Program, National Institutes of Health, DHHS, 5500 Nathan Shock, Baltimore, MD 21224, USA. ekiyatki@intra.nida.nih.gov
Y1  - 2005/12/01/
PY  - 2005
DA  - 2005 Dec 01
SP  - 27
EP  - 56
VL  - 50
IS  - 1
KW  - Adrenergic Uptake Inhibitors
KW  - 0
KW  - Narcotics
KW  - Index Medicus
KW  - Animals
KW  - Adrenergic Uptake Inhibitors -- adverse effects
KW  - Humans
KW  - Narcotics -- adverse effects
KW  - Body Temperature -- physiology
KW  - Fever -- pathology
KW  - Brain Diseases -- chemically induced
KW  - Fever -- physiopathology
KW  - Brain Diseases -- physiopathology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68807323?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Brain+research.+Brain+research+reviews&rft.atitle=Brain+hyperthermia+as+physiological+and+pathological+phenomena.&rft.au=Kiyatkin%2C+Eugene+A&rft.aulast=Kiyatkin&rft.aufirst=Eugene&rft.date=2005-12-01&rft.volume=50&rft.issue=1&rft.spage=27&rft.isbn=&rft.btitle=&rft.title=Brain+research.+Brain+research+reviews&rft.issn=&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-30
N1  - Date created - 2005-11-18
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Molecular mechanisms of hexavalent chromium-induced apoptosis in human bronchoalveolar cells.
AN  - 68806698; 16166740
AB  - Hexavalent chromium (Cr[VI]) is classified by the International Agency for Research on Cancer as a group I carcinogen. Although the U.S. Occupational Safety and Health Administration was obliged to reduce the permissible exposure limit (PEL), it was reported that U.S. workers continue to be exposed to dangerously high Cr(VI) levels. In this study, we examined the role of p53 and target genes in a bronchoalveolar carcinoma isogenic cell line system and in primary human bronchial epithelial cells. p53-Negative parental H358 cell line, the same line in which the wild-type p53 expression vector (pC53-SN3) was introduced, and cells obtained from biopsies of human bronchus were exposed to chromate. Induction of DNA strand breaks were evaluated by alkaline elution assay, and apoptosis was analyzed by gel ladder, annexin V-PI staining, and ELISA, whereas p53 and target genes were evaluated by Western blots. Although Cr(VI) induced DNA strand breaks in both H358 cell clones, apoptosis was present only in the p53-transfected cells (H358p53(+/+)). In these cells, Cr(VI)-induced apoptosis is mediated by p53 upregulation of p53-upregulated modulator of apoptosis (PUMA), BAX translocation to mitochondria, cytochrome c release, and caspase-3 activation. In primary human bronchial epithelial cells expressing functional p53, Cr(VI) induced expression of PUMA and Noxa, which promote apoptosis through BAX. This result establishes p53 as the "necessary" player in Cr(VI)-induced apoptosis. To the best of our knowledge, this is the first report indicating strict correlation of Cr(VI) apoptosis to PUMA induction on primary human bronchoalveolar cells in short-term cultures.
JF  - American journal of respiratory cell and molecular biology
AU  - Russo, Patrizia
AU  - Catassi, Alessia
AU  - Cesario, Alfredo
AU  - Imperatori, Andrea
AU  - Rotolo, Nicola
AU  - Fini, Massimo
AU  - Granone, Pierluigi
AU  - Dominioni, Lorenzo
AD  - Department of Integrated Medical Oncology (DOMI), Laboratory of Translational Research B (Lung Cancer), National Cancer Institute, Largo Rosanna Benzi 10, I-16132 Genoa, Italy. patrizia.russo@istge.it
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 589
EP  - 600
VL  - 33
IS  - 6
SN  - 1044-1549, 1044-1549
KW  - Apoptosis Regulatory Proteins
KW  - 0
KW  - BBC3 protein, human
KW  - Carcinogens, Environmental
KW  - Proto-Oncogene Proteins
KW  - Tumor Suppressor Protein p53
KW  - bcl-2-Associated X Protein
KW  - Chromium
KW  - 0R0008Q3JB
KW  - chromium hexavalent ion
KW  - 18540-29-9
KW  - Cytochromes c
KW  - 9007-43-6
KW  - CASP3 protein, human
KW  - EC 3.4.22.-
KW  - Caspase 3
KW  - Caspases
KW  - Index Medicus
KW  - Cytochromes c -- metabolism
KW  - Humans
KW  - Biopsy
KW  - Bronchi -- drug effects
KW  - Caspases -- metabolism
KW  - bcl-2-Associated X Protein -- metabolism
KW  - DNA Damage -- drug effects
KW  - Epithelial Cells -- metabolism
KW  - Epithelial Cells -- drug effects
KW  - Tumor Cells, Cultured
KW  - Bronchi -- cytology
KW  - Mitochondria -- drug effects
KW  - Enzyme Activation -- drug effects
KW  - Mitochondria -- metabolism
KW  - Enzyme-Linked Immunosorbent Assay
KW  - Up-Regulation
KW  - Bronchi -- metabolism
KW  - Protein Transport
KW  - Adenocarcinoma, Bronchiolo-Alveolar -- drug therapy
KW  - Lung Neoplasms -- drug therapy
KW  - Apoptosis Regulatory Proteins -- metabolism
KW  - Apoptosis -- drug effects
KW  - Proto-Oncogene Proteins -- metabolism
KW  - Adenocarcinoma, Bronchiolo-Alveolar -- metabolism
KW  - Carcinogens, Environmental -- toxicity
KW  - Chromium -- toxicity
KW  - Tumor Suppressor Protein p53 -- metabolism
KW  - Lung Neoplasms -- metabolism
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=American+journal+of+respiratory+cell+and+molecular+biology&rft.atitle=Molecular+mechanisms+of+hexavalent+chromium-induced+apoptosis+in+human+bronchoalveolar+cells.&rft.au=Russo%2C+Patrizia%3BCatassi%2C+Alessia%3BCesario%2C+Alfredo%3BImperatori%2C+Andrea%3BRotolo%2C+Nicola%3BFini%2C+Massimo%3BGranone%2C+Pierluigi%3BDominioni%2C+Lorenzo&rft.aulast=Russo&rft.aufirst=Patrizia&rft.date=2005-12-01&rft.volume=33&rft.issue=6&rft.spage=589&rft.isbn=&rft.btitle=&rft.title=American+journal+of+respiratory+cell+and+molecular+biology&rft.issn=10441549&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-10
N1  - Date created - 2005-11-18
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
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Neoplasma. 2004;51(3):175-80 [15254669]
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Chest. 1994 Mar;105(3 Suppl):67S-74S [8131616]
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Am J Pathol. 1996 Sep;149(3):845-52 [8780388]
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Toxicol Sci. 2000 May;55(1):60-8 [10788560]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Insertional mutagenesis identifies genes that promote the immortalization of primary bone marrow progenitor cells.
AN  - 68805980; 16109773
AB  - Retroviruses can induce hematopoietic disease via insertional mutagenesis of cancer genes and provide valuable molecular tags for cancer gene discovery. Here we show that insertional mutagenesis can also identify genes that promote the immortalization of hematopoietic cells, which normally have only limited self-renewal. Transduction of mouse bone marrow cells with replication-incompetent murine stem cell virus (MSCV) expressing only neo, followed by serial passage in liquid culture containing stem cell factor (SCF) and interleukin-3 (IL-3), produced immortalized immature myeloid cell lines with neutrophil and macrophage differentiation potential in about 50% of the infected cultures. More than half of the lines have MSCV insertions at Evi1 or Prdm16. These loci encode transcription factor homologs and are validated human myeloid leukemia genes. Integrations are located in intron 1 or 2, where they promote expression of truncated proteins lacking the PRDI-BF1-RIZ1 homologous (PR) domain, similar to what is observed in human leukemias with EVI1 or PRDM16 mutations. Evi1 overexpression alone appears sufficient to immortalize immature myeloid cells and does not seem to require any other cooperating mutations. Genes identified by insertional mutagenesis by their nature could also be involved in immortalization of leukemic stem cells, and thus represent attractive drug targets for treating cancer.
JF  - Blood
AU  - Du, Yang
AU  - Jenkins, Nancy A
AU  - Copeland, Neal G
AD  - Mouse Cancer Genetics Program, National Cancer Institute, Center for Cancer Research, Frederick, MD 21702, USA.
Y1  - 2005/12/01/
PY  - 2005
DA  - 2005 Dec 01
SP  - 3932
EP  - 3939
VL  - 106
IS  - 12
SN  - 0006-4971, 0006-4971
KW  - DNA-Binding Proteins
KW  - 0
KW  - MECOM protein, human
KW  - PRDM16 protein, human
KW  - Transcription Factors
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Animals
KW  - Blotting, Northern
KW  - Humans
KW  - Transduction, Genetic
KW  - DNA-Binding Proteins -- genetics
KW  - Cell Differentiation
KW  - Mice
KW  - Transcription Factors -- genetics
KW  - Leukemia -- genetics
KW  - Polymerase Chain Reaction
KW  - Blotting, Southern
KW  - Zinc Fingers -- genetics
KW  - Proto-Oncogenes -- genetics
KW  - Cell Culture Techniques -- methods
KW  - Flow Cytometry
KW  - Retroviridae -- genetics
KW  - Bone Marrow Cells -- virology
KW  - Hematopoietic Stem Cells -- physiology
KW  - Hematopoietic Stem Cells -- virology
KW  - Cell Line, Transformed
KW  - Mutagenesis, Insertional -- genetics
KW  - Bone Marrow Cells -- physiology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Blood&rft.atitle=Insertional+mutagenesis+identifies+genes+that+promote+the+immortalization+of+primary+bone+marrow+progenitor+cells.&rft.au=Du%2C+Yang%3BJenkins%2C+Nancy+A%3BCopeland%2C+Neal+G&rft.aulast=Du&rft.aufirst=Yang&rft.date=2005-12-01&rft.volume=106&rft.issue=12&rft.spage=3932&rft.isbn=&rft.btitle=&rft.title=Blood&rft.issn=00064971&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-18
N1  - Date created - 2005-11-18
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Blood. 2000 Feb 1;95(3):1007-13 [10648416]
Cell. 2000 Jan 7;100(1):57-70 [10647931]
Mol Cell Biol. 2000 Oct;20(20):7419-26 [11003639]
Blood. 2000 Nov 1;96(9):3209-14 [11050005]
Nat Med. 2000 Nov;6(11):1278-81 [11062542]
J Exp Med. 2001 Feb 19;193(4):531-43 [11181704]
Genesis. 2001 Jun;30(2):82-8 [11416868]
Nature. 2001 Nov 1;414(6859):105-11 [11689955]
Haematologica. 2001 Nov;86(11):1124-57 [11694400]
Acta Haematol. 2002;107(2):76-94 [11919388]
Science. 2002 Apr 19;296(5567):497 [11964471]
Mol Cell. 2002 Nov;10(5):1107-17 [12453418]
Proc Natl Acad Sci U S A. 2003 Apr 1;100(7):3983-8 [12629218]
Nature. 2003 May 15;423(6937):255-60 [12714970]
Nature. 2003 May 15;423(6937):302-5 [12714971]
Nat Immunol. 2003 Jun;4(6):525-32 [12717432]
Proc Natl Acad Sci U S A. 2003 Aug 19;100(17):10002-7 [12890867]
Blood Cells Mol Dis. 2003 Sep-Oct;31(2):206-12 [12972028]
Blood. 2003 Nov 1;102(9):3323-32 [12816872]
Haematologica. 2003 Nov;88(11):1221-8 [14607750]
J Biol Chem. 2003 Dec 12;278(50):49806-11 [14555651]
Genes Dev. 2003 Dec 15;17(24):3029-35 [14701873]
Cancer Sci. 2004 Jun;95(6):503-7 [15182431]
N Engl J Med. 2004 Aug 12;351(7):657-67 [15306667]
J Clin Invest. 2004 Sep;114(5):713-9 [15343390]
Blood. 1985 Dec;66(6):1362-70 [4063525]
Blood. 1986 Sep;68(3):652-7 [3461853]
Proc Natl Acad Sci U S A. 1990 Dec;87(23):9202-6 [2251265]
Mol Cell Biol. 1992 Jan;12(1):183-9 [1370341]
Proc Natl Acad Sci U S A. 1992 May 1;89(9):3937-41 [1570317]
J Exp Med. 1992 Oct 1;176(4):1149-63 [1402659]
Proc Natl Acad Sci U S A. 1993 Jul 15;90(14):6454-8 [8341654]
Leukemia. 1993 Oct;7(10):1654-7 [8412328]
Blood. 1994 Oct 15;84(8):2681-8 [7919381]
Leukemia. 1996 May;10(5):788-94 [8656673]
J Exp Med. 1996 May 1;183(5):2283-91 [8642337]
Genomics. 1996 Oct 1;37(1):24-8 [8921366]
Proc Natl Acad Sci U S A. 1996 Nov 26;93(24):14059-64 [8943060]
Genes Dev. 1997 Jan 15;11(2):226-40 [9009205]
Nat Med. 1997 Jul;3(7):730-7 [9212098]
J Biol Chem. 1998 Jun 26;273(26):15933-9 [9632640]
Blood. 1998 Jul 1;92(1):83-92 [9639503]
Immunity. 1998 Jul;9(1):47-57 [9697835]
Proc Natl Acad Sci U S A. 1998 Aug 18;95(17):10129-33 [9707612]
Haematologica. 1999 Aug;84(8):690-4 [10457403]
Cancer Cell. 2004 Dec;6(6):587-96 [15607963]
Blood. 2005 Oct 1;106(7):2530-3 [15933056]
Nature. 1994 Feb 17;367(6464):645-8 [7509044]
Blood. 1994 Aug 15;84(4):1243-8 [8049440]
Genes Dev. 1999 Oct 15;13(20):2678-90 [10541554]
Leukemia. 1999 Nov;13(11):1639-45 [10557037]
Histol Histopathol. 2000 Jan;15(1):109-17 [10668202]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Combined blockade of AMPA and NMDA glutamate receptors reduces levodopa-induced motor complications in animal models of PD.
AN  - 68805518; 16203001
AB  - AMPA and NMDA receptors, abundantly expressed on striatal medium spiny neurons, have been implicated in the regulation of corticostriatal synaptic efficacy. To evaluate the contribution of both glutamate receptor types to the pathogenesis of motor response alterations associated with dopaminergic treatment, we studied the ability of the selective AMPA receptor antagonist GYKI-47261 and the selective NMDA receptor antagonists, MK-801 and amantadine, to mitigate these syndromes in rodent and primate models of Parkinson's disease. The effects of GYKI-47261 and amantadine (or MK-801), alone and in combination, were compared for their ability to modify dyskinesias induced by levodopa. In rats, simultaneous administration of subthreshold doses of AMPA and NMDA receptor antagonists completely normalized the wearing-off response to acute levodopa challenge produced by chronic levodopa treatment (P < 0.05). In primates, the glutamate antagonists GYKI-47261 and amantadine, co-administered at low doses (failing to alter dyskinesia scores), reduced levodopa-induced dyskinesias by 51% (P < 0.05). The simultaneous AMPA and NMDA receptor blockade acts to provide a substantially greater reduction in the response alterations induced by levodopa than inhibition of either of these receptors alone. The results suggest that mechanisms mediated by both ionotropic glutamate receptors make an independent contribution to the pathogenesis of these motor response changes and further that a combination of both drug types may provide relief from these disabling complications at lower and thus safer and more tolerable doses than required when either drug is used alone.
JF  - Experimental neurology
AU  - Bibbiani, F
AU  - Oh, J D
AU  - Kielaite, A
AU  - Collins, M A
AU  - Smith, C
AU  - Chase, T N
AD  - ETB, NINDS, National Institutes of Health, Bethesda, MD 20892, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 422
EP  - 429
VL  - 196
IS  - 2
SN  - 0014-4886, 0014-4886
KW  - Antiparkinson Agents
KW  - 0
KW  - Benzazepines
KW  - Dopamine Agents
KW  - Dopamine Agonists
KW  - Excitatory Amino Acid Antagonists
KW  - GYKI 47261
KW  - Receptors, AMPA
KW  - Receptors, Glutamate
KW  - Receptors, N-Methyl-D-Aspartate
KW  - Benzodiazepines
KW  - 12794-10-4
KW  - Quinpirole
KW  - 20OP60125T
KW  - Levodopa
KW  - 46627O600J
KW  - Dizocilpine Maleate
KW  - 6LR8C1B66Q
KW  - SK&F 82958
KW  - 80751-65-1
KW  - Amantadine
KW  - BF4C9Z1J53
KW  - Index Medicus
KW  - Rotarod Performance Test -- methods
KW  - Animals
KW  - Benzazepines -- pharmacology
KW  - Drug Interactions
KW  - Dose-Response Relationship, Drug
KW  - Receptors, Glutamate -- physiology
KW  - Disease Models, Animal
KW  - Haplorhini
KW  - Behavior, Animal
KW  - Dizocilpine Maleate -- pharmacology
KW  - Excitatory Amino Acid Antagonists -- pharmacology
KW  - Rats
KW  - Rats, Sprague-Dawley
KW  - Quinpirole -- pharmacology
KW  - Dopamine Agonists -- pharmacology
KW  - Motor Activity -- drug effects
KW  - Antiparkinson Agents -- pharmacology
KW  - Amantadine -- pharmacology
KW  - Benzodiazepines -- pharmacology
KW  - Time Factors
KW  - Male
KW  - Parkinson Disease, Secondary -- chemically induced
KW  - Receptors, N-Methyl-D-Aspartate -- physiology
KW  - Receptors, AMPA -- antagonists & inhibitors
KW  - Receptors, N-Methyl-D-Aspartate -- antagonists & inhibitors
KW  - Receptors, AMPA -- physiology
KW  - Dopamine Agents -- adverse effects
KW  - Levodopa -- adverse effects
KW  - Parkinson Disease, Secondary -- drug therapy
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68805518?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Experimental+neurology&rft.atitle=Combined+blockade+of+AMPA+and+NMDA+glutamate+receptors+reduces+levodopa-induced+motor+complications+in+animal+models+of+PD.&rft.au=Bibbiani%2C+F%3BOh%2C+J+D%3BKielaite%2C+A%3BCollins%2C+M+A%3BSmith%2C+C%3BChase%2C+T+N&rft.aulast=Bibbiani&rft.aufirst=F&rft.date=2005-12-01&rft.volume=196&rft.issue=2&rft.spage=422&rft.isbn=&rft.btitle=&rft.title=Experimental+neurology&rft.issn=00144886&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-25
N1  - Date created - 2005-11-18
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Functional characterization of novel allelic variants of CYP2C9 recently discovered in southeast Asians.
AN  - 68801576; 16099926
AB  - CYP2C9 was recently resequenced in 150 Asian subjects from Singapore. Several new coding variants were reported, and these variants are now named CYP2C9*14 (R125H), CYP2C9*15 (S162X), CYP2C9*16 (T299A), CYP2C9*17 (P382S), CYP2C9*18 (D397A), and CYP2C9*19 (Q454H). The CYP2C9*18 variant also contained an I359L change previously associated with the CYP2C9*3 allele. In this study, we assessed the functional consequences of the new coding changes. cDNAs containing each of the new coding changes were constructed by site-directed mutagenesis and expressed in a bacterial cDNA expression system, the allelic proteins were partially purified, and their ability to hydroxylate a prototype CYP2C9 substrate was assayed. Expression of cDNAs in Escherichia coli containing either the D397A change or the S162X (premature stop codon) could not be detected either spectrally or at the apoprotein level. CYP2C9.14 and CYP2C9.16 exhibited 80 to 90% lower catalytic activity toward tolbutamide at two substrate concentrations compared with wild-type CYP2C9.1. Kinetic analysis confirmed that CYP2C9.14 and CYP2C9.16 have a higher Km and a >90% lower intrinsic clearance of tolbutamide compared with wild-type CYP2C9.1. Both CYP2C9.17 and CYP2C9.19 proteins exhibited modest 30 to 40% decreases in catalytic activity toward tolbutamide. Thus, CYP2C9*15 and CYP2C9*18 may represent null alleles, whereas CYP2C9*14 and CYP2C9*16 allelic variants produce proteins that are clearly catalytically defective in vitro, indicating the existence of new defective putative alleles of CYP2C9 in Asians.
JF  - The Journal of pharmacology and experimental therapeutics
AU  - DeLozier, Tracy C
AU  - Lee, Soo-Chin
AU  - Coulter, Sherry J
AU  - Goh, Boon Cher
AU  - Goldstein, Joyce A
AD  - Human Metabolism Section, Laboratory of Pharmacology and Chemistry, National Institute of Environmental Health Sciences, NIH, Research Triangle Park, NC 27709, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1085
EP  - 1090
VL  - 315
IS  - 3
SN  - 0022-3565, 0022-3565
KW  - DNA, Complementary
KW  - 0
KW  - Recombinant Proteins
KW  - Tolbutamide
KW  - 982XCM1FOI
KW  - CYP2C9 protein, human
KW  - EC 1.14.13.-
KW  - Cytochrome P-450 CYP2C9
KW  - Aryl Hydrocarbon Hydroxylases
KW  - EC 1.14.14.1
KW  - Index Medicus
KW  - India -- ethnology
KW  - Humans
KW  - Tolbutamide -- pharmacology
KW  - Tolbutamide -- pharmacokinetics
KW  - Escherichia coli -- genetics
KW  - Hydroxylation
KW  - Mutagenesis, Site-Directed
KW  - Recombinant Proteins -- isolation & purification
KW  - Tolbutamide -- metabolism
KW  - Recombinant Proteins -- metabolism
KW  - Kinetics
KW  - Singapore
KW  - China -- ethnology
KW  - Catalysis
KW  - Genetic Variation
KW  - Polymorphism, Single Nucleotide
KW  - Aryl Hydrocarbon Hydroxylases -- metabolism
KW  - Alleles
KW  - Aryl Hydrocarbon Hydroxylases -- genetics
KW  - Aryl Hydrocarbon Hydroxylases -- isolation & purification
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-23
N1  - Date created - 2005-11-18
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Tau is hyperphosphorylated in the insulin-like growth factor-I null brain.
AN  - 68799875; 16123158
AB  - IGF action has been implicated in the promotion of oxidative stress and aging in invertebrate and murine models. However, some in vitro models suggest that IGF-I specifically prevents neuronal oxidative damage. To investigate whether IGF-I promotes or retards brain aging, we evaluated signs of oxidative stress and neuropathological aging in brains from 400-d-old Igf1-/- and wild-type (WT) mice. Lipofuscin pigment accumulation reflects oxidative stress and aging, but we found no difference in lipofuscin deposition in Igf1-/- and WT brains. Likewise, there was no apparent difference in accumulation of nitrotyrosine residues in Igf1-/- and WT brains, except for layer IV/V of the cerebral cortex, where these proteins were about 20% higher in the Igf1-/- brain (P = 0.03). We found no difference in the levels of oxidative stress-related enzymes, neuronal nitric oxide synthase, inducible nitric oxide synthase, and superoxide dismutase in Igf1-/- and WT brains. Tau is a microtubule-associated protein that causes the formation of neurofibrillary tangles and senile plaques as it becomes hyperphosphorylated in the aging brain. Tau phosphorylation was dramatically increased on two specific residues, Ser-396 and Ser-202, both glycogen synthase kinases target sites implicated in neurodegeneration. These observations indicate that IGF-I has a major role in regulating tau phosphorylation in the aging brain, whereas its role in promoting or preventing oxidative stress remains uncertain.
JF  - Endocrinology
AU  - Cheng, Clara M
AU  - Tseng, Victor
AU  - Wang, Jie
AU  - Wang, Daniel
AU  - Matyakhina, Ludmila
AU  - Bondy, Carolyn A
AD  - Developmental Endocrinology Branch, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892, USA. chengc@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 5086
EP  - 5091
VL  - 146
IS  - 12
SN  - 0013-7227, 0013-7227
KW  - Lipofuscin
KW  - 0
KW  - tau Proteins
KW  - 3-nitrotyrosine
KW  - 3604-79-3
KW  - Tyrosine
KW  - 42HK56048U
KW  - Insulin-Like Growth Factor I
KW  - 67763-96-6
KW  - Nitric Oxide Synthase
KW  - EC 1.14.13.39
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Animals
KW  - Aging -- metabolism
KW  - Phosphorylation
KW  - Oxidative Stress
KW  - Drug Residues -- metabolism
KW  - Mice
KW  - Tyrosine -- metabolism
KW  - Tyrosine -- analogs & derivatives
KW  - Male
KW  - Lipofuscin -- metabolism
KW  - Nitric Oxide Synthase -- biosynthesis
KW  - Mice, Knockout
KW  - Brain -- enzymology
KW  - tau Proteins -- metabolism
KW  - Insulin-Like Growth Factor I -- deficiency
KW  - Brain -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-05
N1  - Date created - 2005-11-18
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Assessment of the integrity of study blindness in a pediatric clinical trial of risperidone.
AN  - 68797858; 16282839
AB  - Controlled clinical trials in pediatric psychopharmacology rely on blinded parents and clinical evaluators for outcome data, but little is known about the success of the masking procedures. The blindness of clinical evaluators and parents was examined in a clinical trial of risperidone in autism.
          Clinical evaluators and parents were asked to guess individual treatment assignments at the end of an 8-week placebo-controlled trial of risperidone in children (aged 5-17 years) with autism. Clinical evaluators did not have access to adverse event data. The rates of correctly guessing individual treatment assignment (risperidone or placebo) were significantly greater than chance for both clinical evaluators and parents (P < 0.001). Clinical evaluators associated improvement with attribution to risperidone, and lack of improvement with attribution to placebo, in both the risperidone and placebo treatment arms. Parents associated improvement with attribution to risperidone only in the placebo treatment arm. Parents reported that adverse events influenced their guesses, but presence of adverse events was not associated with correctness of guess.
          Improvement was associated with attribution to active treatment regardless of actual treatment assignment, and adverse events did not appear to be a threat to study blindness.
JF  - Journal of clinical psychopharmacology
AU  - Vitiello, Benedetto
AU  - Davies, Mark
AU  - Arnold, L Eugene
AU  - McDougle, Christopher J
AU  - Aman, Michael
AU  - McCracken, James T
AU  - Scahill, Lawrence
AU  - Tierney, Elaine
AU  - Posey, David J
AU  - Swiezy, Naomi B
AU  - Koenig, Kathleen
AD  - Division of Services and Intervention Research, National Institute of Mental Health, Bethesda, MD 20892-9633, USA. bvitiell@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 565
EP  - 569
VL  - 25
IS  - 6
SN  - 0271-0749, 0271-0749
KW  - Antipsychotic Agents
KW  - 0
KW  - Risperidone
KW  - L6UH7ZF8HC
KW  - Index Medicus
KW  - Reproducibility of Results
KW  - Humans
KW  - Treatment Outcome
KW  - Child
KW  - Adolescent
KW  - Child, Preschool
KW  - Research Personnel -- psychology
KW  - Double-Blind Method
KW  - Antipsychotic Agents -- therapeutic use
KW  - Autistic Disorder -- drug therapy
KW  - Risperidone -- adverse effects
KW  - Antipsychotic Agents -- adverse effects
KW  - Risperidone -- therapeutic use
KW  - Parents -- psychology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-28
N1  - Date created - 2005-11-11
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Specific recognition and cleavage of the plus-strand primer by reverse transcriptase.
AN  - 68794383; 16282486
AB  - Reverse transcriptases (RTs) of retroviruses and long terminal repeat (LTR)-retrotransposons possess DNA polymerase and RNase H activities. During reverse transcription these activities are necessary for the programmed sequence of events that include template switching and primer processing. Integrase then inserts the completed cDNA into the genome of the host cell. The RT of the LTR-retrotransposon Tf1 was subjected to random mutagenesis, and the resulting transposons were screened with genetic assays to test which mutations reduced reverse transcription and which inhibited integration. We identified a cluster of mutations in the RNase H domain of RT that were surprising because they blocked integration without reducing cDNA levels. The results of immunoblots demonstrated that these mutations did not reduce levels of RT or integrase. DNA blots showed that the mutations did not lower the amounts of full-length cDNA. The sequences of the 3' ends of the cDNA revealed that mutations within the cluster in RNase H specifically reduced the removal of the polypurine tract (PPT) primer from the ends of the cDNA. These results indicate that primer removal is not a necessary component of reverse transcription. The residues mutated in Tf1 RNase H are conserved in human immunodeficiency virus type 1 and make direct contact with DNA opposite the PPT. Thus, our results identify a conserved element in RT that contacts the PPT and is specifically required for PPT removal.
JF  - Journal of virology
AU  - Atwood-Moore, Angela
AU  - Ejebe, Kenechi
AU  - Levin, Henry L
AD  - Section on Eukaryotic Transposable Elements, Laboratory of Gene Regulation and Development, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 14863
EP  - 14875
VL  - 79
IS  - 23
SN  - 0022-538X, 0022-538X
KW  - DNA, Viral
KW  - 0
KW  - RNA primers
KW  - RNA
KW  - 63231-63-0
KW  - HIV Reverse Transcriptase
KW  - EC 2.7.7.49
KW  - RNA-Directed DNA Polymerase
KW  - Ribonuclease H
KW  - EC 3.1.26.4
KW  - Index Medicus
KW  - Saccharomyces cerevisiae -- genetics
KW  - HIV Long Terminal Repeat
KW  - DNA, Viral -- biosynthesis
KW  - Saccharomyces cerevisiae -- metabolism
KW  - HIV Reverse Transcriptase -- metabolism
KW  - Templates, Genetic
KW  - Substrate Specificity
KW  - RNA -- metabolism
KW  - RNA-Directed DNA Polymerase -- chemistry
KW  - RNA -- chemistry
KW  - RNA-Directed DNA Polymerase -- metabolism
KW  - Ribonuclease H -- metabolism
KW  - RNA-Directed DNA Polymerase -- genetics
KW  - RNA -- genetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-23
N1  - Date created - 2005-11-11
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
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Biochemistry. 2002 Apr 16;41(15):4856-65 [11939780]
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Int J Biochem Cell Biol. 2004 Sep;36(9):1752-66 [15183342]
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Cell. 1990 Oct 5;63(1):87-95 [2170022]
EMBO J. 1990 Oct;9(10):3353-62 [1698615]
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Methods Enzymol. 1991;194:795-823 [2005825]
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Proc Natl Acad Sci U S A. 1994 Jan 18;91(2):549-53 [7507249]
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Virology. 1994 Dec;205(2):470-8 [7975248]
Mol Cell Biol. 1995 Jun;15(6):3310-7 [7760826]
Mol Cell Biol. 1996 Jan;16(1):338-46 [8524313]
Mol Cell Biol. 1996 Oct;16(10):5645-54 [8816477]
Genes Dev. 1997 Jan 15;11(2):270-85 [9009208]
J Mol Biol. 1997 Jun 6;269(2):225-39 [9191067]
J Virol. 1998 Feb;72(2):1324-33 [9445033]
Mol Cell Biol. 1998 Feb;18(2):1094-104 [9448007]
J Virol. 1998 Aug;72(8):6490-503 [9658092]
J Virol. 1998 Nov;72(11):9318-22 [9765482]
Mol Cell Biol. 1998 Nov;18(11):6839-52 [9774697]
EMBO J. 2001 Mar 15;20(6):1449-61 [11250910]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Role of CYP2E1 in the epoxidation of acrylamide to glycidamide and formation of DNA and hemoglobin adducts.
AN  - 68794284; 16141435
AB  - Acrylamide (AA) is an animal carcinogen, neurotoxin, and reproductive toxin. AA is formed in baked and fried carbohydrate-rich foods. Metabolism of AA occurs via epoxidation to glycidamide (GA) or direct conjugation with glutathione. Using CYP2E1-null mice, recent studies in this laboratory demonstrated that induction of somatic and germ cell mutagenicity in AA-treated mice is dependent on CYP2E1. We hypothesized that AA metabolism to GA is a prerequisite for the induction of AA-induced mutagenicity. Current studies were undertaken to assess the role of CYP2E1 in the epoxidation of AA to GA and the formation of DNA and hemoglobin (HGB) adducts. AA was administered to CYP2E1-null or wild-type mice at 50 mg/kg ip. Mice were euthanized 6 h later and blood and tissues were collected. Using LC-ES/MS/MS, AA, GA, and DNA- and HGB-adducts were measured. While the plasma levels of AA and GA were 115 +/- 14.0 and 1.7 +/- 0.31 microM in CYP2E1-null mice, they were 0.84 +/- 0.80 and 33.0 +/- 6.3 microM in the plasma of AA-treated wild-type mice. Administration of AA to wild-type mice caused a large increase in N7-GA-Gua and N3-GA-Ade adducts in the liver, lung, and testes. While traces of N7-GA-Gua adducts were measured in the tissues of AA-treated CYP2E1-null mice, these levels were 52- to 66-fold lower than in wild-type mice. Significant elevation of both AA- and GA-HGB adducts was detected in AA-treated wild-type mice. In AA-treated CYP2E1-null mice, levels of AA-HGB adducts were roughly twice as high as those in wild-type mice. In conclusion, current work demonstrated that CYP2E1 is the primary enzyme responsible for the epoxidation of AA to GA, which leads to the formation of GA-DNA and HGB adducts.
JF  - Toxicological sciences : an official journal of the Society of Toxicology
AU  - Ghanayem, Burhan I
AU  - McDaniel, L Patrice
AU  - Churchwell, Mona I
AU  - Twaddle, Nathan C
AU  - Snyder, Rodney
AU  - Fennell, Timothy R
AU  - Doerge, Daniel R
AD  - Laboratory of Pharmacology and Chemistry, National Toxicology Program, NIEHS/NIH, Research Triangle Park, NC 27709, USA. ghanayem@niehs.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 311
EP  - 318
VL  - 88
IS  - 2
SN  - 1096-6080, 1096-6080
KW  - DNA Adducts
KW  - 0
KW  - Epoxy Compounds
KW  - Hemoglobins
KW  - Acrylamide
KW  - 20R035KLCI
KW  - glycidamide
KW  - 6G5ELX5XYN
KW  - DNA
KW  - 9007-49-2
KW  - Cytochrome P-450 CYP2E1
KW  - EC 1.14.13.-
KW  - Index Medicus
KW  - Animals
KW  - Liver -- enzymology
KW  - Lung -- chemistry
KW  - Mice
KW  - Liver -- chemistry
KW  - DNA -- drug effects
KW  - Mice, Knockout
KW  - Testis -- drug effects
KW  - Liver -- drug effects
KW  - Lung -- drug effects
KW  - Mice, Inbred C57BL
KW  - Testis -- enzymology
KW  - Lung -- enzymology
KW  - Testis -- chemistry
KW  - Male
KW  - Hemoglobins -- metabolism
KW  - DNA Adducts -- chemistry
KW  - Cytochrome P-450 CYP2E1 -- deficiency
KW  - Epoxy Compounds -- metabolism
KW  - Epoxy Compounds -- chemistry
KW  - Acrylamide -- metabolism
KW  - Cytochrome P-450 CYP2E1 -- metabolism
KW  - Hemoglobins -- chemistry
KW  - Cytochrome P-450 CYP2E1 -- genetics
KW  - Acrylamide -- toxicity
KW  - DNA Adducts -- metabolism
KW  - Acrylamide -- chemistry
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-10
N1  - Date created - 2005-11-10
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Chemical effects in biological systems--data dictionary (CEBS-DD): a compendium of terms for the capture and integration of biological study design description, conventional phenotypes, and 'omics data.
AN  - 68792840; 16150882
AB  - A critical component in the design of the Chemical Effects in Biological Systems (CEBS) Knowledgebase is a strategy to capture toxicogenomics study protocols and the toxicity endpoint data (clinical pathology and histopathology). A Study is generally an experiment carried out during a period of time for the purpose of obtaining data, and the Study Design Description captures the methods, timing, and organization of the Study. The CEBS Data Dictionary (CEBS-DD) has been designed to define and organize terms in an attempt to standardize nomenclature needed to describe a toxicogenomics Study in a structured yet intuitive format and provide a flexible means to describe a Study as conceptualized by the investigator. The CEBS-DD will organize and annotate information from a variety of sources, thereby facilitating the capture and display of toxicogenomics data in biological context in CEBS, i.e., associating molecular events detected in highly-parallel data with the toxicology/pathology phenotype as observed in the individual Study Subjects and linked to the experimental treatments. The CEBS-DD has been developed with a focus on acute toxicity studies, but with a design that will permit it to be extended to other areas of toxicology and biology with the addition of domain-specific terms. To illustrate the utility of the CEBS-DD, we present an example of integrating data from two proteomics and transcriptomics studies of the response to acute acetaminophen toxicity (A. N. Heinloth et al., 2004, Toxicol. Sci. 80, 193-202).
JF  - Toxicological sciences : an official journal of the Society of Toxicology
AU  - Fostel, Jennifer
AU  - Choi, Danielle
AU  - Zwickl, Craig
AU  - Morrison, Norman
AU  - Rashid, Asif
AU  - Hasan, Atif
AU  - Bao, Wenjun
AU  - Richard, Ann
AU  - Tong, Weida
AU  - Bushel, Pierre R
AU  - Brown, Roger
AU  - Bruno, Maribel
AU  - Cunningham, Michael L
AU  - Dix, David
AU  - Eastin, William
AU  - Frade, Carlos
AU  - Garcia, Alex
AU  - Heinloth, Alexandra
AU  - Irwin, Rick
AU  - Madenspacher, Jennifer
AU  - Merrick, B Alex
AU  - Papoian, Thomas
AU  - Paules, Richard
AU  - Rocca-Serra, Philippe
AU  - Sansone, Assunta-Susanna
AU  - Stevens, James
AU  - Tomer, Kenneth
AU  - Yang, Chihae
AU  - Waters, Michael
AD  - LIMT Lockheed Martin Information Technology (LMIT), Research Triangle Park, NC 27709, USA. fostel@niehs.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 585
EP  - 601
VL  - 88
IS  - 2
SN  - 1096-6080, 1096-6080
KW  - Acetaminophen
KW  - 362O9ITL9D
KW  - Index Medicus
KW  - Administration, Oral
KW  - Animals
KW  - Dose-Response Relationship, Drug
KW  - Proteomics
KW  - Toxicity Tests
KW  - Toxicogenetics
KW  - Acetaminophen -- toxicity
KW  - Biomedical Research
KW  - Systems Biology -- methods
KW  - Databases, Factual
KW  - Terminology as Topic
KW  - Research Design
KW  - Database Management Systems
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Toxicological+sciences+%3A+an+official+journal+of+the+Society+of+Toxicology&rft.atitle=Chemical+effects+in+biological+systems--data+dictionary+%28CEBS-DD%29%3A+a+compendium+of+terms+for+the+capture+and+integration+of+biological+study+design+description%2C+conventional+phenotypes%2C+and+%27omics+data.&rft.au=Fostel%2C+Jennifer%3BChoi%2C+Danielle%3BZwickl%2C+Craig%3BMorrison%2C+Norman%3BRashid%2C+Asif%3BHasan%2C+Atif%3BBao%2C+Wenjun%3BRichard%2C+Ann%3BTong%2C+Weida%3BBushel%2C+Pierre+R%3BBrown%2C+Roger%3BBruno%2C+Maribel%3BCunningham%2C+Michael+L%3BDix%2C+David%3BEastin%2C+William%3BFrade%2C+Carlos%3BGarcia%2C+Alex%3BHeinloth%2C+Alexandra%3BIrwin%2C+Rick%3BMadenspacher%2C+Jennifer%3BMerrick%2C+B+Alex%3BPapoian%2C+Thomas%3BPaules%2C+Richard%3BRocca-Serra%2C+Philippe%3BSansone%2C+Assunta-Susanna%3BStevens%2C+James%3BTomer%2C+Kenneth%3BYang%2C+Chihae%3BWaters%2C+Michael&rft.aulast=Fostel&rft.aufirst=Jennifer&rft.date=2005-12-01&rft.volume=88&rft.issue=2&rft.spage=585&rft.isbn=&rft.btitle=&rft.title=Toxicological+sciences+%3A+an+official+journal+of+the+Society+of+Toxicology&rft.issn=10966080&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-10
N1  - Date created - 2005-11-10
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Research strategies for safety evaluation of nanomaterials, Part III: nanoscale technologies for assessing risk and improving public health.
AN  - 68787783; 16162851
AB  - Risk assessment in the environmental health sciences focuses on understanding the nature of environmental exposures and the potential harm posed by those exposures which in turn is determined by the perturbation of biological pathways and the individual's susceptibility to damage. While there are extensive research efforts ongoing in these areas, progress in each is currently slowed by technological limitations including comprehensive assessment of multiple exposures in real time and dynamic assessment of biological response with high temporal and quantitative resolution. This Forum article discusses recent technological innovations capitalizing on the emergent properties of nanoscale materials and their potential adaptation to improving individual exposure assessment, determination of biological response, and environmental remediation. The ultimate goal is to raise the environmental health science community's awareness of these possibilities and encourage the development of improved strategies for assessing risk and improving public health.
JF  - Toxicological sciences : an official journal of the Society of Toxicology
AU  - Balshaw, David M
AU  - Philbert, Martin
AU  - Suk, William A
AD  - Center for Risk and Integrated Sciences, National Institute of Environmental Health Sciences, National Institutes of Health, US Department of Health and Human Services, Research Triangle Park, NC 27709, USA. Balshaw@niehs.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 298
EP  - 306
VL  - 88
IS  - 2
SN  - 1096-6080, 1096-6080
KW  - Environmental Pollutants
KW  - 0
KW  - Index Medicus
KW  - Biomedical Research
KW  - Humans
KW  - Public Health
KW  - Environmental Pollutants -- toxicity
KW  - Risk Assessment -- methods
KW  - Environmental Monitoring -- methods
KW  - Environmental Health -- methods
KW  - Nanotechnology
KW  - Environmental Monitoring -- instrumentation
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-10
N1  - Date created - 2005-11-10
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Telomeres, telomerase and oral cancer (Review).
AN  - 68772503; 16273215
AB  - Oral squamous cell carcinoma (oral cancer) and many squamous cell carcinomas of the head and neck arise as a consequence of multiple molecular events induced by the effects of various carcinogens related to tobacco use, environmental factors, and viruses in some instances (e.g., mucosal oncogenic human papillomaviruses), against a background of inheritable resistance or susceptibility. Consequent genetic damage affects many chromosomes and genes, and it is the accumulation of these changes that appears to lead to carcinoma. Telomere maintenance by telomerase or, in its absence, alternative lengthening of telomeres protect this acquired altered genetic information ensuring immortality without losing eukaryotic linear DNA; when this does not occur DNA is lost and end-replication problems arise. Telomerase is reactivated in 80-90% of cancers thus attracting the attention of pathologists and clinicians who have explored its use as a target for anticancer therapy and to develop better diagnostic and prognostic markers. In the last few years, valuable research from various laboratories has provided major insights into telomerase and telomeres leading to their use as diagnostic and prognostic markers in several types of cancer. Moreover, many strategies have emerged which inhibit this complex enzyme for anticancer therapy and are one step ahead of clinical trials. This review explains the basic biology and the clinical implications of telomerase-based diagnosis and prognosis, the prospects for its use in anticancer therapy, and the limitations it presents in the context of oral cancer.
JF  - International journal of oncology
AU  - Sebastian, Sinto
AU  - Grammatica, Luciano
AU  - Paradiso, Angelo
AD  - Clinical Experimental Oncology Laboratory, Surgery Department, National Cancer Institute, 70126 Bari, Italy.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1583
EP  - 1596
VL  - 27
IS  - 6
SN  - 1019-6439, 1019-6439
KW  - Telomerase
KW  - EC 2.7.7.49
KW  - Index Medicus
KW  - Humans
KW  - Prognosis
KW  - Models, Biological
KW  - Mouth Neoplasms -- therapy
KW  - Telomere -- genetics
KW  - Mouth Neoplasms -- enzymology
KW  - Telomerase -- metabolism
KW  - Mouth Neoplasms -- genetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2005-11-07
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Thoracic radiation therapy and concomitant low-dose daily paclitaxel in non-small cell lung cancer: a phase I study.
AN  - 68770255; 16273271
AB  - The primary objective of the current study was to determine the maximum tolerated dose of paclitaxel (PTX) that could be added daily to radiation therapy (RT) in patients with non-small cell lung cancer (NSCLC). The secondary objective was to achieve a plasma concentration of PTX estimated to exert a radiosensitizing effect. Eighteen patients with locally advanced NSCLC were treated. 60 Gy of RT were given in 2 Gy fractions, 5 days per week. A daily dose of PTX was delivered by 4-h i.v. infusion before RT. The initial dose level of PTX was 9 mg/m2/day, escalated by 1 mg at each additional patient triplet. Two out of 6 patients experienced acute dose limiting toxicity (DLT) at the 12 mg/m2/day PTX dose level. PTX continuously greater than 10 nM, the estimated radiosensitizing condition, was achieved at the PTX dose level of 12 mg/m2/day. PTX at doses up to 11 mg/m2/day may be safely added to a conventional conformal RT course. Both DLT and the estimated radiosensitizing plasma exposure to PTX were encountered at the 12 mg/m(2)/day dose level.
JF  - Oncology reports
AU  - Gobitti, Carlo
AU  - Franchin, Giovanni
AU  - Minatel, Emilio
AU  - Gigante, Marco
AU  - Basso, Barbara
AU  - Bujor, Laurentiu
AU  - Trovò, Mauro G
AD  - Radiation Oncology Department, Centro di Riferimento Oncologico, National Cancer Institute, 33081 Aviano, Italy. cgobitti@cro.it
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1647
EP  - 1653
VL  - 14
IS  - 6
SN  - 1021-335X, 1021-335X
KW  - Antineoplastic Agents, Phytogenic
KW  - 0
KW  - Paclitaxel
KW  - P88XT4IS4D
KW  - Index Medicus
KW  - Area Under Curve
KW  - Infusions, Intravenous
KW  - Combined Modality Therapy
KW  - Dose-Response Relationship, Drug
KW  - Humans
KW  - Antineoplastic Agents, Phytogenic -- blood
KW  - Aged
KW  - Chromatography, High Pressure Liquid
KW  - Radiotherapy Dosage
KW  - Antineoplastic Agents, Phytogenic -- therapeutic use
KW  - Treatment Outcome
KW  - Middle Aged
KW  - Antineoplastic Agents, Phytogenic -- administration & dosage
KW  - Female
KW  - Male
KW  - Survival Analysis
KW  - Paclitaxel -- administration & dosage
KW  - Lung Neoplasms -- radiotherapy
KW  - Paclitaxel -- pharmacokinetics
KW  - Lung Neoplasms -- drug therapy
KW  - Paclitaxel -- therapeutic use
KW  - Carcinoma, Non-Small-Cell Lung -- drug therapy
KW  - Lung Neoplasms -- pathology
KW  - Carcinoma, Non-Small-Cell Lung -- radiotherapy
KW  - Carcinoma, Non-Small-Cell Lung -- pathology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68770255?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Oncology+reports&rft.atitle=Thoracic+radiation+therapy+and+concomitant+low-dose+daily+paclitaxel+in+non-small+cell+lung+cancer%3A+a+phase+I+study.&rft.au=Gobitti%2C+Carlo%3BFranchin%2C+Giovanni%3BMinatel%2C+Emilio%3BGigante%2C+Marco%3BBasso%2C+Barbara%3BBujor%2C+Laurentiu%3BTrov%C3%B2%2C+Mauro+G&rft.aulast=Gobitti&rft.aufirst=Carlo&rft.date=2005-12-01&rft.volume=14&rft.issue=6&rft.spage=1647&rft.isbn=&rft.btitle=&rft.title=Oncology+reports&rft.issn=1021335X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-09
N1  - Date created - 2005-11-07
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Nitric oxide regulates prolidase activity by serine/threonine phosphorylation.
AN  - 68766098; 16167338
AB  - Prolidase [E.C. 3.4.13.9], a member of the matrix metalloproteinase (MMP) family, is a manganese-dependent cytosolic exopeptidase that cleaves imidodipeptides containing C-terminal proline or hydroxyproline. It plays an important role in collagen metabolism, matrix remodeling and cell growth. Nitric oxide (NO), a versatile signaling molecule, regulates many processes including collagen synthesis and matrix remodeling and, thereby, may modulate angiogenesis, tumor invasiveness, and metastasis. Thus, we considered that prolidase may be an important target of NO regulation. In our study, SIN I and DETA/NO were used as NO donors. Both donors increased prolidase activity in a time-dependent and dose-dependent manner. Prolidase activity increased not only with NO donors but also with endogenous NO in cells transfected with iNOS. The effect of iNOS was abolished by treatment with S-methylisothiourea (SMT), a selective inhibitor of iNOS. However, with either exogenous or endogenous sources of NO, the increase in prolidase activity was not accompanied by increased prolidase expression. Therefore, we suspected phosphorylation of prolidase as a potential mechanism regulating enzyme activation. We observed increased serine/threonine phosphorylation on prolidase protein in cells treated with NO donors and in cells transfected with iNOS. To determinate the pathways that may mediate prolidase induction by NO, we first used 8-Br-cGMP, a cGMP agonist, and found that 8-Br-cGMP strongly and rapidly stimulated prolidase activity accompanied by increased phosphorylation. Rp-8-Br-pCPT-cGMP, an inhibitor of cGMP, reduced NO donor-stimulated prolidase activity to control levels. To test whether the MAPK pathway is involved in this NO-dependent activation, we used an ERK1/2 inhibitor and found that it had no effect on prolidase activity increased by NO donors. These results demonstrate that NO stimulates prolidase activity by increasing serine/threonine phosphorylation through PKG-cGMP pathway, but independent of MAPK and suggest an interaction between inflammatory signaling pathways and regulation of the terminal step of matrix degradation.
          2005 Wiley-Liss, Inc.
JF  - Journal of cellular biochemistry
AU  - Surazynski, Arkadiusz
AU  - Liu, Yongmin
AU  - Miltyk, Wojciech
AU  - Phang, James M
AD  - Metabolism and Cancer Susceptibility Section, Laboratory of Comparative Carcinogenesis, National Cancer Institute at Frederick, Frederick, Maryland 21702, USA.
Y1  - 2005/12/01/
PY  - 2005
DA  - 2005 Dec 01
SP  - 1086
EP  - 1094
VL  - 96
IS  - 5
SN  - 0730-2312, 0730-2312
KW  - DNA, Complementary
KW  - 0
KW  - Peptides
KW  - Threonine
KW  - 2ZD004190S
KW  - Nitric Oxide
KW  - 31C4KY9ESH
KW  - Serine
KW  - 452VLY9402
KW  - Nitric Oxide Synthase Type II
KW  - EC 1.14.13.39
KW  - Mitogen-Activated Protein Kinase 1
KW  - EC 2.7.11.24
KW  - Mitogen-Activated Protein Kinase 3
KW  - Dipeptidases
KW  - EC 3.4.13.-
KW  - proline dipeptidase
KW  - EC 3.4.13.9
KW  - Matrix Metalloproteinases
KW  - EC 3.4.24.-
KW  - Thiourea
KW  - GYV9AM2QAG
KW  - Cyclic GMP
KW  - H2D2X058MU
KW  - Index Medicus
KW  - Animals
KW  - Plasmids -- metabolism
KW  - Dose-Response Relationship, Drug
KW  - Wound Healing
KW  - Immunoprecipitation
KW  - Mice
KW  - NIH 3T3 Cells
KW  - Inflammation
KW  - Mitogen-Activated Protein Kinase 3 -- metabolism
KW  - Blotting, Western
KW  - Cyclic GMP -- metabolism
KW  - Phosphorylation
KW  - Transfection
KW  - Matrix Metalloproteinases -- chemistry
KW  - DNA, Complementary -- metabolism
KW  - Mitogen-Activated Protein Kinase 1 -- metabolism
KW  - Peptides -- chemistry
KW  - Nitric Oxide Synthase Type II -- metabolism
KW  - Neovascularization, Pathologic
KW  - Thiourea -- chemistry
KW  - Time Factors
KW  - Signal Transduction
KW  - Dipeptidases -- biosynthesis
KW  - Threonine -- chemistry
KW  - Gene Expression Regulation, Enzymologic
KW  - Nitric Oxide -- metabolism
KW  - Dipeptidases -- chemistry
KW  - Serine -- chemistry
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=9th+International+Workshop+on+Langerhans+Cells+%28LC+2005%29&rft.atitle=Induction+of+a+Graft-Versus-Host-Like+Skin+Disease+by+Intradermal+Injection+of+Ovalbumin-Peptide-Specific+CD8%2B+%28OT-I%29+T+Cells+into+Keratin+14-Ovalbumin-Expressing+Transgenic+Mice&rft.au=Kim%2C+B+S%3BMiyagawa%2C+F%3BKatz%2C+S+I&rft.aulast=Kim&rft.aufirst=B&rft.date=2005-09-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=9th+International+Workshop+on+Langerhans+Cells+%28LC+2005%29&rft.issn=&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-20
N1  - Date created - 2005-11-03
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Preclinical toxicity of a geldanamycin analog, 17-(dimethylaminoethylamino)-17-demethoxygeldanamycin (17-DMAG), in rats and dogs: potential clinical relevance.
AN  - 68658649; 15986212
AB  - 17-DMAG is a hydrophilic derivative of the molecular chaperone inhibitor 17-(allylamino)-17-demethoxygeldanamycin (17-AAG; NSC-330507), which is currently being evaluated for the treatment of cancer in clinical trials. 17-DMAG offers a potential advantage over 17-AAG because its aqueous solubility eliminates the need for complicated formulations that are currently used for administration of 17-AAG. In addition, 17-DMAG undergoes only limited metabolism compared to 17-AAG. The present results are from preclinical toxicity studies evaluating 17-DMAG in rats and dogs.
          Doses of 0, 2.4, 12 and 24 mg/m2 per day were administered to rats, while dogs received doses of 0, 8 or 16 mg/m2 per day. In both species, 17-DMAG was administered i.v. (slow bolus for rats; 1-h infusion for dogs) daily for 5 days. An additional cohort of dogs received 16 mg/m2 per day orally for 5 days. Clinical observations were noted, and standard hematology and clinical chemistry parameters were monitored. Selected tissues were evaluated microscopically for drug-related lesions. Tissue and plasma 17-DMAG concentrations were measured by HPLC/MS at selected time-points on days 1 and 5. Daily i.v. administration of 17-DMAG at doses of 24 mg/m2 per day in rats or 16 mg/m2 per day in dogs produced lethality on day 6, approximately 24 h following the last dose. Body weight loss was common in rats and dogs. Drug-related gastrointestinal, bone marrow and hepatic toxicities were also common in rats and dogs. Dogs also exhibited signs of renal and gallbladder toxicity. Plasma concentrations of 17-DMAG increased proportionately with dose in rats and disproportionately with dose in dogs. In rat tissues, however, only fourfold to sixfold increases in 17-DMAG concentrations were observed with a tenfold increase in dose. The highest concentrations of 17-DMAG were found in the liver of rats, with progressively lower concentrations in the spleen, lung, kidney and plasma. Regardless of the route of administration, higher drug concentrations were present in plasma (rat and dog) and tissue (rat) samples obtained on day 5 compared to those obtained on day 1. Although plasma concentrations decreased with time, 17-DMAG was still detected in dog plasma for at least 24 h after drug administration.
          With the recent approval of 17-DMAG for clinical use, the data generated from these preclinical studies will provide guidance to clinicians as they administer this drug to their patients. The MTD of 17-DMAG was 12 mg/m2 per day in rats and 8 mg/m2 per day in dogs; therefore, the recommended starting dose for phase I trial is 1.3 mg/m2 per day for 5 days. Gastrointestinal and bone marrow toxicity were dose-limiting in rats, and gastrointestinal, renal, gallbladder and bone marrow toxicity were dose-limiting in dogs. All adverse effects were fully reversible in surviving animals after treatment was complete.
JF  - Cancer chemotherapy and pharmacology
AU  - Glaze, Elizabeth R
AU  - Lambert, Amy L
AU  - Smith, Adaline C
AU  - Page, John G
AU  - Johnson, William D
AU  - McCormick, David L
AU  - Brown, Alan P
AU  - Levine, Barry S
AU  - Covey, Joseph M
AU  - Egorin, Merrill J
AU  - Eiseman, Julie L
AU  - Holleran, Julianne L
AU  - Sausville, Edward A
AU  - Tomaszewski, Joseph E
AD  - Toxicology and Pharmacology Branch, Developmental Therapeutics Program, Division of Cancer Treatment and Diagnosis, National Cancer Institute, Executive Plaza North, Room 8040, Rockville, MD 20852, USA. glazee@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 637
EP  - 647
VL  - 56
IS  - 6
SN  - 0344-5704, 0344-5704
KW  - Antibiotics, Antineoplastic
KW  - 0
KW  - Benzoquinones
KW  - Lactams, Macrocyclic
KW  - Quinones
KW  - 17-(dimethylaminoethylamino)-17-demethoxygeldanamycin
KW  - 001L2FE0M3
KW  - geldanamycin
KW  - Z3K3VJ16KU
KW  - Index Medicus
KW  - Animals
KW  - Recovery of Function
KW  - Rats
KW  - Rats, Inbred F344
KW  - Gastrointestinal Tract -- drug effects
KW  - Clinical Chemistry Tests
KW  - Bone Marrow -- drug effects
KW  - Male
KW  - Administration, Oral
KW  - Bone Marrow -- pathology
KW  - Kidney -- pathology
KW  - Infusions, Intravenous
KW  - Injections, Intravenous
KW  - Dose-Response Relationship, Drug
KW  - Longevity -- drug effects
KW  - Kidney -- drug effects
KW  - Gallbladder -- drug effects
KW  - Hematologic Tests
KW  - Gastrointestinal Tract -- pathology
KW  - Body Weight -- drug effects
KW  - Toxicity Tests
KW  - Dogs
KW  - Species Specificity
KW  - Gallbladder -- pathology
KW  - Female
KW  - Quinones -- pharmacokinetics
KW  - Quinones -- toxicity
KW  - Antibiotics, Antineoplastic -- pharmacokinetics
KW  - Antibiotics, Antineoplastic -- toxicity
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cancer+chemotherapy+and+pharmacology&rft.atitle=Preclinical+toxicity+of+a+geldanamycin+analog%2C+17-%28dimethylaminoethylamino%29-17-demethoxygeldanamycin+%2817-DMAG%29%2C+in+rats+and+dogs%3A+potential+clinical+relevance.&rft.au=Glaze%2C+Elizabeth+R%3BLambert%2C+Amy+L%3BSmith%2C+Adaline+C%3BPage%2C+John+G%3BJohnson%2C+William+D%3BMcCormick%2C+David+L%3BBrown%2C+Alan+P%3BLevine%2C+Barry+S%3BCovey%2C+Joseph+M%3BEgorin%2C+Merrill+J%3BEiseman%2C+Julie+L%3BHolleran%2C+Julianne+L%3BSausville%2C+Edward+A%3BTomaszewski%2C+Joseph+E&rft.aulast=Glaze&rft.aufirst=Elizabeth&rft.date=2005-12-01&rft.volume=56&rft.issue=6&rft.spage=637&rft.isbn=&rft.btitle=&rft.title=Cancer+chemotherapy+and+pharmacology&rft.issn=03445704&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-05
N1  - Date created - 2005-10-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Homozygous germ line mutation in exon 27 of murine Brca2 disrupts the Fancd2-Brca2 pathway in the homologous recombination-mediated DNA interstrand cross-links' repair but does not affect meiosis.
AN  - 68642130; 16127665
AB  - The role of the region encoded by exon 27 of the Brca2 gene in DNA repair was studied in cells and tissues from Brca2Delta27/Delta27 mice. The COOH-terminal truncated Brca2 localized to the nucleus in primary mouse embryo fibroblasts from Brca2Delta27/Delta27 mice. Fluorescence-activated cell sorting (FACS) analysis demonstrated that these fibroblasts were hypersensitive to mitomycin C-induced cross-links, but not to double-strand breaks (DSBs) induced by irradiation. The gammaH2AX appearance kinetics and comet assay showed that DSBs were repaired through non-homologous end joining pathways, while interstrand cross-links were not repaired due to deficient homologous recombination pathways. Immunoprecipitation experiments showed that Fancd2 did not coprecipitate with the mutated Brca2. There were also no detectable Rad51-positive foci formed in these cells after damage. On the other hand, we did not find any difference during gametogenesis in mice harboring exon 27 truncating mutation of the Brca2 gene and control mice, and in both cases, Rad51 localized to the recombination foci. Our results suggest that exon 27 of murine Brca2 is crucial for the interaction of Brca2 and Fancd2 in Rad51-mediated recombination in response to DNA damage, but that this interaction is not taking place in the homologous recombination during meiosis.
          Published 2005 Wiley-Liss, Inc.
JF  - Genes, chromosomes & cancer
AU  - Atanassov, Boyko S
AU  - Barrett, J Carl
AU  - Davis, Barbara J
AD  - Laboratory of Women's Health, National Institute of Environmental Health Sciences, NIH, Research Triangle Park, NC, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 429
EP  - 437
VL  - 44
IS  - 4
SN  - 1045-2257, 1045-2257
KW  - BRCA2 Protein
KW  - 0
KW  - Fanconi Anemia Complementation Group D2 Protein
KW  - Histones
KW  - gamma-H2AX protein, mouse
KW  - Mitomycin
KW  - 50SG953SK6
KW  - Rad51 Recombinase
KW  - EC 2.7.7.-
KW  - Rad51 protein, mouse
KW  - Index Medicus
KW  - Animals
KW  - Comet Assay
KW  - Fibroblasts -- drug effects
KW  - Cell Nucleus -- metabolism
KW  - Exons
KW  - Fluorescent Antibody Technique, Indirect
KW  - Mitomycin -- pharmacology
KW  - Mice
KW  - Rad51 Recombinase -- metabolism
KW  - Blotting, Western
KW  - Cells, Cultured
KW  - Kinetics
KW  - Histones -- metabolism
KW  - Fibroblasts -- radiation effects
KW  - Flow Cytometry
KW  - Embryo, Mammalian
KW  - Female
KW  - Radiation, Ionizing
KW  - DNA Repair
KW  - BRCA2 Protein -- chemistry
KW  - Meiosis
KW  - Recombination, Genetic
KW  - Fanconi Anemia Complementation Group D2 Protein -- metabolism
KW  - BRCA2 Protein -- metabolism
KW  - Germ-Line Mutation
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68642130?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Genes%2C+chromosomes+%26+cancer&rft.atitle=Homozygous+germ+line+mutation+in+exon+27+of+murine+Brca2+disrupts+the+Fancd2-Brca2+pathway+in+the+homologous+recombination-mediated+DNA+interstrand+cross-links%27+repair+but+does+not+affect+meiosis.&rft.au=Atanassov%2C+Boyko+S%3BBarrett%2C+J+Carl%3BDavis%2C+Barbara+J&rft.aulast=Atanassov&rft.aufirst=Boyko&rft.date=2005-12-01&rft.volume=44&rft.issue=4&rft.spage=429&rft.isbn=&rft.btitle=&rft.title=Genes%2C+chromosomes+%26+cancer&rft.issn=10452257&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-06
N1  - Date created - 2005-10-03
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Modulation of cytochrome P450 enzymes by organosulfur compounds from garlic.
AN  - 68622945; 16000231
AB  - Organosulfur compounds (OSCs) derived from garlic have been studied for the ability to inhibit experimental cancer in various animal models, primarily through modification of carcinogen detoxification enzymes, such as cytochrome P450 (CYP) enzymes. OSCs vary in structural and physical properties, and a detailed analysis of these properties has not been performed with respect to their ability of inhibit chemically-induced colon cancer development. Gastric intubation of rats with a single dose of 200 mg/kg diallyl sulfide (DAS), diallyl disulfide (DADS), and allyl methyl sulfide (AMS) decreased hepatic CYP2E1 protein by 45%, 25% and 47%, respectively, and this inhibition was sustained after 1, 4 and 8 weeks of treatment by these compounds. Dipropyl sulfide (DPS), dipropyl disulfide (DPDS), propyl methyl sulfide (PMS) and S-allylcysteine (SAC) did not inhibit hepatic CYP2E1 protein expression, nor did any of the OSCs affect CYP2E1 mRNA levels. A single dose of 200 mg/kg DAS and AMS increased hepatic CYP1A2 protein (but not mRNA) by 282% and 70%, and DAS increased CYP1A1 protein levels by 684%. Daily treatment for 1, 4 and 8 weeks with 200 mg/kg DAS and AMS resulted in time-dependent increases in hepatic CYP1A1 and CYP1A2 protein levels to a maximum of 600% and 50% for DAS, and 1600% and 240% for AMS after 8 weeks. Dosing with 200 mg/kg of each of the OSCs used in this study increased hepatic CYP3A2 protein levels at all time points. Dosing for 8 weeks with 200 mg/kg DAS, but not AMS or lower doses of DAS, induced bile duct obstruction and focal areas of necrosis. These results indicate that OSCs present in garlic, including DAS and AMS, may be beneficial in inhibiting chemically-induced colon cancer, but that longer dosing with higher concentrations of DAS may elicit minor hepatic toxicity.
JF  - Food and chemical toxicology : an international journal published for the British Industrial Biological Research Association
AU  - Davenport, Destiny M
AU  - Wargovich, Michael J
AD  - Department of Pathology and Microbiology, University of South Carolina, School of Medicine and South Carolina Cancer Center, Columbia, SC 29208, USA. matthew2@niehs.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1753
EP  - 1762
VL  - 43
IS  - 12
SN  - 0278-6915, 0278-6915
KW  - Allyl Compounds
KW  - 0
KW  - Anticarcinogenic Agents
KW  - Disulfides
KW  - Sulfides
KW  - Sulfur Compounds
KW  - diallyl disulfide
KW  - 5HI47O6OA7
KW  - allyl sulfide
KW  - 60G7CF7CWZ
KW  - Cytochrome P-450 Enzyme System
KW  - 9035-51-2
KW  - Cytochrome P-450 CYP2E1
KW  - EC 1.14.13.-
KW  - Cytochrome P-450 CYP1A1
KW  - EC 1.14.14.1
KW  - Cytochrome P-450 CYP1A2
KW  - allyl methyl sulfide
KW  - V7QI1R316C
KW  - Index Medicus
KW  - Animals
KW  - Random Allocation
KW  - Dose-Response Relationship, Drug
KW  - Disulfides -- pharmacology
KW  - Cytochrome P-450 CYP1A2 -- metabolism
KW  - Allyl Compounds -- pharmacology
KW  - Cytochrome P-450 CYP1A1 -- metabolism
KW  - Cytochrome P-450 CYP2E1 -- metabolism
KW  - Allyl Compounds -- toxicity
KW  - Rats
KW  - Cytochrome P-450 CYP1A2 -- drug effects
KW  - Rats, Inbred F344
KW  - Carcinogenicity Tests
KW  - Sulfides -- toxicity
KW  - Time Factors
KW  - Sulfides -- pharmacology
KW  - Cytochrome P-450 CYP2E1 -- drug effects
KW  - Male
KW  - Disulfides -- toxicity
KW  - Cytochrome P-450 CYP1A1 -- drug effects
KW  - Anticarcinogenic Agents -- toxicity
KW  - Liver -- pathology
KW  - Liver -- enzymology
KW  - Sulfur Compounds -- toxicity
KW  - Sulfur Compounds -- pharmacology
KW  - Liver -- drug effects
KW  - Anticarcinogenic Agents -- pharmacology
KW  - Cytochrome P-450 Enzyme System -- metabolism
KW  - Cytochrome P-450 Enzyme System -- drug effects
KW  - Garlic -- chemistry
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-29
N1  - Date created - 2005-09-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Signal transduction during environmental stress: InsP8 operates within highly restricted contexts.
AN  - 68572328; 15936174
AB  - Genetic manipulation of diphosphoinositol polyphosphate synthesis impacts many biological processes (reviewed in S.B. Shears, Biochem. J. 377, 2004, 265-280). These observations lacked a cell-signalling context, until the recent discovery that bis-diphosphoinositol tetrakisphosphate ([PP]2-InsP4 or "InsP8") accumulates rapidly in mammalian cells in response to hyperosmotic stress (X. Pesesse, K. Choi, T. Zhang, and S. B. Shears J. Biol. Chem. 279, 2004, 43378-43381). We now investigate how widely applicable is this new stress-response. [PP]2-InsP4 did not respond to mechanical strain or oxidative stress in mammalian cells. Furthermore, despite tight conservation of many molecular stress responses across the phylogenetic spectrum, we show that cellular [PP]2-InsP4 levels do not respond significantly to osmotic imbalance, heat stress and salt toxicity in Saccharomyces cerevisiae. In contrast, we show that [PP]2-InsP4 is a novel sensor of mild thermal stress in mammalian cells: [PP]2-InsP4 levels increased 3-4 fold when cells were cooled from 37 to 33 degrees C, or heated to 42 degrees C. Increases in [PP]2-InsP4 levels following heat-shock were evident <5 min, and reversible (t(1/2)=7 min) once cells were returned to 37 degrees C. These responses were blocked by pharmacological inhibition of the ERK/MEK pathway. Additional control processes may lie upstream of [PP]2-InsP4 synthesis, which was synergistically activated when heat stress and osmotic stress were combined. Our data add to the repertoire of signaling responses following thermal challenges, a topic of current interest for its possible therapeutic value.
JF  - Cellular signalling
AU  - Choi, Kuicheon
AU  - Mollapour, Elahe
AU  - Shears, Stephen B
AD  - Inositide Signaling Group, National Institute of Environmental Health Sciences, NIH, DHHS, Research Triangle Park, PO Box 12233, NC 27709, USA.
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 1533
EP  - 1541
VL  - 17
IS  - 12
SN  - 0898-6568, 0898-6568
KW  - Saccharomyces cerevisiae Proteins
KW  - 0
KW  - p38 Mitogen-Activated Protein Kinases
KW  - EC 2.7.11.24
KW  - MAP Kinase Kinase Kinases
KW  - EC 2.7.11.25
KW  - Phosphotransferases (Phosphate Group Acceptor)
KW  - EC 2.7.4.-
KW  - KCS1 protein, S cerevisiae
KW  - EC 2.7.4.21
KW  - Acid Anhydride Hydrolases
KW  - EC 3.6.-
KW  - diphosphoinositol polyphosphate phosphohydrolase
KW  - EC 3.6.1.-
KW  - Index Medicus
KW  - Saccharomyces cerevisiae Proteins -- metabolism
KW  - Animals
KW  - Osmotic Pressure
KW  - Saccharomyces cerevisiae Proteins -- genetics
KW  - Heat-Shock Response
KW  - Humans
KW  - Saccharomyces cerevisiae -- enzymology
KW  - Myocytes, Smooth Muscle -- metabolism
KW  - p38 Mitogen-Activated Protein Kinases -- metabolism
KW  - Saccharomyces cerevisiae -- genetics
KW  - MAP Kinase Kinase Kinases -- metabolism
KW  - MAP Kinase Kinase Kinases -- antagonists & inhibitors
KW  - p38 Mitogen-Activated Protein Kinases -- antagonists & inhibitors
KW  - Stress, Mechanical
KW  - Oxidative Stress
KW  - Phosphotransferases (Phosphate Group Acceptor) -- metabolism
KW  - Keratinocytes -- metabolism
KW  - Phosphotransferases (Phosphate Group Acceptor) -- genetics
KW  - Cell Line
KW  - Cricetinae
KW  - MAP Kinase Signaling System
KW  - Acid Anhydride Hydrolases -- metabolism
KW  - Signal Transduction
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-10-04
N1  - Date created - 2005-09-12
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The Relationships between Childhood Sexual Abuse, Social Anxiety, and Symptoms of Posttraumatic Stress Disorder in Women
AN  - 60002281; 200614125
AB  - The relationships between childhood sexual abuse, social anxiety, & symptoms of posttraumatic stress disorder were examined in a sample of 313 undergraduate women. Thirty-one percent of the women reported some form of sexual abuse in childhood. Women with a history of sexual abuse reported more symptoms of anxiety, distress in social situations, & posttraumatic stress disorder than other women. Women who experienced attempted or actual intercourse reported more avoidance than women with no history of abuse & women with exposure only, & more PTSD symptoms than all other groups of women. Women who experienced fondling reported more PTSD symptoms than women with no history of abuse. Pressure, age of onset of abuse, abuse by a family friend, & abuse by other perpetrators were all significant abuse characteristics in predicting adult social anxiety. Implications of these results for research & interventions are discussed. Tables, References. Adapted from the source document.
JF  - Journal of Family Violence
AU  - Feerick, Margaret M
AU  - Snow, Kyle L
AD  - National Instit Child Health & Human Development, National Instit Health, Bethesda, MD feerickm@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 409
EP  - 419
PB  - Springer Science+Business Media, Inc, New York, NY
VL  - 20
IS  - 6
SN  - 0885-7482, 0885-7482
KW  - childhood sexual abuse
KW  - long-term effects
KW  - social anxiety
KW  - PTSD
KW  - Symptoms
KW  - Anxiety
KW  - Females
KW  - Posttraumatic Stress Disorder
KW  - Child Sexual Abuse
KW  - article
KW  - 2190: social problems and social welfare; victimology (rape, family violence, & child abuse)
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Asocabs&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Family+Violence&rft.atitle=The+Relationships+between+Childhood+Sexual+Abuse%2C+Social+Anxiety%2C+and+Symptoms+of+Posttraumatic+Stress+Disorder+in+Women&rft.au=Feerick%2C+Margaret+M%3BSnow%2C+Kyle+L&rft.aulast=Feerick&rft.aufirst=Margaret&rft.date=2005-12-01&rft.volume=20&rft.issue=6&rft.spage=409&rft.isbn=&rft.btitle=&rft.title=Journal+of+Family+Violence&rft.issn=08857482&rft_id=info:doi/10.1007%2Fs10896-005-7802-z
LA  - English
DB  - Sociological Abstracts
N1  - Date revised - 2007-04-01
N1  - Number of references - 81
N1  - Last updated - 2016-09-28
N1  - CODEN - JFVIEV
N1  - SubjectsTermNotLitGenreText - Females; Child Sexual Abuse; Anxiety; Posttraumatic Stress Disorder; Symptoms
DO  - http://dx.doi.org/10.1007/s10896-005-7802-z
ER  - 



TY  - JOUR
T1  - Physician Migration: Views from Professionals in Colombia, Nigeria, India, Pakistan and the Philippines
AN  - 57185034; 200610160
AB  - There has been much debate recently about several issues related to the migration of physicians from developing to developed countries. However, few studies have been conducted to address these issues in a systematic fashion. In an attempt to begin the process of generating systematic data, we designed & distributed a questionnaire addressing several core issues surrounding physician migration to respondents selected on the basis of their special expertise or experience in India, Nigeria, Pakistan, Colombia, & the Philippines. The issues addressed relate to the reasons physicians migrate to developed countries, how migration is related to the structure of medical education, the effect that migration has on the health care infrastructure of developing countries, & various policy options for dealing with physician migration. Though responses varied somewhat by country, a desire for increased income, greater access to enhanced technology, an atmosphere of general security & stability, & improved prospects for one's children were the primary motivating factors for physician migration. A majority of respondents believed that physicians in developing counties are provided with highly specialized skills that they can better utilize in developed countries, but respondents were ambivalent with respect to the utility of educational reform. Responses varied significantly by country with regard to whether physician migration results in physician shortages, but there was widespread agreement that it exacerbates shortages in rural & public settings. With respect to policy options, increasing physician income, improving working conditions, requiring physicians to work in their home countries for a period following graduation from medical school, & creating increased collaboration between health ministries in developed & developing countries found the most favor with respondents. 4 Tables, 27 References. [Copyright 2005 Elsevier Ltd.]
JF  - Social Science & Medicine
AU  - Astor, Avraham
AU  - Akhtar, Tasleem
AU  - Matallana, Maria Alexandra
AU  - Muthuswamy, Vasantha
AU  - Olowu, Folarin A
AU  - Tallo, Veronica
AU  - Lie, Reidar K
AD  - c/o Lie -- Dept Clinical Bioethics, National Instit Health, Bethesda, MD
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 2492
EP  - 2500
PB  - Elsevier Science, Amsterdam The Netherlands
VL  - 61
IS  - 12
SN  - 0277-9536, 0277-9536
KW  - Physician migration
KW  - Health policy
KW  - Developing countries
KW  - India
KW  - Pakistan
KW  - Nigeria
KW  - Columbia
KW  - The Philippines
KW  - Doctors
KW  - Migration
KW  - article
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aassia&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Social+Science+%26+Medicine&rft.atitle=Physician+Migration%3A+Views+from+Professionals+in+Colombia%2C+Nigeria%2C+India%2C+Pakistan+and+the+Philippines&rft.au=Astor%2C+Avraham%3BAkhtar%2C+Tasleem%3BMatallana%2C+Maria+Alexandra%3BMuthuswamy%2C+Vasantha%3BOlowu%2C+Folarin+A%3BTallo%2C+Veronica%3BLie%2C+Reidar+K&rft.aulast=Astor&rft.aufirst=Avraham&rft.date=2005-12-01&rft.volume=61&rft.issue=12&rft.spage=2492&rft.isbn=&rft.btitle=&rft.title=Social+Science+%26+Medicine&rft.issn=02779536&rft_id=info:doi/10.1016%2Fj.socscimed.2005.05.003
LA  - English
DB  - Applied Social Sciences Index & Abstracts (ASSIA)
N1  - Date revised - 2006-07-28
N1  - Last updated - 2016-09-27
N1  - CODEN - SSCMAW
N1  - SubjectsTermNotLitGenreText - Doctors; Migration; Health policy; Developing countries
DO  - http://dx.doi.org/10.1016/j.socscimed.2005.05.003
ER  - 



TY  - JOUR
T1  - Dysbindin (DTNBP1, 6p22.3) Is Associated with Childhood-Onset Psychosis and Endophenotypes Measured by the Premorbid Adjustment Scale (PAS)
AN  - 57044953; 200614510
AB  - Straub et al. (2002) recently identified the 6p22.3 gene dysbindin (DTNBP1) through positional cloning as a schizophrenia susceptibility gene. We studied a rare cohort of 102 children with onset of psychosis before age 13. Standardized ratings of early development, medication response, neuropsychological & cognitive performance, premorbid dysfunction & clinical follow-up were obtained. Fourteen SNPs were genotyped in the gene DTNBP1. Family-based pairwise & haplotype transmission disequilibrium test (TDT) analysis with the clinical phenotype, & quantitative transmission disequilibrium test (QTDT) explored endophenotype relationships. One SNP was associated with diagnosis (TDT p=.01). The QTDT analyses showed several significant relationships. Four adjacent SNPs were associated (p values=.0009-.003) with poor premorbid functioning. These findings support the hypothesis that this & other schizophrenia susceptibility genes contribute to early neurodevelopmental impairment. 3 Tables, 38 References. Adapted from the source document.
JF  - Journal of Autism and Developmental Disorders
AU  - Gornick, M C
AU  - Addington, A M
AU  - Sporn, A
AU  - Gogtay, N
AU  - Greenstein, D
AU  - Lenane, M
AU  - Gochman, P
AU  - Ordonez, A
AU  - Balkissoon, R
AU  - Vakkalanka, R
AU  - Weinberger, D R
AU  - Rapoport, J L
AU  - Straub, R E
AD  - c/o Rapoport -- Child Psychiatry Branch, IRP, National Instit Mental Health, Bethesda, MD
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 831
EP  - 838
PB  - Springer, Dordrecht The Netherlands
VL  - 35
IS  - 6
SN  - 0162-3257, 0162-3257
KW  - Candidate gene
KW  - genetic association
KW  - transmission disequilibrium test
KW  - quantitative TDT
KW  - schizophrenia
KW  - DTNBP1
KW  - childhood onset
KW  - Schizophrenia
KW  - Genetics
KW  - Phenotypes
KW  - Psychoses
KW  - Childhood onset
KW  - article
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aassia&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Autism+and+Developmental+Disorders&rft.atitle=Dysbindin+%28DTNBP1%2C+6p22.3%29+Is+Associated+with+Childhood-Onset+Psychosis+and+Endophenotypes+Measured+by+the+Premorbid+Adjustment+Scale+%28PAS%29&rft.au=Gornick%2C+M+C%3BAddington%2C+A+M%3BSporn%2C+A%3BGogtay%2C+N%3BGreenstein%2C+D%3BLenane%2C+M%3BGochman%2C+P%3BOrdonez%2C+A%3BBalkissoon%2C+R%3BVakkalanka%2C+R%3BWeinberger%2C+D+R%3BRapoport%2C+J+L%3BStraub%2C+R+E&rft.aulast=Gornick&rft.aufirst=M&rft.date=2005-12-01&rft.volume=35&rft.issue=6&rft.spage=831&rft.isbn=&rft.btitle=&rft.title=Journal+of+Autism+and+Developmental+Disorders&rft.issn=01623257&rft_id=info:doi/10.1007%2Fs10803-005-0028-3
LA  - English
DB  - Applied Social Sciences Index & Abstracts (ASSIA)
N1  - Date revised - 2006-10-02
N1  - Last updated - 2016-09-27
N1  - CODEN - JADDDQ
N1  - SubjectsTermNotLitGenreText - Genetics; Psychoses; Phenotypes; Schizophrenia; Childhood onset
DO  - http://dx.doi.org/10.1007/s10803-005-0028-3
ER  - 



TY  - CPAPER
T1  - Genetic Marking Studies in Non-Human Primates: Insights into Hematopoiesis and Leukemogenesis
T2  - 2005 Euroconference on Gene and Cell Therapy
AN  - 40099002; 4041880
JF  - 2005 Euroconference on Gene and Cell Therapy
AU  - Dunbar, Cynthia E
Y1  - 2005/12/01/
PY  - 2005
DA  - 2005 Dec 01
KW  - Leukemogenesis
KW  - Hemopoiesis
KW  - Primates
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Euroconference+on+Gene+and+Cell+Therapy&rft.atitle=Genetic+Marking+Studies+in+Non-Human+Primates%3A+Insights+into+Hematopoiesis+and+Leukemogenesis&rft.au=Dunbar%2C+Cynthia+E&rft.aulast=Dunbar&rft.aufirst=Cynthia&rft.date=2005-12-01&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Euroconference+on+Gene+and+Cell+Therapy&rft.issn=&rft_id=info:doi/
L2  - http://www.pasteur.fr/applications/euroconf/geneandcelltherapy/gene-program me.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Addiction and its brain science
AN  - 37698390; 3253554
AB  - Aims To illustrate how modern neurobiological approaches will help to identify the neurocircuits and genes involved in addictive behavior.    Background The current disorder concept of addiction includes neurobiological foundations and neurobiological research assuming irreversible molecular and structural changes within the brain dopamine reinforcement system, constituting the 'molecular and structural switch' from controlled drug intake to compulsive drug abuse. However, those irreversible changes have not so far been identified and it is suggested that in addition to the mesolimbic dopamine system, other brain systems including the mesocortical and nigrostriatal pathways as well as their non-dopaminergic feedback-loops might be involved in addictive behavior.    Neurobiological approach A three-step neurobiological approach is described that allows in a first step via novel animal models and imaging techniques to identify the neuroanatomical sites mediating voluntary drug intake, reinstatement of drug-seeking behavior, relapse, loss of control and drug intake despite negative consequences. In a subsequent step, forward genetic approaches including quantitative trait loci (QTL)-analysis and gene expression profiling are helpful in identifying so-called candidate genes. In a final step, conditional animal mutants and selective pharmacological tools are used to functionally validate candidate genes. Following this validation process, the transfer to the human situation has to be made and candidate genes have to be verified further in well-phenotyped cohorts of addicted patients.    Conclusion This three-step neurobiological approach, that must involve an interdisciplinary team including experimental psychologists, geneticists, molecular biologists and finally clinical addiction researchers, will allow us to understand where and how the addicted brain goes awry. Reprinted by permission of Blackwell Publishing
JF  - Addiction
AU  - Spanagel, Rainer
AU  - Heilig, Markus
AD  - University of Heidelberg ; National Institute on Alcohol Abuse and Alcoholism
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1813
EP  - 1822
VL  - 100
IS  - 12
SN  - 0965-2140, 0965-2140
KW  - Sociology
KW  - Genetics
KW  - Behavioural psychology
KW  - Brain
KW  - Social problems
KW  - Health
KW  - Addiction
KW  - Drugs
KW  - Neurology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/37698390?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Addiction&rft.atitle=Addiction+and+its+brain+science&rft.au=Spanagel%2C+Rainer%3BHeilig%2C+Markus&rft.aulast=Spanagel&rft.aufirst=Rainer&rft.date=2005-12-01&rft.volume=100&rft.issue=12&rft.spage=1813&rft.isbn=&rft.btitle=&rft.title=Addiction&rft.issn=09652140&rft_id=info:doi/10.1111%2Fj.1360-0443.2005.01260.x
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 5772; 11893 11979; 561 6220; 1750 1678; 8635; 1540 1543 10404; 3755; 5460 1615 8573 11325
DO  - http://dx.doi.org/10.1111/j.1360-0443.2005.01260.x
ER  - 



TY  - JOUR
T1  - Developmental differences in the function and use of anatomical dolls during interviews with alleged sexual abuse victims
AN  - 36524710; 3315465
AB  - The impact of anatomical dolls on reports provided by 3- to 12-year-old alleged sexual abuse victims (N = 178) was examined. Children produced as many details in response to open-ended invitations with and without the dolls. In response to directive questions, the 3- to 6-year-olds were more likely to reenact behaviorally than to report verbally, whereas the 7- to 12-year-olds produced more verbal details than enactments when using the dolls. With the dolls, the younger children were more likely than the older children to play suggestively and to contradict details provided without the dolls, whereas the older children were more likely to provide details that were consistent. Children in both age groups produced proportionally more fantastic details with the dolls than without the dolls. Reprinted by permission of the American Psychological Association
JF  - Journal of consulting and clinical psychology
AU  - Thierry, Karen L
AU  - Lamb, Michael E
AU  - Orbach, Yael
AU  - Pipe, Margaret-Ellen
AD  - State University of New Jersey ; University of Cambridge ; National Institute of Child Health and Human Development
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1125
EP  - 1134
VL  - 73
IS  - 6
SN  - 0022-006X, 0022-006X
KW  - Sociology
KW  - Body
KW  - Memory
KW  - Social psychology
KW  - Sexual abuse
KW  - Childhood
KW  - Behavioural psychology
KW  - Interviews
KW  - Psychopathology
KW  - Anatomy
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/36524710?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+consulting+and+clinical+psychology&rft.atitle=Developmental+differences+in+the+function+and+use+of+anatomical+dolls+during+interviews+with+alleged+sexual+abuse+victims&rft.au=Thierry%2C+Karen+L%3BLamb%2C+Michael+E%3BOrbach%2C+Yael%3BPipe%2C+Margaret-Ellen&rft.aulast=Thierry&rft.aufirst=Karen&rft.date=2005-12-01&rft.volume=73&rft.issue=6&rft.spage=1125&rft.isbn=&rft.btitle=&rft.title=Journal+of+consulting+and+clinical+psychology&rft.issn=0022006X&rft_id=info:doi/10.1037%2F0022-006X.73.6.1125
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 10409; 2211 652 5676 646 6091 2212; 1540 1543 10404; 11901 10404; 11559 11540 3015 11881; 7930; 6832 10919; 981 1615 8573 11325; 1678
DO  - http://dx.doi.org/10.1037/0022-006X.73.6.1125
ER  - 



TY  - JOUR
T1  - Evidence for a gene-environment interaction in predicting behavioral inhibition in middle childhood
AN  - 36488019; 3298343
AB  - Gene-environment interactions are presumed to shape human behavior during early development. However, no human research has demonstrated that such interactions lead to stable individual differences in fear responses. We tested this possibility by focusing on a polymorphism in the promoter region of the gene for the serotonin transporter (5-HTT). This polymorphism has been linked to many indices of serotonin activity. Specifically, we tested the hypothesis that an interaction between children's 5-HTT status and maternal reports of social support predicts inhibited behavior with unfamiliar peers in middle childhood. Results were consistent with this hypothesis: Children with the combination of the short 5-HTT allele and low social support had increased risk for behavioral inhibition in middle childhood. Reprinted by permission of Sage Publications
JF  - Psychological science
AU  - Fox, Nathan A
AU  - Nichols, Kate E
AU  - Henderson, Heather A
AU  - Rubin, Kenneth
AU  - Schmidt, Louis
AU  - Hamer, Dean
AU  - Ernst, Monique
AU  - Pine, Daniel S
AD  - University of Maryland ; University of Miami ; McMaster University ; National Cancer Institute
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 921
EP  - 926
VL  - 16
IS  - 12
SN  - 0956-7976, 0956-7976
KW  - Sociology
KW  - Genetics
KW  - Childhood
KW  - Behavioural psychology
KW  - Social environment
KW  - Psychopathology
KW  - Developmental psychology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/36488019?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Psychological+science&rft.atitle=Evidence+for+a+gene-environment+interaction+in+predicting+behavioral+inhibition+in+middle+childhood&rft.au=Fox%2C+Nathan+A%3BNichols%2C+Kate+E%3BHenderson%2C+Heather+A%3BRubin%2C+Kenneth%3BSchmidt%2C+Louis%3BHamer%2C+Dean%3BErnst%2C+Monique%3BPine%2C+Daniel+S&rft.aulast=Fox&rft.aufirst=Nathan&rft.date=2005-12-01&rft.volume=16&rft.issue=12&rft.spage=921&rft.isbn=&rft.btitle=&rft.title=Psychological+science&rft.issn=09567976&rft_id=info:doi/
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 10409; 11829 6077 4309; 2211 652 5676 646 6091 2212; 1540 1543 10404; 3518 10404; 5460 1615 8573 11325
ER  - 



TY  - JOUR
T1  - Opinion: A candidate gene approach to searching for low-penetrance breast and prostate cancer genes
AN  - 275118034; 16341085
AB  - Most cases of breast and prostate cancer are not associated with mutations in known high-penetrance genes, indicating the involvement of multiple low-penetrance risk alleles. Studies that have attempted to identify these genes have met with limited success. The National Cancer Institute Breast and Prostate Cancer Cohort Consortium--a pooled analysis of multiple large cohort studies with a total of more than 5,000 cases of breast cancer and 8,000 cases of prostate cancer--was therefore initiated. The goal of this consortium is to characterize variations in approximately 50 genes that mediate two pathways that are associated with these cancers--the steroid-hormone metabolism pathway and the insulin-like growth factor signalling pathway--and to associate these variations with cancer risk.
JF  - Nature Reviews. Cancer
AU  - Hunter, David
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 977
EP  - 85
CY  - London
PB  - Nature Publishing Group
VL  - 5
IS  - 12
SN  - 1474175X
KW  - Medical Sciences--Oncology
KW  - Gonadal Steroid Hormones
KW  - Prostatic Neoplasms -- metabolism
KW  - Humans
KW  - Cohort Studies
KW  - Gonadal Steroid Hormones -- metabolism
KW  - Breast Neoplasms -- metabolism
KW  - Male
KW  - Female
KW  - Breast Neoplasms -- genetics
KW  - Penetrance
KW  - Genes, Neoplasm
KW  - Prostatic Neoplasms -- genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/275118034?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ahealthcompleteshell&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Nature+Reviews.+Cancer&rft.atitle=Opinion%3A+A+candidate+gene+approach+to+searching+for+low-penetrance+breast+and+prostate+cancer+genes&rft.au=Hunter%2C+David&rft.aulast=Hunter&rft.aufirst=David&rft.date=2005-12-01&rft.volume=5&rft.issue=12&rft.spage=977&rft.isbn=&rft.btitle=&rft.title=Nature+Reviews.+Cancer&rft.issn=1474175X&rft_id=info:doi/10.1038%2Fnrc1754
LA  - English
DB  - ProQuest Central
N1  - Copyright - Copyright Nature Publishing Group Dec 2005
N1  - Last updated - 2014-04-30
DO  - http://dx.doi.org/10.1038/nrc1754
ER  - 



TY  - JOUR
T1  - In vivo single-shot, proton-localized 13C MRS of rhesus monkey brain
AN  - 21067891; 8632097
AB  - A single-shot, proton-localized, polarization transfer 13C spectroscopic method was proposed and implemented on a 4.7T scanner for studying rhesus monkey brains. The polarization transfer sequence was mostly adiabatic, minimizing signal loss due to B1 inhomogeneity. RF pulses in polarization transfer were also used for voxel selection of protons with gradient fields. The transferred 13C magnetization was refocused by additional refocusing adiabatic pulses. With the intravenous infusion of D-[1-13C]glucose solution, 13C NMR spectra from a 30mL voxel were acquired for the resonances of C1 of glucose, C2,3,4 of glutamate and glutamine. The time-resolved turnover of glutamate, glutamine and aspartate from intravenously infused D-[1-13C]glucose at a temporal resolution of 12min was demonstrated with excellent spectral resolution and signal-to-noise ratio. Typically, the half-height linewidth of the decoupled 13C peaks was 4Hz. Data obtained with infusion of sodium [2-13C]acetate using the proposed polarization transfer method and data from the carboxylic carbon region using non-localized acquisition are also presented. Published in 2005 by John Wiley & Sons, Ltd.
JF  - NMR in Biomedicine
AU  - Li, Shizhe
AU  - Chen, Zhengguang
AU  - Zhang, Yan
AU  - Lizak, Martin
AU  - Bacher, John
AU  - Innis, Robert B
AU  - Shen, Jun
AD  - National Institute of Mental Health, National Institutes of Health, Bethesda, MD 20892, USA, shenj@intra.nimh.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 560
EP  - 569
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 18
IS  - 8
SN  - 0952-3480, 0952-3480
KW  - CSA Neurosciences Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Glutamine
KW  - Glucose
KW  - Carbon
KW  - N.M.R.
KW  - Macaca mulatta
KW  - Intravenous administration
KW  - Data processing
KW  - Protons
KW  - Brain
KW  - Polarization
KW  - Sodium
KW  - Adiabatic
KW  - Glutamic acid
KW  - W 30910:Imaging
KW  - N3 11029:Neurophysiology & biophysics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/21067891?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=NMR+in+Biomedicine&rft.atitle=In+vivo+single-shot%2C+proton-localized+13C+MRS+of+rhesus+monkey+brain&rft.au=Li%2C+Shizhe%3BChen%2C+Zhengguang%3BZhang%2C+Yan%3BLizak%2C+Martin%3BBacher%2C+John%3BInnis%2C+Robert+B%3BShen%2C+Jun&rft.aulast=Li&rft.aufirst=Shizhe&rft.date=2005-12-01&rft.volume=18&rft.issue=8&rft.spage=560&rft.isbn=&rft.btitle=&rft.title=NMR+in+Biomedicine&rft.issn=09523480&rft_id=info:doi/10.1002%2Fnbm.993
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-12-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - Macaca mulatta; Polarization; Glutamic acid; Data processing; Brain; N.M.R.; Adiabatic; Glutamine; Carbon; Sodium; Intravenous administration; Glucose; Protons
DO  - http://dx.doi.org/10.1002/nbm.993
ER  - 



TY  - JOUR
T1  - A diffusion tensor imaging analysis of gender differences in water diffusivity within human skeletal muscle
AN  - 21063363; 8632089
AB  - The diffusive properties of adjacent muscles at rest were evaluated in male (n=12) and female (n=12) subjects using diffusion tensor imaging (DTI). The principle, second and third eigenvalues, trace of the diffusion tensor [Tr(D)], and two anisotropic parameters, ellipsoid eccentricity (e) and fractional anisotropy (FA), of various muscles in the human calf were calculated from the diffusion tensor. Seven muscles were investigated in this study from images acquired of the left calf: the soleus, lateral gastrocnemius, medial gastrocnemius, posterior tibialis, anterior tibialis, extensor digitorum longus and peroneus longus. A mathematical model was also derived that relates the eigenvalues of the diffusion tensor to the muscle fiber volume fraction, which is defined as the volume of muscle fibers within a well-defined arbitrary muscle volume. Females on average had higher eigenvalues and Tr(D) compared with males, with the majority of muscles being statistically different between the sexes. In contrast, males on average had higher e and FA than females, with the large plantar flexors-soleus, lateral gastrocnemius, and medial gastrocnemius-producing statistically different results. The behavior of the mathematical model for variations in fiber volume fraction produced similar trends to those seen when the experimental data were fit to the model. The model predicts that a larger volume fraction of skeletal muscle in males is devoted to fibers than in females, but the true underlying source of the gender discrepancy remains unclear. Although the model does not fully account for other transport processes, it does provide some insight into the limiting factors that affect the diffusion of water in skeletal muscle measured by DTI.
JF  - NMR in Biomedicine
AU  - Galban, Craig J
AU  - Maderwald, Stefan
AU  - Uffmann, Kai
AU  - Ladd, Mark E
AD  - Department of Diagnostic and Interventional Radiology, University Hospital Essen, Hufelandstrasse 55, D-45122 Essen, Germany, galbanc@ors.od.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 489
EP  - 498
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 18
IS  - 8
SN  - 0952-3480, 0952-3480
KW  - Biotechnology and Bioengineering Abstracts
KW  - Data processing
KW  - Anisotropy
KW  - Mathematical models
KW  - Magnetic resonance imaging
KW  - Diffusion
KW  - N.M.R.
KW  - Skeletal muscle
KW  - Limiting factors
KW  - Sex differences
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/21063363?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=NMR+in+Biomedicine&rft.atitle=A+diffusion+tensor+imaging+analysis+of+gender+differences+in+water+diffusivity+within+human+skeletal+muscle&rft.au=Galban%2C+Craig+J%3BMaderwald%2C+Stefan%3BUffmann%2C+Kai%3BLadd%2C+Mark+E&rft.aulast=Galban&rft.aufirst=Craig&rft.date=2005-12-01&rft.volume=18&rft.issue=8&rft.spage=489&rft.isbn=&rft.btitle=&rft.title=NMR+in+Biomedicine&rft.issn=09523480&rft_id=info:doi/10.1002%2Fnbm.975
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-12-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - Skeletal muscle; Mathematical models; Anisotropy; Magnetic resonance imaging; Sex differences; Data processing; N.M.R.; Diffusion; Limiting factors
DO  - http://dx.doi.org/10.1002/nbm.975
ER  - 



TY  - JOUR
T1  - CpG-containing oligodeoxynucleotide promotes microglial cell uptake of amyloid ss 1-42 peptide by up-regulating the expression of the G-protein-coupled receptor mFPR2
AN  - 21053094; 7327148
AB  - Inflammation contributes to the pathogenic process of Alzheimer's disease (AD). We previously discovered that a human G-protein-coupled formyl peptide receptor-like 1 (FPRL1) and its mouse homologue mFPR2 mediate the chemotaxis and activation of mononuclear phagocytes in response to a variety of peptide agonists, including amyloid ss 1-42 (Ass sub(42)), which is neurotoxic and a key mediator of inflammatory responses in AD. Since mFPR2 is up-regulated in mouse microglia by lipopolysaccharide (LPS), a Toll-like receptor 4 ligand, the aim of this study is to investigate whether TLR9, which is activated by CpG-containing oligodeoxynucleotide (ODN) as well as by potential agonists released by damaged host cells, may also enhance the expression and function of mFPR2, thereby affecting the progress of AD.
JF  - FASEB Journal
AU  - Iribarren, P
AU  - Chen, K
AU  - Hu, J
AU  - Gong, W
AU  - Cho, E H
AU  - Lockett, S
AU  - Uranchimeg, B
AU  - Wang, J M
AD  - Laboratory of Molecular Immunoregulation, Center for Cancer Research, National Cancer Institute at Frederick, Bldg. 560, Room 31-40, Frederick, MD 21702-1201, USA, wangji@mail.ncifcrf.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 2032
EP  - 2034
VL  - 19
IS  - 14
SN  - 0892-6638, 0892-6638
KW  - CSA Neurosciences Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Alzheimer's disease
KW  - Chemotaxis
KW  - Oligonucleotides
KW  - ^b-Amyloid
KW  - G protein-coupled receptors
KW  - Phagocytes
KW  - Lipopolysaccharides
KW  - Microglial cells
KW  - TLR4 protein
KW  - TLR9 protein
KW  - Microglia
KW  - Inflammation
KW  - Neurodegenerative diseases
KW  - Neurotoxicity
KW  - formyl peptide receptor-like 1
KW  - ^AG protein-coupled receptors
KW  - Toll-like receptors
KW  - b-Amyloid
KW  - N3 11028:Neuropharmacology & toxicology
KW  - W 30915:Pharmaceuticals & Vaccines
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/21053094?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=FASEB+Journal&rft.atitle=CpG-containing+oligodeoxynucleotide+promotes+microglial+cell+uptake+of+amyloid+ss+1-42+peptide+by+up-regulating+the+expression+of+the+G-protein-coupled+receptor+mFPR2&rft.au=Iribarren%2C+P%3BChen%2C+K%3BHu%2C+J%3BGong%2C+W%3BCho%2C+E+H%3BLockett%2C+S%3BUranchimeg%2C+B%3BWang%2C+J+M&rft.aulast=Iribarren&rft.aufirst=P&rft.date=2005-12-01&rft.volume=19&rft.issue=14&rft.spage=2032&rft.isbn=&rft.btitle=&rft.title=FASEB+Journal&rft.issn=08926638&rft_id=info:doi/10.1096%2Ffj.05-4578fje
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-04-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - Alzheimer's disease; Neurodegenerative diseases; Oligonucleotides; Lipopolysaccharides; Inflammation; Toll-like receptors; b-Amyloid; Phagocytes; Microglia; formyl peptide receptor-like 1; TLR9 protein; TLR4 protein; Microglial cells; Chemotaxis; G protein-coupled receptors; Neurotoxicity; ^b-Amyloid; ^AG protein-coupled receptors
DO  - http://dx.doi.org/10.1096/fj.05-4578fje
ER  - 



TY  - JOUR
T1  - Conjugates of Group A and W135 Capsular Polysaccharides of Neisseria meningitidis Bound to Recombinant Staphylococcus aureus Enterotoxin C1: Preparation, Physicochemical Characterization, and Immunological Properties in Mice
AN  - 20986440; 7142798
AB  - Neisseria meningitidis groups A (GAM) and W135 capsular polysaccharides (CPs) were bound to recombinant Staphylococcus aureus enterotoxin C1 (rSEC). The CPs were activated with 1-cyano-4-dimethylaminopyridinium tetrafluoroborate and then bound to adipic acid dihydrazide derivatives of rSEC. Syntheses were conducted with native GAM CP (GAMP), W135 CP (W135P), and ultrasonicated or hydrazine-treated W135P at various concentrations of reactants, pHs, and ionic strengths. The conjugates were characterized by compositional and serologic analyses, high-performance size-exclusion chromatography with multi-angle laser light scattering detection, and immunogenicity in 5- to 6-week-old mice. Conjugates injected subcutaneously in phosphate-buffered saline elicited immunoglobulin G (IgG) responses against their respective CPs and rSEC, whereas GAMP and W135P alone did not induce detectable CP antibodies. The O-acetyl content of W135P was low, and its removal had no adverse effect upon the conjugate's immunogenicity. Reduction of the molecular size of W135P by treatment with hydrazine improved the immunogenicity of W135P-rSEC. IgG anti-CP elicited by the conjugates showed complement-dependent bactericidal activity against their respective organisms, and IgG anti-rSEC neutralized the T-cell proliferative activity of native SEC. A bivalent formulation of GAMP-rSEC and W135P-rSEC elicited IgG anti-CP at comparable levels to those induced by the conjugates administered separately.
JF  - Infection and Immunity
AU  - Jin, Zhigang
AU  - Bohach, Gregory A
AU  - Shiloach, Joseph
AU  - Norris, Scott E
AU  - Freedberg, Daron I
AU  - Deobald, Claudia
AU  - Coxon, Bruce
AU  - Robbins, John B
AU  - Schneerson, Rachel
AD  - National Institute of Child Health and Human Development. National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland 20892. Department of Microbiology, Molecular Biology and Biochemistry, University of Idaho, Moscow, Idaho 83844. Center for Biologics Evaluation and Research, Food and Drug Administration, Bethesda, Maryland 20892
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 7887
EP  - 7893
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 73
IS  - 12
SN  - 0019-9567, 0019-9567
KW  - Immunology Abstracts; Microbiology Abstracts B: Bacteriology
KW  - Ionic strength
KW  - Hydrazine
KW  - Chromatography
KW  - Light scattering
KW  - Neisseria meningitidis
KW  - Adipic acid dihydrazide
KW  - Polysaccharides
KW  - Immunogenicity
KW  - Lymphocytes T
KW  - Immunoglobulin G
KW  - Lasers
KW  - Enterotoxins
KW  - Staphylococcus aureus
KW  - Bactericidal activity
KW  - Capsular polysaccharides
KW  - Side effects
KW  - J 02350:Immunology
KW  - F 06910:Microorganisms & Parasites
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20986440?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Infection+and+Immunity&rft.atitle=Conjugates+of+Group+A+and+W135+Capsular+Polysaccharides+of+Neisseria+meningitidis+Bound+to+Recombinant+Staphylococcus+aureus+Enterotoxin+C1%3A+Preparation%2C+Physicochemical+Characterization%2C+and+Immunological+Properties+in+Mice&rft.au=Jin%2C+Zhigang%3BBohach%2C+Gregory+A%3BShiloach%2C+Joseph%3BNorris%2C+Scott+E%3BFreedberg%2C+Daron+I%3BDeobald%2C+Claudia%3BCoxon%2C+Bruce%3BRobbins%2C+John+B%3BSchneerson%2C+Rachel&rft.aulast=Jin&rft.aufirst=Zhigang&rft.date=2005-12-01&rft.volume=73&rft.issue=12&rft.spage=7887&rft.isbn=&rft.btitle=&rft.title=Infection+and+Immunity&rft.issn=00199567&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Hydrazine; Ionic strength; Chromatography; Light scattering; Polysaccharides; Adipic acid dihydrazide; Immunogenicity; Immunoglobulin G; Lymphocytes T; Enterotoxins; Lasers; Capsular polysaccharides; Bactericidal activity; Side effects; Neisseria meningitidis; Staphylococcus aureus
ER  - 



TY  - JOUR
T1  - PfCG2, a Plasmodium falciparum protein peripherally associated with the parasitophorous vacuolar membrane, is expressed in the period of maximum hemoglobin uptake and digestion by trophozoites
AN  - 20957324; 8338134
AB  - A Plasmodium falciparum gene closely linked to the chloroquine resistance locus encodes PfCG2, a predicted 320-330 kDa protein. In the parasitized erythrocyte, PfCG2 expression rises sharply in the trophozoite stage and is detected in electron-dense patches along the parasitophorous vacuolar membrane (PVM), in the cytoplasm and in the digestive vacuole (DV). Results of extraction and partitioning experiments show that PfCG2 is a peripheral membrane protein. Exposure of trophozoite-infected erythrocytes to trypsin-containing buffer after streptolysin O permeabilization indicates that PfCG2 is exposed to the erythrocyte cytosol at the outer face of the PVM. PfCG2 is highly susceptible to hydrolysis by aspartic and cysteine proteases and shows dose-dependent accumulation in the presence of protease inhibitors. These results suggest that PfCG2 is delivered from the outside face of the PVM to the DV, where it is broken down by parasite proteases. PfCG2 interacts with erythrocyte cytoplasm and may be associated with processes of hemoglobin uptake and digestion by erythrocytic-stage parasites.
JF  - Molecular and Biochemical Parasitology
AU  - Cooper, Roland A
AU  - Papakrivos, Janni
AU  - Lane, Kristin D
AU  - Fujioka, Hisashi
AU  - Lingelbach, Klaus
AU  - Wellems, Thomas E
AD  - Laboratory of Malaria and Vector Research, Twinbrook III, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892-8132, USA, twellems@niaid.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - December 2005
SP  - 167
EP  - 176
PB  - Elsevier Science, P.O. Box 211 Amsterdam 1000 AE Netherlands, [mailto:nlinfo-f@elsevier.nl]
VL  - 144
IS  - 2
SN  - 0166-6851, 0166-6851
KW  - Genetics Abstracts; Microbiology Abstracts C: Algology, Mycology & Protozoology; ASFA 3: Aquatic Pollution & Environmental Quality; ASFA 1: Biological Sciences & Living Resources
KW  - Malaria
KW  - Endocytosis
KW  - Phagocytosis
KW  - Protein trafficking
KW  - Proteases
KW  - Parasites
KW  - Proteinase inhibitors
KW  - Erythrocytes
KW  - Chloroquine
KW  - Plasmodium falciparum
KW  - Membrane proteins
KW  - Hydrolysis
KW  - Hemoglobin
KW  - Digestion
KW  - Bioaccumulation
KW  - Cysteine
KW  - Cytoplasm
KW  - Vacuoles
KW  - Cytosol
KW  - Proteins
KW  - Haemoglobins
KW  - Trophozoites
KW  - Cysteine proteinase
KW  - G 07880:Human Genetics
KW  - Q1 08484:Species interactions: parasites and diseases
KW  - Q5 08501:General
KW  - K 03320:Cell Biology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20957324?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aasfaaquaticpollution&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Molecular+and+Biochemical+Parasitology&rft.atitle=PfCG2%2C+a+Plasmodium+falciparum+protein+peripherally+associated+with+the+parasitophorous+vacuolar+membrane%2C+is+expressed+in+the+period+of+maximum+hemoglobin+uptake+and+digestion+by+trophozoites&rft.au=Cooper%2C+Roland+A%3BPapakrivos%2C+Janni%3BLane%2C+Kristin+D%3BFujioka%2C+Hisashi%3BLingelbach%2C+Klaus%3BWellems%2C+Thomas+E&rft.aulast=Cooper&rft.aufirst=Roland&rft.date=2005-12-01&rft.volume=144&rft.issue=2&rft.spage=167&rft.isbn=&rft.btitle=&rft.title=Molecular+and+Biochemical+Parasitology&rft.issn=01666851&rft_id=info:doi/10.1016%2Fj.molbiopara.2005.07.009
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-07-01
N1  - Last updated - 2016-05-27
N1  - SubjectsTermNotLitGenreText - Digestion; Parasites; Bioaccumulation; Cysteine; Cytoplasm; Erythrocytes; Proteins; Hydrolysis; Haemoglobins; Hemoglobin; Vacuoles; Proteinase inhibitors; Cytosol; Chloroquine; Membrane proteins; Cysteine proteinase; Trophozoites; Plasmodium falciparum
DO  - http://dx.doi.org/10.1016/j.molbiopara.2005.07.009
ER  - 



TY  - JOUR
T1  - Dependence on diffusion time of apparent diffusion tensor of ex vivo calf tongue and heart
AN  - 20859707; 8367966
AB  - The time dependence of the apparent diffusion tensor of ex vivo calf heart and tongue was measured for diffusion times (d) between 32 and 810 ms. The results showed evidence of restricted diffusion in the muscle tissues of both organs. In regions where the myofibers are parallel, the largest eigenvalue (1) of the diffusion tensor remained the same for all diffusion times measured, while the other eigenvalues (2, 3) decreased by 29-36% between d = 32 ms and d = 400 ms. In regions where the fibers cross, the 1 also changed, decreasing by 17% between d = 32 ms and d = 400 ms. The restricting compartment size and volume fraction were effectively estimated by fitting the time courses of the eigenvalues to a model consisting of a nonrestricted compartment and a cylindrically restricted compartment. To our knowledge, this study is the first demonstrating diffusion time dependence of measured water diffusion tensor in muscular tissue. With improvement in scanning technology, future studies may permit noninvasive, in vivo detection of changes in muscle myoarchitecture due to disease, treatment, and exercise.
JF  - Magnetic Resonance in Medicine
AU  - Kim, Sungheon
AU  - Chi-Fishman, Gloria
AU  - Barnett, Alan S
AU  - Pierpaoli, Carlo
AD  - Physical Disabilities Branch, Department of Rehabilitation Medicine, Clinical Research Center, National Institutes of Health, Bethesda, Maryland, USA, sungheonk@cc.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1387
EP  - 1396
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 54
IS  - 6
SN  - 0740-3194, 0740-3194
KW  - Biotechnology and Bioengineering Abstracts
KW  - Heart
KW  - Scanning
KW  - Muscles
KW  - N.M.R.
KW  - Tongue
KW  - Diffusion
KW  - Models
KW  - Physical training
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20859707?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Magnetic+Resonance+in+Medicine&rft.atitle=Dependence+on+diffusion+time+of+apparent+diffusion+tensor+of+ex+vivo+calf+tongue+and+heart&rft.au=Kim%2C+Sungheon%3BChi-Fishman%2C+Gloria%3BBarnett%2C+Alan+S%3BPierpaoli%2C+Carlo&rft.aulast=Kim&rft.aufirst=Sungheon&rft.date=2005-12-01&rft.volume=54&rft.issue=6&rft.spage=1387&rft.isbn=&rft.btitle=&rft.title=Magnetic+Resonance+in+Medicine&rft.issn=07403194&rft_id=info:doi/10.1002%2Fmrm.20676
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-08-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - Diffusion; Heart; Muscles; Tongue; N.M.R.; Scanning; Physical training; Models
DO  - http://dx.doi.org/10.1002/mrm.20676
ER  - 



TY  - JOUR
T1  - Single heartbeat cardiac tagging for the evaluation of transient phenomena
AN  - 20859474; 8367974
AB  - Many cardiac abnormalities are of a transient nature, creating a beat-to-beat variation in myocardial function. This work presents the cardiac imaging technique for the measurement of regional function during transient cardiac phenomena. All information necessary for the reconstruction of a cine loop is acquired within a single heartbeat, avoiding the temporal blurring introduced by segmented imaging due to the assumption of cardiac cycle periodicity. This method incorporates a gradient-optimized, high-efficiency EPI-SSFP sequence and TSENSE parallel imaging. For acquisitions with readout resolutions of 128,160, 192, and 256 points, the technique produced images with average temporal resolution of 35, 39, 43, and 52 ms and average spatial resolutions of 2.65, 2.12, 1.77, and 1.32 mm in the readout direction, respectively, and 2.88 and 2.08 mm in the phase encode direction for acceleration rates of 3 and 4, respectively. Local apparent strains in the single slice and measurements of ventricular end-systolic and end-diastolic areas were used as quantitative measures to validate the single heartbeat technique. To demonstrate the utility of the sequence, movie loops were acquired for multiple heartbeats in non-breath-held acquisitions as well as during a Valsalva maneuver. A heartbeat-interleaved acquisition allowed for the reconstruction of nonaccelerated images from R contiguous heartbeats. Images reconstructed from such data displayed tag blurring and reduced tag persistence due to motion and interheartbeat variability. Images acquired during the Valsalva maneuver demonstrated apparent beat-to-beat variability, visible both in the images and as changing strain patterns and ventricular volumes.
JF  - Magnetic Resonance in Medicine
AU  - Herzka, Daniel A
AU  - Derbyshire, J Andrew
AU  - Kellman, Peter
AU  - McVeigh, Elliot R
AD  - Department of Biomedical Engineering, Johns Hopkins University School of Medicine Baltimore, Maryland, USA, herzkad@nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1455
EP  - 1464
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 54
IS  - 6
SN  - 0740-3194, 0740-3194
KW  - Biotechnology and Bioengineering Abstracts
KW  - Heart
KW  - Data processing
KW  - Image processing
KW  - Periodicity
KW  - spatial discrimination
KW  - N.M.R.
KW  - imaging
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20859474?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Magnetic+Resonance+in+Medicine&rft.atitle=Single+heartbeat+cardiac+tagging+for+the+evaluation+of+transient+phenomena&rft.au=Herzka%2C+Daniel+A%3BDerbyshire%2C+J+Andrew%3BKellman%2C+Peter%3BMcVeigh%2C+Elliot+R&rft.aulast=Herzka&rft.aufirst=Daniel&rft.date=2005-12-01&rft.volume=54&rft.issue=6&rft.spage=1455&rft.isbn=&rft.btitle=&rft.title=Magnetic+Resonance+in+Medicine&rft.issn=07403194&rft_id=info:doi/10.1002%2Fmrm.20719
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-08-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - Heart; imaging; N.M.R.; Data processing; Image processing; spatial discrimination; Periodicity
DO  - http://dx.doi.org/10.1002/mrm.20719
ER  - 



TY  - JOUR
T1  - Image reconstruction in SNR units: A general method for SNR measurement
AN  - 20859112; 8367972
AB  - The method for phased array image reconstruction of uniform noise images may be used in conjunction with proper image scaling as a means of reconstructing images directly in SNR units. This facilitates accurate and precise SNR measurement on a per pixel basis. This method is applicable to root-sum-of-squares magnitude combining, B1-weighted combining, and parallel imaging such as SENSE. A procedure for image reconstruction and scaling is presented, and the method for SNR measurement is validated with phantom data. Alternative methods that rely on noise only regions are not appropriate for parallel imaging where the noise level is highly variable across the field-of-view. The purpose of this article is to provide a nuts and bolts procedure for calculating scale factors used for reconstructing images directly in SNR units. The procedure includes scaling for noise equivalent bandwidth of digital receivers, FFTs and associated window functions (raw data filters), and array combining.
JF  - Magnetic Resonance in Medicine
AU  - Kellman, Peter
AU  - McVeigh, Elliot R
AD  - Laboratory of Cardiac Energetics, National Heart, Lung and Blood Institute, National Institutes of Health, DHHS, Bethesda, Maryland 20892-1061, USA, kellman@nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1439
EP  - 1447
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 54
IS  - 6
SN  - 0740-3194, 0740-3194
KW  - Biotechnology and Bioengineering Abstracts
KW  - Filters
KW  - Data processing
KW  - Nuts
KW  - Image processing
KW  - N.M.R.
KW  - imaging
KW  - Scaling
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20859112?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Magnetic+Resonance+in+Medicine&rft.atitle=Image+reconstruction+in+SNR+units%3A+A+general+method+for+SNR+measurement&rft.au=Kellman%2C+Peter%3BMcVeigh%2C+Elliot+R&rft.aulast=Kellman&rft.aufirst=Peter&rft.date=2005-12-01&rft.volume=54&rft.issue=6&rft.spage=1439&rft.isbn=&rft.btitle=&rft.title=Magnetic+Resonance+in+Medicine&rft.issn=07403194&rft_id=info:doi/10.1002%2Fmrm.20713
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-08-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - Scaling; Image processing; Data processing; imaging; N.M.R.; Filters; Nuts
DO  - http://dx.doi.org/10.1002/mrm.20713
ER  - 



TY  - JOUR
T1  - Absolute oxygen tension (pO2) in murine fatty and muscle tissue as determined by EPR
AN  - 20856783; 8367981
AB  - The absolute partial pressure of oxygen (pO2) in the mammary gland pad and femoral muscle of female mice was measured using EPR oximetry at 700 MHz. A small quantity of lithium phthalocyanine (LiPc) crystals was implanted in both mammary and femoral muscle tissue of female C3H mice. Subsequent EPR measurements were carried out 1-30 days after implantation with or without control of core body temperature. The pO2 values in the tissue became stable 2 weeks after implantation of LiPc crystals. The pO2 level was found to be higher in the femoral muscle than in the mammary tissue. However, the pO2 values showed a strong dependence on the core body temperature of the mice. The pO2 values were responsive to carbogen (95% O2, 5% CO2) breathing even 44-58 days after the implantation of LiPc. The LiPc linewidth was also sensitive to changes in the blood supply even 60 days after implantation of the crystals. This study further validates the use of LiPc crystals and EPR oximetry for long-term non-invasive assessment of pO2 levels in tissues, underscores the importance of maintaining normal body core temperature during the measurements, and demonstrates that mammary tissue functions at a lower pO2 level than muscle in female C3H mice.
JF  - Magnetic Resonance in Medicine
AU  - Matsumoto, Atsuko
AU  - Matsumoto, Shingo
AU  - Sowers, Anastasia L
AU  - Koscielniak, Janusz W
AU  - Trigg, Nancy J
AU  - Kuppusamy, Periannan
AU  - Mitchell, James B
AU  - Subramanian, Sankaran
AU  - Krishna, Murali C
AU  - Matsumoto, Ken-ichiro
AD  - Radiation Biology Branch, Center for Cancer Research, National Cancer Institute, Bethesda, MD, USA, murali@helix.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1530
EP  - 1535
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 54
IS  - 6
SN  - 0740-3194, 0740-3194
KW  - Biotechnology and Bioengineering Abstracts
KW  - Oxygen tension
KW  - Body temperature
KW  - Mammary gland
KW  - Respiration
KW  - Muscles
KW  - Crystals
KW  - Femur
KW  - Blood
KW  - N.M.R.
KW  - Pressure
KW  - Carbon dioxide
KW  - Lithium
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20856783?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Magnetic+Resonance+in+Medicine&rft.atitle=Absolute+oxygen+tension+%28pO2%29+in+murine+fatty+and+muscle+tissue+as+determined+by+EPR&rft.au=Matsumoto%2C+Atsuko%3BMatsumoto%2C+Shingo%3BSowers%2C+Anastasia+L%3BKoscielniak%2C+Janusz+W%3BTrigg%2C+Nancy+J%3BKuppusamy%2C+Periannan%3BMitchell%2C+James+B%3BSubramanian%2C+Sankaran%3BKrishna%2C+Murali+C%3BMatsumoto%2C+Ken-ichiro&rft.aulast=Matsumoto&rft.aufirst=Atsuko&rft.date=2005-12-01&rft.volume=54&rft.issue=6&rft.spage=1530&rft.isbn=&rft.btitle=&rft.title=Magnetic+Resonance+in+Medicine&rft.issn=07403194&rft_id=info:doi/10.1002%2Fmrm.20714
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-08-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Muscles; Crystals; Femur; Body temperature; Carbon dioxide; Blood; Oxygen tension; N.M.R.; Respiration; Mammary gland; Lithium; Pressure
DO  - http://dx.doi.org/10.1002/mrm.20714
ER  - 



TY  - JOUR
T1  - Real-time blood flow imaging using autocalibrated spiral sensitivity encoding
AN  - 20854987; 8367986
AB  - A novel spiral phase contrast (PC) technique was developed for high temporal resolution imaging of blood flow without cardiac gating. An autocalibrated spiral sensitivity encoding (SENSE) method is introduced and used to reconstruct PC images. Numerical simulations and a flow phantom study were performed to validate the technique. To study the accuracy of the flow measurement in vivo, a high-resolution cardiac experiment was performed and a subset of undersampled SENSE reconstructed data were reconstructed. Good agreement between the velocity measurement from the fully-sampled and undersampled data was achieved. Real-time experiments were performed to measure blood velocity in the ascending aorta and aortic valve, and during a Valsalva maneuver. The results demonstrate the potential of this technique for real-time flow imaging.
JF  - Magnetic Resonance in Medicine
AU  - Nezafat, Reza
AU  - Kellman, Peter
AU  - Derbyshire, J Andrew
AU  - McVeigh, Elliot R
AD  - Department of Biomedical Engineering, Johns Hopkins University, Baltimore, Maryland, USA, nezafatr@nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1557
EP  - 1561
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 54
IS  - 6
SN  - 0740-3194, 0740-3194
KW  - Biotechnology and Bioengineering Abstracts
KW  - Heart
KW  - Data processing
KW  - Aortic valve
KW  - Aorta
KW  - Gating
KW  - N.M.R.
KW  - imaging
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20854987?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Magnetic+Resonance+in+Medicine&rft.atitle=Real-time+blood+flow+imaging+using+autocalibrated+spiral+sensitivity+encoding&rft.au=Nezafat%2C+Reza%3BKellman%2C+Peter%3BDerbyshire%2C+J+Andrew%3BMcVeigh%2C+Elliot+R&rft.aulast=Nezafat&rft.aufirst=Reza&rft.date=2005-12-01&rft.volume=54&rft.issue=6&rft.spage=1557&rft.isbn=&rft.btitle=&rft.title=Magnetic+Resonance+in+Medicine&rft.issn=07403194&rft_id=info:doi/10.1002%2Fmrm.20690
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-08-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - imaging; Data processing; Heart; N.M.R.; Gating; Aortic valve; Aorta
DO  - http://dx.doi.org/10.1002/mrm.20690
ER  - 



TY  - JOUR
T1  - In vivo carbon-13 magnetization transfer effect. Detection of aspartate aminotransferase reaction
AN  - 20852952; 8367958
AB  - One of the most remarkable achievements of in vivo NMR spectroscopy has been the detection of rapid enzyme-catalyzed exchange reactions using phosphorus-31 magnetic resonance spectroscopy-based magnetization transfer experiments. In this paper, we report, for the first time, the in vivo carbon magnetization transfer (CMT) effect and in vivo detection of the CMT effects of the -ketoglutarate glutamate and the oxaloacetate aspartate reactions, both of which are catalyzed by aspartate aminotransferase. By saturating the carbonyl carbon of -ketoglutarate at 206 ppm in -chloralose anesthetized adult rat brain, the unidirectional glutamate -ketoglutarate flux was determined to be 78 - 9 mol/g/min (mean - SD, n = 11) following i.v. infusion of [1,6-13C2]D-glucose. Contribution from aspartate aminotransferase-catalyzed partial reactions to the observed CMT effects was emphasized. Because of the large chemical shift separation between the -carbons of the amino acids and the carbonyl carbons of the corresponding cognate keto acids, the spillover of the saturation radiofrequency pulses to the -carbon resonances was negligible. The results indicate that the magnetization transfer effects of aspartate aminotransferase-catalyzed reactions can be used as new biomarkers accessible to non-invasive in vivo magnetic resonance spectroscopy techniques.
JF  - Magnetic Resonance in Medicine
AU  - Shen, Jun
AD  - Molecular Imaging Branch, National Institute of Mental Health, Bethesda, Maryland, USA, shenj@intra.nimh.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1321
EP  - 1326
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 54
IS  - 6
SN  - 0740-3194, 0740-3194
KW  - Biotechnology and Bioengineering Abstracts
KW  - Amino acids
KW  - Carbon
KW  - Aspartate aminotransferase
KW  - Acids
KW  - Magnetic resonance spectroscopy
KW  - Brain
KW  - N.M.R.
KW  - Glutamic acid
KW  - biomarkers
KW  - carbonyls
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20852952?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Magnetic+Resonance+in+Medicine&rft.atitle=In+vivo+carbon-13+magnetization+transfer+effect.+Detection+of+aspartate+aminotransferase+reaction&rft.au=Shen%2C+Jun&rft.aulast=Shen&rft.aufirst=Jun&rft.date=2005-12-01&rft.volume=54&rft.issue=6&rft.spage=1321&rft.isbn=&rft.btitle=&rft.title=Magnetic+Resonance+in+Medicine&rft.issn=07403194&rft_id=info:doi/10.1002%2Fmrm.20709
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-08-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - Carbon; Magnetic resonance spectroscopy; Glutamic acid; N.M.R.; carbonyls; Aspartate aminotransferase; Amino acids; biomarkers; Brain; Acids
DO  - http://dx.doi.org/10.1002/mrm.20709
ER  - 



TY  - JOUR
T1  - Immune-Related Conditions and Immune-Modulating Medications as Risk Factors for Non-Hodgkin's Lymphoma: A Case-Control Study
AN  - 20715076; 6576056
AB  - In immunosuppressed or autoimmune disease states, disordered immune responses may lead to non-Hodgkin's lymphoma (NHL). In a US population-based case-control study of NHL (1998-2000), the authors collected personal histories of immune-related conditions and use of immune-modulating therapies as well as family histories of autoimmune conditions. The study included 1,321 NHL cases and 1,057 controls; only half received some questionnaire components. NHL was associated with Sjoegren's syndrome (odds ratio (OR) = 13, 95% confidence interval (CI): 1.7, 100) and lupus (OR = 4.2, 95% CI: 1.2, 15). Two specific NHL subtypes were strongly associated with Sjoegren's syndrome: salivary gland (OR = 290, 95% CI: 33, 2600) and marginal zone (OR = 75, 95% CI: 9.1, 610). NHL was less convincingly associated with receipt of an organ transplant (OR = 2.0, 95% CI: 0.4, 11). Other autoimmune conditions were too rare to evaluate or not associated with NHL. Corticosteroid use was unrelated to NHL (OR = 1.0, 95% CI: 0.8, 1.2), but methotrexate use was marginally associated (OR = 2.3, 95% CI: 0.7, 7.5). Family history of dermatomyositis was associated with NHL (7 cases vs. 0 controls, OR = infinite; two-sided p = 0.02), but dermatomyositis was absent in cases themselves. Family history of remaining conditions was unrelated to NHL. Results suggest that disordered immunity in some immune-related conditions can lead to NHL.
JF  - American Journal of Epidemiology
AU  - Engels, Eric A
AU  - Cerhan, James R
AU  - Linet, Martha S
AU  - Cozen, Wendy
AU  - Colt, Joanne S
AU  - Davis, Scott
AU  - Gridley, Gloria
AU  - Severson, Richard K
AU  - Hartge, Patricia
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, Department of Health and Human Services, Rockville, MD
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1153
EP  - 1161
PB  - Oxford University Press, Oxford Journals Health, Great Clarendon Street Oxford OX2 6DP UK, [mailto:jnl.samples@oup.co.uk], [URL:http://www3.oup.co.uk/jnls/]
VL  - 162
IS  - 12
SN  - 0002-9262, 0002-9262
KW  - Risk Abstracts; Immunology Abstracts
KW  - non-Hodgkin's lymphoma
KW  - Historical account
KW  - Inventories
KW  - Autoimmune diseases
KW  - autoimmune diseases
KW  - Immunity
KW  - Salivary gland
KW  - Organs
KW  - Immunomodulation
KW  - Sjogren's syndrome
KW  - Genetics
KW  - Non-Hodgkin's lymphoma
KW  - Corticoids
KW  - Dermatomyositis
KW  - Risk factors
KW  - Methotrexate
KW  - Drugs
KW  - corticoids
KW  - R2 23060:Medical and environmental health
KW  - F 06920:Transplantation
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ariskabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=American+Journal+of+Epidemiology&rft.atitle=Immune-Related+Conditions+and+Immune-Modulating+Medications+as+Risk+Factors+for+Non-Hodgkin%27s+Lymphoma%3A+A+Case-Control+Study&rft.au=Engels%2C+Eric+A%3BCerhan%2C+James+R%3BLinet%2C+Martha+S%3BCozen%2C+Wendy%3BColt%2C+Joanne+S%3BDavis%2C+Scott%3BGridley%2C+Gloria%3BSeverson%2C+Richard+K%3BHartge%2C+Patricia&rft.aulast=Engels&rft.aufirst=Eric&rft.date=2005-12-01&rft.volume=162&rft.issue=12&rft.spage=1153&rft.isbn=&rft.btitle=&rft.title=American+Journal+of+Epidemiology&rft.issn=00029262&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-07-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Sjogren's syndrome; Corticoids; Inventories; Non-Hodgkin's lymphoma; Dermatomyositis; Risk factors; Autoimmune diseases; Methotrexate; Immunity; Salivary gland; Immunomodulation; non-Hodgkin's lymphoma; Historical account; Genetics; autoimmune diseases; Drugs; Organs; corticoids
ER  - 



TY  - JOUR
T1  - Countermeasures to the Bioterrorist Threat of Smallpox
AN  - 20305551; 7653965
AB  - Variola, the agent of smallpox, is a bioterrorist threat, as is monkeypox virus, which also occurs naturally in Africa. Development of countermeasures, in the form of improved vaccines, antiviral drugs, and other therapeutic strategies are a high priority. Recent advances in molecular biology and in animal model development have provided fresh insight into the virulence determinants for smallpox and the pathophysiology of disease. The complex replication cycle for orthopoxviruses, and the pivotal role for viralspecific immunomodulatory proteins which contribute to escape from immunologic surveillance, provide many unique targets for therapeutic intervention. The "toxemia" of smallpox has been elucidated in part by variola- infected primate studies which revealed the central role of apoptosis and the evolution of a cytokine storm leading to hemorrhagic diathesis, resembling fulminent "black" smallpox. This suggests a potential role for therapeutic strategies developed for septic shock, in treatment of smallpox. Drugs licensed for other viruses which share molecular targets with orthopoxviruses (e.g. Cidofovir) or cancer drugs (e.g. Gleevec and other tyrosine kinase inhibitors) have immediate application for treatment of smallpox and monkeypox and provide leads for second generation drugs with higher therapeutic indices. Recent advances in identification of virulence determinants and immune evasion genes facilitate the design of alternative vaccines to replace live vaccinia strains that are unsuitable for a large proportion of individuals in a mass immunization campaign.
JF  - Current Molecular Medicine
AU  - Jahrling, Peter B
AU  - Fritz, Elizabeth A
AU  - Hensley, Lisa E
AD  - National Institute of Allergy and Infectious Diseases, National Institutes of Health, 6700-B Rockledge Drive, Bethesda, MD 20892-7609, USA.
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 817
EP  - 826
PB  - Bentham Science Publishers B.V., P.O. Box 1673 Hilversum 1200 BR The Netherlands, [mailto:shidding@worldonline.nl], [URL:http://www.bentham.org]
VL  - 5
IS  - 8
SN  - 1566-5240, 1566-5240
KW  - Primates
KW  - Virology & AIDS Abstracts; Immunology Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Therapeutic applications
KW  - Hemorrhage
KW  - Virulence
KW  - Protein-tyrosine kinase
KW  - Variola
KW  - Monkeypox virus
KW  - Replication
KW  - Vaccinia
KW  - Drug development
KW  - Septic shock
KW  - Immunization
KW  - Vaccines
KW  - Apoptosis
KW  - Animal models
KW  - Immunosuppressive agents
KW  - Antiviral agents
KW  - Cytokines
KW  - Cidofovir
KW  - Monkeypox
KW  - Toxemia
KW  - Cancer
KW  - Smallpox
KW  - Evolution
KW  - F 06905:Vaccines
KW  - V 22350:Immunology
KW  - W 30915:Pharmaceuticals & Vaccines
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Current+Molecular+Medicine&rft.atitle=Countermeasures+to+the+Bioterrorist+Threat+of+Smallpox&rft.au=Jahrling%2C+Peter+B%3BFritz%2C+Elizabeth+A%3BHensley%2C+Lisa+E&rft.aulast=Jahrling&rft.aufirst=Peter&rft.date=2005-12-01&rft.volume=5&rft.issue=8&rft.spage=817&rft.isbn=&rft.btitle=&rft.title=Current+Molecular+Medicine&rft.issn=15665240&rft_id=info:doi/10.2174%2F156652405774962326
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-11-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Monkeypox virus; Variola; Primates; Smallpox; Antiviral agents; Immunosuppressive agents; Vaccines; Virulence; Monkeypox; Protein-tyrosine kinase; Vaccinia; Hemorrhage; Cytokines; Apoptosis; Cancer; Replication; Therapeutic applications; Animal models; Evolution; Drug development; Toxemia; Immunization; Septic shock; Cidofovir
DO  - http://dx.doi.org/10.2174/156652405774962326
ER  - 



TY  - JOUR
T1  - Perfusion-based fMRI: Insights from animal models
AN  - 20243437; 7456810
AB  - Modern functional neuroimaging techniques, including functional magnetic resonance imaging (fMRI), positron emission tomography (PET), and optical imaging of intrinsic signals (OIS), rely on a tight coupling between neural activity and cerebral blood flow (CBF) to visualize brain activity using CBF as a surrogate marker. Because CBF is a uniquely defined physiological parameter, fMRI techniques based on CBF contrast have the advantage of being specific to tissue signal change, and the potential to provide more direct and quantitative measures of brain activation than blood oxygenation level-dependent (BOLD)- or cerebral blood volume (CBV)-based techniques. The changes in CBF elicited by increased neural activity are an excellent index of the magnitude of electrical activity. Increases in CBF are more closely localized to the foci of increased electrical activity, and occur more promptly to the stimulus than BOLD- or CBV- based contrast. In addition, CBF-based fMRI is less affected by confounds from venous drainage common to BOLD. Animal studies of brain activation have yielded considerable insights into the advantages of CBF-based fMRI. Based on results provided by animal studies, CBF fMRI may offer a means of better assessing the magnitude, spatial extent, and temporal response of neural activity, and may be more specific to tissue state. These properties are expected to be particularly useful for longitudinal and quantitative fMRI studies. J. Magn. Reson. Imaging 2005. Published 2005 Wiley-Liss, Inc.
JF  - Journal of Magnetic Resonance Imaging
AU  - Silva, Afonso C
AD  - Cerebral Microcirculation Unit, Laboratory of Functional and Molecular Imaging, National Institute of Neurological Disorders and Stroke, Bethesda, Maryland, USA, silvaa@ninds.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 745
EP  - 750
PB  - John Wiley & Sons, Inc., 111 River Street Hoboken NJ 07030 USA, [mailto:custserv@wiley.com], [URL:http://www.wiley.com/]
VL  - 22
IS  - 6
SN  - 1053-1807, 1053-1807
KW  - Biotechnology and Bioengineering Abstracts; CSA Neurosciences Abstracts
KW  - functional magnetic resonance imaging
KW  - arterial spin labeling
KW  - animal models
KW  - cerebral blood flow
KW  - spatial resolution
KW  - temporal resolution
KW  - Brain mapping
KW  - Neuroimaging
KW  - Functional magnetic resonance imaging
KW  - Positron emission tomography
KW  - Animal models
KW  - Cerebral blood flow
KW  - W 30910:Imaging
KW  - N3 11027:Neurology & neuropathology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Magnetic+Resonance+Imaging&rft.atitle=Perfusion-based+fMRI%3A+Insights+from+animal+models&rft.au=Silva%2C+Afonso+C&rft.aulast=Silva&rft.aufirst=Afonso&rft.date=2005-12-01&rft.volume=22&rft.issue=6&rft.spage=745&rft.isbn=&rft.btitle=&rft.title=Journal+of+Magnetic+Resonance+Imaging&rft.issn=10531807&rft_id=info:doi/10.1002%2Fjmri.20461
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Brain mapping; Neuroimaging; Functional magnetic resonance imaging; Animal models; Positron emission tomography; Cerebral blood flow
DO  - http://dx.doi.org/10.1002/jmri.20461
ER  - 



TY  - JOUR
T1  - Technological advances in MRI measurement of brain perfusion
AN  - 20242018; 7456807
AB  - Measurement of brain perfusion using arterial spin labeling (ASL) or dynamic susceptibility contrast (DSC) based MRI has many potential important clinical applications. However, the clinical application of perfusion MRI has been limited by a number of factors, including a relatively poor spatial resolution, limited volume coverage, and low signal-to-noise ratio (SNR). It is difficult to improve any of these aspects because both ASL and DSC methods require rapid image acquisition. In this report, recent methodological developments are discussed that alleviate some of these limitations and make perfusion MRI more suitable for clinical application. In particular, the availability of high magnetic field strength systems, increased gradient performance, the use of RF coil arrays and parallel imaging, and increasing pulse sequence efficiency allow for increased image acquisition speed and improved SNR. The use of parallel imaging facilitates the trade-off of SNR for increases in spatial resolution. As a demonstration, we obtained DSC and ASL perfusion images at 3.0 T and 7.0 T with multichannel RF coils and parallel imaging, which allowed us to obtain high-quality images with in-plane voxel sizes of 1.5 X 1.5 mm super(2). J. Magn. Reson. Imaging 2005. Published 2005 Wiley-Liss, Inc.
JF  - Journal of Magnetic Resonance Imaging
AU  - Duyn, Jeff H
AU  - Van Gelderen, Peter
AU  - Talagala, Lalith
AU  - Koretsky, Alan
AU  - De Zwart, Jacco A
AD  - Advanced MRI Laboratory, National Institutes of Health, Bethesda, Maryland, USA, jhd@helix.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 751
EP  - 753
PB  - John Wiley & Sons, Inc., 111 River Street Hoboken NJ 07030 USA, [mailto:custserv@wiley.com], [URL:http://www.wiley.com/]
VL  - 22
IS  - 6
SN  - 1053-1807, 1053-1807
KW  - Biotechnology and Bioengineering Abstracts; CSA Neurosciences Abstracts
KW  - MR imaging
KW  - perfusion
KW  - resolution
KW  - coil arrays
KW  - parallel imaging
KW  - Magnetic fields
KW  - Neuroimaging
KW  - Perfusion
KW  - Magnetic resonance imaging
KW  - Brain
KW  - spatial discrimination
KW  - W 30910:Imaging
KW  - N3 11027:Neurology & neuropathology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Magnetic+Resonance+Imaging&rft.atitle=Technological+advances+in+MRI+measurement+of+brain+perfusion&rft.au=Duyn%2C+Jeff+H%3BVan+Gelderen%2C+Peter%3BTalagala%2C+Lalith%3BKoretsky%2C+Alan%3BDe+Zwart%2C+Jacco+A&rft.aulast=Duyn&rft.aufirst=Jeff&rft.date=2005-12-01&rft.volume=22&rft.issue=6&rft.spage=751&rft.isbn=&rft.btitle=&rft.title=Journal+of+Magnetic+Resonance+Imaging&rft.issn=10531807&rft_id=info:doi/10.1002%2Fjmri.20450
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Magnetic fields; Neuroimaging; Perfusion; Magnetic resonance imaging; Brain; spatial discrimination
DO  - http://dx.doi.org/10.1002/jmri.20450
ER  - 



TY  - JOUR
T1  - Nano-sized MRI contrast agents with dendrimer cores
AN  - 20219549; 7199800
AB  - Gadolinium-based MRI contrast agents (CAs) can be effective at a 100-fold lower concentration of Gadolinium ions in comparison to the concentration of Iodine atoms required for CT imaging. Therefore, a number of dendrimer based macromolecular MRI CAs of various sizes and properties prepared employing relatively simple chemistry are readily available that can provide sufficient contrast enhancement for various applications. Molecules up to 20 nm in diameter behave differently in the body depending on their size. Even if these molecules possess similar chemical properties, small changes in size can greatly impact their pharmacokinetics. Changes in molecular size up to 15 nm in diameter altered permeability across the vascular wall, excretion route, and recognition by the reticuloendothelial system. Smaller sized polyamidoamine (PAMAM) dendrimer-based contrast agents, i.e., less than 3 nm in diameter, easily "leak" across the vascular wall resulting in rapid perfusion throughout the body. Contrast agents 3-6 nm in diameter were quickly excreted through the kidney indicating these agents to be potentially suitable as functional renal contrast agents. Contrast agents 7-12 nm in diameter were retained in circulation and were better suited for use as blood pool contrast agents. Hydrophobic variants of CAs formed with polypropylenimine diaminobutane (DAB) dendrimer cores quickly accumulated in the liver and potentially have use as liver contrast agents. Larger hydrophilic agents have suitable characteristics for lymphatic imaging. Finally, contrast agents conjugated with either monoclonal antibodies or with avidin are able to function as tumor-specific contrast agents and might also be employed as either gadolinium neutron capture therapy or in conjunction with radioimmunotherapy.
JF  - Advanced Drug Delivery Reviews
AU  - Kobayashi, Hisataka
AU  - Brechbiel, Martin W
AD  - Molecular Imaging Program, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Building 10, Room 1B40, 10 Center Drive, Bethesda, MD 20892-1088, USA, Kobayash@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 2271
EP  - 2286
PB  - Elsevier Science Ltd., The Boulevard Langford Lane Kidlington Oxford OX5 1GB UK, [mailto:usinfo-f@elsevier.com], [URL:http://www.elsevier.nl]
VL  - 57
IS  - 15
SN  - 0169-409X, 0169-409X
KW  - Biotechnology Research Abstracts (through 1992)
KW  - Drug delivery
KW  - Ions
KW  - Macromolecules
KW  - Perfusion
KW  - Monoclonal antibodies
KW  - polyamidoamines
KW  - Gadolinium
KW  - Magnetic resonance imaging
KW  - Hydrophobicity
KW  - Reticuloendothelial system
KW  - Pharmacokinetics
KW  - Neutrons
KW  - Blood
KW  - Avidin
KW  - Permeability
KW  - Reviews
KW  - Computed tomography
KW  - Liver
KW  - Kidney
KW  - Contrast media
KW  - Iodine
KW  - Excretion
KW  - Vascular system
KW  - W 30915:Pharmaceuticals & Vaccines
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20219549?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Advanced+Drug+Delivery+Reviews&rft.atitle=Nano-sized+MRI+contrast+agents+with+dendrimer+cores&rft.au=Kobayashi%2C+Hisataka%3BBrechbiel%2C+Martin+W&rft.aulast=Kobayashi&rft.aufirst=Hisataka&rft.date=2005-12-01&rft.volume=57&rft.issue=15&rft.spage=2271&rft.isbn=&rft.btitle=&rft.title=Advanced+Drug+Delivery+Reviews&rft.issn=0169409X&rft_id=info:doi/10.1016%2Fj.addr.2005.09.016
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Contrast media; Magnetic resonance imaging; Kidney; Gadolinium; Liver; Vascular system; Macromolecules; Hydrophobicity; Reticuloendothelial system; Neutrons; Ions; Perfusion; Excretion; Permeability; Reviews; Avidin; Monoclonal antibodies; Iodine; Drug delivery; Pharmacokinetics; polyamidoamines; Computed tomography; Blood
DO  - http://dx.doi.org/10.1016/j.addr.2005.09.016
ER  - 



TY  - JOUR
T1  - Replication of Coxiella burnetii Is Inhibited in CHO K-1 Cells Treated with Inhibitors of Cholesterol Metabolism
AN  - 20198015; 6715703
AB  - Coxiella burnetii directs the synthesis of a large parasitophorous vacuole (PV) that is required for its replication. While some lysosomal characteristics of the PV have been described, the origin and composition of the PV membrane remain largely undefined. Cholesterol is an essential component of mammalian membranes where it lends mechanical stability and serves as a platform for signaling proteins. Using infected Chinese hamster ovary cells as a model, we examined whether cholesterol is trafficked to the C. burnetii PV membrane and the effects of inhibitors of cholesterol metabolism on C. burnetii replication. When infected cells were stained with filipin, a fluorescent polyene antifungal agent that binds cholesterol, obvious staining of PV was observed indicating the PV membrane is cholesterol-rich. Furthermore, replication of C. burnetii was significantly inhibited in cells treated with the cholesterol metabolism inhibitors lovastatin, ketoconazole, imipramine, progesterone, and U18666A. These data suggest that cholesterol is an important component of the C. burnetii PV membrane and that normal cellular cholesterol metabolism is required for optimal C. burnetii replication.
JF  - Annals of the New York Academy of Sciences
AU  - Howe, Dale
AU  - Heinzen, Robert A
AD  - Coxiella Pathogenesis Section, Laboratory of Intracellular Parasites, Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Hamilton, Montana 59840, USA
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 123
EP  - 129
PB  - New York Academy of Sciences, 2 East 63rd Street New York NY 10021 USA, [mailto:publications@nyas.org], [URL:http://www.nyas.org]
VL  - 1063
SN  - 0077-8923, 0077-8923
KW  - Microbiology Abstracts C: Algology, Mycology & Protozoology; Microbiology Abstracts B: Bacteriology
KW  - Antifungal agents
KW  - Data processing
KW  - Progesterone
KW  - Replication
KW  - Cholesterol
KW  - Ketoconazole
KW  - Lipid metabolism
KW  - parasitophorous vacuole
KW  - Coxiella burnetii
KW  - polyenes
KW  - imipramine
KW  - Lovastatin
KW  - Signal transduction
KW  - J 02320:Cell Biology
KW  - K 03420:Plant Diseases
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20198015?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Annals+of+the+New+York+Academy+of+Sciences&rft.atitle=Replication+of+Coxiella+burnetii+Is+Inhibited+in+CHO+K-1+Cells+Treated+with+Inhibitors+of+Cholesterol+Metabolism&rft.au=Howe%2C+Dale%3BHeinzen%2C+Robert+A&rft.aulast=Howe&rft.aufirst=Dale&rft.date=2005-12-01&rft.volume=1063&rft.issue=&rft.spage=123&rft.isbn=&rft.btitle=&rft.title=Annals+of+the+New+York+Academy+of+Sciences&rft.issn=00778923&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-12-01
N1  - Last updated - 2015-03-27
N1  - SubjectsTermNotLitGenreText - parasitophorous vacuole; Antifungal agents; Data processing; Progesterone; imipramine; polyenes; Replication; Cholesterol; Ketoconazole; Lovastatin; Signal transduction; Lipid metabolism; Coxiella burnetii
ER  - 



TY  - JOUR
T1  - Immunochemical detection of flucloxacillin adduct formation in livers of treated rats
AN  - 20193767; 6906342
AB  - Flucloxacillin is a semi-synthetic penicillin widely used in the prophylaxis and treatment of staphylococcal infections. Severe liver reactions, characterised by delayed cholestatic hepatitis and a prolonged course of recovery, are associated with flucloxacillin therapy. Clinical findings are suggestive of an immune mediated reaction but there exists little supporting experimental evidence. The formation of drug modified hepatic protein adducts has been proposed to play an important role in the hepatotoxicity of many drugs. The aim of the present study was to investigate whether flucloxacillin treatment results in adduct formation in vivo. Flucloxacillin was conjugated to rabbit serum albumin by formation of a penicilloyl determinant and used as an immunogen to raise a polyclonal antiserum specific for flucloxacillin-modified proteins. Antibody specificity was confirmed by competitive enzyme-linked immunosorbent assay (ELISA) with free drug. The antiserum was used in combination with western blotting to detect adduct formation in the livers of flucloxacillin treated rats. Western blot analysis of rat liver subcellular fractions revealed the formation of six flucloxacillin adducts in various subcellular fractions. These studies demonstrate for the first time that treatment with flucloxacillin results in the formation of hepatic protein adducts.
JF  - Toxicology
AU  - Carey, Michelle A
AU  - Van Pelt, Frank NAM
AD  - Department of Pharmacology & Therapeutics, University College Cork, Ireland, carey1@niehs.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 41
EP  - 48
PB  - Elsevier Science Ireland Ltd., P.O. Box 85 Limerick Ireland
VL  - 216
IS  - 1
SN  - 0300-483X, 0300-483X
KW  - Virology & AIDS Abstracts; Microbiology Abstracts B: Bacteriology; Toxicology Abstracts
KW  - Flucloxacillin
KW  - Cholestasis
KW  - Drug-adduct
KW  - Immunoblotting
KW  - ELISA
KW  - Western blotting
KW  - Enzyme-linked immunosorbent assay
KW  - Infection
KW  - Immunosuppressive agents
KW  - Penicillin
KW  - hepatotoxicity
KW  - Hepatitis
KW  - Antibodies
KW  - Protein adducts
KW  - Albumin
KW  - Prophylaxis
KW  - Liver
KW  - Drugs
KW  - V 22350:Immunology
KW  - X 24115:Pathology
KW  - J 02350:Immunology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20193767?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Toxicology&rft.atitle=Immunochemical+detection+of+flucloxacillin+adduct+formation+in+livers+of+treated+rats&rft.au=Carey%2C+Michelle+A%3BVan+Pelt%2C+Frank+NAM&rft.aulast=Carey&rft.aufirst=Michelle&rft.date=2005-12-01&rft.volume=216&rft.issue=1&rft.spage=41&rft.isbn=&rft.btitle=&rft.title=Toxicology&rft.issn=0300483X&rft_id=info:doi/10.1016%2Fj.tox.2005.07.015
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-07-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Western blotting; Enzyme-linked immunosorbent assay; Infection; Immunosuppressive agents; hepatotoxicity; Penicillin; Hepatitis; Antibodies; Protein adducts; Albumin; Liver; Prophylaxis; Flucloxacillin; Drugs
DO  - http://dx.doi.org/10.1016/j.tox.2005.07.015
ER  - 



TY  - JOUR
T1  - An amino acid substitution in a capsid protein enhances phage survival in mouse circulatory system more than a 1000-fold
AN  - 20156733; 6634439
AB  - In experiments with germ free mice, free from adaptive antibodies to the bacterial virus lambda phage, titers of the virus in the circulatory system have been reported to decrease by more than 10 super(9)pfu within 48h of intraperitoneal intravenous or oral administration. Based on these observations, serial passage techniques have been used to select lambda phage mutants, with 13,000-16,000-fold greater capacity to remain in the mouse circulatory system 24h after intraperitoneal injection. In these prior studies the ''long-circulating'' phage, designated lambda Argo phage, had at least three mutations including one in the major phage capsid (E) protein, which resulted in the change of glutamic acid to a lysine at residue 158. In the current study, we demonstrate that this single specific substitution in the E protein is sufficient to confer the ''long-circulating'' phenotype. The isogenic pair of phage developed in this study consisting of the long-circulating marker-rescued lambda Argo phage, and the parental wild type phage can be used for studies of viral recognition mechanisms of the innate immune system and for the development of more effective antibacterial therapeutic phage strains.
JF  - Virus Research
AU  - Vitiello, CL
AU  - Merril, C R
AU  - Adhya, S
AD  - National Institutes of Mental Health, National Institutes of Health, Bethesda, MD 20892, USA, merrilc@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 101
EP  - 103
VL  - 114
IS  - 1-2
SN  - 0168-1702, 0168-1702
KW  - Microbiology Abstracts B: Bacteriology; Virology & AIDS Abstracts
KW  - Phages
KW  - Capsids
KW  - Intravenous administration
KW  - Amino acid substitution
KW  - Immune system
KW  - Oral administration
KW  - Survival
KW  - Lysine
KW  - Antibodies
KW  - double prime E protein
KW  - Glutamic acid
KW  - Mutation
KW  - Capsid protein
KW  - Circulatory system
KW  - V 22070:Phage-host interactions including lysogeny & transduction
KW  - J 02340:Antibiotics & Antimicrobials
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20156733?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Virus+Research&rft.atitle=An+amino+acid+substitution+in+a+capsid+protein+enhances+phage+survival+in+mouse+circulatory+system+more+than+a+1000-fold&rft.au=Vitiello%2C+CL%3BMerril%2C+C+R%3BAdhya%2C+S&rft.aulast=Vitiello&rft.aufirst=CL&rft.date=2005-12-01&rft.volume=114&rft.issue=1-2&rft.spage=101&rft.isbn=&rft.btitle=&rft.title=Virus+Research&rft.issn=01681702&rft_id=info:doi/10.1016%2Fj.virusres.2005.05.014
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Capsids; Phages; Intravenous administration; Amino acid substitution; Immune system; Oral administration; Lysine; Survival; Antibodies; double prime E protein; Glutamic acid; Mutation; Circulatory system; Capsid protein
DO  - http://dx.doi.org/10.1016/j.virusres.2005.05.014
ER  - 



TY  - JOUR
T1  - Population Pharmacokinetics of Amphotericin B Lipid Complex in Neonates
AN  - 19983169; 7139858
AB  - The pharmacokinetics of amphotericin B lipid complex (ABLC) were investigated in neonates with invasive candidiasis enrolled in a phase II multicenter trial. Sparse blood (153 samples; 1 to 9 per patient, 1 to 254 h after the dose) and random urine and cerebrospinal fluid (CSF) samples of 28 neonates (median weight [WT], 1.06 kg; range, 0.48 to 4.9 kg; median gestational age, 27 weeks; range, 24 to 41 weeks) were analyzed. Patients received intravenous ABLC at 2.5 (n = 15) or 5 (n = 13) mg/kg of body weight once a day over 1 or 2 h, respectively, for a median of 21 days (range, 4 to 47 days). Concentrations of amphotericin B were quantified as total drug by high-performance liquid chromatography. Blood data for time after dose (TAD) of 24 h revealed a terminal half-life of 395 h. Mean concentrations in the urine after 1, 2, and 3 weeks ranged from 0.082 to 0.430 mu g/ml, and those in CSF ranged from undetectable to 0.074 mu g/ml. The disposition of ABLC in neonates was similar to that observed in other age groups: weight was the only factor that influenced clearance. Based on these results and previously published safety and efficacy data, we recommend a daily dosage between 2.5 and 5.0 mg/kg for treatment of invasive Candida infections in neonates.
JF  - Antimicrobial Agents & Chemotherapy
AU  - Wuerthwein, Gudrun
AU  - Groll, Andreas H
AU  - Hempel, Georg
AU  - Adler-Shohet, Felice C
AU  - Lieberman, Jay M
AU  - Walsh, Thomas J
AD  - Infectious Disease Research Program, Center for Bone Marrow Transplantation and Department of Pediatric Hematology/Oncology, Children's University Hospital, Muenster, Federal Republic of Germany. Clinical Pharmacokinetics Section, Coordinating Centre for Clinical Trials (KKS), University Hospital, Muenster, Federal Republic of Germany. Millers Children's Hospital, Long Beach, California. Immunocompromised Host Section, Pediatric Oncology Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 5092
EP  - 5098
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 49
IS  - 12
SN  - 0066-4804, 0066-4804
KW  - Microbiology Abstracts A: Industrial & Applied Microbiology; Microbiology Abstracts C: Algology, Mycology & Protozoology
KW  - High-performance liquid chromatography
KW  - Amphotericin B
KW  - Intravenous administration
KW  - Age
KW  - Gestational age
KW  - Mathematical models
KW  - Data processing
KW  - Candidiasis
KW  - Lipids
KW  - Candida
KW  - Disposition
KW  - Infection
KW  - Clinical trials
KW  - Pharmacokinetics
KW  - Antimicrobial agents
KW  - Models
KW  - Blood
KW  - Cerebrospinal fluid
KW  - Body weight
KW  - Urine
KW  - Neonates
KW  - Drugs
KW  - A 01340:Antibiotics & Antimicrobials
KW  - K 03400:Human Diseases
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19983169?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologya&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Antimicrobial+Agents+%26+Chemotherapy&rft.atitle=Population+Pharmacokinetics+of+Amphotericin+B+Lipid+Complex+in+Neonates&rft.au=Wuerthwein%2C+Gudrun%3BGroll%2C+Andreas+H%3BHempel%2C+Georg%3BAdler-Shohet%2C+Felice+C%3BLieberman%2C+Jay+M%3BWalsh%2C+Thomas+J&rft.aulast=Wuerthwein&rft.aufirst=Gudrun&rft.date=2005-12-01&rft.volume=49&rft.issue=12&rft.spage=5092&rft.isbn=&rft.btitle=&rft.title=Antimicrobial+Agents+%26+Chemotherapy&rft.issn=00664804&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - High-performance liquid chromatography; Amphotericin B; Age; Intravenous administration; Data processing; Mathematical models; Gestational age; Candidiasis; Lipids; Disposition; Infection; Clinical trials; Pharmacokinetics; Models; Antimicrobial agents; Blood; Cerebrospinal fluid; Body weight; Urine; Neonates; Drugs; Candida
ER  - 



TY  - JOUR
T1  - The Conserved Poxvirus L3 Virion Protein Is Required for Transcription of Vaccinia Virus Early Genes
AN  - 19964683; 7144483
AB  - We provide the initial characterization of the product of the vaccinia virus L3L open reading frame (VACWR090), which is conserved in all sequenced members of the poxvirus family. The predicted polypeptide contains no motifs or other features that provided a clue to the role of the L3 protein, and no functional information was available regarding a homolog discovered in Plasmodium falciparum. The L3 protein was expressed following viral DNA replication, a finding consistent with a putative late promoter sequence, and was packaged as a non-membrane protein in mature virus particles. A recombinant virus, in which the L3L gene was regulated by the Escherichia coli lac operator/repressor system, had a conditional lethal phenotype. The virus replicated in the presence of inducer, but in its absence, the yields of infectious virus were reduced by 99%. When cells were infected without inducer, however, no defect in gene expression or morphogenesis was noted. Virus particles lacking L3, which assembled in the absence of inducer, were indistinguishable from wild-type virions with regard to morphology, major structural proteins, and DNA content but were noninfectious. L3-deficient virions were able to bind and penetrate cells but produced extremely small amounts of viral early mRNA. A defect in transcription was demonstrated by in vitro studies with permeabilized virions, but soluble extracts of L3-deficient virions showed normal levels of template-dependent transcriptional activity, indicating that only transcription of the packaged genome is impaired.
JF  - Journal of Virology
AU  - Resch, Wolfgang
AU  - Moss, Bernard
AD  - Laboratory of Viral Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland 20892
Y1  - 2005/12/01/
PY  - 2005
DA  - 2005 Dec 01
SP  - 14719
EP  - 14729
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 79
IS  - 23
SN  - 0022-538X, 0022-538X
KW  - Genetics Abstracts; Microbiology Abstracts C: Algology, Mycology & Protozoology; Microbiology Abstracts B: Bacteriology; Virology & AIDS Abstracts; Biochemistry Abstracts 2: Nucleic Acids
KW  - Virions
KW  - Genomes
KW  - DNA biosynthesis
KW  - Replication
KW  - Nucleotide sequence
KW  - Morphogenesis
KW  - Transcription
KW  - Plasmodium falciparum
KW  - Structural proteins
KW  - Operators
KW  - Promoters
KW  - Vaccinia virus
KW  - Poxvirus
KW  - Escherichia coli
KW  - Repressors
KW  - Open reading frames
KW  - N 14820:DNA Metabolism & Structure
KW  - J 02320:Cell Biology
KW  - G 07770:Bacteria
KW  - V 22310:Genetics, Taxonomy & Structure
KW  - K 03420:Plant Diseases
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Virology&rft.atitle=The+Conserved+Poxvirus+L3+Virion+Protein+Is+Required+for+Transcription+of+Vaccinia+Virus+Early+Genes&rft.au=Resch%2C+Wolfgang%3BMoss%2C+Bernard&rft.aulast=Resch&rft.aufirst=Wolfgang&rft.date=2005-12-01&rft.volume=79&rft.issue=23&rft.spage=14719&rft.isbn=&rft.btitle=&rft.title=Journal+of+Virology&rft.issn=0022538X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Operators; Genomes; Virions; DNA biosynthesis; Promoters; Replication; Nucleotide sequence; Morphogenesis; Transcription; Repressors; Structural proteins; Open reading frames; Vaccinia virus; Poxvirus; Escherichia coli; Plasmodium falciparum
ER  - 



TY  - JOUR
T1  - Lack of Dendritic Cell Maturation Following Infection by Coxiella burnetii Synthesizing Different Lipopolysaccharide Chemotypes
AN  - 19939656; 6715708
AB  - Coxiella burnetii is an obligate intracellular bacterium and the etiologic agent of the zoonotic disease Q fever. Symptomatic infection is normally characterized by flu-like symptoms; however, in some cases, a persistent infection can ensue that may reactivate months or years after initial exposure to cause chronic disease. The mechanisms by which this obligate parasite evades clearance by the host immune response during persistent infection are unknown. We have previously demonstrated that lipopolysaccharide (LPS) length is critical in determining the response of human dendritic cells (DC) to C. burnetii. Here, we investigated whether LPS chemotype affects DC maturation or activation. Immature human DC were infected with three virulent strains of C. burnetii (Nine Mile phase I, S, or Priscilla) that produce chemically distinct LPS molecules. None of these strains stimulated significant upregulation of cell surface markers of DC maturation. Moreover, these strains were equally deficient in inducing DC IL-12p70 production or p38 mitogen-activated protein kinase phosphorylation. Infection of DC by virulent C. burnetii without stimulating significant maturation or inflammatory cytokine production may be a mechanism of immune evasion that results in persistent infection of an otherwise immunocompetent host. Our data indicate that LPS chemotype is not a determinant of DC maturation or cytokine production in response to C. burnetii.
JF  - Annals of the New York Academy of Sciences
AU  - Shannon, Jeffrey G
AU  - Howe, Dale
AU  - Heinzen, Robert A
AD  - Coxiella Pathogenesis Section, Laboratory of Intracellular Parasites, Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Hamilton, Montana 59840, USA
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 154
EP  - 160
PB  - New York Academy of Sciences, 2 East 63rd Street New York NY 10021 USA, [mailto:publications@nyas.org], [URL:http://www.nyas.org]
VL  - 1063
SN  - 0077-8923, 0077-8923
KW  - Microbiology Abstracts B: Bacteriology; Immunology Abstracts
KW  - Parasites
KW  - Cell surface
KW  - MAP kinase
KW  - Data processing
KW  - double prime Q fever
KW  - Persistent infection
KW  - Cell activation
KW  - Inflammation
KW  - Coxiella burnetii
KW  - Interleukin 12
KW  - Dendritic cells
KW  - Phosphorylation
KW  - Chronic infection
KW  - Cytokines
KW  - Lipopolysaccharides
KW  - J 02350:Immunology
KW  - F 06910:Microorganisms & Parasites
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Annals+of+the+New+York+Academy+of+Sciences&rft.atitle=Lack+of+Dendritic+Cell+Maturation+Following+Infection+by+Coxiella+burnetii+Synthesizing+Different+Lipopolysaccharide+Chemotypes&rft.au=Shannon%2C+Jeffrey+G%3BHowe%2C+Dale%3BHeinzen%2C+Robert+A&rft.aulast=Shannon&rft.aufirst=Jeffrey&rft.date=2005-12-01&rft.volume=1063&rft.issue=&rft.spage=154&rft.isbn=&rft.btitle=&rft.title=Annals+of+the+New+York+Academy+of+Sciences&rft.issn=00778923&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-04-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Cell surface; Parasites; MAP kinase; Data processing; Persistent infection; double prime Q fever; Inflammation; Cell activation; Dendritic cells; Interleukin 12; Phosphorylation; Chronic infection; Lipopolysaccharides; Cytokines; Coxiella burnetii
ER  - 



TY  - JOUR
T1  - BMP2 and FGF2 cooperate to induce neural-crest-like fates from fetal and adult CNS stem cells
AN  - 19931233; 6577582
AB  - CNS stem cells are best characterized by their ability to self-renew and to generate multiple differentiated derivatives, but the effect of mitogenic signals, such as fibroblast growth factor 2 (FGF2), on the positional identity of these cells is not well understood. Here, we report that bone morphogenetic protein 2 (BMP2) induces telencephalic CNS stem cells to fates characteristic of neural crest and choroid plexus mesenchyme, a cell type of undetermined lineage in rodents. This induction occurs both in dissociated cell culture and cortical explants of embryonic day 14.5 (E14.5) embryos, but only when cells have been exposed to FGF2. Neither EGF nor IGF1 can substitute for FGF2. An early step in this response is activation of beta -catenin, a mediator of Wnt activity. The CNS stem cells first undergo an epithelial-to-mesenchymal transition and subsequently differentiate to smooth-muscle and non-CNS glia cells. Similar responses are seen with stem cells from E14.5 cortex, E18.5 cortex and adult subventricular zone, but with a progressive shift toward gliogenesis that is characteristic of normal development. These data indicate that FGF2 confers competence for dorsalization independently of its mitogenic action. This rapid and efficient induction of dorsal fates may allow identification of positional identity effectors that are co-regulated by FGF2 and BMP2.
JF  - Journal of Cell Science
AU  - Sailer, Martin HM
AU  - Hazel, Thomas G
AU  - Panchision, David M
AU  - Hoeppner, Daniel J
AU  - Schwab, Martin E
AU  - McKay, Ronald DG
AD  - Laboratory of Molecular Biology, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD 20892, USA. Brain Research Institute, University of Zurich, 8057 Zurich, Switzerland. Department of Biology, Swiss Federal Institute of Technology, 8057 Zurich, Switzerland. Center for Neuroscience Research, Children's Research Institute, Children's National Medical Center, Washington DC, 20010, USA
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 5849
EP  - 5860
PB  - Company of Biologists, 140 Cowley Road Cambridge CB4 0DL UK, [URL:http://www.biologists.com/web/index.html]
VL  - 118
IS  - 24
SN  - 0021-9533, 0021-9533
KW  - Biotechnology and Bioengineering Abstracts; CSA Neurosciences Abstracts
KW  - Smooth muscle
KW  - Central nervous system
KW  - Insulin-like growth factor I
KW  - Wnt protein
KW  - Data processing
KW  - subventricular zone
KW  - Cell culture
KW  - Choroid plexus
KW  - Fetuses
KW  - Stem cells
KW  - catenin
KW  - Glia
KW  - Telencephalon
KW  - Embryos
KW  - Bone morphogenetic protein 2
KW  - Epidermal growth factor
KW  - Mesenchyme
KW  - Fibroblast growth factor 2
KW  - Explants
KW  - Neural crest
KW  - Gliogenesis
KW  - N3 11070:Neurochemistry and cellular biology
KW  - W 30945:Fermentation & Cell Culture
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19931233?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Cell+Science&rft.atitle=BMP2+and+FGF2+cooperate+to+induce+neural-crest-like+fates+from+fetal+and+adult+CNS+stem+cells&rft.au=Sailer%2C+Martin+HM%3BHazel%2C+Thomas+G%3BPanchision%2C+David+M%3BHoeppner%2C+Daniel+J%3BSchwab%2C+Martin+E%3BMcKay%2C+Ronald+DG&rft.aulast=Sailer&rft.aufirst=Martin&rft.date=2005-12-01&rft.volume=118&rft.issue=24&rft.spage=5849&rft.isbn=&rft.btitle=&rft.title=Journal+of+Cell+Science&rft.issn=00219533&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-07-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Smooth muscle; Insulin-like growth factor I; Central nervous system; Data processing; Wnt protein; subventricular zone; Cell culture; Choroid plexus; Fetuses; Stem cells; catenin; Glia; Embryos; Telencephalon; Bone morphogenetic protein 2; Fibroblast growth factor 2; Mesenchyme; Epidermal growth factor; Explants; Gliogenesis; Neural crest
ER  - 



TY  - JOUR
T1  - Crystal structure of human T cell leukemia virus protease, a novel target for anticancer drug design
AN  - 19924921; 6578666
AB  - The successful development of a number of HIV-1 protease (PR) inhibitors for the treatment of AIDS has validated the utilization of retroviral PRs as drug targets and necessitated their detailed structural study. Here we report the structure of a complex of human T cell leukemia virus type 1 (HTLV-1) PR with a substrate-based inhibitor bound in subsites P5 through P5'. Although HTLV-1 PR exhibits an overall fold similar to other retroviral PRs, significant structural differences are present in several loop areas, which include the functionally important flaps, previously considered to be structurally highly conserved. Potential key residues responsible for the resistance of HTLV-1 PR to anti-HIV drugs are identified. We expect that the knowledge accumulated during the development of anti-HIV drugs, particularly in overcoming drug resistance, will help in designing a novel class of antileukemia drugs targeting HTLV-1 PR and in predicting their drug-resistance profile. The structure presented here can be used as a starting point for the development of such anticancer therapies.
JF  - Proceedings of the National Academy of Sciences, USA
AU  - Li, Mi
AU  - Laco, Gary S
AU  - Jaskolski, Mariusz
AU  - Rozycki, Jan
AU  - Alexandratos, Jerry
AU  - Wlodawer, Alexander
AU  - Gustchina, Alla
AD  - Protein Structure Section, Macromolecular Crystallography Laboratory, National Cancer Institute, Frederick, MD 21702
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 18332
EP  - 18337
PB  - National Academy of Sciences, 2101 Constitution Ave. Washington DC 20418 USA
VL  - 102
IS  - 51
SN  - 0027-8424, 0027-8424
KW  - HIV-1
KW  - Biotechnology and Bioengineering Abstracts; Oncogenes & Growth Factors Abstracts; Virology & AIDS Abstracts
KW  - Drug delivery
KW  - Acquired immune deficiency syndrome
KW  - Human immunodeficiency virus
KW  - Drug resistance
KW  - Human T-lymphotropic virus 1
KW  - Human immunodeficiency virus 1
KW  - Proteinase inhibitors
KW  - Lymphocytes T
KW  - Crystal structure
KW  - Drug development
KW  - Proteinase
KW  - V 22032:Viral proteins
KW  - W 30915:Pharmaceuticals & Vaccines
KW  - B 26285:Retroviruses
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19924921?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Drug delivery; Acquired immune deficiency syndrome; Drug resistance; Proteinase inhibitors; Crystal structure; Lymphocytes T; Proteinase; Drug development; Human immunodeficiency virus; Human immunodeficiency virus 1; Human T-lymphotropic virus 1
ER  - 



TY  - JOUR
T1  - Potent Antiviral Activity of North-Methanocarbathymidine against Kaposi's Sarcoma-Associated Herpesvirus
AN  - 19839571; 7139840
AB  - Kaposi's sarcoma-associated herpesvirus (KSHV) infection is a prerequisite for the development of Kaposi's sarcoma (KS). Blocking lytic KSHV replication may hinder KS tumorigenesis. Here, we report potent in vitro anti-KSHV activity of 2'-exo-methanocarbathymidine [North-methanocarbathymidine (N-MCT)], a thymidine analog with a pseudosugar ring locked in the northern conformation, which has previously been shown to block the replication of herpes simplex virus types 1 and 2. N-MCT inhibited KSHV virion production in lytically induced KSHV-infected BCBL-1 cells with a substantially lower 50% inhibitory concentration (IC sub(50)) than those of cidofovir (CDV) and ganciclovir (GCV) (IC sub(50), mean plus or minus standard deviation: 0.08 plus or minus 0.03, 0.42 plus or minus 0.07, and 0.96 plus or minus 0.49 mu M for N-MCT, CDV, and GCV, respectively). The reduction in KSHV virion production was accompanied by a corresponding decrease in KSHV DNA levels in the N-MCT-treated BCBL-1 cells, indicating that the compound blocked lytic KSHV DNA replication. A time- and dose-dependent accumulation of N-MCT-triphosphate (TP) was demonstrated in lytically induced BCBL-1 cells, while uninfected cells showed virtually no accumulation. The levels of N-MCT-TP were significantly decreased in the presence of 5'-ethynylthymidine, a potent inhibitor of herpesvirus thymidine kinase, resulting in the abrogation of anti-KSHV activity of N-MCT. N-MCT-TP more effectively blocked in vitro DNA synthesis by KSHV DNA polymerase with an IC sub(50) of 6.24 plus or minus 0.08 mu M (mean plus or minus standard deviation) compared to CDV-diphosphate (14.70 plus or minus 2.47 mu M) or GCV-TP (24.59 plus or minus 5.60 mu M). Taken together, N-MCT is a highly potent and target-specific anti-KSHV agent which inhibits lytic KSHV DNA synthesis through its triphosphate metabolite produced in KSHV-infected cells expressing a virally encoded thymidine kinase.
JF  - Antimicrobial Agents & Chemotherapy
AU  - Zhu, Weimin
AU  - Burnette, Angela
AU  - Dorjsuren, Dorjbal
AU  - Roberts, Paula E
AU  - Huleihel, Mahmoud
AU  - Shoemaker, Robert H
AU  - Marquez, Victor E
AU  - Agbaria, Riad
AU  - Sei, Shizuko
AD  - Laboratory of Antiviral Drug Mechanisms, SAIC-Frederick, Frederick, Maryland. National Institute for Biotechnology and Department of Virology, Faculty of Health Sciences, Ben-Gurion University of the Negev, Beer-Sheva, Israel. Screening Technologies Branch, Developmental Therapeutics Program, NCI-Frederick, Frederick, Maryland. Laboratory of Medicinal Chemistry, Center for Cancer Research, NCI-Frederick, Frederick, Maryland. Department of Clinical Pharmacology, Faculty of Health Sciences, Ben-Gurion University of the Negev, Beer-Sheva, Israel
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 4965
EP  - 4973
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 49
IS  - 12
SN  - 0066-4804, 0066-4804
KW  - HSV
KW  - Microbiology Abstracts A: Industrial & Applied Microbiology; Virology & AIDS Abstracts
KW  - Cidofovir
KW  - Virions
KW  - DNA biosynthesis
KW  - Human herpesvirus 8
KW  - Replication
KW  - Tumorigenesis
KW  - Kaposi's sarcoma-associated herpesvirus
KW  - Metabolites
KW  - Ganciclovir
KW  - Thymidine kinase
KW  - Infection
KW  - Antiviral activity
KW  - Antimicrobial agents
KW  - Standard deviation
KW  - Kaposi's sarcoma
KW  - DNA-directed DNA polymerase
KW  - Herpes simplex virus
KW  - Thymidine
KW  - Conformation
KW  - A 01340:Antibiotics & Antimicrobials
KW  - V 22370:Oncology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Virions; Cidofovir; DNA biosynthesis; Replication; Tumorigenesis; Thymidine kinase; Ganciclovir; Metabolites; Antiviral activity; Infection; Antimicrobial agents; Standard deviation; Kaposi's sarcoma; DNA-directed DNA polymerase; Thymidine; Conformation; Human herpesvirus 8; Kaposi's sarcoma-associated herpesvirus; Herpes simplex virus
ER  - 



TY  - JOUR
T1  - Enzymatic Redesigning of Biologically Active Heparan Sulfate
AN  - 19825825; 6577430
AB  - Heparan sulfate carries a wide range of biological activities, regulating blood coagulation, cell differentiation, and inflammatory responses. The sulfation patterns of the polysaccharide are essential for the biological activities. In this study, we report an enzymatic method for the sulfation of multimilligram amounts of heparan sulfate with specific functions using immobilized sulfotransferases combined with a 3'-phosphoadenosine 5'-phosphosulfate regeneration system. By selecting appropriate enzymatic modification steps, an inactive precursor has been converted to the heparan sulfate having three distinct biological activities, associated with binding to antithrombin, fibroblast growth factor-2, and herpes simplex virus envelope glycoprotein D. Because the recombinant sulfotransferases are expressed in bacteria, and the method uses a low cost sulfo donor, it can be readily utilized to synthesize large quantities of anticoagulant heparin drug or other biologically active heparan sulfates.
JF  - Journal of Biological Chemistry
AU  - Chen, Jinghua
AU  - Avci, Fikri Y
AU  - Munoz, Eva M
AU  - McDowell, Lynda M
AU  - Chen, Miao
AU  - Pedersen, Lars C
AU  - Zhang, Lijuan
AU  - Linhardt, Robert J
AU  - Liu, Jian
AD  - Division of Medicinal Chemistry and Natural Products, School of Pharmacy, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599, the Department of Chemistry and Chemical Biology, Biology and Chemical and Biological Engineering, Rensselaer Polytechnic Institute, Troy, New York 12180, the Department of Pathology and Immunology, Washington University School of Medicine, St. Louis, Missouri 63110, and the Laboratory of Structural Biology, NIEHS, National Institutes of Health, Research Triangle Park, North Carolina 27709
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 42817
EP  - 42825
PB  - American Society for Biochemistry and Molecular Biology, 9650 Rockville Pike Bethesda MD 20814-3996 USA, [mailto:asbmb@asbmb.faseb.org], [URL:http://www.jbc.org]
VL  - 280
IS  - 52
SN  - 0021-9258, 0021-9258
KW  - HSV
KW  - Virology & AIDS Abstracts; Biotechnology and Bioengineering Abstracts; Medical and Pharmaceutical Biotechnology Abstracts
KW  - Anticoagulants
KW  - Sulfotransferase
KW  - Polysaccharides
KW  - Heparan sulfate
KW  - Inflammation
KW  - glycoprotein D
KW  - Differentiation
KW  - Blood coagulation
KW  - Envelopes
KW  - Fibroblast growth factor 2
KW  - Herpes simplex virus
KW  - Drugs
KW  - Heparin
KW  - antithrombin
KW  - W 30965:Miscellaneous, Reviews
KW  - V 22310:Genetics, Taxonomy & Structure
KW  - W3 33390:Products: Others
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Sulfotransferase; Anticoagulants; Polysaccharides; Heparan sulfate; glycoprotein D; Inflammation; Differentiation; Blood coagulation; Envelopes; Fibroblast growth factor 2; Heparin; Drugs; antithrombin; Herpes simplex virus
ER  - 



TY  - JOUR
T1  - A Role for TLRs in the Regulation of Immune Cell Migration by First Trimester Trophoblast Cells
AN  - 19820311; 6577908
AB  - Normal pregnancy is characterized by the presence of innate immune cells at the maternal-fetal interface. Originally, it was postulated that the presence of these leukocytes was due to an immune response toward paternal Ags expressed by the invading trophoblasts. Instead, we and others postulate that these innate immune cells are necessary for successful implantation and pregnancy. However, elevated leukocyte infiltration may be an underlying cause of pregnancy complications, such as preterm labor or preeclampsia. Furthermore, such conditions have been attributed to an intrauterine infection. Therefore, we hypothesize that first trimester trophoblast cells, upon recognition of microbes through TLRs, may coordinate an immune response by recruiting cells of the innate immune system to the maternal-fetal interface. In this study, we have demonstrated that human first trimester trophoblast cells constitutively secrete the chemokines growth-related oncogene, growth-related oncogene alpha , IL-8, and MCP-1 and are able to recruit monocytes and NK cells, and to a lesser degree, neutrophils. Following the ligation of TLR-3 by the viral ligand, poly(I:C), or TLR-4 by bacterial LPS, trophoblast secretion of chemokines is significantly increased and this in turn results in elevated monocyte and neutrophil chemotaxis. In addition, TLR-3 stimulation also induces trophoblast cells to secrete RANTES. These results suggest a novel mechanism by which first trimester trophoblast cells may differentially modulate the maternal immune system during normal pregnancy and in the presence of an intrauterine infection. Such altered trophoblast cell responses might contribute to the pathogenesis of certain pregnancy complications.
JF  - Journal of Immunology
AU  - Abrahams, Vikki M
AU  - Visintin, Irene
AU  - Aldo, Paulomi B
AU  - Guller, Seth
AU  - Romero, Roberto
AU  - Mor, Gil
AD  - Department of Obstetrics, Gynecology & Reproductive Sciences, Yale University School of Medicine, New Haven, CT 06520. Perinatology Research Branch, National Institute of Child Health and Human Development, Detroit, MI 48202
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 8096
EP  - 8104
PB  - American Association of Immunologists, 9650 Rockville Pike Bethesda MD 20814-3998 USA, [URL:http://www.jimmunol.org/]
VL  - 175
IS  - 12
SN  - 0022-1767, 0022-1767
KW  - Microbiology Abstracts B: Bacteriology; Virology & AIDS Abstracts; Immunology Abstracts
KW  - Chemokines
KW  - Monocyte chemoattractant protein 1
KW  - Immune system
KW  - Leukocytes (neutrophilic)
KW  - Natural killer cells
KW  - Trophoblasts
KW  - RANTES
KW  - Infection
KW  - Chemotaxis
KW  - Interleukin 8
KW  - Pregnancy
KW  - Gro protein
KW  - Pregnancy complications
KW  - Pre-eclampsia
KW  - Lipopolysaccharides
KW  - Immune response
KW  - Monocytes
KW  - Cell migration
KW  - V 22350:Immunology
KW  - J 02350:Immunology
KW  - F 06378:Reproductive System: Clinical
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Chemokines; Monocyte chemoattractant protein 1; Immune system; Natural killer cells; Leukocytes (neutrophilic); RANTES; Trophoblasts; Infection; Chemotaxis; Interleukin 8; Pregnancy; Pregnancy complications; Gro protein; Pre-eclampsia; Lipopolysaccharides; Cell migration; Monocytes; Immune response
ER  - 



TY  - JOUR
T1  - Invasive Infections with Haemophilus influenzae Serotype a Containing an IS1016-bexA Partial Deletion: Possible Association with Virulence
AN  - 19773333; 6841846
AB  - Recent reports of invasive Haemophilus influenzae non-b capsular serotypes in the era since development of conjugate vaccines have prompted concern about serotype replacement. Unusual clusters of invasive infection due to H. influenzae serotype a with clinical features that resemble those of infection due to H. influenzae serotype b have been described. A unique feature often associated with more-virulent H. influenzae serotype a isolates is the IS1016-bexA partial deletion, which was previously identified in the capsule locus of H. influenzae serotype b strains. We report the clinical, epidemiologic, and molecular genetic features of 2 cases of severe disease caused by H. influenzae serotype a. Invasive H. influenzae isolates were serotyped with standard serological methods, and molecular typing was done with PCR. The capsular genotype of each isolate was characterized with PCR, partial sequencing, and Southern blot hybridization. Further strain typing was performed with pulsed-field gel electrophoresis. We identified 2 children with severe invasive disease due to H. influenzae serotype a. Both H. influenzae serotype a isolates contained the identical pulsed-field gel electrophoresis pattern and capsular genotype. An IS1016-bexA partial deletion in the capsule gene locus similar to that found in H. influenzae serotype b was identified in both isolates by means of PCR and sequencing of the IS1016-bexA junction. We describe 2 cases of severe invasive disease due to H. influenzae serotype a with the putative virulence-enhancing IS1016-bexA partial deletion and duplication of the capsule locus. Our data support the hypothesis that this mutation may be associated with virulence in non-b capsular serotypes of H. influenzae.
JF  - Clinical Infectious Diseases
AU  - Kapogiannis, B G
AU  - Satola, S
AU  - Keyserling, H L
AU  - Farley, M M
AD  - Pediatric, Adolescent, and Maternal AIDS Branch, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, MD, USA
Y1  - 2005/12/01/
PY  - 2005
DA  - 2005 Dec 01
SP  - e97
EP  - e103
VL  - 41
IS  - 11
SN  - 1058-4838, 1058-4838
KW  - Virology & AIDS Abstracts; Microbiology Abstracts B: Bacteriology
KW  - Haemophilus influenzae
KW  - Serotypes
KW  - Data processing
KW  - Genotypes
KW  - Children
KW  - Infection
KW  - Virulence
KW  - Gene deletion
KW  - Typing
KW  - Pulsed-field gel electrophoresis
KW  - Polymerase chain reaction
KW  - Vaccines
KW  - Mutation
KW  - J 02834:Vaccination and immunization
KW  - V 22400:Human Diseases
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+Infectious+Diseases&rft.atitle=Invasive+Infections+with+Haemophilus+influenzae+Serotype+a+Containing+an+IS1016-bexA+Partial+Deletion%3A+Possible+Association+with+Virulence&rft.au=Kapogiannis%2C+B+G%3BSatola%2C+S%3BKeyserling%2C+H+L%3BFarley%2C+M+M&rft.aulast=Kapogiannis&rft.aufirst=B&rft.date=2005-12-01&rft.volume=41&rft.issue=11&rft.spage=e97&rft.isbn=&rft.btitle=&rft.title=Clinical+Infectious+Diseases&rft.issn=10584838&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-06-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Virulence; Gene deletion; Data processing; Typing; Serotypes; Pulsed-field gel electrophoresis; Polymerase chain reaction; Vaccines; Genotypes; Infection; Children; Mutation; Haemophilus influenzae
ER  - 



TY  - JOUR
T1  - Cancer Incidence among Male Pesticide Applicators in the Agricultural Health Study Cohort Exposed to Diazinon
AN  - 19772670; 7140979
AB  - Little is known about the potential carcinogenicity associated with routine application of diazinon, a common organophosphate insecticide. The authors explored a possible association of diazinon exposure with cancer risk in the Agricultural Health Study, a prospective cohort of licensed pesticide applicators in Iowa and North Carolina enrolled in 1993-1997. A total of 23,106 male applicators provided information in a self-administered questionnaire. Among 4,961 applicators who reported using diazinon, 301 incident cancer cases were diagnosed during the follow-up period ending December 2002 compared with 968 cases among 18,145 participants who reported no use. Poisson regression was used to calculate rate ratios and 95% confidence intervals. Two quantitative exposure metrics were used: lifetime exposure days and intensity-weighted lifetime exposure days, a measure that incorporates probability of pesticide exposure with lifetime pesticide application frequency. When lifetime exposure days were used, increased risks for the highest tertile of exposure and significant tests for trend for lung cancer and leukemia were observed. No other cancer site showed an association with diazinon for the highest tertile of exposure. Because these results were based on small numbers, additional analyses are necessary as more cases accrue to clarify whether diazinon is associated with cancer risk in humans.
JF  - American Journal of Epidemiology
AU  - Beane Freeman, Laura E
AU  - Bonner, Matthew R
AU  - Blair, Aaron
AU  - Hoppin, Jane A
AU  - Sandler, Dale P
AU  - Lubin, Jay H
AU  - Dosemeci, Mustafa
AU  - Lynch, Charles F
AU  - Knott, Charles
AU  - Alavanja, Michael CR
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Department of Health and Human Services, Rockville, MD
Y1  - 2005/12/01/
PY  - 2005
DA  - 2005 Dec 01
SP  - 1070
EP  - 1079
PB  - Oxford University Press, Oxford Journals Health, Great Clarendon Street Oxford OX2 6DP UK, [mailto:jnl.samples@oup.co.uk], [URL:http://www3.oup.co.uk/jnls/]
VL  - 162
IS  - 11
SN  - 0002-9262, 0002-9262
KW  - Toxicology Abstracts; Risk Abstracts; Health & Safety Science Abstracts
KW  - Agriculture
KW  - USA, North Carolina
KW  - Inventories
KW  - Organophosphates
KW  - males
KW  - organophosphates
KW  - Cancer
KW  - Pesticide applications
KW  - Leukemia
KW  - Insecticides
KW  - USA, Iowa
KW  - Carcinogenicity
KW  - Risk factors
KW  - Pesticides
KW  - Diazinon
KW  - Occupational exposure
KW  - Lung cancer
KW  - H 5000:Pesticides
KW  - R2 23060:Medical and environmental health
KW  - X 24330:Agrochemicals
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Inventories; Leukemia; Insecticides; Carcinogenicity; Risk factors; Pesticides; organophosphates; Diazinon; Pesticide applications; Lung cancer; Agriculture; Organophosphates; males; Occupational exposure; Cancer; USA, North Carolina; USA, Iowa
ER  - 



TY  - JOUR
T1  - A review of evidence from short-term studies leading to the prediction that diazoaminobenzene (1,3-diphenyltriazine) is a carcinogen
AN  - 19727108; 7516658
AB  - The National Toxicology Program (NTP) is responsible for providing comprehensive toxicology evaluations of substances, while at the same time incorporating approaches to reduce, refine or replace laboratory animals in routine toxicity/carcinogenicity studies. Consistent with this, a series of metabolism studies in rodents and human liver slices, electron spin resonance spectroscopy (ESR) studies, short-term dermal toxicity studies in rodents, and acute bone marrow micronucleus studies in mice were performed on diazoaminobenzene (DAAB, also known as 1,3-diphenyltriazine). These studies demonstrated that DAAB is metabolized and shares similar genotoxic and toxicological properties to the known human carcinogen, benzene, and the known rodent carcinogen, aniline. These data were used to evaluate the potential carcinogenicity of DAAB without doing a 2-year rodent bioassay. Based on this analysis, DAAB was predicted to be carcinogenic if evaluated in a 2-year rodent bioassay. These data were evaluated to support listing DAAB in the NTP Report on Carcinogens as a substance reasonably anticipated to be a human carcinogen. The purpose of this article is to review the data developed for predicting the carcinogenicity of DAAB. Published in 2005 by John Wiley & Sons, Ltd.
JF  - Journal of Applied Toxicology
AU  - Bordelon, Nancy R
AU  - Chhabra, Rajendra
AU  - Bucher, John R
AD  - National Toxicology Program, National Institute of Environmental Health Sciences, P.O. Box 12233, Research Triangle Park, NC 27709, USA, bucher@niehs.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 514
EP  - 521
PB  - John Wiley & Sons, Ltd., Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 25
IS  - 6
SN  - 0260-437X, 0260-437X
KW  - Toxicology Abstracts
KW  - Skin
KW  - Genotoxicity
KW  - Laboratory animals
KW  - Bone marrow
KW  - Toxicity
KW  - Carcinogens
KW  - Spectroscopy
KW  - Benzene
KW  - Carcinogenicity
KW  - Reviews
KW  - Liver
KW  - Metabolism
KW  - Aniline
KW  - X 24350:Industrial Chemicals
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19727108?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxicologyabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Applied+Toxicology&rft.atitle=A+review+of+evidence+from+short-term+studies+leading+to+the+prediction+that+diazoaminobenzene+%281%2C3-diphenyltriazine%29+is+a+carcinogen&rft.au=Bordelon%2C+Nancy+R%3BChhabra%2C+Rajendra%3BBucher%2C+John+R&rft.aulast=Bordelon&rft.aufirst=Nancy&rft.date=2005-12-01&rft.volume=25&rft.issue=6&rft.spage=514&rft.isbn=&rft.btitle=&rft.title=Journal+of+Applied+Toxicology&rft.issn=0260437X&rft_id=info:doi/10.1002%2Fjat.1087
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-08-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Skin; Genotoxicity; Bone marrow; Laboratory animals; Carcinogens; Toxicity; Spectroscopy; Benzene; Carcinogenicity; Reviews; Liver; Metabolism; Aniline
DO  - http://dx.doi.org/10.1002/jat.1087
ER  - 



TY  - JOUR
T1  - n-Alkyl glucopyranosides completely inhibit ultrasound-induced cytolysis
AN  - 19467651; 7983929
AB  - The mechanism(s) responsible for sudden cytolysis observed when cells are exposed to ultrasound could be mechanical and/or free radical in nature. Free radical reactions are initiated in the core and in the interfacial regions of collapsing acoustic cavitation bubbles. Because cyclic sugars are known to inhibit free radical chain reactions, we investigated the effects of n-alkyl- beta -d-glucopyranosides of varying hydrophobicity on ultrasound (1.057 MHz)-induced cytolysis of HL-60 cells in vitro. n-Alkyl glucopyranosides with hexyl- (5 mM), heptyl- (3 mM), or octyl- (2 mM) n-alkyl chains protected 100% of the cell population from ultrasound-induced cytolysis under a range of conditions that resulted in 35 to 100% cytolysis in the absence of glucopyranosides. The protected cell populations also possessed long-term reproductive viability. However, the hydrophilic methyl- beta -d-glucopyranoside could not protect cells, even up to a concentration of 30 mM. Furthermore, none of the glucopyranosides could prevent cytolysis of cells from a mechanically induced shear stress. Spin trapping and electron spin resonance experiments confirmed the presence of inertial cavitation in cell suspensions both in the presence and in the absence of the surfactants. It is concluded that surface-active glucopyranosides efficiently quench cytotoxic radicals and/or their precursors at the gas/solution interface of collapsing cavitation bubbles.
JF  - Free Radical Biology and Medicine
AU  - Sostaric, Joe Z
AU  - Miyoshi, Norio
AU  - Riesz, Peter
AU  - Degraff, William G
AU  - Mitchell, James B
AD  - Radiation Biology Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892-1002, USA, sostaric.2@osu.edu
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1539
EP  - 1548
PB  - Elsevier Science, The Boulevard Langford Lane Kidlington Oxford OX5 1GB UK, [mailto:nlinfo-f@elsevier.nl], [URL:http://www.elsevier.nl]
VL  - 39
IS  - 12
SN  - 0891-5849, 0891-5849
KW  - Biotechnology and Bioengineering Abstracts
KW  - Free radicals
KW  - EKW ESR
KW  - Sonoporation
KW  - Sonophoresis
KW  - Sonochemistry
KW  - Radiolysis
KW  - HIFU
KW  - Ultrasound
KW  - Surfactants
KW  - HL-60
KW  - Protection
KW  - Sonoprotection
KW  - Cytolysis
KW  - Sonolysis
KW  - Sonication
KW  - Glucopyranoside
KW  - Sugars
KW  - Bioreactors
KW  - Cell suspensions
KW  - Sugar
KW  - Acoustics
KW  - Hydrophobicity
KW  - Trapping
KW  - Mechanical stimuli
KW  - Cytotoxicity
KW  - Cavitation
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19467651?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Free+Radical+Biology+and+Medicine&rft.atitle=n-Alkyl+glucopyranosides+completely+inhibit+ultrasound-induced+cytolysis&rft.au=Sostaric%2C+Joe+Z%3BMiyoshi%2C+Norio%3BRiesz%2C+Peter%3BDegraff%2C+William+G%3BMitchell%2C+James+B&rft.aulast=Sostaric&rft.aufirst=Joe&rft.date=2005-12-01&rft.volume=39&rft.issue=12&rft.spage=1539&rft.isbn=&rft.btitle=&rft.title=Free+Radical+Biology+and+Medicine&rft.issn=08915849&rft_id=info:doi/10.1016%2Fj.freeradbiomed.2005.07.020
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-01-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Cell suspensions; Sugar; Cytotoxicity; Cavitation; Acoustics; Free radicals; Cytolysis; Hydrophobicity; Trapping; Surfactants; Ultrasound; Mechanical stimuli
DO  - http://dx.doi.org/10.1016/j.freeradbiomed.2005.07.020
ER  - 



TY  - JOUR
T1  - Arginine-rich cell penetrating peptides: from endosomal uptake to nuclear delivery
AN  - 19440765; 6706627
AB  - Delivery of macromolecules into living cells by arginine-rich cell penetrating peptides (AR-CPPs) is an important new avenue for the development of novel therapeutic strategies. However, to date the mechanism of this delivery remains elusive. Recent data implicate endocytosis in the internalization of AR-CPPs and their macromolecular cargo and also indicate limited delivery of macromolecules into the cell cytoplasm and nucleus. Different types of endocytosis - clathrin-dependent endocytosis, raft/caveolin-dependent endocytosis and macropinocytosis - are all implicated in the uptake of AR-CPPs and their cargo into different cells. Cationic AR-CPPs dramatically increase uptake of conjugated molecules through efficient binding to surface proteogly-cans. Whether this increase in binding can assure delivery of a sufficient amount of functionally active macromolecules into the cytoplasm and nucleus or whether there is a specific mechanism by which AR-CPPs facilitate the escape of conjugated cargo from endosomes remains to be understood.
JF  - Cellular and Molecular Life Sciences
AU  - Melikov, K
AU  - Chernomordik, LV
AD  - Section on Membrane Biology, Laboratory of Cellular and Molecular Biophysics, NICHD, National Institutes of Health, Bldg.10/Rm.10D05, 10 Center Drive, Bethesda, Maryland 20892-1855 (USA), melikovk@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 2739
EP  - 2749
VL  - 62
IS  - 23
SN  - 1420-682X, 1420-682X
KW  - Biotechnology and Bioengineering Abstracts
KW  - Endocytosis
KW  - endosomes
KW  - Macromolecules
KW  - Cytoplasm
KW  - Nuclei
KW  - W 30915:Pharmaceuticals & Vaccines
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19440765?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cellular+and+Molecular+Life+Sciences&rft.atitle=Arginine-rich+cell+penetrating+peptides%3A+from+endosomal+uptake+to+nuclear+delivery&rft.au=Melikov%2C+K%3BChernomordik%2C+LV&rft.aulast=Melikov&rft.aufirst=K&rft.date=2005-12-01&rft.volume=62&rft.issue=23&rft.spage=2739&rft.isbn=&rft.btitle=&rft.title=Cellular+and+Molecular+Life+Sciences&rft.issn=1420682X&rft_id=info:doi/10.1007%2Fs00018-005-5293-y
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Endocytosis; Macromolecules; Nuclei; Cytoplasm; endosomes
DO  - http://dx.doi.org/10.1007/s00018-005-5293-y
ER  - 



TY  - JOUR
T1  - Finding New Tricks For Old Drugs: An Efficient Route For Public-Sector Drug Discovery
AN  - 19427848; 6702402
AB  - With the annotation of the human genome approaching completion, public- sector researchers-spurred in part by various National Institutes of Health Roadmap Initiatives-have become increasingly engaged in drug discovery and development efforts. Although large and diverse chemical libraries of 'drug- like' compounds can be readily screened to yield chemically novel scaffolds, transforming these 'chemical probes' into drugs is a daunting endeavour. A more efficient approach involves screening libraries of approved and off-patent medications; both phenotypic- and molecular target-based screening of 'old drugs' can readily yield compounds that could be immediately used in clinical trials. Using case studies, we describe how this approach has rapidly identified candidate medications suitable for clinical trials in disorders such as progressive multifocal leukoencephalopathy and amyotrophic lateral sclerosis. This approach has also led to the discovery of the molecular targets responsible for serious drug side effects, thereby allowing efficient 'counter-screening' to avoid these side effects.
JF  - Nature Reviews: Drug Discovery
AU  - O'Connor, Kerry A
AU  - Roth, Bryan L
AD  - Departments of Biochemistry, Psychiatry, Neurosciences, Comprehensive Cancer Center and National Institute of Mental Health Psychoactive Drug Screening Program, 2109 Adelbert Road, Case Western Reserve University Medical School, Cleveland, Ohio 44106, USA., bryan.roth@case.edu
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1005
EP  - 1014
PB  - Nature Publishing Group, The Macmillan Building 4 Crinan Street London N1 9XW UK, [mailto:feedback@nature.com], [URL:http://www.nature.com/]
VL  - 4
IS  - 12
SN  - 1474-1776, 1474-1776
KW  - Biotechnology and Bioengineering Abstracts
KW  - Genomes
KW  - Drug discovery
KW  - Amyotrophic lateral sclerosis
KW  - DNA probes
KW  - Reviews
KW  - Drug screening
KW  - Progressive multifocal leukoencephalopathy
KW  - Clinical trials
KW  - Drugs
KW  - scaffolds
KW  - Side effects
KW  - W 30915:Pharmaceuticals & Vaccines
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19427848?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Nature+Reviews%3A+Drug+Discovery&rft.atitle=Finding+New+Tricks+For+Old+Drugs%3A+An+Efficient+Route+For+Public-Sector+Drug+Discovery&rft.au=O%27Connor%2C+Kerry+A%3BRoth%2C+Bryan+L&rft.aulast=O%27Connor&rft.aufirst=Kerry&rft.date=2005-12-01&rft.volume=4&rft.issue=12&rft.spage=1005&rft.isbn=&rft.btitle=&rft.title=Nature+Reviews%3A+Drug+Discovery&rft.issn=14741776&rft_id=info:doi/10.1038%2Fnrd1900
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Drugs; Drug discovery; Side effects; Clinical trials; Reviews; Genomes; Drug screening; Progressive multifocal leukoencephalopathy; Amyotrophic lateral sclerosis; scaffolds; DNA probes
DO  - http://dx.doi.org/10.1038/nrd1900
ER  - 



TY  - JOUR
T1  - Staphylococcal Protein A Deletes B-1a and Marginal Zone B Lymphocytes Expressing Human Immunoglobulins: An Immune Evasion Mechanism
AN  - 19379852; 7144053
AB  - Protein A (SpA) of Staphylococcus aureus is endowed with the capacity to interact with the H chain variable region (V sub(H)) of human Abs and to target >40% of B lymphocytes. To investigate whether this property represents a virulence factor and to determine the in vivo consequences of the confrontation of SpA with B lymphocytes, we used transgenic mice expressing fully human Abs. We found that administration of soluble SpA reduces B-1a lymphocytes of the peritoneal cavity and marginal zone B lymphocytes of the spleen, resulting in a markedly deficient type 2 humoral response. Single-cell PCR analysis and sequencing of the Ab V sub(H) gene repertoire revealed a significant reduction of V sub(H)3 super(+) marginal zone B cells. Since the two B lymphocyte subsets targeted are involved in innate immune functions, our data suggest that crippling of humoral immunity by S. aureus represents an immune evasion mechanism that may aggravate recurrent infections.
JF  - Journal of Immunology
AU  - Viau, Muriel
AU  - Longo, Nancy S
AU  - Lipsky, Peter E
AU  - Zouali, Moncef
AD  - Institut National de Sante et de Recherche Medicale Unite 430, Immunopathologie Humaine, Paris, France. National Institute of Arthritis and Musculoskeletal and Skin Diseases, Bethesda, MD 20892
Y1  - 2005/12/01/
PY  - 2005
DA  - 2005 Dec 01
SP  - 7719
EP  - 7727
PB  - American Association of Immunologists, 9650 Rockville Pike Bethesda MD 20814-3998 USA, [URL:http://www.jimmunol.org/]
VL  - 175
IS  - 11
SN  - 0022-1767, 0022-1767
KW  - Virology & AIDS Abstracts; Microbiology Abstracts B: Bacteriology; Immunology Abstracts
KW  - Data processing
KW  - virulence factors
KW  - Lymphocytes B
KW  - protein A
KW  - Peritoneum
KW  - Spleen
KW  - Transgenic mice
KW  - Immunity (humoral)
KW  - Polymerase chain reaction
KW  - Recurrent infection
KW  - Immune response
KW  - Staphylococcus aureus
KW  - Immune response (humoral)
KW  - Immunoglobulins
KW  - Variable region
KW  - V 22350:Immunology
KW  - J 02350:Immunology
KW  - F 06910:Microorganisms & Parasites
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19379852?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Immunology&rft.atitle=Staphylococcal+Protein+A+Deletes+B-1a+and+Marginal+Zone+B+Lymphocytes+Expressing+Human+Immunoglobulins%3A+An+Immune+Evasion+Mechanism&rft.au=Viau%2C+Muriel%3BLongo%2C+Nancy+S%3BLipsky%2C+Peter+E%3BZouali%2C+Moncef&rft.aulast=Viau&rft.aufirst=Muriel&rft.date=2005-12-01&rft.volume=175&rft.issue=11&rft.spage=7719&rft.isbn=&rft.btitle=&rft.title=Journal+of+Immunology&rft.issn=00221767&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Data processing; virulence factors; Lymphocytes B; protein A; Peritoneum; Spleen; Transgenic mice; Immunity (humoral); Polymerase chain reaction; Recurrent infection; Immune response; Immune response (humoral); Variable region; Immunoglobulins; Staphylococcus aureus
ER  - 



TY  - JOUR
T1  - Plant-Based Vaccine: Mice Immunized with Chloroplast-Derived Anthrax Protective Antigen Survive Anthrax Lethal Toxin Challenge
AN  - 19379141; 7142842
AB  - The currently available human vaccine for anthrax, derived from the culture supernatant of Bacillus anthracis, contains the protective antigen (PA) and traces of the lethal and edema factors, which may contribute to adverse side effects associated with this vaccine. Therefore, an effective expression system that can provide a clean, safe, and efficacious vaccine is required. In an effort to produce anthrax vaccine in large quantities and free of extraneous bacterial contaminants, PA was expressed in transgenic tobacco chloroplasts by inserting the pagA gene into the chloroplast genome. Chloroplast integration of the pagA gene was confirmed by PCR and Southern analysis. Mature leaves grown under continuous illumination contained PA as up to 14.2% of the total soluble protein. Cytotoxicity measurements in macrophage lysis assays showed that chloroplast-derived PA was equal in potency to PA produced in B. anthracis. Subcutaneous immunization of mice with partially purified chloroplast-derived or B. anthracis-derived PA with adjuvant yielded immunoglobulin G titers up to 1:320,000, and both groups of mice survived (100%) challenge with lethal doses of toxin. An average yield of about 150 mg of PA per plant should produce 360 million doses of a purified vaccine free of bacterial toxins edema factor and lethal factor from 1 acre of land. Such high expression levels without using fermenters and the immunoprotection offered by the chloroplast-derived PA should facilitate development of a cleaner and safer anthrax vaccine at a lower production cost. These results demonstrate the immunogenic and immunoprotective properties of plant-derived anthrax vaccine antigen.
JF  - Infection and Immunity
AU  - Koya, Vijay
AU  - Moayeri, Mahtab
AU  - Leppla, Stephen H
AU  - Daniell, Henry
AD  - Department of Molecular Biology and Microbiology, University of Central Florida, Biomolecular Science Building 20, Room 336, Orlando, Florida 32816-2364. Microbial Pathogenesis Section, National Institute of Allergy and Infectious Diseases, NIH, Building 30, Room 303, 30 Convent Dr., Bethesda, Maryland 20892-4349
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 8266
EP  - 8274
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 73
IS  - 12
SN  - 0019-9567, 0019-9567
KW  - Toxicology Abstracts; Microbiology Abstracts B: Bacteriology; Biotechnology and Bioengineering Abstracts; Immunology Abstracts
KW  - Genomes
KW  - Macrophages
KW  - Fermenters
KW  - Plant protection
KW  - Lethal factor
KW  - Edema
KW  - Adjuvants
KW  - Bacillus anthracis
KW  - Transgenic plants
KW  - Integration
KW  - Tobacco
KW  - Anthrax
KW  - Polymerase chain reaction
KW  - Anthrax lethal toxin
KW  - protective antigen
KW  - Leaves
KW  - Chloroplasts
KW  - Immunization
KW  - Cytotoxicity
KW  - Illumination
KW  - Immunogenicity
KW  - Immunoglobulin G
KW  - Plants
KW  - Vaccines
KW  - Contaminants
KW  - Side effects
KW  - Lethal dose
KW  - X 24380:Social Poisons & Drug Abuse
KW  - F 06905:Vaccines
KW  - W 30915:Pharmaceuticals & Vaccines
KW  - J 02350:Immunology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19379141?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Infection+and+Immunity&rft.atitle=Plant-Based+Vaccine%3A+Mice+Immunized+with+Chloroplast-Derived+Anthrax+Protective+Antigen+Survive+Anthrax+Lethal+Toxin+Challenge&rft.au=Koya%2C+Vijay%3BMoayeri%2C+Mahtab%3BLeppla%2C+Stephen+H%3BDaniell%2C+Henry&rft.aulast=Koya&rft.aufirst=Vijay&rft.date=2005-12-01&rft.volume=73&rft.issue=12&rft.spage=8266&rft.isbn=&rft.btitle=&rft.title=Infection+and+Immunity&rft.issn=00199567&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Macrophages; Genomes; Fermenters; Plant protection; Lethal factor; Edema; Adjuvants; Transgenic plants; Integration; Tobacco; Polymerase chain reaction; Anthrax; Anthrax lethal toxin; protective antigen; Leaves; Chloroplasts; Immunization; Cytotoxicity; Illumination; Immunogenicity; Plants; Immunoglobulin G; Vaccines; Contaminants; Side effects; Lethal dose; Bacillus anthracis
ER  - 



TY  - JOUR
T1  - Drinking Water and Dietary Sources of Nitrate and Nitrite and Risk of Glioma
AN  - 17481361; 6677734
AB  - Dietary nitrite has been associated with increased glioma risk; however, drinking water nitrate has not been extensively evaluated. We conducted a population-based case-control study of adult glioma in Nebraska. Water utility nitrate measurements were linked to residential water source histories. We computed average nitrate exposure over a 20-year period. A food frequency questionnaire was used to assess dietary nitrate and nitrite. Increasing quartiles of the average nitrate level in drinking water were not significantly associated with risk (adjusted odd ratios: 1.4, 1.2, 1.3). Risk was similar among those with both higher and lower intakes of vitamin C, an inhibitor of N-nitroso compound formation. Dietary nitrite intake was not associated with risk. Our study does not support a role for drinking water and dietary sources of nitrate and nitrite in risk of adult glioma.
JF  - Journal of Occupational and Environmental Medicine
AU  - Ward, M H
AU  - Heineman, E F
AU  - McComb, R D
AU  - Weisenburger, D D
AD  - Occupational and Environmental Epidemiology Branch, National Cancer Institute, 6120 Executive Blvd, EPS-8104, Bethesda, MD 20892-7240, USA, wardm@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1260
EP  - 1267
VL  - 47
IS  - 12
SN  - 1076-2752, 1076-2752
KW  - glioma
KW  - Water Resources Abstracts; Toxicology Abstracts; Risk Abstracts; Health & Safety Science Abstracts; Pollution Abstracts
KW  - Nitrate
KW  - Food
KW  - Intakes
KW  - Water quality
KW  - Dietary intake
KW  - Utilities
KW  - Public health
KW  - Drinking Water
KW  - History
KW  - Vitamins
KW  - Glioma
KW  - Nitrite
KW  - Nitrates
KW  - Ingestion
KW  - Ascorbic acid
KW  - Brain tumors
KW  - Risk
KW  - Foods
KW  - N-Nitroso compounds
KW  - Nitrites
KW  - USA, Nebraska
KW  - Drinking water
KW  - X 24120:Food, additives & contaminants
KW  - SW 3060:Water treatment and distribution
KW  - R2 23060:Medical and environmental health
KW  - H 12000:Epidemiology and Public Health
KW  - P 6000:TOXICOLOGY AND HEALTH
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17481361?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ariskabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Occupational+and+Environmental+Medicine&rft.atitle=Drinking+Water+and+Dietary+Sources+of+Nitrate+and+Nitrite+and+Risk+of+Glioma&rft.au=Ward%2C+M+H%3BHeineman%2C+E+F%3BMcComb%2C+R+D%3BWeisenburger%2C+D+D&rft.aulast=Ward&rft.aufirst=M&rft.date=2005-12-01&rft.volume=47&rft.issue=12&rft.spage=1260&rft.isbn=&rft.btitle=&rft.title=Journal+of+Occupational+and+Environmental+Medicine&rft.issn=10762752&rft_id=info:doi/10.1097%2F01.jom.0000184879.67736.ae
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-08-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Brain tumors; Nitrate; N-Nitroso compounds; Food; Glioma; Drinking water; Nitrite; Dietary intake; Ascorbic acid; Nitrites; Nitrates; Ingestion; Water quality; Public health; Risk; Foods; Drinking Water; History; Vitamins; Intakes; Utilities; USA, Nebraska
DO  - http://dx.doi.org/10.1097/01.jom.0000184879.67736.ae
ER  - 



TY  - JOUR
T1  - Metabolism and disposition of juglone in male F344 rats
AN  - 17474426; 6678353
AB  - The metabolism and disposition of super(14)C-labelled juglone in male F344 rats following oral, intravenous and dermal administration were studied. Approximately 40-50% of an oral dose (0.1 to 10 mg kg super(-1)) and less than 20% of the dermal dose (4 mg kg super(-1)) were absorbed within 24 h. Most of the oral dose was excreted in faeces and urine within 24 h and only 1-3% remained in the tissues. High concentrations of juglone-derived radioactivity were found in kidney for all three dosing routes. The accumulation in kidney can be attributed to covalent binding of juglone and/or metabolites to cytosolic protein. Five metabolites were identified in the urine of rats treated with an oral dose: 1,4,5-trihydroxynaphthalene di-glucuronide, 1,4,5-trihydroxynaphthalene mono-glucuronide mono-sulfate, 2-sulfo-2,3-dihydrojuglone, 4,8-dihydroxy-1-tetralone mono-glucuronide and 1,4,5-trihydroxynaphthalene mono-glucuronide. Liver microsomal incubations of juglone in the presence of NAD(P)H and UDP-glucuronic acid gave rise to two 1,4,5-trihydroxynaphthalene mono-glucuronides.
JF  - Xenobiotica
AU  - Chen, L-J
AU  - Lebetkin, E H
AU  - Burka, L T
AD  - Laboratory of Pharmacology and Chemistry, National Institute of Environmental Health Sciences, Research Triangle Park, NC, USA
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1019
EP  - 1034
VL  - 35
IS  - 10-11
SN  - 0049-8254, 0049-8254
KW  - Toxicology Abstracts
KW  - Intravenous administration
KW  - Skin
KW  - Urine
KW  - Kidney
KW  - Liver
KW  - Metabolites
KW  - Disposition
KW  - Radioactivity
KW  - Feces
KW  - Metabolism
KW  - X 24172:Plants
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17474426?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxicologyabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Xenobiotica&rft.atitle=Metabolism+and+disposition+of+juglone+in+male+F344+rats&rft.au=Chen%2C+L-J%3BLebetkin%2C+E+H%3BBurka%2C+L+T&rft.aulast=Chen&rft.aufirst=L-J&rft.date=2005-12-01&rft.volume=35&rft.issue=10-11&rft.spage=1019&rft.isbn=&rft.btitle=&rft.title=Xenobiotica&rft.issn=00498254&rft_id=info:doi/10.1080%2F00498250500356621
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Intravenous administration; Skin; Urine; Liver; Kidney; Disposition; Metabolites; Radioactivity; Feces; Metabolism
DO  - http://dx.doi.org/10.1080/00498250500356621
ER  - 



TY  - JOUR
T1  - Resistance and functional training reduces knee extensor position fluctuations in functionally limited older adults
AN  - 17469256; 6654941
AB  - The purpose of this study was to determine the effect of task-specificity on knee extensor steadiness adaptations in functionally limited older adults. Twenty-four functionally limited older adults (74.6 plus or minus 7.6 years: 22 women, 2 men) completed a 10-week control period followed by 10 weeks (2 days/week) of resistance (RT), functional (FT) (practicing everyday tasks, i.e., chair rises) or functional + resistance (FRT) training, which featured both shortening and lengthening movements. During testing, subjects performed a steady isometric [10, 25, 50% of maximal voluntary contraction (MVC)] and shortening/lengthening (5, 30, 65% of MVC) knee extensor contractions. There were no steadiness (isometric, shortening or lengthening contractions) changes in the control period and no adaptations in isometric steadiness due to training. RT induced a 37% reduction in shortening fluctuations at 5% of MVC and 35% reduction in lengthening fluctuations at both 30% and 65% of MVC. FRT induced a 60% reduction in shortening fluctuations at 30% of MVC. No adaptations in dynamic steadiness were observed in the FT group. Further analysis indicated that those who were the least steady at baseline showed the greatest training effects during isometric (RT: R super(2)=0.25, FRT: R super(2)=0.49, FT: R super(2)=0.38), shortening (RT: R super(2)=0.36, FRT: R super(2)=0.36, FT: R super(2)=0.35) and lengthening (RT: r super(2)=0.29, FRT: r super(2)=0.44) contractions. In conclusion, steadiness improvements in groups performing resistance exercise, without a concomitant improvement in the FT group, supports a role for task-specificity in explaining steadiness adaptations, particularly for unsteady older adults.
JF  - European Journal of Applied Physiology
AU  - Manini, T M
AU  - Clark, B C
AU  - Tracy, B L
AU  - Burke, J
AU  - Ploutz-Snyder, L
AD  - Musculoskeletal Research Laboratory, Syracuse University, Syracuse, NY, USA, maninit@mail.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 436
EP  - 446
PB  - Springer-Verlag (New York), P.O. Box 2485 Secaucus NJ 07096-2485 USA, [mailto:orders@springer-ny.com], [URL:http://www.springer-ny.com/]
VL  - 95
IS  - 5-6
SN  - 1439-6319, 1439-6319
KW  - Physical Education Index
KW  - Exercise physiology
KW  - Men
KW  - Analysis
KW  - Women
KW  - Gerontology
KW  - Knees
KW  - Isometrics
KW  - Adults
KW  - Resistance exercise
KW  - Movement
KW  - PE 090:Sports Medicine & Exercise Sport Science
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aphysicaleducation&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=European+Journal+of+Applied+Physiology&rft.atitle=Resistance+and+functional+training+reduces+knee+extensor+position+fluctuations+in+functionally+limited+older+adults&rft.au=Manini%2C+T+M%3BClark%2C+B+C%3BTracy%2C+B+L%3BBurke%2C+J%3BPloutz-Snyder%2C+L&rft.aulast=Manini&rft.aufirst=T&rft.date=2005-12-01&rft.volume=95&rft.issue=5-6&rft.spage=436&rft.isbn=&rft.btitle=&rft.title=European+Journal+of+Applied+Physiology&rft.issn=14396319&rft_id=info:doi/10.1007%2Fs00421-005-0048-x
LA  - English
DB  - Physical Education Index
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Exercise physiology; Men; Analysis; Women; Knees; Gerontology; Isometrics; Resistance exercise; Adults; Movement
DO  - http://dx.doi.org/10.1007/s00421-005-0048-x
ER  - 



TY  - JOUR
T1  - ORIGINAL ARTICLE: Selective inhibition by rottlerin of macropinocytosis in monocyte-derived dendritic cells
AN  - 17447082; 6550918
AB  - We present here the analysis of fluid-phase endocytosis (FPE) in human blood monocytes and monocyte-derived dendritic cells (MDDC) facilitated by our serendipitous identification of rottlerin as an efficient inhibitor of dendritic cell FPE (IC sub(50) of 0.4 mu M). Rottlerin was found to be an excellent tool for FPE analysis: rapid-acting, irreversible and selective for FPE (as opposed to receptor-mediated endocytosis) at concentrations of 3 mu M and below. The inhibitory effect was not due to toxicity or visible change in membrane ruffles, but affects on cytoskeletal reorganization were evident in MDDC treated with relevant rottlerin concentrations during adhesion. A marked increase in FPE was observed in 1 hr interleukin (IL)-4 and granulocyte macrophage-colony stimulating factor (GM-CSF)-stimulated monocytes. Moreover, rottlerin inhibited the augmented FPE of 1-day cytokine treated monocytes and their augmented ability to induce T cell proliferative responses to tetanus toxoid. We conclude that rottlerin is a useful tool for investigating FPE and its functional importance.
JF  - Immunology
AU  - Sarkar, Kakali
AU  - Kruhlak, Michael J
AU  - Erlandsen, Stanley L
AU  - Shaw, Stephen
AD  - Experimental Immunology Branch, National Cancer Institute, National Institutes of Health, Bethesda, MD, sshaw@nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 513
EP  - 524
PB  - Blackwell Publishing Ltd., 9600 Garsington Road Oxford OX4 2DQ UK, [URL:http://www.blackwellpublishing.com]
VL  - 116
IS  - 4
SN  - 0019-2805, 0019-2805
KW  - rottlerin
KW  - Microbiology Abstracts B: Bacteriology; Immunology Abstracts
KW  - Interleukins
KW  - Granulocyte-macrophage colony-stimulating factor
KW  - Toxoids
KW  - Toxicity
KW  - Tetanus
KW  - Cytoskeleton
KW  - Blood
KW  - Endocytosis
KW  - Dendritic cells
KW  - Pinocytosis
KW  - Lymphocytes T
KW  - Vaccines
KW  - Monocytes
KW  - J 02350:Immunology
KW  - F 06622:Dendritic cells (plasmacytoid, monocyte-derived, Langerhans)
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17447082?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Immunology&rft.atitle=ORIGINAL+ARTICLE%3A+Selective+inhibition+by+rottlerin+of+macropinocytosis+in+monocyte-derived+dendritic+cells&rft.au=Sarkar%2C+Kakali%3BKruhlak%2C+Michael+J%3BErlandsen%2C+Stanley+L%3BShaw%2C+Stephen&rft.aulast=Sarkar&rft.aufirst=Kakali&rft.date=2005-12-01&rft.volume=116&rft.issue=4&rft.spage=513&rft.isbn=&rft.btitle=&rft.title=Immunology&rft.issn=00192805&rft_id=info:doi/10.1111%2Fj.1365-2567.2005.02253.x
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - SuppNotes - Figures, 10; references, 46.
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Granulocyte-macrophage colony-stimulating factor; Interleukins; Toxicity; Toxoids; Tetanus; Cytoskeleton; Dendritic cells; Endocytosis; Blood; Pinocytosis; Lymphocytes T; Monocytes; Vaccines
DO  - http://dx.doi.org/10.1111/j.1365-2567.2005.02253.x
ER  - 



TY  - JOUR
T1  - Bacterial metal detectors
AN  - 17438677; 6555897
AB  - Gram negative bacteria can detect environmental iron using outer membrane transporters (OMTs), and then regulate certain transport genes to take advantage of a readily available iron source. This process begins with an iron complex being bound by an OMT, and results in a signal being sent across the outer membrane, the periplasmic space, and the inner membrane, to a sigma factor that interacts with RNA polymerase and initiates transcription of relevant genes. Many of the interactions contributing to signalling have been observed by genetic and biochemical studies, but structural studies, which potentially show these interactions in molecular detail, have been limited. In this issue, Garcia-Herrero and Vogel describe an NMR structure of the periplasmic domain of an OMT, which had not been seen in previous X-ray crystal structures. This domain transmits the 'iron availability' signal to the next protein in the signal transduction cascade, which sits in the inner membrane and extends into the periplasm. The new structure extends our knowledge of transporter architecture and suggests how signalling may occur across the outer membrane.
JF  - Molecular Microbiology
AU  - Buchanan, Susan K
AD  - Laboratory of Molecular Biology, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Department of Health and Human Services, Bethesda, MD 20892, USA, skbuchan@helix.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1205
EP  - 1209
PB  - Blackwell Publishing Ltd., 9600 Garsington Road Oxford OX4 2DQ UK, [URL:http://www.blackwellpublishing.com]
VL  - 58
IS  - 5
SN  - 0950-382X, 0950-382X
KW  - Microbiology Abstracts A: Industrial & Applied Microbiology; Microbiology Abstracts B: Bacteriology
KW  - Bacteria
KW  - Metals
KW  - Periplasmic space
KW  - Heavy metals
KW  - Outer membranes
KW  - Transcription
KW  - DNA-directed RNA polymerase
KW  - Ionizing radiation
KW  - Gram-negative bacteria
KW  - Inner membranes
KW  - Crystal structure
KW  - N.M.R.
KW  - Sigma factor
KW  - Iron
KW  - periplasm
KW  - Signal transduction
KW  - J 02721:Cell cycle, morphology and motility
KW  - A 01450:Environmental Pollution & Waste Treatment
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - SuppNotes - Figures, 3; references, 14.
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Metals; Heavy metals; Periplasmic space; Outer membranes; Transcription; DNA-directed RNA polymerase; Inner membranes; Gram-negative bacteria; Ionizing radiation; Crystal structure; N.M.R.; Sigma factor; periplasm; Iron; Signal transduction; Bacteria
DO  - http://dx.doi.org/10.1111/j.1365-2958.2005.04904.x
ER  - 



TY  - JOUR
T1  - Differential cis-regulation of human versus mouse TERT gene expression in vivo: Identification of a human-specific repressive element
AN  - 17438513; 6578684
AB  - In vivo expression of human telomerase is significantly different from that of mouse telomerase. To assess the basis for this difference, a bacterial artificial chromosome clone containing the entire hTERT (human telomerase reverse transcriptase) gene was introduced in mice. In these transgenic mice, expression of the hTERT transgene was similar to that of endogenous hTERT in humans, rather than endogenous mTERT (mouse telomerase reverse transcriptase). In tissues and cells showing a striking difference in expression levels between hTERT in humans and mTERT in mice (i.e., liver, kidney, lung, uterus, and fibroblasts), expression of the hTERT transgene in transgenic mice was repressed, mimicking hTERT in humans. The transcriptional activity of the hTERT promoter was much lower than that of the mTERT promoter in mouse embryonic fibroblasts or human fibroblasts. Mutational analysis of the hTERT and mTERT promoters revealed that a nonconserved GC-box within the hTERT promoter was responsible for the human-specific repression. These results reveal that a difference in cis-regulation of transcription, rather than transacting transcription factors, is critical to species differences in tissue-specific TERT expression. Our data also suggest that the GC-box-mediated, human-specific mechanism for TERT repression is impaired in human cancers. This study represents a detailed characterization of the functional difference in a gene promoter of mice versus humans and provides not only important insight into species-specific regulation of telomerase and telomeres but also an experimental basis for generating mice humanized for telomerase enzyme and its pattern of expression.
JF  - Proceedings of the National Academy of Sciences, USA
AU  - Horikawa, Izumi
AU  - Chiang, YJeffrey
AU  - Patterson, Tricia
AU  - Feigenbaum, Lionel
AU  - Leem, Sun-Hee
AU  - Michishita, Eriko
AU  - Larionov, Vladimir
AU  - Hodes, Richard J
AU  - Barrett, JCarl
AD  - Laboratory of Biosystems and Cancer and Experimental Immunology Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 18437
EP  - 18442
PB  - National Academy of Sciences, 2101 Constitution Ave. Washington DC 20418 USA
VL  - 102
IS  - 51
SN  - 0027-8424, 0027-8424
KW  - mice
KW  - Genetics Abstracts; Microbiology Abstracts B: Bacteriology; Oncogenes & Growth Factors Abstracts; Biochemistry Abstracts 2: Nucleic Acids
KW  - Mimicry
KW  - Uterus
KW  - Data processing
KW  - Transgenes
KW  - Enzymes
KW  - telomerase reverse transcriptase
KW  - Transgenic mice
KW  - Cancer
KW  - Fibroblasts
KW  - Gene expression
KW  - Bacterial artificial chromosomes
KW  - Telomeres
KW  - Promoters
KW  - Lung
KW  - Transcription factors
KW  - Embryo fibroblasts
KW  - Liver
KW  - Kidney
KW  - Embryos
KW  - Telomerase reverse transcriptase
KW  - J 02310:Genetics & Taxonomy
KW  - B 26248:DNA repair
KW  - N 14045:Transcriptional regulation
KW  - G 07770:Bacteria
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Proceedings+of+the+National+Academy+of+Sciences%2C+USA&rft.atitle=Differential+cis-regulation+of+human+versus+mouse+TERT+gene+expression+in+vivo%3A+Identification+of+a+human-specific+repressive+element&rft.au=Horikawa%2C+Izumi%3BChiang%2C+YJeffrey%3BPatterson%2C+Tricia%3BFeigenbaum%2C+Lionel%3BLeem%2C+Sun-Hee%3BMichishita%2C+Eriko%3BLarionov%2C+Vladimir%3BHodes%2C+Richard+J%3BBarrett%2C+JCarl&rft.aulast=Horikawa&rft.aufirst=Izumi&rft.date=2005-12-01&rft.volume=102&rft.issue=51&rft.spage=18437&rft.isbn=&rft.btitle=&rft.title=Proceedings+of+the+National+Academy+of+Sciences%2C+USA&rft.issn=00278424&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-04-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Mimicry; Uterus; Data processing; Transgenes; Enzymes; telomerase reverse transcriptase; Transgenic mice; Cancer; Fibroblasts; Bacterial artificial chromosomes; Gene expression; Promoters; Telomeres; Lung; Transcription factors; Embryo fibroblasts; Kidney; Liver; Embryos; Telomerase reverse transcriptase
ER  - 



TY  - JOUR
T1  - Cocaine-induced CREB phosphorylation in nucleus accumbens of cocaine-sensitized rats is enabled by enhanced activation of extracellular signal-related kinase, but not protein kinase A
AN  - 17435276; 6552992
AB  - Repeated cocaine administration to rats outside their home cages sensitizes the behavioral effects of the drug, and enhances induction of the immediate early gene product Fos in nucleus accumbens. We hypothesized that the same treatment regimen would also enhance cocaine-induced activation of intracellular signaling kinases that phosphorylate cyclic AMP-regulated element-binding protein (CREB), an important mediator of c-fos transcription. Phosphorylation levels of extracellular signal-regulated kinase (ERK)-mitogen-activated protein kinase (MAPK), calcium-calmodulin kinases (CaMKs) II and IV, and CREB were used to assess endogenous functional activity of these signaling molecules in rats behaviorally sensitized outside their home cages. Protein kinase A (PKA)-specific phosphorylation of Ser845 in the alpha -amino-3-hydroxy-5-methylisoxazole-4-propionate (AMPA) receptor subunit GluR1 was used to assess endogenous functional activity of PKA. Using western blots and immunohistochemistry, we detected cocaine-induced CREB phosphorylation after repeated cocaine administration, but not after repeated saline administration. Using western blots and MAPK activity assays, we found that cocaine-induced phosphorylation and activation of ERK, but not of CaMKs II or IV or GluR1, was augmented in nucleus accumbens of cocaine-sensitized rats. Unilateral infusions of the MAPK kinase inhibitor U0126 into nucleus accumbens attenuated cocaine-induced ERK and CREB phosphorylation in cocaine-sensitized rats. In contrast, unilateral infusions of the PKA inhibitor Rp-isomer of adenosine-3',5'-cyclicmonophosphorothioate (Rp-cAMPs) did not affect cocaine-induced CREB phosphorylation. Therefore, enhanced activation of ERK, but not PKA, enables and mediates cocaine-induced CREB phosphorylation in nucleus accumbens of rats that are sensitized by repeated cocaine administration outside their home cages.
JF  - Journal of Neurochemistry
AU  - Mattson, Brandi J
AU  - Bossert, Jennifer M
AU  - Simmons, Danielle E
AU  - Nozaki, Naohito
AU  - Nagarkar, Deepti
AU  - Kreuter, Justin D
AU  - Hope, Bruce T
AD  - Behavioral Neuroscience Branch, Intramural Research Program, National Institute on Drug Abuse, National Institutes of Health, Department of Health and Human Services, Baltimore, Maryland, USA, bhope@intra.nida.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1481
EP  - 1494
PB  - Blackwell Publishing Ltd., 9600 Garsington Road Oxford OX4 2DQ UK, [URL:http://www.blackwellpublishing.com]
VL  - 95
IS  - 5
SN  - 0022-3042, 0022-3042
KW  - rats
KW  - Toxicology Abstracts; CSA Neurosciences Abstracts
KW  - Intracellular signalling
KW  - Western blotting
KW  - Nucleus accumbens
KW  - MAP kinase
KW  - Protein kinase A
KW  - Transcription
KW  - c-Fos protein
KW  - Drug abuse
KW  - alpha -Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptors
KW  - Glutamic acid receptors (ionotropic)
KW  - Fos protein
KW  - Extracellular signal-regulated kinase
KW  - Phosphorylation
KW  - alpha -Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid
KW  - Cocaine
KW  - Ca super(2+)/calmodulin-dependent protein kinase II
KW  - Immunohistochemistry
KW  - Cyclic AMP response element-binding protein
KW  - Signal transduction
KW  - N3 11106:Neurobiology of drug abuse
KW  - X 24180:Social poisons & drug abuse
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-06-01
N1  - SuppNotes - Figures, 9; references, 65.
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Nucleus accumbens; Western blotting; Intracellular signalling; Protein kinase A; MAP kinase; Transcription; c-Fos protein; Drug abuse; alpha -Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptors; Glutamic acid receptors (ionotropic); Fos protein; Extracellular signal-regulated kinase; Phosphorylation; alpha -Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid; Cocaine; Immunohistochemistry; Ca super(2+)/calmodulin-dependent protein kinase II; Signal transduction; Cyclic AMP response element-binding protein
DO  - http://dx.doi.org/10.1111/j.1471-4159.2005.03500.x
ER  - 



TY  - JOUR
T1  - Crystal structures of T cell receptor beta chains related to rheumatoid arthritis
AN  - 17429726; 6581427
AB  - The crystal structures of the V beta 17 super(+) beta chains of two human T cell receptors (TCRs), originally derived from the synovial fluid (SF4) and tissue (C5-1) of a patient with rheumatoid arthritis (RA), have been determined in native (SF4) and mutant (C5-1 sub(F104 arrow right Y/C187 arrow right S)) forms, respectively. These TCR beta chains form homo-dimers in solution and in crystals. Structural comparison reveals that the main-chain conformations in the CDR regions of the C5-1 and SF4 V beta 17 closely resemble those of a V beta 17 JM22 in a bound form; however, the CDR3 region shows different conformations among these three V beta 17 structures. At the side-chain level, conformational differences were observed at the CDR2 regions between our two ligand-free forms and the bound JM22 form. Other significant differences were observed at the V beta regions 8-12, 40-44, and 82-88 between C5-1/SF4 and JM22 V beta 17, implying that there is considerable variability in the structures of very similar beta chains. Structural alignments also reveal a considerable variation in the V beta -C beta associations, and this may affect ligand recognition. The crystal structures also provide insights into the structure basis of T cell recognition of Mycoplasma arthritidis mitogen (MAM), a superantigen that may be implicated in the development of human RA. Structural comparisons of the V beta domains of known TCR structures indicate that there are significant similarities among V beta regions that are MAM-reactive, whereas there appear to be significant structural differences among those V beta regions that lack MAM-reactivity. It further reveals that CDR2 and framework region (FR) 3 are likely to account for the binding of TCR to MAM.
JF  - Protein Science
AU  - Li, Hongmin
AU  - Van Vranken, Sandra
AU  - Zhao, Yiwei
AU  - Li, Zhong
AU  - Guo, Yi
AU  - Eisele, Leslie
AU  - Li, Yixin
AD  - Wadsworth Center, New York State Department of Health, and Department of Biomedical Sciences, School of Public Health, University at Albany, State University of New York, Empire State Plaza, Albany, New York 12201-0509, USA. Stroke Branch, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892, USA
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 3025
EP  - 3038
PB  - Cold Spring Harbor Laboratory Press, [mailto:cshpress@cshl.org], [URL:http://www.cshl.org/]
VL  - 14
IS  - 12
SN  - 0961-8368, 0961-8368
KW  - Microbiology Abstracts B: Bacteriology
KW  - complementarity-determining region 3
KW  - Rheumatoid arthritis
KW  - Superantigens
KW  - Synovial fluid
KW  - double prime T-cell receptor
KW  - Mycoplasma arthritidis
KW  - Crystal structure
KW  - Lymphocytes T
KW  - Proteins
KW  - Mitogens
KW  - Crystals
KW  - J 02727:Amino acids, peptides and proteins
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17429726?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Protein+Science&rft.atitle=Crystal+structures+of+T+cell+receptor+beta+chains+related+to+rheumatoid+arthritis&rft.au=Li%2C+Hongmin%3BVan+Vranken%2C+Sandra%3BZhao%2C+Yiwei%3BLi%2C+Zhong%3BGuo%2C+Yi%3BEisele%2C+Leslie%3BLi%2C+Yixin&rft.aulast=Li&rft.aufirst=Hongmin&rft.date=2005-12-01&rft.volume=14&rft.issue=12&rft.spage=3025&rft.isbn=&rft.btitle=&rft.title=Protein+Science&rft.issn=09618368&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-06-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - complementarity-determining region 3; Superantigens; Rheumatoid arthritis; Synovial fluid; double prime T-cell receptor; Lymphocytes T; Crystal structure; Mitogens; Proteins; Crystals; Mycoplasma arthritidis
ER  - 



TY  - JOUR
T1  - TLR9 regulates Th1 responses and cooperates with TLR2 in mediating optimal resistance to Mycobacterium tuberculosis
AN  - 17428442; 6577859
AB  - To investigate the role of Toll-like receptor (TLR)9 in the immune response to mycobacteria as well as its cooperation with TLR2, a receptor known to be triggered by several major mycobacterial ligands, we analyzed the resistance of TLR9 super(-/-) as well as TLR2/9 double knockout mice to aerosol infection with Mycobacterium tuberculosis. Infected TLR9 super(-/-) but not TLR2 super(-/-) mice displayed defective mycobacteria-induced interleukin (IL)-12p40 and interferon (IFN)- gamma responses in vivo, but in common with TLR2 super(-/-) animals, the TLR9 super(-/-) mice exhibited only minor reductions in acute resistance to low dose pathogen challenge. When compared with either of the single TLR-deficient animals, TLR2/9 super(-/-) mice displayed markedly enhanced susceptibility to infection in association with combined defects in proinflammatory cytokine production in vitro, IFN- gamma recall responses ex vivo, and altered pulmonary pathology. Cooperation between TLR9 and TLR2 was also evident at the level of the in vitro response to live M. tuberculosis, where dendritic cells and macrophages from TLR2/9 super(-/-) mice exhibited a greater defect in IL-12 response than the equivalent cell populations from single TLR9-deficient animals. These findings reveal a previously unappreciated role for TLR9 in the host response to M. tuberculosis and illustrate TLR collaboration in host resistance to a major human pathogen.
JF  - Journal of Experimental Medicine
AU  - Bafica, Andre
AU  - Scanga, Charles A
AU  - Feng, Carl G
AU  - Leifer, Cynthia
AU  - Cheever, Allen
AU  - Sher, Alan
AD  - Immunobiology Section, Laboratory of Parasitic Diseases. Experimental Immunology Branch, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892. Laboratorio de Imunorregulacao e Microbiologia, Centro de Pesquisas Goncalo Moniz, FIOCRUZ, Bahia 40296-710, Brazil. Biomedical Research Institute, Rockville, MD 20852
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 1715
EP  - 1724
PB  - Rockefeller University Press, 1114 First Avenue New York NY 10021-8325 USA, [mailto:Bruce.Lyons@rockefeller.edu], [URL:http://www.rockefeller.edu/rupress]
VL  - 202
IS  - 12
SN  - 0022-1007, 0022-1007
KW  - Microbiology Abstracts B: Bacteriology; Immunology Abstracts
KW  - gamma -Interferon
KW  - Aerosols
KW  - TLR9 protein
KW  - TLR2 protein
KW  - Pathogens
KW  - Infection
KW  - Inflammation
KW  - Interleukin 12
KW  - Dendritic cells
KW  - Tuberculosis
KW  - Toll-like receptors
KW  - Mycobacterium tuberculosis
KW  - J 02833:Immune response and immune mechanisms
KW  - F 06106:Bacteria
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17428442?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Experimental+Medicine&rft.atitle=TLR9+regulates+Th1+responses+and+cooperates+with+TLR2+in+mediating+optimal+resistance+to+Mycobacterium+tuberculosis&rft.au=Bafica%2C+Andre%3BScanga%2C+Charles+A%3BFeng%2C+Carl+G%3BLeifer%2C+Cynthia%3BCheever%2C+Allen%3BSher%2C+Alan&rft.aulast=Bafica&rft.aufirst=Andre&rft.date=2005-12-01&rft.volume=202&rft.issue=12&rft.spage=1715&rft.isbn=&rft.btitle=&rft.title=Journal+of+Experimental+Medicine&rft.issn=00221007&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Dendritic cells; Interleukin 12; gamma -Interferon; Aerosols; TLR9 protein; TLR2 protein; Tuberculosis; Pathogens; Infection; Toll-like receptors; Inflammation; Mycobacterium tuberculosis
ER  - 



TY  - JOUR
T1  - The Genome of Bacteriophage K1F, a T7-Like Phage That Has Acquired the Ability To Replicate on K1 Strains of Escherichia coli
AN  - 17424341; 6577046
AB  - Bacteriophage K1F specifically infects Escherichia coli strains that produce the K1 polysaccharide capsule. Like several other K1 capsule-specific phages, K1F encodes an endo-neuraminidase (endosialidase) that is part of the tail structure which allows the phage to recognize and degrade the polysaccharide capsule. The complete nucleotide sequence of the K1F genome reveals that it is closely related to bacteriophage T7 in both genome organization and sequence similarity. The most striking difference between the two phages is that K1F encodes the endosialidase in the analogous position to the T7 tail fiber gene. This is in contrast with bacteriophage K1-5, another K1-specific phage, which encodes a very similar endosialidase which is part of a tail gene "module" at the end of the phage genome. It appears that diverse phages have acquired endosialidase genes by horizontal gene transfer and that these genes or gene products have adapted to different genome and virion architectures.
JF  - Journal of Bacteriology
AU  - Scholl, Dean
AU  - Merril, Carl
AD  - National Institute of Mental Health, National Institutes of Health, Bethesda, Maryland 20892
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 8499
EP  - 8503
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 187
IS  - 24
SN  - 0021-9193, 0021-9193
KW  - Microbiology Abstracts B: Bacteriology; Genetics Abstracts; Virology & AIDS Abstracts
KW  - phage K1F
KW  - Phages
KW  - Virions
KW  - Endo- alpha -sialidase
KW  - Genomes
KW  - Tails
KW  - Nucleotide sequence
KW  - Polysaccharides
KW  - Genetic relationship
KW  - Gene transfer
KW  - Escherichia coli
KW  - Tail fibers
KW  - Genetic structure
KW  - G 07312:Phages
KW  - J 02750:Phage-host interactions
KW  - V 22070:Phage-host interactions including lysogeny & transduction
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17424341?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Bacteriology&rft.atitle=The+Genome+of+Bacteriophage+K1F%2C+a+T7-Like+Phage+That+Has+Acquired+the+Ability+To+Replicate+on+K1+Strains+of+Escherichia+coli&rft.au=Scholl%2C+Dean%3BMerril%2C+Carl&rft.aulast=Scholl&rft.aufirst=Dean&rft.date=2005-12-01&rft.volume=187&rft.issue=24&rft.spage=8499&rft.isbn=&rft.btitle=&rft.title=Journal+of+Bacteriology&rft.issn=00219193&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Genomes; Endo- alpha -sialidase; Virions; Genetic relationship; Phages; Tails; Gene transfer; Nucleotide sequence; Tail fibers; Polysaccharides; Genetic structure; phage K1F; Escherichia coli
ER  - 



TY  - JOUR
T1  - A detailed behavioral analysis of the acute motor effects of caffeine in the rat: involvement of adenosine A sub(1) and A sub(2A) receptors
AN  - 17205255; 6889206
AB  - Rationale: There is no consensus on the contribution of adenosine A sub(1) and A sub(2A) receptor blockade to motor-activating effects of caffeine. Objective: Our aim was to use a detailed and continuous observational method to compare the motor effects induced by caffeine with those induced by selective A sub(1) and A sub(2A) receptor antagonists. Methods: The behavioral repertoire induced by systemic administration of caffeine (3, 10, and 30 mg/kg), A sub(1) receptor antagonist 8-cyclopentyl-1,3-dimethylxanthine (CPT; 1.2, 4.8 and 7.2 mg/kg), and A sub(2A) receptor antagonist 3-(3-hydroxypropyl)-8-(m-methoxystyryl)-7-methyl-1-propargylxan thine phosphate disodium salt (MSX-3; 1, 3, and 10 mg/kg) was analyzed. The effects of pretreatment with the selective A sub(1) receptor agonist N super(6)-cyclopentyladenosine (CPA; 0.1 mg/g) and the selective A sub(2A) receptor agonist 2-p-(2-carboxyethyl)phenethylamino-5'-N-ethylcarboxyamidoad enosine (CGS 21680; 0.2 mg/kg) on the pattern of motor activation induced by caffeine, CPT, or MSX-3 were also examined. Results: The pattern of behavioral activation induced by caffeine was better mimicked by CPT than by MSX-3. Coadministration of CPT and MSX-3 gave different results depending on the dose and the type of behavioral response. CPA was more effective at decreasing the activating effects of caffeine and CPT than those of CGS 21680. On the other hand, CGS 21680 was more effective at decreasing the activating effects of MSX-3 than those of caffeine or CPT. Factor analysis revealed a complex three-dimensional behavioral profile for caffeine that was similar to the profile for CPT and was different from the profile for MSX-3. Conclusions: The results indicate a predominant role for A sub(1) receptors in the motor-activating effects of acutely administered caffeine.
JF  - Psychopharmacology
AU  - Antoniou, Katerina
AU  - Papadopoulou-Daifoti, Zeta
AU  - Hyphantis, Thomas
AU  - Papathanasiou, Georgia
AU  - Bekris, Efstathios
AU  - Marselos, Marios
AU  - Panlilio, Leigh
AU  - Mueller, Christa E
AU  - Goldberg, Steven R
AU  - Ferre, Sergi
AD  - Behavioral Neuroscience Branch, National Institute on Drug Abuse Intramural Research Program, National Institutes of Health, Department of Health and Human Services, Baltimore, MD, 21224, USA, sferre@intra.nida.nih.gov
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 154
EP  - 162
PB  - Springer-Verlag (Berlin), Heidelberger Platz 3 Berlin 14197 Germany, [mailto:subscriptions@springer.de], [URL:http://www.springer.de/]
VL  - 183
IS  - 2
SN  - 0033-3158, 0033-3158
KW  - Factor analysis
KW  - rats
KW  - CSA Neurosciences Abstracts; Animal Behavior Abstracts; Toxicology Abstracts
KW  - Motor activity
KW  - Caffeine
KW  - Adenosine A1 receptors
KW  - Adenosine A2A receptors
KW  - Y 25777:Mammals (excluding primates)
KW  - X 24180:Social poisons & drug abuse
KW  - N3 11139:Toxicological and psychoactive drug correlates
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxicologyabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Psychopharmacology&rft.atitle=A+detailed+behavioral+analysis+of+the+acute+motor+effects+of+caffeine+in+the+rat%3A+involvement+of+adenosine+A+sub%281%29+and+A+sub%282A%29+receptors&rft.au=Antoniou%2C+Katerina%3BPapadopoulou-Daifoti%2C+Zeta%3BHyphantis%2C+Thomas%3BPapathanasiou%2C+Georgia%3BBekris%2C+Efstathios%3BMarselos%2C+Marios%3BPanlilio%2C+Leigh%3BMueller%2C+Christa+E%3BGoldberg%2C+Steven+R%3BFerre%2C+Sergi&rft.aulast=Antoniou&rft.aufirst=Katerina&rft.date=2005-12-01&rft.volume=183&rft.issue=2&rft.spage=154&rft.isbn=&rft.btitle=&rft.title=Psychopharmacology&rft.issn=00333158&rft_id=info:doi/10.1007%2Fs00213-005-0173-6
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-09-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Motor activity; Adenosine A1 receptors; Caffeine; Adenosine A2A receptors
DO  - http://dx.doi.org/10.1007/s00213-005-0173-6
ER  - 



TY  - JOUR
T1  - Characterization of Both MTBE and BTEX in the Ambient Air of Night Markets in Southern Taiwan
AN  - 17135377; 6756488
AB  - To characterize concentrations of volatile organic compounds (VOCs) at the night markets in southern Taiwan, four representative night markets and one background location were selected for this study. The VOCs measured included methyl tertiary-butyl ether (MTBE) and BTEX (the acronym for benzene, toluene, ethylbenzene, and xylene). The results indicated that the measured concentrations of MTBE and BTEX were typically on the order of one to two times higher at night market level than at the background site. It is clear that the night market activities in all sampling sites affected the distribution of MTBE and BTEX. During non-night market activities, the average MTBE-BTEX ratios of Liu-Ho, Rui-Guang, Ping-Tung and Chao-Zhou were (13.9: 2.2: 10.1: 1.0: 6.1), (4.9: 3.8: 13.7: 1.0: 7.9), (10.3: 1.7: 8.2: 1.0: 3.9) and (87.4: 10: 46: 1.0: 9.1), respectively. However, during the night market activities, the average MTBE-BTEX ratios shifted to (27.4: 1.9: 21.9: 1.0: 4.3), (23.1: 3.9: 16.5: 1.0: 3.2), (38.6: 6.8: 30.1: 1.0: 14.9), and (38.6: 7.8: 24.3: 1.0: 5.1), respectively.
JF  - Aerosol and Air Quality Resarch
AU  - Hsieh, Lien-Te
AU  - Yang, His-Hsieh
AU  - Chen, Ho-Wen
AD  - Department of Environmental Engineering and Science, National Pingtung University of Science and Technology, Nei Pu 912, Ping Tung, Taiwan, Lthsieh@.mail.npust.edu.tw
Y1  - 2005/12//
PY  - 2005
DA  - Dec 2005
SP  - 154
EP  - 170
VL  - 5
IS  - 2
SN  - 1680-8584, 1680-8584
KW  - Meteorological & Geoastrophysical Abstracts; Pollution Abstracts
KW  - Taiwan
KW  - Aerosols
KW  - Atmospheric pollution
KW  - MTBE
KW  - Toluene
KW  - Acronyms
KW  - Air quality
KW  - Benzene
KW  - Xylene
KW  - Chemical speciation
KW  - Volatile organic compounds
KW  - M2 551.510.42:Air Pollution (551.510.42)
KW  - P 0000:AIR POLLUTION
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17135377?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Apollution&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Aerosol+and+Air+Quality+Resarch&rft.atitle=Characterization+of+Both+MTBE+and+BTEX+in+the+Ambient+Air+of+Night+Markets+in+Southern+Taiwan&rft.au=Hsieh%2C+Lien-Te%3BYang%2C+His-Hsieh%3BChen%2C+Ho-Wen&rft.aulast=Hsieh&rft.aufirst=Lien-Te&rft.date=2005-12-01&rft.volume=5&rft.issue=2&rft.spage=154&rft.isbn=&rft.btitle=&rft.title=Aerosol+and+Air+Quality+Resarch&rft.issn=16808584&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-09-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Atmospheric pollution; Acronyms; Air quality; Aerosols; Xylene; Toluene; Chemical speciation; MTBE; Benzene; Volatile organic compounds; Taiwan
ER  - 



TY  - JOUR
T1  - Post insult enriched housing improves the 8-arm radial maze performance but not the Morris water maze task in ventral subicular lesioned rats.
AN  - 68881836; 16324686
AB  - The present study attempted to evaluate the efficacy of enriched housing conditions in promoting behavioral recovery following subicular lesion. Rats with bilateral ibotenic acid lesions of ventral subiculum were exposed to either enriched housing conditions or standard housing for 6 h daily for 10 days. The performance of the lesioned rats reared in standard housing conditions was severely impaired in both 8-arm radial maze and water maze tasks. Lesioned rats exposed to enriched housing showed behavioral recovery in the 8-arm radial maze but not in the water maze. Our study suggests the possibility that recovery may be based on the functional demand of spatial tasks and may require more appropriate environmental stimulation.
JF  - Brain research
AU  - Bindu, B
AU  - Rekha, J
AU  - Kutty, Bindu M
AD  - Department of Neurophysiology, National Institute of Mental Health and Neuro Sciences (NIMHANS), P.O. Box No.2900, Hosur Road, Bangalore-560 029, India.
Y1  - 2005/11/30/
PY  - 2005
DA  - 2005 Nov 30
SP  - 121
EP  - 131
VL  - 1063
IS  - 2
SN  - 0006-8993, 0006-8993
KW  - Excitatory Amino Acid Agonists
KW  - 0
KW  - Ibotenic Acid
KW  - 2552-55-8
KW  - Index Medicus
KW  - Rats
KW  - Animals
KW  - Housing, Animal
KW  - Rats, Wistar
KW  - Recovery of Function -- physiology
KW  - Ibotenic Acid -- toxicity
KW  - Excitatory Amino Acid Agonists -- toxicity
KW  - Male
KW  - Environment Design
KW  - Maze Learning -- physiology
KW  - Nerve Degeneration -- physiopathology
KW  - Nerve Degeneration -- pathology
KW  - Nerve Degeneration -- chemically induced
KW  - Hippocampus -- physiopathology
KW  - Behavior, Animal -- physiology
KW  - Hippocampus -- pathology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68881836?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Brain+research&rft.atitle=Post+insult+enriched+housing+improves+the+8-arm+radial+maze+performance+but+not+the+Morris+water+maze+task+in+ventral+subicular+lesioned+rats.&rft.au=Bindu%2C+B%3BRekha%2C+J%3BKutty%2C+Bindu+M&rft.aulast=Bindu&rft.aufirst=B&rft.date=2005-11-30&rft.volume=1063&rft.issue=2&rft.spage=121&rft.isbn=&rft.btitle=&rft.title=Brain+research&rft.issn=00068993&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-15
N1  - Date created - 2005-12-12
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - A quantitative slot blot assay for host cell protein impurities in recombinant proteins expressed in E. coli
AN  - 17451757; 6637944
AB  - Residual host cell protein impurities in recombinant proteins intended for human use must be accurately quantified to help establish their safety. We describe a novel means of host cell protein quantitation, in which a slot blot system was employed together with scanning laser densitometry to allow picogram level sensitivity in detection of residual host cell proteins in unpurified fermentation products and final purified bulk samples. Two allelic forms of merozoite surface protein 1, a promising malaria vaccine candidate antigen currently undergoing evaluation in clinical trials, were expressed in E. coli as clinical grade proteins, refolded, and carried through several chromatographic purification steps. Several lots of these proteins were analyzed with this generic quantitative assay that uses rat polyclonal antibodies generated against soluble and insoluble E. coli proteins. The assay had a detection range of 6.1-1562 ng/mL, with a detection limit of 6.1 ng/mL, comparable to reported ELISA-based methods. This assay proved simple yet very sensitive and accurate, giving highly reproducible results. Thus it is suitable for evaluating host cell protein levels in clinical grade recombinant proteins expressed in E. coli. electrophoresis
JF  - Journal of Immunological Methods
AU  - Zhu, D
AU  - Saul, A J
AU  - Miles, A P
AD  - National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rockville, MD 20852, USA, dzhu@niaid.nih.gov
Y1  - 2005/11/30/
PY  - 2005
DA  - 2005 Nov 30
SP  - 40
EP  - 50
PB  - Elsevier B.V.
VL  - 306
IS  - 1-2
SN  - 0022-1759, 0022-1759
KW  - Microbiology Abstracts C: Algology, Mycology & Protozoology; Biotechnology and Bioengineering Abstracts; Medical and Pharmaceutical Biotechnology Abstracts; Immunology Abstracts
KW  - Enzyme-linked immunosorbent assay
KW  - Electrophoresis
KW  - Fermentation
KW  - Impurities
KW  - Merozoite surface protein 1
KW  - Malaria
KW  - protein purification
KW  - Clinical trials
KW  - Antibodies
KW  - Escherichia coli
KW  - Vaccines
KW  - Quantitation
KW  - Densitometry
KW  - K 03410:Animal Diseases
KW  - W 30965:Miscellaneous, Reviews
KW  - W3 33250:Methods: Others
KW  - F 06708:Other methods
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17451757?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Immunological+Methods&rft.atitle=A+quantitative+slot+blot+assay+for+host+cell+protein+impurities+in+recombinant+proteins+expressed+in+E.+coli&rft.au=Zhu%2C+D%3BSaul%2C+A+J%3BMiles%2C+A+P&rft.aulast=Zhu&rft.aufirst=D&rft.date=2005-11-30&rft.volume=306&rft.issue=1-2&rft.spage=40&rft.isbn=&rft.btitle=&rft.title=Journal+of+Immunological+Methods&rft.issn=00221759&rft_id=info:doi/10.1016%2Fj.jim.2005.07.021
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Enzyme-linked immunosorbent assay; Antibodies; Electrophoresis; Fermentation; Impurities; Malaria; Merozoite surface protein 1; Vaccines; protein purification; Quantitation; Clinical trials; Densitometry; Escherichia coli
DO  - http://dx.doi.org/10.1016/j.jim.2005.07.021
ER  - 



TY  - JOUR
T1  - Knockout of caspase-like gene, YCA1, abrogates apoptosis and elevates oxidized proteins in Saccharomyces cerevisiae.
AN  - 68845691; 16301538
AB  - In our previous study, we established that inhibition of apoptosis by the general caspase inhibitor is associated with an increase in the level of oxidized proteins in a multicellular eukaryotic system. To gain further insight into a potential link between oxidative stress and apoptosis, we carried out studies with Saccharomyces cerevisiae, which contains a gene (YCA1) that encodes synthesis of metacaspase, a homologue of the mammalian caspase, and is known to play a crucial role in the regulation of yeast apoptosis. We show that upon exposure to H(2)O(2), the accumulation of protein carbonyls is much greater in a Delta yca1 strain lacking the YCA1 gene than in the wild type and that apoptosis was abrogated in the Delta yca1 strain, whereas wild type underwent apoptosis as measured by externalization of phosphatidylserine and the display of TUNEL-positive nuclei. We also show that H(2)O(2)-mediated stress leads to up-regulation of the 20S proteasome and suppression of ubiquitinylation activities. These findings suggest that deletion of the apoptotic-related caspase-like gene leads to a large H(2)O(2)-dependent accumulation of oxidized proteins and up-regulation of 20S proteasome activity.
JF  - Proceedings of the National Academy of Sciences of the United States of America
AU  - Khan, Mohammed A S
AU  - Chock, P Boon
AU  - Stadtman, Earl R
AD  - Laboratory of Biochemistry, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, MD 20892-8012, USA.
Y1  - 2005/11/29/
PY  - 2005
DA  - 2005 Nov 29
SP  - 17326
EP  - 17331
VL  - 102
IS  - 48
SN  - 0027-8424, 0027-8424
KW  - Phosphatidylserines
KW  - 0
KW  - Saccharomyces cerevisiae Proteins
KW  - Hydrogen Peroxide
KW  - BBX060AN9V
KW  - Caspases
KW  - EC 3.4.22.-
KW  - MCA1 protein, S cerevisiae
KW  - Proteasome Endopeptidase Complex
KW  - EC 3.4.25.1
KW  - Index Medicus
KW  - Protein Carbonylation -- drug effects
KW  - Hydrogen Peroxide -- toxicity
KW  - In Situ Nick-End Labeling
KW  - Immunoblotting
KW  - Phosphatidylserines -- metabolism
KW  - Up-Regulation -- drug effects
KW  - Proteasome Endopeptidase Complex -- drug effects
KW  - Flow Cytometry
KW  - Saccharomyces cerevisiae -- genetics
KW  - Apoptosis -- genetics
KW  - Saccharomyces cerevisiae -- physiology
KW  - Saccharomyces cerevisiae Proteins -- genetics
KW  - Oxidative Stress -- genetics
KW  - Caspases -- genetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-05-22
N1  - Date created - 2005-11-30
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
J Biol Chem. 2000 Mar 10;275(10):7337-42 [10702305]
Curr Genet. 2002 Jul;41(4):208-16 [12172961]
Annu Rev Neurosci. 2000;23:73-87 [10845059]
Biochimie. 2001 Mar-Apr;83(3-4):301-10 [11295490]
Mol Biol Cell. 2001 Aug;12(8):2422-32 [11514626]
Proc Natl Acad Sci U S A. 2001 Nov 6;98(23):12920-5 [11606777]
Electrophoresis. 2004 May;25(9):1334-41 [15174056]
Proc Natl Acad Sci U S A. 2004 Aug 10;101(32):11560-5 [15284441]
FEMS Yeast Res. 2004 Nov;5(2):111-7 [15489193]
FEMS Yeast Res. 2004 Nov;5(2):141-7 [15489197]
J Biol Chem. 1985 Oct 15;260(23):12600-6 [2864341]
Curr Top Cell Regul. 1986;28:291-337 [2878793]
J Biol Chem. 1987 Jun 15;262(17):8227-34 [3597373]
J Biol Chem. 1987 Jul 15;262(20):9895-901 [3036875]
Annu Rev Biochem. 1993;62:797-821 [8352601]
FEBS Lett. 2002 Sep 25;528(1-3):23-6 [12297273]
Free Radic Biol Med. 2002 Nov 1;33(9):1209-20 [12398929]
Science. 2003 Mar 14;299(5613):1751-3 [12610228]
Proc Natl Acad Sci U S A. 2003 Nov 25;100(24):14327-32 [14623979]
J Cell Biol. 2004 Feb 16;164(4):501-7 [14970189]
Chem Res Toxicol. 1993 Jul-Aug;6(4):430-3 [8374038]
Methods Enzymol. 1994;233:346-57 [8015469]
Yeast. 1994 Sep;10(9):1141-55 [7754704]
Pharmacol Ther. 1996;72(1):37-50 [8981570]
Proc Natl Acad Sci U S A. 1996 Dec 24;93(26):15036-40 [8986759]
Microsc Res Tech. 1997 Jan 15;36(2):123-9 [9015258]
Drug Metab Rev. 1998 May;30(2):225-43 [9606602]
Biochem J. 1998 Nov 1;335 ( Pt 3):637-42 [9794805]
Nature. 1998 Nov 12;396(6707):119-22 [9823889]
Exp Cell Res. 1999 May 1;248(2):381-90 [10222130]
J Cell Biol. 1999 May 17;145(4):757-67 [10330404]
J Biol Chem. 2004 Dec 10;279(50):52623-9 [15381697]
Biochim Biophys Acta. 2005 Jan 17;1703(2):261-6 [15680234]
J Biol Chem. 2005 Apr 15;280(15):14691-9 [15691845]
Mol Cell. 2002 Apr;9(4):911-7 [11983181]
Hum Exp Toxicol. 2002 Feb;21(2):83 [12102501]
Arch Biochem Biophys. 2002 Aug 15;404(2):279-84 [12147266]
J Gerontol A Biol Sci Med Sci. 2000 May;55(5):B220-7 [10819308]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - An inhibitor of TRPV1 channels isolated from funnel Web spider venom.
AN  - 68812062; 16300403
AB  - Capsaicin receptor channels (TRPV1) are nonselective cation channels that integrate multiple noxious stimuli in sensory neurons. In an effort to identify new inhibitors of these channels we screened a venom library for activity against TRPV1 channels and found robust inhibitory activity in venom from Agelenopsis aperta, a north American funnel web spider. Fractionation of the venom using reversed-phase HPLC resulted in the purification of two acylpolyamine toxins, AG489 and AG505, which inhibit TRPV1 channels from the extracellular side of the membrane. The activity of AG489 was characterized further, and the toxin was found to inhibit TRPV1 channels with a K(i) of 0.3 microM at -40 mV. Inhibition of TRPV1 channels by AG489 is strongly voltage-dependent, with relief of inhibition at positive voltages, consistent with the toxin inhibiting the channel through a pore-blocking mechanism. We used scanning mutagenesis throughout the TM5-TM6 linker, a region thought to form the outer pore of TRPV1 channels, to identify pore mutations that alter toxin affinity. Four mutants dramatically decrease toxin affinity and several mutants increase toxin affinity, consistent with the notion that the TM5-TM6 linker forms the outer vestibule of TRPV1 channels and that AG489 is a pore blocker.
JF  - Biochemistry
AU  - Kitaguchi, Tetsuya
AU  - Swartz, Kenton J
AD  - Molecular Physiology and Biophysics Section, Porter Neuroscience Research Center, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/11/29/
PY  - 2005
DA  - 2005 Nov 29
SP  - 15544
EP  - 15549
VL  - 44
IS  - 47
SN  - 0006-2960, 0006-2960
KW  - Agatoxins
KW  - 0
KW  - FTX, spider toxin
KW  - Polyamines
KW  - Spider Venoms
KW  - TRPV Cation Channels
KW  - Trpv1 protein, rat
KW  - agatoxin-489
KW  - 128549-96-2
KW  - Index Medicus
KW  - Animals
KW  - Models, Molecular
KW  - Chemical Fractionation
KW  - Spider Venoms -- chemistry
KW  - Electrophysiology
KW  - Mutagenesis
KW  - Rats
KW  - Transfection
KW  - Xenopus
KW  - Oocytes
KW  - Spider Venoms -- genetics
KW  - Spider Venoms -- pharmacology
KW  - Polyamines -- pharmacology
KW  - Polyamines -- chemistry
KW  - TRPV Cation Channels -- antagonists & inhibitors
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Biochemistry&rft.atitle=An+inhibitor+of+TRPV1+channels+isolated+from+funnel+Web+spider+venom.&rft.au=Kitaguchi%2C+Tetsuya%3BSwartz%2C+Kenton+J&rft.aulast=Kitaguchi&rft.aufirst=Tetsuya&rft.date=2005-11-29&rft.volume=44&rft.issue=47&rft.spage=15544&rft.isbn=&rft.btitle=&rft.title=Biochemistry&rft.issn=00062960&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2005-11-22
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Modulation of Werner syndrome protein function by a single mutation in the conserved RecQ domain.
AN  - 68815968; 16150736
AB  - Naturally occurring mutations in the human RECQ3 gene result in truncated Werner protein (WRN) and manifest as a rare premature aging disorder, Werner syndrome. Cellular and biochemical studies suggest a multifaceted role of WRN in DNA replication, DNA repair, recombination, and telomere maintenance. The RecQ C-terminal (RQC) domain of WRN was determined previously to be the major site of interaction for DNA and proteins. By using site-directed mutagenesis in the WRN RQC domain, we determined which amino acids might be playing a critical role in WRN function. A site-directed mutation at Lys-1016 significantly decreased WRN binding to fork or bubble DNA substrates. Moreover, the Lys-1016 mutation markedly reduced WRN helicase activity on fork, D-loop, and Holliday junction substrates in addition to reducing significantly the ability of WRN to stimulate FEN-1 incision activities. Thus, DNA binding mediated by the RQC domain is crucial for WRN helicase and its coordinated functions. Our nuclear magnetic resonance data on the three-dimensional structure of the wild-type RQC and Lys-1016 mutant proteins display a remarkable similarity in their structures.
JF  - The Journal of biological chemistry
AU  - Lee, Jae Wan
AU  - Kusumoto, Rika
AU  - Doherty, Kevin M
AU  - Lin, Guang-Xin
AU  - Zeng, Wangyong
AU  - Cheng, Wen-Hsing
AU  - von Kobbe, Cayetano
AU  - Brosh, Robert M
AU  - Hu, Jin-Shan
AU  - Bohr, Vilhelm A
AD  - Laboratory of Molecular Gerontology, NIA, National Institutes of Health, Baltimore, Maryland 21224-6825, USA.
Y1  - 2005/11/25/
PY  - 2005
DA  - 2005 Nov 25
SP  - 39627
EP  - 39636
VL  - 280
IS  - 47
SN  - 0021-9258, 0021-9258
KW  - Recombinant Proteins
KW  - 0
KW  - DNA
KW  - 9007-49-2
KW  - Exodeoxyribonucleases
KW  - EC 3.1.-
KW  - Adenosine Triphosphatases
KW  - EC 3.6.1.-
KW  - RECQL protein, human
KW  - DNA Helicases
KW  - EC 3.6.4.-
KW  - RecQ Helicases
KW  - EC 3.6.4.12
KW  - WRN protein, human
KW  - Werner Syndrome Helicase
KW  - Index Medicus
KW  - Humans
KW  - Mutagenesis, Site-Directed
KW  - Werner Syndrome -- etiology
KW  - Amino Acid Motifs
KW  - Recombinant Proteins -- metabolism
KW  - In Vitro Techniques
KW  - Molecular Sequence Data
KW  - Adenosine Triphosphatases -- chemistry
KW  - Recombinant Proteins -- chemistry
KW  - Sequence Homology, Amino Acid
KW  - Adenosine Triphosphatases -- genetics
KW  - Adenosine Triphosphatases -- metabolism
KW  - Amino Acid Sequence
KW  - Recombinant Proteins -- genetics
KW  - Mutation, Missense
KW  - Werner Syndrome -- metabolism
KW  - Base Sequence
KW  - Conserved Sequence
KW  - Nuclear Magnetic Resonance, Biomolecular
KW  - DNA -- genetics
KW  - Protein Structure, Tertiary
KW  - Werner Syndrome -- genetics
KW  - Cell Line
KW  - DNA Helicases -- chemistry
KW  - DNA Helicases -- metabolism
KW  - DNA Helicases -- genetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2005-11-21
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The entomological inoculation rate and Plasmodium falciparum infection in African children
AN  - 17093271; 6718753
AB  - Malaria is an important cause of global morbidity and mortality. The fact that some people are bitten more often than others has a large effect on the relationship between risk factors and prevalence of vector-borne diseases. Here we develop a mathematical framework that allows us to estimate the heterogeneity of infection rates from the relationship between rates of infectious bites and community prevalence. We apply this framework to a large, published data set that combines malaria measurements from more than 90 communities. We find strong evidence that heterogeneous biting or heterogeneous susceptibility to infection are important and pervasive factors determining the prevalence of infection: 20% of people receive 80% of all infections. We also find that individual infections last about six months on average, per infectious bite, and children who clear infections are not immune to new infections. The results have important implications for public health interventions: the success of malaria control will depend heavily on whether efforts are targeted at those who are most at risk of infection.
JF  - Nature
AU  - Smith, D L
AU  - Dushoff, J
AU  - Snow, R W
AU  - Hay, SI
AD  - Fogarty International Center, National Institutes of Health, Building 16, 16 Center Drive, Bethesda, Maryland 20892, USA, smitdave@helix.nih.gov
Y1  - 2005/11/24/
PY  - 2005
DA  - 2005 Nov 24
SP  - 492
EP  - 495
PB  - Nature Publishing Group, The Macmillan Building 4 Crinan Street London N1 9XW UK, [mailto:feedback@nature.com]
VL  - 438
IS  - 7067
SN  - 0028-0836, 0028-0836
KW  - African children
KW  - Mosquitoes
KW  - Entomology Abstracts; Microbiology Abstracts C: Algology, Mycology & Protozoology; ASFA 3: Aquatic Pollution & Environmental Quality
KW  - Biological vectors
KW  - Human diseases
KW  - Vector-borne diseases
KW  - Disease control
KW  - Culicidae
KW  - Malaria
KW  - Plasmodium falciparum
KW  - Infection
KW  - Risks
KW  - Public health
KW  - Disease transmission
KW  - Socioeconomic aspects
KW  - Biting
KW  - Africa
KW  - K 03090:Protozoa: human
KW  - Z 05206:Medical & veterinary entomology
KW  - Q5 08524:Public health, medicines, dangerous organisms
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-05-01
N1  - Last updated - 2016-05-27
N1  - SubjectsTermNotLitGenreText - Biological vectors; Human diseases; Socioeconomic aspects; Disease control; Malaria; Risks; Disease transmission; Public health; Biting; Vector-borne diseases; Infection; Culicidae; Plasmodium falciparum; Africa
DO  - http://dx.doi.org/10.1038/nature04024
ER  - 



TY  - JOUR
T1  - Decreased levels of CXC-chemokines in serum of benzene-exposed workers identified by array-based proteomics.
AN  - 68821798; 16286641
AB  - Benzene is an important industrial chemical and environmental contaminant that causes leukemia. To obtain mechanistic insight into benzene's mechanism of action, we examined the impact of benzene on the human serum proteome in a study of exposed healthy shoe-factory workers and unexposed controls. Two sequential studies were performed, each using sera from 10 workers exposed to benzene (overall mean benzene air level >30 ppm) and 10 controls. Serum samples were subjected to anion-exchange fractionation and bound to three types of ProteinChip arrays (Ciphergen Biosystems, Fremont, CA) [hydrophobic (H50), metal affinity (IMAC3-Cu), and cation exchange (WCX2)]. Protein-expression patterns were detected by surface-enhanced laser desorption/ionization (SELDI)-TOF MS. Three proteins (4.1, 7.7, and 9.3 kDa) were consistently down-regulated in exposed compared with control subjects in both studies. All proteins were highly inversely correlated with individual estimates of benzene exposure (r > 0.75). The 7.7- and 9.3-kDa proteins were subsequently identified as platelet factor (PF)4 and connective tissue activating peptide (CTAP)-III. Initial proteomic results for PF4 and CTAP-III were subsequently confirmed in a single experiment using a ProteinChip-array-based immunoassay(Ciphergen Biosystems). The altered expression of the platelet-derived CXC-chemokines (40% and 63% for PF4 and CTAP-III, respectively) could not be explained by changes in absolute platelet counts. Thus, SELDI-TOF analysis of a limited number of exposed and unexposed subjects revealed that lowered expression of PF4 and CTAP-III proteins is a potential biomarker of benzene's early biologic effects and may play a role in the immunosuppressive effects of benzene.
JF  - Proceedings of the National Academy of Sciences of the United States of America
AU  - Vermeulen, Roel
AU  - Lan, Qing
AU  - Zhang, Luoping
AU  - Gunn, Laura
AU  - McCarthy, Diane
AU  - Woodbury, Ronald L
AU  - McGuire, Marielena
AU  - Podust, Vladimir N
AU  - Li, Guilan
AU  - Chatterjee, Nilanjan
AU  - Mu, Ruidong
AU  - Yin, Songnian
AU  - Rothman, Nathaniel
AU  - Smith, Martyn T
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Department of Health and Human Services, 6120 Executive Boulevard, Rockville, MD 20852, USA. vermeulr@mail.nih.gov
Y1  - 2005/11/22/
PY  - 2005
DA  - 2005 Nov 22
SP  - 17041
EP  - 17046
VL  - 102
IS  - 47
SN  - 0027-8424, 0027-8424
KW  - Biomarkers
KW  - 0
KW  - Chemokines, CXC
KW  - Benzene
KW  - J64922108F
KW  - Index Medicus
KW  - Protein Array Analysis
KW  - Humans
KW  - Linear Models
KW  - Biomarkers -- blood
KW  - Proteomics
KW  - Occupational Exposure -- adverse effects
KW  - Chemokines, CXC -- blood
KW  - Benzene -- adverse effects
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Proceedings+of+the+National+Academy+of+Sciences+of+the+United+States+of+America&rft.atitle=Decreased+levels+of+CXC-chemokines+in+serum+of+benzene-exposed+workers+identified+by+array-based+proteomics.&rft.au=Vermeulen%2C+Roel%3BLan%2C+Qing%3BZhang%2C+Luoping%3BGunn%2C+Laura%3BMcCarthy%2C+Diane%3BWoodbury%2C+Ronald+L%3BMcGuire%2C+Marielena%3BPodust%2C+Vladimir+N%3BLi%2C+Guilan%3BChatterjee%2C+Nilanjan%3BMu%2C+Ruidong%3BYin%2C+Songnian%3BRothman%2C+Nathaniel%3BSmith%2C+Martyn+T&rft.aulast=Vermeulen&rft.aufirst=Roel&rft.date=2005-11-22&rft.volume=102&rft.issue=47&rft.spage=17041&rft.isbn=&rft.btitle=&rft.title=Proceedings+of+the+National+Academy+of+Sciences+of+the+United+States+of+America&rft.issn=00278424&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-12
N1  - Date created - 2005-11-23
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Am J Epidemiol. 1988 Mar;127(3):419-39 [3277397]
Environ Health Perspect. 2005 Jun;113(6):801-7 [15929907]
Am J Ind Med. 1996 Mar;29(3):236-46 [8833776]
J Leukoc Biol. 2000 Apr;67(4):471-8 [10770278]
J Biol Chem. 2000 Jul 7;275(27):20374-81 [10877842]
Blood. 2000 Nov 1;96(9):2965-72 [11049972]
Immunol Rev. 2000 Oct;177:204-16 [11138777]
Curr Opin Rheumatol. 2001 May;13(3):202-8 [11333349]
Transfus Med. 2001 Dec;11(6):403-17 [11851938]
J Immunol. 2002 Jul 15;169(2):770-7 [12097379]
Am J Ind Med. 2002 Oct;42(4):275-85 [12271475]
Semin Immunol. 2003 Feb;15(1):15-21 [12495637]
Lung Cancer. 2003 Jun;40(3):267-79 [12781425]
BJU Int. 2003 Aug;92(3):223-5 [12887471]
Arch Otolaryngol Head Neck Surg. 2004 Jan;130(1):98-104 [14732777]
Ann Occup Hyg. 2004 Mar;48(2):105-16 [14990432]
Novartis Found Symp. 2004;256:173-84; discussion 184-8, 259-69 [15027490]
Lab Invest. 2004 Jul;84(7):845-56 [15107802]
Am J Ind Med. 1985;7(5-6):395-402 [4003402]
Toxicol Appl Pharmacol. 1985 Sep 30;80(3):502-10 [2863880]
Environ Health Perspect. 1996 Dec;104 Suppl 6:1339-41 [9118917]
Environ Health Perspect. 1996 Dec;104 Suppl 6:1349-52 [9118919]
Am J Ind Med. 1997 Mar;31(3):287-95 [9055951]
Blood. 1997 Apr 1;89(7):2328-35 [9116276]
J Natl Cancer Inst. 1997 Jul 16;89(14):1065-71 [9230889]
Science. 2004 Dec 3;306(5702):1774-6 [15576619]
Stat Med. 1990 Jul;9(7):811-8 [2218183]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Immunohistochemical evaluation of heat shock proteins in normal and preinvasive lesions of the cervix.
AN  - 68689266; 16112431
AB  - Heat Shock Proteins (HSPs) are molecular chaperons with multiple functions relating to cellular homeostasis. Primary, HSPs are expressed in response to cellular stresses that may also include carcinogenesis. Patterns of expression have not been extensively evaluated in the multi-step carcinogenesis of cervical cancer (Normal --> HPV infection --> Cervical Precancer --> Cancer). We evaluated the expression of HSP40, HSP60, HSP70, and HSP90 in normal tissues (N=30), in cervical intraepithelial neoplasia grade 1 (CIN1)(synonymous with productive HPV infections) (N=32), and in CIN3 (cervical precancer)(N=25) by immunohistochemistry staining (graded 0-3) and compared the results to p16INK4a, a biomarker of oncogenic HPV infections and CIN3. We found strong patterns of increased HSP40, HSP60, and HSP70 immunostaining with increasing severity of the lesion in a manner similar to p16INK4a (P(Trend)<0.0005). No difference in staining intensity by grade of lesion was observed for HSP90 (P(Trend)=0.8). Tissue patterns in CIN3 of diffuse immunostaining for HSP40 and HSP70 were analogous to those observed for p16INK4a; HSP60 immunostaining appeared more punctate within cells than for other antigens although similar tissue patterns were observed. We conclude that HSP40, HSP60, and HSP70 expressions are up-regulated in response to the development of CIN3 akin to p16INK4a expression.
JF  - Cancer letters
AU  - Castle, Philip E
AU  - Ashfaq, Raheela
AU  - Ansari, Faryal
AU  - Muller, Carolyn Y
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, NIH, DHHS, Bethesda, MD, USA. castlep@mail.nih.gov
Y1  - 2005/11/18/
PY  - 2005
DA  - 2005 Nov 18
SP  - 245
EP  - 252
VL  - 229
IS  - 2
SN  - 0304-3835, 0304-3835
KW  - Biomarkers, Tumor
KW  - 0
KW  - Cyclin-Dependent Kinase Inhibitor p16
KW  - Heat-Shock Proteins
KW  - Index Medicus
KW  - Humans
KW  - Papillomavirus Infections -- complications
KW  - Precancerous Conditions -- metabolism
KW  - Precancerous Conditions -- pathology
KW  - Precancerous Conditions -- virology
KW  - Cyclin-Dependent Kinase Inhibitor p16 -- biosynthesis
KW  - Tumor Virus Infections -- metabolism
KW  - Biomarkers, Tumor -- analysis
KW  - Up-Regulation
KW  - Immunohistochemistry
KW  - Female
KW  - Papillomavirus Infections -- metabolism
KW  - Tumor Virus Infections -- complications
KW  - Cervical Intraepithelial Neoplasia -- pathology
KW  - Uterine Cervical Neoplasms -- metabolism
KW  - Cervical Intraepithelial Neoplasia -- metabolism
KW  - Heat-Shock Proteins -- biosynthesis
KW  - Cervical Intraepithelial Neoplasia -- virology
KW  - Uterine Cervical Neoplasms -- pathology
KW  - Uterine Cervical Neoplasms -- virology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-11
N1  - Date created - 2005-10-14
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Potential hazard of pharmacokinetic interactions between lopinavir-ritonavir protease inhibitors and irinotecan
AN  - 21046234; 6585921
AB  - The use of concomitant chemotherapy and highly active antiretroviral therapy (HAART) has been demonstrated to be feasible and effective in reducing morbidity associated with opportunistic infections and to improve overall survival in patients with HIV-related malignances. However, such combination therapy causes severe toxicity, including neutropenia. It has been hypothesized that such unpredictable toxicity can be related to pharmacokinetic interactions.
JF  - AIDS
AU  - Corona, G
AU  - Vaccher, E
AU  - Cattarossi, G
AU  - Sartor, I
AU  - Toffoli, G
AD  - Division of Medical Oncology A, National Cancer Institute CRO-IRCCS, Aviano (PN), Italy
Y1  - 2005/11/18/
PY  - 2005
DA  - 2005 Nov 18
SP  - 2043
EP  - 2044
VL  - 19
IS  - 17
SN  - 0269-9370, 0269-9370
KW  - HIV
KW  - irinotecan
KW  - lopinavir-ritonavir protease inhibitors
KW  - Immunology Abstracts; Health & Safety Science Abstracts; Toxicology Abstracts; Virology & AIDS Abstracts
KW  - Acquired immune deficiency syndrome
KW  - Chemotherapy
KW  - Proteinase inhibitors
KW  - Irinotecan
KW  - Survival
KW  - Toxicity
KW  - chemotherapy
KW  - Pharmacokinetics
KW  - Morbidity
KW  - Opportunist infection
KW  - Neutropenia
KW  - Human immunodeficiency virus
KW  - highly active antiretroviral therapy
KW  - antiretroviral agents
KW  - infection
KW  - Side effects
KW  - X 24114:Metabolism
KW  - V 22002:AIDS: Molecular and in vitro aspects
KW  - F 06910:Microorganisms & Parasites
KW  - H 4000:Food and Drugs
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Neutropenia; highly active antiretroviral therapy; Chemotherapy; Irinotecan; Proteinase inhibitors; Survival; Toxicity; Morbidity; Pharmacokinetics; Opportunist infection; Acquired immune deficiency syndrome; antiretroviral agents; infection; Side effects; chemotherapy; Human immunodeficiency virus
ER  - 



TY  - CPAPER
T1  - Production of Reactive Oxygen Species in Both Human and Mouse Mast Cells is Lipoxygenase-Dependent and Plays a Facilitatory Role in Antigen Mediated Cytokine Secretion
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39768844; 4051721
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Coleman, John W
AU  - Metcalfe, Dean D
AU  - Swindle, Emily J
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Mast cells
KW  - Reactive oxygen species
KW  - Cytokines
KW  - Secretion
KW  - Antigens
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Biting the Hand that Feeds: Use of a Novel DMPO-Protein Antibody in Detection of a Drug-Induced Myeloperoxidase Radical Adduct Upon Myeloperoxidase-Catalyzed Peroxidation of Aminoglutethimide
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39768211; 4051644
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Bonini, Marcelo G
AU  - Mason, Ronald P
AU  - Siraki, Arno G
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Feeds
KW  - Adducts
KW  - Biting
KW  - Peroxidation
KW  - Antibodies
KW  - Radicals
KW  - Peroxidase
KW  - Hand
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Imaging Tissue Redox Staus Using MRI and Redox Sensitive Paramagnetic Contrast Agents: Applications for Tumor Imaging
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39767150; 4051800
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Hyodo, Fuminori
AU  - Matsumoto, Ken-ichiro
AU  - Matsumoto, Atsuko
AU  - Mitchell, James
AU  - Murali, Cherukuri
AU  - Subramanian, Sankaran
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Magnetic resonance imaging
KW  - Contrast media
KW  - Redox reactions
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Nitrite Regulates Mitochondrial Respiration and Limits Reperfusion Injury
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39763672; 4052082
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Gladwin, Mark
AU  - Huang, Zhi
AU  - Lefer, David
AU  - Ringwood, Lorna
AU  - Sack, Michael
AU  - Shiva, Sruti
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Nitrite
KW  - Respiration
KW  - Injuries
KW  - Mitochondria
KW  - Reperfusion
KW  - Electron transport
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Catalase Inactivation by Hypochlorite Correlates with Protein Radical Formation, Aggregation and Heme Modification
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39755226; 4051626
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Atanassov, Boyko S
AU  - Bonini, Marcelo G
AU  - Mason, Ronald P
AU  - Siraki, Arno G
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Heme
KW  - Catalase
KW  - Radicals
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Mass Spectral Analysis of Protein-Based Radicals Using Stable Nitroxide Radicals: The Spin Scavenging Approach
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39754566; 4051813
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Deterding, Leesa
AU  - Lardinois, Olivier
AU  - Mason, Ronald
AU  - Tomer, Kenneth
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Radicals
KW  - Nitroxide
KW  - Spectral analysis
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39754566?accountid=14244
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L2  - http://submissions.miracd.com/sfrbm2005/Itinerary/SearchHome.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Novel Pharmacokinetic Measurement Using Electron Paramagnetic Resonance Spectroscopy and Simulation of in Vivo Decay of Various Nitroxyl Radicals in Mouse Blood
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39750890; 4051805
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Krishna, Murali
AU  - Matsumoto, Ken-ichiro
AU  - Mitchell, James
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Decay
KW  - Blood
KW  - Spectroscopy
KW  - Simulation
KW  - Pharmacokinetics
KW  - E.S.R.
KW  - Radicals
KW  - Resonance
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39750890?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Atorvastatin Therapy Restores Nitric Oxide-Dependent Vascular Responsiveness in Patients with Sickle Cell Disease
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39750799; 4051778
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Cannon, Richard
AU  - Dejam, Andre
AU  - Gladwin, Mark
AU  - Hunter, Christian
AU  - Hunter, Lori
AU  - Kato, Gregory
AU  - Lin, Elaina
AU  - Machado, Roberto
AU  - Mack, Kyle
AU  - Sachdev, Vandana
AU  - Tremonti, Carole
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Vascular system
KW  - Sickle cell disease
KW  - Atorvastatin
KW  - Therapy
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39750799?accountid=14244
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L2  - http://submissions.miracd.com/sfrbm2005/Itinerary/SearchHome.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Noninvasive EPR Assessment of Tissue Oxygenation Using Water Soluble Paramagnetic Probes
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39747266; 4051810
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Devasahayam, Nallathamby
AU  - Hyodo, Fuminori
AU  - Koscielniak, Janusz
AU  - Krishna, Murali
AU  - Matsumoto, Atsuko
AU  - Matsumoto, Ken-ichiro
AU  - Mitchell, James
AU  - Sowers, Anastasia
AU  - Subramanian, Sankaran
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Oxygenation
KW  - Probes
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Estimation of Redox Status of a Tumor Tissue in Mice Using Paramagnetic Nitroxyl Contrast Agent
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39747239; 4051806
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Cook, John
AU  - Hyodo, Fuminori
AU  - Krishna, Murali
AU  - Matsumoto, Ken-ichiro
AU  - Matsumoto, Atsuko
AU  - Mitchell, James
AU  - Murugesan, Ramachandran
AU  - Sowers, Anastasia
AU  - Subramanian, Sankaran
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Mice
KW  - Contrast media
KW  - Redox reactions
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Copper Catalyzed Protein Oxidation and its Modulation by Carbon Dioxide: Enhancement of Protein Radicals in Functioning Cells
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39720913; 4052037
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Mejiba, Sandra Gomez
AU  - Mason, Ronald
AU  - Ramirez, Dario
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Copper
KW  - Oxidation
KW  - Carbon dioxide
KW  - Radicals
KW  - U 2000:Biological Sciences
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L2  - http://submissions.miracd.com/sfrbm2005/Itinerary/SearchHome.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Superoxide Fluxes Control NO-Induced Post-Translational Regulation of sGC, p53, and HIF-1a
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39712942; 4051917
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Thomas, Douglas
AU  - Wink, David
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Hypoxia-inducible factor 1^a
KW  - P53 protein
KW  - Superoxide
KW  - Post-translation
KW  - U 2000:Biological Sciences
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L2  - http://submissions.miracd.com/sfrbm2005/Itinerary/SearchHome.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Hydroethidine is Efficiently Oxidized by Singlet Oxygen
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39712257; 4051796 DE:
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Bilski, Piotr
AU  - Chignell, Colin F
AU  - DeRose, Eugene F
AU  - Karriker, Brian
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - U 2000:Biological Sciences
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L2  - http://submissions.miracd.com/sfrbm2005/Itinerary/SearchHome.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Proteomic Identification of Dysregulated Apolipoprotein Expression in Pulmonary Hypertension Secondary to Sickle Cell Disease
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39712164; 4051777
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Gladwin, Mark
AU  - Hoehn, Gerard
AU  - Kato, Gregory
AU  - Munson, Peter
AU  - Suffredini, Anthony
AU  - Xu, Xiuli
AU  - Yuditskaya, Susan
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - Hypertension
KW  - Apolipoproteins
KW  - Proteomics
KW  - Sickle cell disease
KW  - U 2000:Biological Sciences
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L2  - http://submissions.miracd.com/sfrbm2005/Itinerary/SearchHome.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Nitroxides Inhibit the TNF-Alpha Initiated NF-kB Cytoplasmic to Nuclear Translocation
T2  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AN  - 39709074; 4051867
JF  - 12th Annual Meeting of Society for Free Radical Biology and Medicine (SFRBM's 12th)
AU  - Cook, John
AU  - Grimes, Kelly
AU  - Mitchell, James
Y1  - 2005/11/16/
PY  - 2005
DA  - 2005 Nov 16
KW  - NF-^KB protein
KW  - Nuclear transport
KW  - Nitroxide
KW  - U 2000:Biological Sciences
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L2  - http://submissions.miracd.com/sfrbm2005/Itinerary/SearchHome.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - The p53 tumor suppressor network is a key responder to microenvironmental components of chronic inflammatory stress.
AN  - 68805004; 16288013
AB  - Activation of the p53 network plays a central role in the inflammatory stress response associated with ulcerative colitis and may modulate cancer risk in patients afflicted with this chronic disease. Here, we describe the gene expression profiles associated with four microenvironmental components of the inflammatory response (NO*, H2O2, DNA replication arrest, and hypoxia) that result in p53 stabilization and activation. Isogenic HCT116 and HCT116 TP53-/- colon cancer cells were exposed to the NO* donor Sper/NO, H2O2, hypoxia, or hydroxyurea, and their mRNA was analyzed using oligonucleotide microarrays. Overall, 1,396 genes changed in a p53-dependent manner (P < 0.001), with the majority representing a "unique" profile for each condition. Only 14 genes were common to all four conditions. Included were eight known p53 target genes. Hierarchical sample clustering distinguished early (1 and 4 hours) from late responses (8, 12, and 24 hours), and each treatment was differentiated from the others. Overall, NO* and hypoxia stimulated similar transcriptional responses. Gene ontology analysis revealed cell cycle as a key feature of stress responses and confirmed the similarity between NO* and hypoxia. Cell cycle profiles analyzed by flow cytometry showed that NO* and hypoxia induced quiescent S-phase and G2-M arrest. Using a novel bioinformatic algorithm, we identified several putative p53-responsive elements among the genes induced in a p53-dependent manner, including four [KIAA0247, FLJ12484, p53CSV (HSPC132), and CNK (PLK3)] common to all exposures. In summary, the inflammatory stress response is a complex, integrated biological network in which p53 is a key molecular node regulating gene expression.
JF  - Cancer research
AU  - Staib, Frank
AU  - Robles, Ana I
AU  - Varticovski, Lyuba
AU  - Wang, Xin W
AU  - Zeeberg, Barry R
AU  - Sirotin, Michail
AU  - Zhurkin, Victor B
AU  - Hofseth, Lorne J
AU  - Hussain, S Perwez
AU  - Weinstein, John N
AU  - Galle, Peter R
AU  - Harris, Curtis C
AD  - Laboratories of Human Carcinogenesis, Center for Cancer Research, National Cancer Institute, NIH, Bethesda, Maryland 20892-4255, USA.
Y1  - 2005/11/15/
PY  - 2005
DA  - 2005 Nov 15
SP  - 10255
EP  - 10264
VL  - 65
IS  - 22
SN  - 0008-5472, 0008-5472
KW  - Nitric Oxide Donors
KW  - 0
KW  - Nitrogen Oxides
KW  - TP53 protein, human
KW  - Tumor Suppressor Protein p53
KW  - spermine nitric oxide complex
KW  - 136587-13-8
KW  - Spermine
KW  - 2FZ7Y3VOQX
KW  - Hydrogen Peroxide
KW  - BBX060AN9V
KW  - Index Medicus
KW  - Humans
KW  - Oxidative Stress -- genetics
KW  - HCT116 Cells
KW  - Cell Hypoxia
KW  - Reverse Transcriptase Polymerase Chain Reaction
KW  - Gene Expression Profiling
KW  - Oxidative Stress -- physiology
KW  - Spermine -- analogs & derivatives
KW  - Flow Cytometry
KW  - Cell Cycle
KW  - Tumor Suppressor Protein p53 -- biosynthesis
KW  - Inflammation -- etiology
KW  - Inflammation -- genetics
KW  - Inflammation -- metabolism
KW  - Tumor Suppressor Protein p53 -- genetics
KW  - Tumor Suppressor Protein p53 -- metabolism
KW  - Tumor Suppressor Protein p53 -- deficiency
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-18
N1  - Date created - 2005-11-18
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
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N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Yin-yang: balancing act of prostaglandins with opposing functions to regulate inflammation.
AN  - 68765371; 16272277
AB  - For many years, cyclooxygenase-2 (COX-2), a critical enzyme for PG production, has been the favorite target for anti-inflammatory drug development. However, recent revelations regarding the adverse effects of selective COX-2 inhibitors have stimulated intense debate. Interestingly, in the early phase of inflammation, COX-2 facilitates inflammatory PG production while in the late phase it has anti-inflammatory effects. Moreover, although some PGs are proinflammatory, others have anti-inflammatory effects. Thus, it is likely that PGs with opposing effects maintain homeostasis, although the molecular mechanism(s) remains unclear. We report here that an inflammatory PG, PGD2, via its receptor, mediates the activation of NF-kappaB stimulating COX-2 gene expression. Most interestingly, an anti-inflammatory PG (PGA1) suppresses NF-kappaB activation and inhibits COX-2 gene expression. We propose that while pro- and anti-inflammatory PGs counteract each other to maintain homeostasis, selective COX-2 inhibitors may disrupt this balance, thereby resulting in reported adverse effects.
JF  - Journal of immunology (Baltimore, Md. : 1950)
AU  - Mandal, Asim K
AU  - Zhang, Zhongjian
AU  - Kim, Sung-Jo
AU  - Tsai, Pei-Chih
AU  - Mukherjee, Anil B
AD  - Section on Developmental Genetics, Heritable Disorders Branch, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, MD 20892, USA.
Y1  - 2005/11/15/
PY  - 2005
DA  - 2005 Nov 15
SP  - 6271
EP  - 6273
VL  - 175
IS  - 10
SN  - 0022-1767, 0022-1767
KW  - Cyclooxygenase 2 Inhibitors
KW  - 0
KW  - NF-kappa B
KW  - Prostaglandins
KW  - Prostaglandins A
KW  - RNA, Messenger
KW  - Cyclooxygenase 2
KW  - EC 1.14.99.1
KW  - Prostaglandin D2
KW  - RXY07S6CZ2
KW  - prostaglandin A1
KW  - VYR271N44P
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Gene Expression -- drug effects
KW  - Animals
KW  - Cyclooxygenase 2 -- physiology
KW  - Cyclooxygenase 2 Inhibitors -- adverse effects
KW  - Prostaglandins A -- pharmacology
KW  - Cyclooxygenase 2 -- genetics
KW  - Cyclooxygenase 2 Inhibitors -- pharmacology
KW  - Mice
KW  - RNA, Messenger -- genetics
KW  - Homeostasis -- drug effects
KW  - NF-kappa B -- genetics
KW  - NIH 3T3 Cells
KW  - Prostaglandin D2 -- pharmacology
KW  - RNA, Messenger -- metabolism
KW  - NF-kappa B -- metabolism
KW  - Prostaglandins -- physiology
KW  - Inflammation -- physiopathology
KW  - Inflammation -- genetics
KW  - Inflammation -- drug therapy
KW  - Inflammation -- immunology
KW  - Prostaglandins -- immunology
KW  - Prostaglandins -- pharmacology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-03
N1  - Date created - 2005-11-07
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The antileukemia effect of HLA-matched NK and NK-T cells in chronic myelogenous leukemia involves NKG2D-target-cell interactions.
AN  - 68755532; 16046526
AB  - To study natural killer (NK) cell-mediated antileukemic activity in chronic myelogenous leukemia (CML), we investigated the ability of HLA-matched and mismatched CD56(+) cells to inhibit granulocyte macrophage-colony-forming unit (CFU-GM) formation by leukemic CD34(+) cells. In 14 HLA-identical donor-recipient pairs, donor CD56(+) cells inhibited CML CFU-GM comparably to effectors from 14 HLA-mismatched unrelated individuals (mean inhibition 42% +/- 9% vs 39.5% +/- 7% at a 10:1 effector-to-target (E/T) ratio), suggesting that killer inhibitory receptor (KIR) incompatibility was not essential for an antileukemic effect. Both CD56(+)CD3(-) (natural killer [NK]) and CD56(+)CD3(+)(NK-T) cells inhibited CFU-GM growth of CML but not normal CD34(+) cells. A mechanism for this leukemia-specific cytotoxicity was suggested by the abnormal overexpression of major histocompatibility class I chain-related gene A or gene B (MICA/B) on CML CD34 cells and their ability to bind the NK activation ligand NKG2D. However, in vivo, CML cells may avoid NK-cell-mediated immune destruction by immune escape, shedding MICA into the plasma, thereby down-regulating NKG2D on CML CD56(+) cells.
JF  - Blood
AU  - Sconocchia, Giuseppe
AU  - Lau, Michelle
AU  - Provenzano, Maurizio
AU  - Rezvani, Katayoun
AU  - Wongsena, Wachanan
AU  - Fujiwara, Hiroshi
AU  - Hensel, Nancy
AU  - Melenhorst, Jos
AU  - Li, Jonming
AU  - Ferrone, Soldano
AU  - Barrett, A John
AD  - Stem Cell Allotransplantation Section, Hematology Branch, National Heart Lung and Blood Institute, Department of Transfusion Medicine, Clinical Center, National Institutes of Health (NIH), Bethesda, MD 20892, USA.
Y1  - 2005/11/15/
PY  - 2005
DA  - 2005 Nov 15
SP  - 3666
EP  - 3672
VL  - 106
IS  - 10
SN  - 0006-4971, 0006-4971
KW  - Antigens, CD
KW  - 0
KW  - HLA Antigens
KW  - Histocompatibility Antigens Class I
KW  - KLRK1 protein, human
KW  - MHC class I-related chain A
KW  - MICB antigen
KW  - NK Cell Lectin-Like Receptor Subfamily K
KW  - Receptors, Immunologic
KW  - Receptors, Natural Killer Cell
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Cytotoxicity Tests, Immunologic -- methods
KW  - Humans
KW  - Histocompatibility Antigens Class I -- immunology
KW  - Tumor Cells, Cultured
KW  - Histocompatibility Testing -- methods
KW  - Adult
KW  - Case-Control Studies
KW  - HLA Antigens -- immunology
KW  - Antigens, CD -- immunology
KW  - Female
KW  - Male
KW  - Receptors, Immunologic -- immunology
KW  - Leukemia, Myelogenous, Chronic, BCR-ABL Positive -- immunology
KW  - Neoplastic Stem Cells -- immunology
KW  - T-Lymphocytes -- immunology
KW  - Killer Cells, Natural -- immunology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-15
N1  - Date created - 2005-11-03
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
J Exp Med. 2000 Apr 17;191(8):1259-62 [10770793]
Neoplasia. 2004 Sep-Oct;6(5):558-68 [15548365]
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Cancer Res. 2002 Nov 1;62(21):6178-86 [12414645]
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Hum Immunol. 2003 Feb;64(2):183-93 [12559621]
Blood. 2003 Aug 1;102(3):814-9 [12689936]
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Med Clin (Barc). 1995 Jun 10;105(2):50-3 [7603094]
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Immunol Today. 2000 May;21(5):228-34 [10782054]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Breast cancer risk following radiotherapy for Hodgkin lymphoma: modification by other risk factors.
AN  - 68755152; 16051739
AB  - The importance of genetic and other risk factors in the development of breast cancer after radiotherapy (RT) for Hodgkin lymphoma (HL) has not been determined. We analyzed data from a breast cancer case-control study (105 patients, 266 control subjects) conducted among 3 817 survivors of HL diagnosed at age 30 years or younger in 6 population-based cancer registries. Odds ratios (ORs) and excess relative risks (ERRs) were calculated using conditional regression. Women who received RT exposure (> or = 5 Gy radiation dose to the breast) had a 2.7-fold increased breast cancer risk (95% confidence interval (CI) 1.4-5.2), compared with those given less than 5 Gy. RT exposure (> or = 5 Gy) was associated with an OR of 0.8 (95% CI, 0.2-3.4) among women with a first- or second-degree family history of breast or ovarian cancer, and 5.8 (95% CI, 2.1-16.3) among all other women (interaction P = .03). History of a live birth appeared to increase the breast cancer risk associated with RT among women not treated with ovarian-damaging therapies. Breast cancer risk following RT varied little according to other factors. The additional increased relative risk of breast cancer after RT for HL is unlikely to be larger among women with a family history of breast or ovarian cancer than among other women.
JF  - Blood
AU  - Hill, Deirdre A
AU  - Gilbert, Ethel
AU  - Dores, Graça M
AU  - Gospodarowicz, Mary
AU  - van Leeuwen, Flora E
AU  - Holowaty, Eric
AU  - Glimelius, Bengt
AU  - Andersson, Michael
AU  - Wiklund, Tom
AU  - Lynch, Charles F
AU  - Van't Veer, Mars
AU  - Storm, Hans
AU  - Pukkala, Eero
AU  - Stovall, Marilyn
AU  - Curtis, Rochelle E
AU  - Allan, James M
AU  - Boice, John D
AU  - Travis, Lois B
AD  - Division of Cancer Epidemiology and Genetics and Division of Cancer Prevention, National Cancer Institute, National Institutes of Health, Department of Health and Human Services, Bethesda, MD, USA. dahill@salud.unm.edu
Y1  - 2005/11/15/
PY  - 2005
DA  - 2005 Nov 15
SP  - 3358
EP  - 3365
VL  - 106
IS  - 10
SN  - 0006-4971, 0006-4971
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Odds Ratio
KW  - Risk Factors
KW  - Radiotherapy Dosage
KW  - Humans
KW  - Adult
KW  - Retrospective Studies
KW  - Middle Aged
KW  - Female
KW  - Hodgkin Disease -- radiotherapy
KW  - Breast Neoplasms -- mortality
KW  - Neoplasms, Radiation-Induced -- etiology
KW  - Neoplasms, Second Primary -- etiology
KW  - Breast Neoplasms -- etiology
KW  - Neoplasms, Radiation-Induced -- mortality
KW  - Neoplasms, Second Primary -- mortality
KW  - Hodgkin Disease -- complications
KW  - Hodgkin Disease -- mortality
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-15
N1  - Date created - 2005-11-03
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Lancet. 2001 Oct 27;358(9291):1389-99 [11705483]
Cancer Causes Control. 1994 Mar;5(2):167-76 [8167264]
J Clin Oncol. 2002 Aug 15;20(16):3484-94 [12177110]
Clin Cancer Res. 2002 Dec;8(12):3813-9 [12473594]
Cancer Epidemiol Biomarkers Prev. 2003 Apr;12(4):289-94 [12692102]
Cancer Causes Control. 2003 Mar;14(2):151-60 [12749720]
J Natl Cancer Inst. 2003 Jul 2;95(13):971-80 [12837833]
JAMA. 2003 Jul 23;290(4):465-75 [12876089]
Mol Cell. 2003 Nov;12(5):1087-99 [14636569]
J Clin Oncol. 2003 Dec 1;21(23):4386-94 [14645429]
Radiat Res. 2003 Dec;160(6):707-17 [14640793]
Blood. 2004 Jan 1;103(1):283-90 [12969974]
Epidemiology. 2004 Jul;15(4):422-7 [15232402]
J Natl Cancer Inst. 1980 Jun;64(6):1459-66 [6929382]
Prev Med. 1980 Nov;9(6):815-22 [7454704]
N Engl J Med. 1994 Jul 7;331(1):5-9 [8202106]
BMJ. 1994 Jun 25;308(6945):1672-4 [8025460]
J Natl Cancer Inst Monogr. 1994;(16):15-24 [7999458]
Br J Cancer. 1995 Aug;72(2):480-4 [7640236]
Science. 1999 Nov 5;286(5442):1162-6 [10550055]
J Clin Oncol. 1999 Apr;17(4):1259 [10561187]
Cancer Epidemiol Biomarkers Prev. 1999 Dec;8(12):1043-50 [10613335]
Carcinogenesis. 2000 May;21(5):1043-50 [10783331]
Int J Radiat Biol. 2000 May;76(5):693-8 [10866292]
Am J Epidemiol. 2000 Sep 15;152(6):514-27 [10997541]
Proc Natl Acad Sci U S A. 2001 Apr 24;98(9):5134-9 [11320250]
Br J Cancer. 2001 Aug 3;85(3):362-6 [11487266]
Cancer Causes Control. 1995 Jul;6(4):283-91 [7548715]
J Natl Cancer Inst. 1996 Mar 20;88(6):359-64 [8609645]
Radiat Res. 1996 Jun;145(6):708-13 [8643830]
Nature. 1997 Apr 24;386(6627):804-10 [9126738]
Am J Hum Genet. 1998 Feb;62(2):334-45 [9463314]
J Clin Oncol. 1998 Jul;16(7):2417-25 [9667259]
J Natl Cancer Inst. 1999 Jun 2;91(11):943-9 [10359546]
Cancer. 1983 Aug 1;52(3):435-8 [6688036]
J Natl Cancer Inst. 1986 Sep;77(3):689-96 [3462410]
Int J Cancer. 1989 Jul 15;44(1):7-16 [2744900]
Arch Intern Med. 1990 Jan;150(1):191-4 [2297287]
Br J Cancer. 1990 Jul;62(1):122-6 [2390471]
N Engl J Med. 1992 Mar 19;326(12):781-5 [1538720]
J Natl Cancer Inst. 1992 Aug 19;84(16):1245-50 [1640483]
J Natl Cancer Inst. 1993 Oct 20;85(20):1679-85 [8411245]
Int J Cancer. 1994 Feb 1;56(3):413-7 [8314329]
Int J Cancer. 1994 Mar 15;56(6):793-801 [8119768]
Radiat Res. 2002 Aug;158(2):220-35 [12105993]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Autonomic activity in relation to symptom ratings and reaction time in unmedicated patients with schizophrenia.
AN  - 68721907; 16006104
AB  - High autonomic base levels and low responsivity are frequently observed in unmedicated patients with schizophrenia. We previously reported that patients in the present cohort, compared to normal controls, had high autonomic tonic baselines and low reactivity to the meaningful stimuli in a reaction time (RT) task but not to novel but innocuous stimuli. This paper explores further the role of autonomic activity in the pathogenesis of schizophrenia by relating differences in the autonomic variables among patients to symptom ratings and RT.
          Electrodermal activity and heart rate were recorded during rest, a tone series, and a RT task in 73 patients with schizophrenia taking placebo. Symptoms were rated with the Brief Psychiatric Rating Scale. Patients with higher autonomic baselines both at rest and under mild stress and those with greater electrodermal responsivity to both simple tones and the RT stimuli had more severe positive, "active", and total symptoms than patients with lower baselines and responsivity. RT was slower in patients with higher baselines. High autonomic activity in general, reactivity as well as base levels, under all conditions used in this study was associated with symptom severity independent of differences from controls. Thus elevated autonomic activity and responsivity may themselves be disturbing or index states that are disturbing in schizophrenia. Some patients might attempt to cope with novel or demanding situations and stimuli by a passive-avoidant strategy of low attention and effort in order to attenuate their responsivity. Less symptomatic patients may better cope in this manner.
JF  - Schizophrenia research
AU  - Zahn, Theodore P
AU  - Pickar, David
AD  - Laboratory of Brain and Cognition, National Institutes of Health, Bldg. 10. Rm. 4C104, MSC 1366, Bethesda, MD 20892-1366, USA. tpz@mail.nih.gov
Y1  - 2005/11/15/
PY  - 2005
DA  - 2005 Nov 15
SP  - 257
EP  - 270
VL  - 79
IS  - 2-3
SN  - 0920-9964, 0920-9964
KW  - Index Medicus
KW  - Depression -- physiopathology
KW  - Analysis of Variance
KW  - Humans
KW  - Retrospective Studies
KW  - Anxiety -- physiopathology
KW  - Reflex, Startle -- physiology
KW  - Dose-Response Relationship, Radiation
KW  - Acoustic Stimulation -- methods
KW  - Depression -- etiology
KW  - Adult
KW  - Cohort Studies
KW  - Heart Rate -- physiology
KW  - Reflex, Startle -- radiation effects
KW  - Male
KW  - Anxiety -- etiology
KW  - Female
KW  - Functional Laterality
KW  - Galvanic Skin Response -- physiology
KW  - Brief Psychiatric Rating Scale -- statistics & numerical data
KW  - Autonomic Nervous System -- physiopathology
KW  - Schizophrenia -- physiopathology
KW  - Schizophrenia -- complications
KW  - Reaction Time -- physiology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-14
N1  - Date created - 2005-10-24
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Polymorphisms of the Toll-Like Receptors and Human Disease
AN  - 17080627; 6707956
AB  - The Toll-like receptor (TLR) family regulates both innate and adaptive immune responses. Given its broad effect on immunity, the function of TLRs in various human diseases has been investigated largely by comparing the incidence of disease among persons with different polymorphisms in the genes that participate in TLR signaling. These studies demonstrate that TLR function affects several diseases, including sepsis, immunodeficiencies, atherosclerosis, and asthma. These findings have resulted in new opportunities to study the pathogenesis of disease, identify subpopulations at greater risk of disease, and, potentially, identify novel therapeutic approaches.
JF  - Clinical Infectious Diseases
AU  - Schwartz, DA
AU  - Cook, D N
AD  - National Institute of Environmental Health Sciences, Research Triangle Park, NC, USA
Y1  - 2005/11/15/
PY  - 2005
DA  - 2005 Nov 15
SP  - S403
EP  - S407
VL  - 41
SN  - 1058-4838, 1058-4838
KW  - Microbiology Abstracts B: Bacteriology; Immunology Abstracts
KW  - Risk assessment
KW  - Sepsis
KW  - Gene polymorphism
KW  - Subpopulations
KW  - Immunodeficiency
KW  - Asthma
KW  - Arteriosclerosis
KW  - Immunity
KW  - Immune response
KW  - Toll-like receptors
KW  - Signal transduction
KW  - J 02350:Immunology
KW  - F 06950:Immunogenetics, MHC, HLA
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+Infectious+Diseases&rft.atitle=Polymorphisms+of+the+Toll-Like+Receptors+and+Human+Disease&rft.au=Schwartz%2C+DA%3BCook%2C+D+N&rft.aulast=Schwartz&rft.aufirst=DA&rft.date=2005-11-15&rft.volume=41&rft.issue=&rft.spage=S403&rft.isbn=&rft.btitle=&rft.title=Clinical+Infectious+Diseases&rft.issn=10584838&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Risk assessment; Sepsis; Subpopulations; Gene polymorphism; Immunodeficiency; Asthma; Immune response; Immunity; Arteriosclerosis; Toll-like receptors; Signal transduction
ER  - 



TY  - CPAPER
T1  - Live Cell-Based Assays for Compound Screening
T2  - Second Annual Conference on Fluorescent Proteins for Cellular Imaging and Drug Development
AN  - 40129077; 4041394
JF  - Second Annual Conference on Fluorescent Proteins for Cellular Imaging and Drug Development
AU  - Inglese, James
Y1  - 2005/11/14/
PY  - 2005
DA  - 2005 Nov 14
KW  - Screening
KW  - U 2000:Biological Sciences
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L2  - http://www.healthtech.com/2005/gfp/index.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Frontiers in Fluorescent Protein Imaging in Living Cells
T2  - Second Annual Conference on Fluorescent Proteins for Cellular Imaging and Drug Development
AN  - 40110722; 4041388
JF  - Second Annual Conference on Fluorescent Proteins for Cellular Imaging and Drug Development
AU  - Patterson, George
Y1  - 2005/11/14/
PY  - 2005
DA  - 2005 Nov 14
KW  - Imaging techniques
KW  - U 2000:Biological Sciences
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ER  - 



TY  - CPAPER
T1  - Analysis and Application of RNAi against Cancer Associated Genes
T2  - AACR-NCI-EORTC Conference on Molecular Targets and Cancer Therapeutics: Discovery, Biology, and Clinical Applications
AN  - 40055475; 4016049
JF  - AACR-NCI-EORTC Conference on Molecular Targets and Cancer Therapeutics: Discovery, Biology, and Clinical Applications
AU  - Caplen, Natasha
Y1  - 2005/11/14/
PY  - 2005
DA  - 2005 Nov 14
KW  - RNA-mediated interference
KW  - Cancer
KW  - U 2000:Biological Sciences
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N1  - Date revised - 2007-09-05
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ER  - 



TY  - CPAPER
T1  - Preclinical Development of Halichondrin B and its Derivative Eisai E7389
T2  - AACR-NCI-EORTC Conference on Molecular Targets and Cancer Therapeutics: Discovery, Biology, and Clinical Applications
AN  - 40051612; 4016006
JF  - AACR-NCI-EORTC Conference on Molecular Targets and Cancer Therapeutics: Discovery, Biology, and Clinical Applications
AU  - Newman, D J
Y1  - 2005/11/14/
PY  - 2005
DA  - 2005 Nov 14
KW  - Drug discovery
KW  - U 2000:Biological Sciences
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LA  - English
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N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - MMP2 Activates TGF-ss1 and Augments TssRII Signaling within the Aged Arterial Wall: Relevance to Matrix Deposition with Aging
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 40004478; 4110583
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Wang, Mingyi
AU  - Zhao, Di
AU  - Spinetti, Gaia
AU  - Zhang, Jing
AU  - Jiang, Li-Qun
AU  - Pintus, Gianfranco
AU  - Monticone, Robert E
AU  - Lakatta, Edward G
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Aging
KW  - Signal transduction
KW  - Gelatinase A
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Indices of Ventricular Relaxation are Not Related to Objective Measures of Exercise Capacity in Non-Obstructive Hypertrophic Cardiomyopathy
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39960896; 4109006
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Owens, David S
AU  - Arena, Ross A
AU  - Smith, Kevin
AU  - Mohiddin, Saidi A
AU  - McAreavey, Dorothea
AU  - Bacharach, Steve L
AU  - Ulisney, Karen L
AU  - Fananapazir, Lameh
AU  - Hadi, Mohiuddin
AU  - Plehn, Jonathan F
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Cardiomyopathy
KW  - Physical training
KW  - Circulatory system
KW  - Heart
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39960896?accountid=14244
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LA  - English
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Tnf Receptor-Associated Factor 2 (TRAF2) is an Important Adaptor in Activation of Nuclear Factor (NF-KB) and Activation Protein (AP-1) Pathways in Human B Cells
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39960211; 4104232
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Martins, Diana C
AU  - Zhang, Wen
AU  - Zhang, Xuan
AU  - He, Liusheng
AU  - Lipsky, Peter E
AU  - Grammer, Amrie C
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Cell activation
KW  - Lymphocytes B
KW  - Tumor necrosis factor
KW  - NF-^KB protein
KW  - TRAF2 protein
KW  - Adaptor proteins
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Bone Density and Metabolism in Patients with NOMID after 12 Months of Treatment with the IL-1 Receptor-Antagonist Anakinra/kineretRG
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39944745; 4103101
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Canna, S
AU  - Gelabert, A
AU  - Jones, J
AU  - Dailey, N J
AU  - Kastner, D
AU  - Reynolds, J
AU  - Goldbach-Mansky, R
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Bone density
KW  - Metabolism
KW  - Interleukin 1
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Impact of Rheumatoid Arthritis (RA) Core Set Measures on Rheumatologists Judgment of Disease Activity
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39941991; 4103343
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Aletaha, Daniel
AU  - Machold, Klaus P
AU  - Nell, Valerie P.K.
AU  - Smolen, Josef S
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Cores
KW  - Rheumatoid arthritis
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Prevalence of Infarct and Non-Infarct as the Etiology in Impaired Left Ventricular Systolic Function in the Elderly: A Gadolinium Enhanced Cardiac MRI Study
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39908609; 4108648
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Cao, Jie J
AU  - Sigurdsson, Sigurdur
AU  - Vincent, Pamela
AU  - Padmanabhan, Sriram
AU  - Holly, Jessica
AU  - Launer, Lenore
AU  - Aletras, Anthony H
AU  - Eiriksdottir, Gudny
AU  - Thorgeirsson, Gudmundur
AU  - Aspelund, Thor
AU  - Gudnason, Vilmundur
AU  - Harris, Tamara
AU  - Arai, Andrew E
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Gadolinium
KW  - Elderly
KW  - Etiology
KW  - Magnetic resonance imaging
KW  - Heart
KW  - Geriatrics
KW  - Aetiology
KW  - Circulatory system
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Heterogeneous Skeletal Muscle Perfusion Recovery after Stenting: Insight into Regional Ischemic Blood Flow Control
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39907826; 4107904
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Aviles, Ronnier J
AU  - Thompson, Richard B
AU  - Ozturk, Cengizhan
AU  - Raval, Amish N
AU  - DeSilva, Ranil
AU  - Stine, Annette
AU  - Wright, Victor
AU  - Raman, Venkatesh K
AU  - Balaban, Robert S
AU  - Lederman, Robert J
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Blood circulation
KW  - Ischemia
KW  - Perfusion
KW  - Skeletal muscle
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39907826?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Scientific+Sessions+of+the+American+Heart+Association&rft.atitle=Heterogeneous+Skeletal+Muscle+Perfusion+Recovery+after+Stenting%3A+Insight+into+Regional+Ischemic+Blood+Flow+Control&rft.au=Aviles%2C+Ronnier+J%3BThompson%2C+Richard+B%3BOzturk%2C+Cengizhan%3BRaval%2C+Amish+N%3BDeSilva%2C+Ranil%3BStine%2C+Annette%3BWright%2C+Victor%3BRaman%2C+Venkatesh+K%3BBalaban%2C+Robert+S%3BLederman%2C+Robert+J&rft.aulast=Aviles&rft.aufirst=Ronnier&rft.date=2005-11-13&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Scientific+Sessions+of+the+American+Heart+Association&rft.issn=&rft_id=info:doi/
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LA  - English
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Contribution of Hepatic and Extrahepatic ABCA1 to Plasma HDL-C and ApoB-Containing Lipoprotein Cholesterol in Transgenic Mice
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39892224; 4110770
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Liu, Lijuan
AU  - Joyce, Charles
AU  - Vaisman, Boris
AU  - Basso, Federica
AU  - Amar, Marcelo J A
AU  - Shamburek, Robert D
AU  - Santamarina-Fojo, Silvia
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Mice
KW  - Lipoproteins
KW  - Cholesterol
KW  - Liver
KW  - Transgenic mice
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Simple and Rapid Quantification of Mechanical Dyssynchrony for Cardiac Resynchronization Therapy
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39885360; 4109192
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Ashikaga, Hiroshi
AU  - Kellman, Peter
AU  - Mickelsen, Steven R
AU  - McVeigh, Elliot R
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Heart
KW  - Therapy
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Microalbuminuria and the Risk of Cardiovascular Events and All-Cause Mortality in the Elderly, the Cardiovascular Health Study
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39884722; 4108306
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Cao, Jie J
AU  - Biggs, Mary L
AU  - Barzilay, Joshua
AU  - Konen, Joseph
AU  - Psaty, Bruce M
AU  - Kuller, Lewis
AU  - Bleyer, Anthony J
AU  - Olson, Jean
AU  - Wexler, Jason
AU  - Summerson, John
AU  - Cushman, Mary
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Elderly
KW  - Mortality
KW  - Geriatrics
KW  - Cardiovascular diseases
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - An SLE-Associated Mutation in CD40 Alters Human B Cell Function
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39883841; 4104233
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Zhang, Wen
AU  - Fischer, Randy
AU  - He, Luisheng
AU  - Pisitkun, Prapaporn
AU  - Gaffney, P
AU  - Behrens, T
AU  - Lipsky, Peter E
AU  - Grammer, Amrie C
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Mutation
KW  - CD40 antigen
KW  - Lymphocytes B
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Gene Expression, Phenotypic and Proteomic Profile of Ig-Secreting Plasma Cells in the Periphery of Patients with Active Sle
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39880237; 4104228
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Lugar, Patricia
AU  - Slota, Rebecca
AU  - Fischer, Randy
AU  - Phillips, Terry
AU  - Brescia, AnneMarie
AU  - Lipsky, Peter
AU  - Grammer, Amrie C
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Gene expression
KW  - Plasma cells
KW  - Proteomics
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Performance-Based Assessment of Functional Limitation and Muscle Endurance: Reliability of the Adult Myositis Assessment Tool
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39877001; 4103852
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Harris-Love, Michael
AU  - Joe, Galen
AU  - Abbett, Kristen
AU  - Koziol, Dee
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Muscles
KW  - Myositis
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Amplified Profiling of Platelet Transcriptome in Sickle Cell Disease Reveals Global Activation and Dysregulated Arginine Processing
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39876908; 4110543
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Raghahavachari, Nalini
AU  - Villagra, Jose
AU  - Harris, Amy
AU  - Logun, Carolea
AU  - Xu, Xiuli
AU  - Munson, Peter
AU  - Kato, Gregory
AU  - Solomon, Michael A
AU  - Danner, Robert A
AU  - Gladwin, Mark T
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Platelets
KW  - Sickle cell disease
KW  - Arginine
KW  - Profiling
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Inducible Mitochondrial Uncoupling - An Endogenous Regulatory Mechanism Augmenting Tolerance to Cardiac Ischemia
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39875551; 4109711
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - McLeod, Christopher J
AU  - McCoy Jr, J Philip
AU  - Aziz, Abdulhameed
AU  - Sack, Michael N
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Ischemia
KW  - Mitochondria
KW  - Heart
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Specific Occupational Activities Associated with Functional Limitations in Patients with Long-Standing Ankylosing Spondylitis
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39875424; 4103603
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Ward, Michael M
AU  - Reveille, John D
AU  - Davis, John C
AU  - Weisman, Michael
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Ankylosing spondylitis
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - The Met66 Variant of the Functional Val66Met Polymorphism in the Brain-Derived Neurotrophic Factor Gene Confers Protection against Cognitive Dysfunction in Systemic Lupus Erythematosus (SLE)
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39869735; 4103569
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Lapteva, Larissa
AU  - Oroszi, Gabor
AU  - Davis, Elizabeth
AU  - Yarboro, Cheryl H
AU  - Lipsky, Peter E
AU  - Goldman, David
AU  - Hu, Xian-Zhang
AU  - Lipsky, Robert
AU  - Illei, Gabor G
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Systemic lupus erythematosus
KW  - Gene polymorphism
KW  - Brain-derived neurotrophic factor
KW  - Cognitive ability
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - The Impact of In Vivo Anti IL-6 Receptor Blockade on Circulating T and B Cell Subsets in Patients with Systemic Lupus Erythematosus
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39869133; 4103159
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Shirota, Yuko
AU  - Yarboro, Cheryl
AU  - Sims, Gary
AU  - Fritsch, Ruth
AU  - Ettinger, Rachel
AU  - Valencia, Xavier
AU  - Fischer, Randy
AU  - Grammer, Amrie
AU  - Pham, Tuyet-Hang
AU  - Lipsky, Peter E
AU  - Illei, Gabor G
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Lymphocytes B
KW  - Systemic lupus erythematosus
KW  - Interleukin 6 receptors
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Contribution of Nitric Oxide to Endothelial Progenitor Cell Mobilization, Survival and Differentiation Potential in Patients with Coronary Artery Disease Undergoing Cardiac Rehabilitation
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39865050; 4110264
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Rodrigo, Maria E
AU  - Benjamin, Moshe
AU  - Carlow, Andrea
AU  - Annavajjhala, Vidhya
AU  - Dejam, Andre
AU  - Paul, Jonathan D
AU  - Powell, Tiffany M
AU  - Thompson, Michael
AU  - McCoy, J Philip
AU  - Zalos, Gloria
AU  - Murphy, Mandy
AU  - Hill, Jonathan M
AU  - Gladwin, Mark
AU  - Orlic, Donald
AU  - Cannon III, Richard O
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Nitric oxide
KW  - Heart diseases
KW  - Coronary heart disease
KW  - Differentiation
KW  - Rehabilitation
KW  - Cell survival
KW  - Stem cells
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - S-Nitrosylation of the L-type Ca@@u2+@ Channel is Involved in Cardioprotection in Female Hearts
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39863819; 4107206
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Sun, Junhui
AU  - Picht, Eckard
AU  - Bers, Donald
AU  - Steenbergen, Charles
AU  - Murphy, Elizabeth
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Calcium channels (L-type)
KW  - Heart
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Accuracy of Glomerular Filtration Rate (GFR) Prediction Equations in Patients with Immune-Mediated Glomerulonephritides (GN)
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39860142; 4104083
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Illei, Gabor G
AU  - Jacobs, Geneva
AU  - Austin, Howard
AU  - Ward, Michael
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Filtration
KW  - Glomerular filtration rate
KW  - Mathematical models
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Trends in Diabetes as a Cardiovascular Disease Risk Factor: the Framingham Heart Study
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39857965; 4108325
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Fox, Caroline S
AU  - Coady, Sean
AU  - Sorlie, Paul D
AU  - D'Agostino Sr, Ralph B
AU  - Vasan, Ramachandran S
AU  - Meigs, James B
AU  - Levy, Daniel
AU  - Savage, Peter J
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Cardiovascular diseases
KW  - Risk factors
KW  - Diabetes mellitus
KW  - Heart
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Myeloperoxidase (MPO) Modulates Risk for Developing Congestive Heart Failure (CHF)
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39852900; 4109162
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Aviles, Ronnier J
AU  - Brennan, Marie-Luise
AU  - Mann, Shirley
AU  - Tracy, Russell P
AU  - Psaty, Bruce M
AU  - Hazen, Stanley L
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Congestive heart failure
KW  - Risk factors
KW  - Peroxidase
KW  - Heart
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - ABCG1-Modifed Plasma Membrane Lipid Domains Mediate Cellular Cholesterol Efflux to HDL
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39850818; 4110632
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Neufeld, Edward B
AU  - O'Brien, Katherine G
AU  - Demosky Jr, Stephen J
AU  - Stonik, John A
AU  - Sabol, Steven L
AU  - Malide, Daniela
AU  - Combs, Christian A
AU  - Remaley, Alan T
AU  - Santamarina-Fojo, Silvia
AU  - Brewer Jr, H Bryan
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Lipid rafts
KW  - Plasma membranes
KW  - Cholesterol
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Validity of the Myositis Disease Activity Assessment Tool (MDAAT) for Assessing Extra-Muscular Disease Activity in Adult and Juvenile Idiopathic Inflammatory Myopathies (IIM)
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39848655; 4103891
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Rider, Lisa
AU  - Villalba, Maria
AU  - Adams, Elizabeth
AU  - Joe, Galen
AU  - Harris-Love, Michael
AU  - Hill, Suvimol
AU  - James-Newton, Laura
AU  - Hicks, Jeanne
AU  - Plotz, Paul
AU  - Lachenbruch, Peter
AU  - Miller, Frederick
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Myositis
KW  - Inflammation
KW  - Myopathy
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Treatment of 4 Patients with Cryopyrin-Associated Periodic Syndromes with the Long-Acting Il-1 Inhibitor Il-1 Trap
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39846580; 4102932
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Canna, S
AU  - Gelabert, A
AU  - Aksentijevich, I
AU  - Mellis, S
AU  - Radin, A
AU  - Papadopoulos, J
AU  - Barham, B
AU  - Wilson, M
AU  - Hawkins, P
AU  - Kastner, D
AU  - Goldbach-Mansky, R
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Interleukin 1
KW  - Inhibitors
KW  - Symptoms
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Seasonal Birth Patterns in Subgroups of Myositis Suggest a Role for Perinatal Environmental Factors in Etiology
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39845595; 4103649
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Vegosen, Leora
AU  - Weinberg, Clarice
AU  - O'Hanlon, Terrance
AU  - Targoff, Ira
AU  - Koneru, Bhanu
AU  - Mamyrova, Gulnara
AU  - Miller, Frederick
AU  - Rider, Lisa
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Seasonal variations
KW  - Etiology
KW  - Sulfur dioxide
KW  - Myositis
KW  - Birth
KW  - Environmental factors
KW  - Aetiology
KW  - Parturition
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Analysis of Multiple Serum Cytokines and Chemokines in SLE Patients Demonstrates that They Highly Correlate to Each Other and Fails to Identify a Principal Effector Molecule
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39844877; 4103585
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Illei, Gabor G
AU  - Phillips, Terry M
AU  - Yarboro, Cheryl
AU  - Pham, Tuyet-Hang
AU  - Sun, Hong-Wei
AU  - Lipsky, Peter E
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Cytokines
KW  - Chemokines
KW  - Serum
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Defective Suppressor Function of CD4+CD25hi T Regulatory Cells in Active SLE
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39842472; 4104666
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Valencia, Xavier
AU  - Vogt, Samantha L
AU  - Simone, James
AU  - Yarboro, Cheryl
AU  - Illei, Gabor
AU  - Lipsky, Peter E
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Lymphocytes T
KW  - Immunoregulation
KW  - Suppressors
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Myocardial Iron Is Not Significantly Abnormal in Patients with Minimally Symptomatic Hereditary Hemochromatosis
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39840634; 4108717
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Padmanabhan, Sriram
AU  - Shizukuda, Yukitaka
AU  - Aletras, Anthony H
AU  - Mordini, Federico
AU  - Ingkanisorn, W Patricia
AU  - Cao, Jie
AU  - Tripodi, Dottie
AU  - Rosing, Douglas R
AU  - Bolan, Charles D
AU  - Leitman, Susan F
AU  - Arai, Andrew E
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Iron
KW  - Hemochromatosis
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Comparison of Patients' Judgments of Improvement in Rheumatoid Arthritis with ACR and EULAR Response Criteria
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39840550; 4103351
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Ward, Michael M
AU  - Guthrie, Lori C
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Rheumatoid arthritis
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Changes in Selected Proteins Associated with Osteoarthritis Development in the Baltimore Longitudinal Study of Aging (BLSA)
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39839031; 4103180
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Ling, Shari M
AU  - Patel, Dhavalkumar
AU  - Zhan, Ming
AU  - Taub, Dennis
AU  - Muller, Denis
AU  - Bathon, Joan
AU  - Hochberg, Marc
AU  - Abernethy, Darrell
AU  - Metter, E
AU  - Ferrucci, Luigi
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - USA, Maryland, Baltimore
KW  - Aging
KW  - Osteoarthritis
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Functional Characteristics of Children with Neonatal Onset Multisystem Inflammatory Disease (NOMID)
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39835976; 4104861
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Canna, Scott
AU  - Paul, Scott M
AU  - Hildenbrand, Hanna
AU  - Jain, Mina
AU  - Smith, Michaele R
AU  - Comis, Leora
AU  - Goldbach-Mansky, Raphaela
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Children
KW  - Neonates
KW  - Inflammatory diseases
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Transcript Profiling of Peripheral Blood Circulating Endothelial Cells
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39827602; 4107574
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Raghavachari, Nalini
AU  - Khan, Sameena S
AU  - Elshal, Mohamed
AU  - Barb, Jennifer
AU  - Logun, Carolea
AU  - Munson, Peter J
AU  - Gladwin, Mark T
AU  - McCoy, J Philip
AU  - Danner, Robert L
AU  - Solomon, Michael A
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Peripheral blood
KW  - Blood circulation
KW  - Transcription
KW  - Endothelial cells
KW  - Profiling
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Ghrelin Improves Endothelial Function in Patients with Metabolic Syndrome
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39825983; 4108032
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Iantorno, Micaela
AU  - Schinzari, Francesca
AU  - Tesauro, Manfredi
AU  - Rizza, Stefano
AU  - Melina, Domenico
AU  - Lauro, Davide
AU  - Cardillo, Carmine
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Ghrelin
KW  - Symptoms
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Cardiac-Specific Ablation of the Na@@u+@/Ca@@u2+@ Exchanger Confers Protection against Ischemia-Reperfusion Injury
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39811868; 4109747
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Imahashi, Kenichi
AU  - Steenbergen, Charles
AU  - Philipson, Kenneth D
AU  - Murphy, Elizabeth
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Injuries
KW  - Na@u+/Ca@@u2+@-exchanging ATPase
KW  - Calcium
KW  - Ablation
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - DRB1*0301 and the Second Hypervariable Region DRB1 Motif, @@u70@QKRGR@@u74@ are HLA Risk Factors for Dermatomyositis (DM) in African-American (AA) Patients
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39804491; 4103872
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Mamyrova, Gulnara
AU  - O'Hanlon, Terrance
AU  - Carrick, Danielle
AU  - Malley, James
AU  - Miller, Frederick
AU  - Rider, Lisa
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Africa
KW  - Histocompatibility antigen HLA
KW  - Dermatomyositis
KW  - Risk factors
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Relative Importance of Immunogenetic Risk and Protective Factors for the Development of Juvenile Dermatomyositis (JDM) in European American (EA) Patients
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39801202; 4103873
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Mamyrova, Gulnara
AU  - Carrick, Danielle
AU  - O'Hanlon, Terrance
AU  - Malley, James
AU  - Reed, Ann
AU  - Sherry, David
AU  - Wallace, Carol
AU  - James-Newton, Laura
AU  - Zemel, Lawrence
AU  - Perez, Maria
AU  - Lindsley, Carol
AU  - Miller, Frederick
AU  - Rider, Lisa
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Immunogenetics
KW  - Dermatomyositis
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Functional Outcomes of Treatment of Neonatal Onset Multisystem Inflammatory Disease (NOMID) with Anakinra: Preliminary Results
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39798493; 4104439
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Paul, Scott M
AU  - Hildenbrand, Hanna
AU  - Jain, Mina
AU  - Smith, Michaele R
AU  - Canna, Scott
AU  - Comis, Leora
AU  - Wiggs, Edith
AU  - Goldbach-Mansky, Raphaela
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Neonates
KW  - Inflammatory diseases
KW  - Disease control
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Functional and Phenotypic Characterization of Anergic B Cells Circulating in the Periphery of Patients with Systemic Lupus Erythematosus
T2  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AN  - 39798303; 4103583
JF  - 69th Annual Meeting of the American College of Rheumatology and 40th Annual Meeting of the Association of Rheumatology Health Professionals
AU  - Fischer, Randy T
AU  - Slota, Rebecca
AU  - Longo, Nancy
AU  - Lugar, Patricia
AU  - Sohn, Hae Won
AU  - Illei, Gabor
AU  - Phillips, Terry
AU  - Lipsky, Peter
AU  - Grammer, Amrie
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Lymphocytes B
KW  - Systemic lupus erythematosus
KW  - Anergy
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39798303?accountid=14244
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Activation of CaMKII at Mitochondria Triggers Apoptotic Cardiomyocyte Death
T2  - 2005 Scientific Sessions of the American Heart Association
AN  - 39782301; 4109821
JF  - 2005 Scientific Sessions of the American Heart Association
AU  - Zhu, Weizhong
AU  - yang, Dongmei
AU  - Crow, Mike T
AU  - Xiao, Rui-Ping
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - Mortality
KW  - Apoptosis
KW  - Cardiomyocytes
KW  - Mitochondria
KW  - Ca@@u2+@/calmodulin-dependent protein kinase II
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Advancing Environmental Toxicogenomics.
T2  - 26th Annual Meeting of the Society of Environmental Toxicology and Chemistry
AN  - 39721616; 4024402 DE:
JF  - 26th Annual Meeting of the Society of Environmental Toxicology and Chemistry
AU  - Waters, M
Y1  - 2005/11/13/
PY  - 2005
DA  - 2005 Nov 13
KW  - U 2000:Biological Sciences
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Brainstem Immunoreactivity Response to Chronic Laryngeal Inflammation in the Rat
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 40010434; 4132688
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Simonyan, K
AU  - Buckholdt, K
AU  - Ludlow, C L
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Immunoreactivity
KW  - Inflammation
KW  - Brain stem
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Offspring of VIP/PHI - Deficient Mice Exhibit Developmental Delays
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 40003083; 4128515
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Cuasay, K
AU  - May, V
AU  - Waschek, J A
AU  - Hill, J M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Offspring
KW  - Mice
KW  - Progeny
KW  - Vasoactive intestinal peptide
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Comparison of Human Corticospinal Input - output Characteristics Related to Motor Learning and PAS Intervention
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 40000535; 4129493
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Meunier, S O
AU  - Russmann, H
AU  - Hallett, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Motor skill learning
KW  - Pyramidal tracts
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Characterization of the Hereditary Spastic Paraplegia 3A ( SPG3A ) Protein Atlastin - 1 and Related Family Members
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39998942; 4126440
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Soderblom, C
AU  - Zhu, P
AU  - Stadler, J
AU  - Blackstone, C D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Spastic paraplegia
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Distinct NMDA Receptor Subtypes at ON and OFF Inputs to Retinal Ganglion Cells
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39995709; 4127269
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kalbaugh, T L
AU  - Diamond, J S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Retinal ganglion cells
KW  - Glutamic acid receptors
KW  - N-Methyl-D-aspartic acid receptors
KW  - Ganglia
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39995709?accountid=14244
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Membrane - Targeting of Phosducin or Phosducin Like - Protein Occludes Voltage - Dependent Inhibition of N - Type Calcium Channels in Rat Superior Cervical Ganglia Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39995516; 4127253
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Partridge, J G
AU  - Ikeda, S R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Membranes
KW  - Phosducin
KW  - Calcium channels
KW  - Ganglia
KW  - Calcium channels (voltage-gated)
KW  - Neurons
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Isolation and Characterization of an Enriched Preparation of Oligodendrocyte Progenitor Cell Membranes from Rat Cortex
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39993310; 4134345
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Weerth, S H
AU  - Hauser, J
AU  - Russell, J T
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Cell membranes
KW  - Glial stem cells
KW  - Cortex
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Social Experience Facilitates Aggression in Mice Lacking a Functional Vasopressin 1b Receptor Gene
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39991386; 4121039
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Caldwell, H K
AU  - Young, W S
AU  - Wersinger, S R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mice
KW  - Aggression
KW  - Vasopressin
KW  - Aggressive behaviour
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Neuronal Avalanche Dynamics are Independent of Initiating Event Size and Maintain Event Size Memory
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39988805; 4130851
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Thiagarajan, T C
AU  - Plenz, D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Avalanches
KW  - Memory
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - PICK1 is Required for Presynaptic Mossy Fiber - - CA3 Interneuron LTD
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39986171; 4125571
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Pelkey, K A
AU  - Racca, C
AU  - Takamiya, K
AU  - Xia, J
AU  - Huganir, R L
AU  - McBain, C J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Fibers
KW  - Long-term depression
KW  - Interneurons
KW  - Mossy fibers
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Activity - Related Redistribution of Presynaptic Proteins at the Active Zone
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39985713; 4118968
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Tao-Cheng, J H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Proteins
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - New Cellular Mechanisms for Multiple Time - Scale Adaptation in Cerebellum
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39983780; 4120013
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Hong, S Y
AU  - Optican, L M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Adaptations
KW  - Cerebellum
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Unique Execution of NO - Mediated Toxicity within Naive and NGF - Differentiated PC12 Cells
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39939662; 4134945
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Brynczka, C
AU  - Merrick, B
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Toxicity
KW  - Pheochromocytoma cells
KW  - Nerve growth factor
KW  - Nitric oxide
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Self - Renewal of Rat Neural Stem Cells at the Beginning of Cortical Neurogenesis Does Not Require the Contribution of Endogenous Endothelial Cells
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39934827; 4132115
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Maric, D
AU  - Chang, Y H
AU  - Barker, J L
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Neurogenesis
KW  - Endothelial cells
KW  - Neural stem cells
KW  - Self
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Enhanced Slow Oscillations in Neuronal Activity of Basal Ganglia Output Nuclei after Dopamine Cell Lesion in Urethane Anesthetized Rats: Exploring Effects on Ventrolateral Thalamus and Motor Cortex
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39934800; 4124504
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Parr-Brownlie, L C
AU  - Bergstrom, D A
AU  - Itoga, C A
AU  - Hu, D.
AU  - Smith, C.P.S.
AU  - Walters, J R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Carbamate compounds
KW  - Lesions
KW  - Rats
KW  - Oscillations
KW  - Basal ganglia
KW  - Urethane
KW  - Cortex (motor)
KW  - Thalamus
KW  - Dopamine
KW  - Ganglia
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Inhibition of GSK - 3 or HDAC Increases the Activity of BDNF Promoter III
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39934001; 4131901
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Yasuda, S
AU  - Liang, M H
AU  - Chuang, D M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Promoters
KW  - Histone deacetylase
KW  - Brain-derived neurotrophic factor
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Neuronal Activity Promotes Conversion of Pro - to Mature Brain - Derived Neurotrophic Factor (BDNF) in the Dendrites of Hippocampal Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39932163; 4125353
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Nagappan, G
AU  - Zaitsev, E
AU  - Chang, J H
AU  - Lu, B.
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain-derived neurotrophic factor
KW  - Neurotrophic factors
KW  - Hippocampus
KW  - Neurons
KW  - Dendrites
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Identification of Cardiotrophin - 1 As a VIP and Choline Acetyltransferase - Inducing Factor in Extracts of Rat Footpads
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39930332; 4125330
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Coulombe, J N
AU  - Habecker, B
AU  - Guidry, G
AU  - McKinnon, L
AU  - Jaffe, H
AU  - Sun, Y E
AU  - Landis, S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Vasoactive intestinal peptide
KW  - Choline O-acetyltransferase
KW  - Choline
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39930332?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Behavioral Phenotypes of Galanin Receptor Subtype 2 Null Mutant Mice
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39930111; 4134839
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Bailey, K R
AU  - Hohmann, J G
AU  - Pavlova, M
AU  - Crawley, J N
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mice
KW  - Mutants
KW  - Galanin receptors
KW  - Phenotypes
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Identification of a Novel Transmembrane Protein Important for Oligodendrocyte Membrane Formation Using Gene Expression Profiling
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39928010; 4132212
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Nielsen, J A
AU  - Maric, D
AU  - Lau, P
AU  - Barker, J L
AU  - Hudson, L D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Membrane proteins
KW  - Gene expression
KW  - Oligodendrocytes
KW  - Profiling
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Task Channels Mediate Leak Currents That Modulate Respiratory Rhythm Generation In Vitro
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39926956; 4132755
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Smerin, S E
AU  - Koizumi, H
AU  - Zhang, R
AU  - Moorjani, B
AU  - Smith, J C
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Channels
KW  - Respiration
KW  - Rhythms
KW  - Metabolism
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Specific Endosomal Associations During the Trafficking of Synaptic Glutamate Receptors
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39926613; 4133922
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Petralia, R S
AU  - Dunbar, L A
AU  - Wang, Y
AU  - Wenthold, R J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Glutamic acid receptors
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Peripheral Nerve Stimulation (PNS) Enhances Learning of a Functional Motor Task in Chronic Stroke Patients
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39925938; 4129490
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Celnik, P A
AU  - Hummel, F
AU  - Harris-Love, M
AU  - Cohen, L G
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Peripheral nerves
KW  - Learning
KW  - Stroke
KW  - Peripheral nervous system
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Characterization of the Pituitary Adenylate Cyclase Activating Polypeptide (PACAP) Receptor in Bovine Chromaffin Cells that Mediates Calcium - dependent Secretion
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39924423; 4130665
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Mustafa, T
AU  - Eiden, L E
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Calcium
KW  - Secretion
KW  - Pituitary adenylate cyclase-activating polypeptide
KW  - Chromaffin cells
KW  - Pituitary adenylate cyclase-activating polypeptide receptors
KW  - Polypeptides
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Degenerative Changes in the Peripheral Retina of Transgenic Animals Containing the Mutated Mouse Myocilin Gene
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39924328; 4126453
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Senatorov, V V
AU  - Malyukova, I V
AU  - Fariss, R N
AU  - Wawrousek, E F
AU  - Swaminathan, S
AU  - Sharan, S K
AU  - Tomarev, S I
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Retina
KW  - Transgenic animals
KW  - U 7000:Multidisciplinary
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Effect of Catechol - O - Methyltransferase val158met Genotype on Attentional Control
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39923908; 4132951
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Blasi, G
AU  - Mattay, V S
AU  - Bertolino, A
AU  - Elvevag, B
AU  - Callicott, J H
AU  - Das, S
AU  - Kolachana, B S
AU  - Egan, M F
AU  - Goldberg, T E
AU  - Weinberger, D R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Attention
KW  - Genotypes
KW  - Methyltransferase
KW  - Catechol
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Mouse Disabled - 1 Regulates Neuronal Nuclear Positioning in a Drosophila Eye Model
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39923901; 4132154
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Pramatarova, A
AU  - Ochalski, P G
AU  - Matsuki, T
AU  - Lee, C H
AU  - Howell, B W
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Eye
KW  - Positioning systems
KW  - Drosophila
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Lithium Normalizes Dendritic Localization of val66met Polymorphism of Brain - derived Neurotrophic Factor ( BDNFmet ): Therapeutic Implications
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39923787; 4131893
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Du, J.
AU  - Suzuki, K
AU  - Guhan, N
AU  - Wei, Y
AU  - Wu, J.
AU  - Lu, B.
AU  - Manji, H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Lithium
KW  - Brain
KW  - Neurotrophic factors
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - 5'UTR of BDNF Transcript Dictates mRNA Trafficking and Local Translation in Dendrites of Hippocampal Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39922370; 4125352
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Zaitsev, E N
AU  - Guhan, N
AU  - Yang, F
AU  - Lu, B.
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Translation
KW  - Transcription
KW  - 5' Untranslated regions
KW  - Brain-derived neurotrophic factor
KW  - Hippocampus
KW  - Neurons
KW  - Dendrites
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Striatal Volumes in Young Alcoholics and Children of Alcoholics
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39921822; 4121745
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Hommer, D W
AU  - Momenan, R
AU  - Bjork, J M
AU  - Kerich, M J
AU  - Israe, M E
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Children
KW  - Alcoholics
KW  - Neostriatum
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Measurement of Trophins, Peptides and Cytokines in Blood of Down Syndrome and Autistic Newborns and Controls
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39919058; 4128513
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Nelson, P G
AU  - Kuddo, T
AU  - Song, E
AU  - Dambrosia, J
AU  - Kohler, S
AU  - Satyanarayana, G
AU  - VanDunk, C
AU  - Grether, J
AU  - Nelson, K B
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Blood
KW  - Cytokines
KW  - Down's syndrome
KW  - Neonates
KW  - Peptides
KW  - Symptoms
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Odorant - induced Activity Accelerates Glomerular Refinement in the Mammalian Olfactory Bulb
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39918816; 4129011
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kerr, M A
AU  - Belluscio, L
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Odors
KW  - Odorants
KW  - Olfactory bulb
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Endogenous and Exogenous Cannabinoids Potentiate Glycine Receptor - mediated Responses Through a CB Receptor Independent Mechanism in Xenopus Oocytes
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39918365; 4130648
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Sun, H
AU  - Hejazi, N
AU  - Oz, M.
AU  - Zhang, L
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Oocytes
KW  - Glycine receptors
KW  - Amphibiotic species
KW  - Xenopus
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - A Novel Experimental Strategy that Allows the Identification of Functionally Critical Amino Acids in the M3 Muscarinic Acetylcholine Receptor 149 G-Protein-Linked Receptors: Muscarinic
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39918180; 4122106
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Li, B.
AU  - Scarselli, M
AU  - Knudsen, C D
AU  - McMillin, S M
AU  - Wess, J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Amino acids
KW  - Acetylcholine receptors (muscarinic)
KW  - Neurotransmitters
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Maturation of GABA@@dA@ Receptor - Mediated Synaptic Transmission in Adult - Born Dentate Gyrus Granule Cells
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39917578; 4121992
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Karten, Y.J.G.
AU  - Brewer, M D
AU  - Dayer, A G
AU  - Cameron, H A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Granule cells
KW  - ^g-Aminobutyric acid A receptors
KW  - Synaptic transmission
KW  - Dentate gyrus
KW  - Sexual maturity
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Are Task Channels a Target for Muscarinic Modulation in Hippocampal Interneurons?
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39917298; 4128928
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Torborg, C L
AU  - Lawrence, J
AU  - Jeffries, B
AU  - Berg, A P
AU  - Bayliss, D A
AU  - McBain, C J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Channels
KW  - Interneurons
KW  - Hippocampus
KW  - Acetylcholine receptors (muscarinic)
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Reduced Prefrontal g - Aminobutyric Acid Levels in Patients with Current Major Depression Determined by Proton Magnetic Resonance Spectroscopy
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39913630; 4119166
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Hasler, G
AU  - van der Veen, J
AU  - Tumonis, T
AU  - Shen, J
AU  - Drevets, W
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Spectroscopy
KW  - Depression
KW  - Magnetic resonance spectroscopy
KW  - Resonance
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Dynamics of Ca@@u2+@ Signals in Soma and Dendrities Due to Activation of Nicotinic Acetylcholine Receptors in Rat Hippocampal Interneurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39913496; 4133986
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Fayuk, D A
AU  - Yakel, J L
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Acetylcholine receptors (nicotinic)
KW  - Interneurons
KW  - Hippocampus
KW  - Calcium signalling
KW  - Neurotransmitters
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Effects of Local Protein Synthesis on Axonal Mitochondria in Superior Cervical Ganglion Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39912995; 4127094
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Hillefors, M S
AU  - Gioio, A E
AU  - Kaplan, B B
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Superior cervical ganglion
KW  - Protein biosynthesis
KW  - Mitochondria
KW  - Neurons
KW  - Protein synthesis
KW  - Ganglia
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Modulation of Neuronal Activity in the Pre - Botzinger Complex by Medullary Raphe Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39912747; 4127796
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Ptak, K
AU  - Milescu, L S
AU  - Richerson, G B
AU  - Smith, J C
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Neuromodulation
KW  - Neurons
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - A Role for PICK1 - Dependent GluR2 Trafficking in Depolarization - Induced Depression (DID) at Hippocampal Mossy Fiber - - CA3 Pyramid Synapses
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39911516; 4125572
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Ho, T W
AU  - Pelkey, K A
AU  - Takamiya, K
AU  - Xia, J
AU  - Huganir, R L
AU  - McBain, C J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Fibers
KW  - Depression
KW  - Synaptic depression
KW  - ^a-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptors
KW  - Hippocampus
KW  - Mossy fibers
KW  - Synapses
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Neuregulin - 1 Depotentiates LTP at Hippocampal CA1 Synapses
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39911235; 4127329
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Buonanno, A
AU  - Kwon, O
AU  - Longart, M
AU  - Hoffman, D
AU  - Vullhorst, D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Long-term potentiation
KW  - Neuregulin
KW  - Synapses
KW  - Hippocampus
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Characterization of a Truncated Isoform of Human Metabotropic Glutamate Receptor 3
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39910629; 4120241
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Sartorius, L J
AU  - Lipska, B K
AU  - Sei, Y
AU  - Ren-Patterson, R
AU  - Kleinman, J E
AU  - Harrison, P J
AU  - Weinberger, D R
AU  - Lu, B.
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Glutamic acid receptors (metabotropic)
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Human Motor Cortical Oscillatory Activation Patterns in Ipsilateral Versus Contralateral Self - Paced Movements: An ECoG Study
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39909418; 4124561
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Mari, Z
AU  - Matsuhashi, M
AU  - Wheaton, L
AU  - Sato, S
AU  - Hallett, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Self
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Neuronal Excess of Ferroxidase - active Ferritin Causes Late - onset Neurodegeneration in Drosophila
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39908579; 4129957
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Missirlis, F
AU  - Kosmidis, S
AU  - Botella, J A
AU  - Schnewuly, S
AU  - Skoulakis, E.M.C.
AU  - Rouault, T A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Neurodegeneration
KW  - Ferritin
KW  - Ferroxidase
KW  - Drosophila
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - GnRH - 1 Regulates GnRH - 1 Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39907769; 4127755
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Duittoz, A
AU  - Constantin, S
AU  - Skinner, D
AU  - Wray, S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Gonadotropin-releasing hormone
KW  - Neurons
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Inhibition of Corticotrophin - Releasing Hormone Transcription by Inducible cAMP Early Repressor(ICER)
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39906280; 4119158
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Liu, Y
AU  - Aguilera, G
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Hormones
KW  - Transcription
KW  - Cyclic AMP
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - The Effects of Cholecystokinin on Ventral Neurons in the Spinal Cord of the Neonatal Rat and Mouse
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39906265; 4129288
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Yang, K
AU  - Morales, M
AU  - Renaud, L P
AU  - O'Donovan, M J
AU  - Lupica, C R
AU  - Oz, M.
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Spinal cord
KW  - Cholecystokinin
KW  - Neonates
KW  - Neurons
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - EEG Coherence Analysis of Visuomotor Networks: Distinguishable Paths in the Brain for Varying Processing Demands
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39905777; 4124273
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Wheaton, L A
AU  - Hattori, N
AU  - Hallett, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain
KW  - Oculomotor behavior
KW  - EEG
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Rhesus Monkeys with Orbital Prefrontal Cortex Lesions can Learn to Inhibit Prepotent Responses in the Reversed - Reward Contingency Task
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39903525; 4134857
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Chudasama, Y
AU  - Kralik, J D
AU  - Murray, E A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Lesions
KW  - Reinforcement
KW  - Contingency
KW  - Cortex (prefrontal)
KW  - Macaca mulatta
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39903525?accountid=14244
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - PKC and GRK Regulation of D@@d1@ Dopamine Receptor Signaling
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39903158; 4120259
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Rankin, M L
AU  - Sibley, D R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Signal transduction
KW  - Dopamine D1 receptors
KW  - Protein kinase C
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - D@@d1@ Dopamine Receptor Expression is Regulated by Direct Interaction with the Chaperone Protein Calnexin
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39903095; 4120258
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Free, R B
AU  - Hazelwood, L A
AU  - Cabrera, D M
AU  - Spalding, H N
AU  - Sibley, D R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Chaperones
KW  - Dopamine D1 receptors
KW  - Calnexin
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Two Neural Circuits for Learning DNMS with Short Delays
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39902440; 4120885
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Malloy, M M
AU  - Turchi, J
AU  - Lowther, R
AU  - Yu, D.
AU  - Saunders, R C
AU  - Mishkin, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Learning
KW  - Neural networks
KW  - U 7000:Multidisciplinary
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Dissociation of Emotion-Laden and Cognitive Prefrontal Cortical Activity
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39901759; 4122904
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Goldman, A L
AU  - Pezawas, L
AU  - Chen, G
AU  - Meyer-Lindenberg, A
AU  - Goldberg, T E
AU  - Saad, Z S
AU  - Mattay, V S
AU  - Weinberger, D R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Cognitive ability
KW  - Dissociation
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Suppressive Effect of Peripheral Stimulation on Corticospinal Excitability Decreases for Muscle Involved in a Motor - Learning Task
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39901378; 4122563
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Russmann, H
AU  - Meunier, S O
AU  - Hallett, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Muscles
KW  - Motor skill learning
KW  - Pyramidal tracts
KW  - Excitability
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39901378?accountid=14244
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Brain Metabolic Fluctuations During Sleep
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39900839; 4122826
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Fukunaga, M
AU  - Horovitz, S G
AU  - van Gelderen, P
AU  - de Zwart, J.A.
AU  - Duyn, J H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain
KW  - Sleep
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Oxidative Modifications of CaMKII Inhibit its Autophosphorylation
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39900460; 4123301
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Shetty, P K
AU  - Huang, F
AU  - Huang, K
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Ca@@u2+@/calmodulin-dependent protein kinase II
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Functional Identification of Distinct Populations of Neurons Involved in Drosophila Wing Expansion
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39899903; 4120670
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Lemon, W C
AU  - Luan, H
AU  - Nitabach, M N
AU  - Holmes, T C
AU  - White, B H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Wings
KW  - Neurons
KW  - Drosophila
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Scopolamine Differentially Modulates Attention and Emotion
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39899850; 4128009
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Furey, M L
AU  - Drevets, W C
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Scopolamine
KW  - Emotions
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Microglial NADPH Oxidase is the Target of Femtomolar Neuroprotection Against Oxidative Stress for GIF, Tripeptide of PACAP - 38
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39899791; 4133904
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Yang, S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Stress
KW  - Oxidative stress
KW  - NADPH oxidase
KW  - Pituitary adenylate cyclase-activating polypeptide
KW  - Neuroprotection
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Functional Neuroimaging of Ambiguous Haplotypes Reveals Impact of Genetic Variation in COMT on Prefrontal Function
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39899419; 4126070
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Meyer-Lindenberg, A S
AU  - Nichols, T
AU  - Callicott, J
AU  - Ding, J
AU  - Kolachana, B
AU  - Buckholtz, J
AU  - Straub, R
AU  - Mattay, V S
AU  - Egan, M
AU  - Weinberger, D R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Neuroimaging
KW  - Haplotypes
KW  - Genetic diversity
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - COMT val@@u158@met Polymorphism Impacts on Reactivity of Amygdala to Emotion - Laden Stimuli
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39899068; 4123022
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Mattay, V S
AU  - Blasi, G
AU  - Alce, G
AU  - Das, S
AU  - Callicott, J H
AU  - Kolachana, B S
AU  - Egan, M F
AU  - Sambataro, F
AU  - Meyer-Lindenberg, A
AU  - Hariri, A R
AU  - Weinberger, D R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Amygdala
KW  - Emotions
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Ethanol Inhibits BDNF - Stimulated ERK Activation in Cerebellar Granule Cells
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39898550; 4123670
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Davis, M I
AU  - Ohrtman, J D
AU  - Stancik, E K
AU  - Lovinger, D M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Ethanol
KW  - Granule cells
KW  - Cerebellum
KW  - Brain-derived neurotrophic factor
KW  - Extracellular signal-regulated kinase
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Rapid Antibody Staining of GnRH - 1 Neurons for Subsequent Laser - Capture Microdissection and RT - PCR Analysis
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39898340; 4127754
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Reuss, A E
AU  - Wray, S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Lasers
KW  - Antibodies
KW  - Polymerase chain reaction
KW  - Neurons
KW  - Gonadotropin-releasing hormone
KW  - Nucleotide sequence
KW  - Staining
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39898340?accountid=14244
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TY  - CPAPER
T1  - Action Potential - Dependent Signaling between Axons and Glia
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39897675; 4125649
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Lee, P R
AU  - Fields, R D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Signal transduction
KW  - Action potential
KW  - Glia
KW  - Axons
KW  - Neurons
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Kinetics of Penetration Influence the Apparent Potency of Vanilloids on TRPV1
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39896380; 4125787
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Lazar, J
AU  - Braun, D C
AU  - Toth, A
AU  - Wang, Y
AU  - Pearce, L V
AU  - Pavlyukovets, V A
AU  - Choi, H
AU  - Lee, J
AU  - Blumberg, P M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Kinetics
KW  - Capsaicin receptors
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Selectivity for Cyclopean Contours in Macaque V2 Reflects Properties of a Simple Mechanism, Rather than High - Level Edge Representation
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39896310; 4119578
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Bredfeldt, C E
AU  - Cumming, B G
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Macaca
KW  - U 7000:Multidisciplinary
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - COMT Val158Met Genotype and IQ Interact to Predict BOLD Response to Working Memory Challenge in Prefrontal Cortex
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39894790; 4126068
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Buckholtz, J W
AU  - Meyer-Lindenberg, A
AU  - Tan, H Y
AU  - Sust, S
AU  - Egan, M F
AU  - Goldberg, T E
AU  - Mattay, V S
AU  - Kolachana, B
AU  - Weinberger, D R
AU  - Callicott, J H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Short term memory
KW  - Cortex (prefrontal)
KW  - Genotypes
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - A Chemical - Library Approach to Mining the Receptorome
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39893866; 4125398
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Roth, B L
AU  - Birkes, J A
AU  - Evans, J
AU  - Kroeze, W K
AU  - Fan, Y
AU  - Beeler, A A
AU  - Panek, J S
AU  - Schaus, S E
AU  - Snyder, J K
AU  - Porco, J A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mining
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Distinct Electrophysiological Properties of Hippocampal CA2 Neurons 162 LTP Postsynaptic Mechanisms: Cellular Physiology
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39893501; 4122326
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Zhao, M
AU  - Dudek, S M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Physiology
KW  - Long-term potentiation
KW  - Hippocampus
KW  - Neurons
KW  - Electrophysiology
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - In Situ Hybridization Analysis of Changes in Heteronuclear Oxytocin and Vasopressin RNA During Lactation and the Estrous Cycle in the Rat Hypothalamus
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39893324; 4134728
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Scordalakes, E M
AU  - Yue, C
AU  - Mutsuga, N
AU  - Gainer, H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Lactation
KW  - RNA
KW  - Oxytocin
KW  - Vasopressin
KW  - Hybridization analysis
KW  - Hypothalamus
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Gene Expression Analysis in Adult Rat Hypothalamus Using an In Vivo Electroporation Technique
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39893212; 4134707
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Mutsuga-Nakayama, N
AU  - Wei, F
AU  - Fields, R L
AU  - Gainer, H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Electroporation
KW  - Gene expression
KW  - Hypothalamus
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - In the Act of Feeding: A Model of Reward, Decision, and Inhibitory Control
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39892836; 4134856
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kralik, J D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Reinforcement
KW  - Feeding
KW  - Models
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39892836?accountid=14244
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Repopulation of Dentate Granule Neurons Following Trimethyltin - Induced Injury in the Adolescent Mouse
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39891989; 4128299
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Aoyama, M
AU  - Wine, R N
AU  - McPherson, C A
AU  - Harry, G J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Adolescents
KW  - Injuries
KW  - Granule cells
KW  - Trimethyltin
KW  - Repopulation
KW  - Neurons
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - PKB Phosphorylation of the NMDA Receptor NR2C Subunit and Binding to 14 - 3 - 3e
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39891084; 4132395
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Chen, B
AU  - Roche, K W
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Glutamic acid receptors
KW  - N-Methyl-D-aspartic acid receptors
KW  - Phosphorylation
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39891084?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Modeling the Behavior of Monkeys in Reward Schedules with Context - Dependent and Adaptive Reinforcement Learning
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39889622; 4134853
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - La Camera, G.
AU  - Zeng, L
AU  - Pritchett, D L
AU  - Richmond, B J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Reinforcement
KW  - Learning
KW  - Learning behaviour
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39889622?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Cue and Reward Signals Carried by Monkey Entorhinal Neurons during Reward Schedules
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39889573; 4134852
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Sugase-Miyamoto, Y
AU  - Richmond, B J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Reinforcement
KW  - Neurons
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39889573?accountid=14244
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Co - Existence of g - Oscillations and Neuronal Avalanches in Cortical Networks
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39889543; 4134283
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Gireesh, E.Dharmaraj
AU  - Plenz, D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Avalanches
KW  - Oscillations
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Rolipram Rescues Spatial Memory Deficits in Galanin - Overexpressing Transgenic Mice
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39889529; 4134838
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Rustay, N R
AU  - Crawley, J N
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mice
KW  - Galanin
KW  - Spatial memory
KW  - Rolipram
KW  - Transgenic mice
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Does Superior Colliculus Stimulation Directly Shift Attention or Produce a Visual Cue?
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39889504; 4122379
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Cavanaugh, J
AU  - Alvarez, B D
AU  - Wurtz, R H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Attention
KW  - Superior colliculus
KW  - Visual stimuli
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - High - and Low - Frequency Stimuli Preferentially Activate Different Steps in the ERK Cascade
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39889118; 4134206
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Hongpaisan, J
AU  - Winters, C A
AU  - Andrews, S B
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Extracellular signal-regulated kinase
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39889118?accountid=14244
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LA  - English
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Identification and Characterization of pA134, a Novel Squid Axonal mrna and its Cognate Protein in the Mammalian Brain
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39888892; 4134175
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Mameza, M G
AU  - Lockard, J
AU  - Gioio, A E
AU  - Hillefors, M
AU  - Lavino, Z.Scotto
AU  - Kaplan, B B
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain
KW  - MRNA
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Lateralized Conceptual Processing in the Perirhinal Cortex During Object Naming Revealed using High - Resolution Fmri.
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39888286; 4119250
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Bellgowan, P.S.F.
AU  - Raymundo, N
AU  - Bodurka, J
AU  - Martin, A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Functional magnetic resonance imaging
KW  - Cortex
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Disruption of mGluR8a - Mediated Calcium Channel Inhibition by Fluorophore - Asssisted Light Inactivation in Rat Sympathetic Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39888042; 4123821
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Guo, J
AU  - Chen, H
AU  - Puhl, H L
AU  - Ikeda, S R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Sympathetic nerves
KW  - Fluorophores
KW  - Calcium channels
KW  - Neurons
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Interaction of the Hereditary Spastic Paraplegia ( SPG20 ) Protein Spartin with Eps15
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39887736; 4135083
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Bakowska, J C
AU  - Russell, J W
AU  - Pendleton, J
AU  - Blackstone, C
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Spastic paraplegia
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - A Centrally Acting Angiotensin II AT@@d1@ Receptor Antagonist Prevents the Isolation Stress - Induced Decrease in Cortical CRH@@d1@ Receptor and Benzodiazepine Binding
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39887473; 4122787
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Pavel, J
AU  - Armando, I
AU  - Bregonzio, C
AU  - Juorio, A
AU  - Macova, M
AU  - Saavedra, J M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Stress
KW  - Benzodiazepine
KW  - Angiotensin II
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - BDNF Gene Expression is Differentially Regulated by Postsynaptic Activity Correlated and Uncorrelated with Synaptic Input to CA1 Hippocampal Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39886367; 4127336
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Fields, R D
AU  - Cohen, J E
AU  - Lee, P R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain-derived neurotrophic factor
KW  - Hippocampus
KW  - Neurons
KW  - Gene expression
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Different Spatiotemporal Profiles in the Gamma Band for Processing Fearful, Angry, and Neutral Expressions: An MEG Study
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39886238; 4120036 DE:
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Luo, Q
AU  - Holroyd, T
AU  - Jones, M
AU  - Hendler, T
AU  - Blair, J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - The Pheromone Androstenol ( 5a - androst - 16 - en - 3a - ol ) is a Neurosteroid
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39884327; 4123793
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kaminski, R M
AU  - Marini, H
AU  - Ortinski, P I
AU  - Yonekawa, W
AU  - Vicini, S
AU  - Rogawski, M A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Pheromones
KW  - Neurosteroids
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Medial Temporal Removals Preserve Projections From Auditory Belt and Parabelt to Frontal Cortex
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39883802; 4120854
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Munoz, M
AU  - Saunders, R C
AU  - Mishkin, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Cortex (temporal)
KW  - Cortex (frontal)
KW  - Cortex (auditory)
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39883802?accountid=14244
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TY  - CPAPER
T1  - Developmental Changes in Visual Selective Attention: Comparison of Children with Healthy Adults
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39883046; 4132933
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Friedman-Hill, S R
AU  - Gex, S E
AU  - Towbin, K E
AU  - Pine, D S
AU  - Leibenluft, E
AU  - Ungerleider, L G
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Children
KW  - Attention
KW  - Visual perception
KW  - Developmental stages
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Activation in the Premotor Cortex During Perceiving Successive Stimuli With or Without Explicit Counting
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39882990; 4132914
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kansaku, K
AU  - Grillon, M
AU  - Johnson, A
AU  - Sadato, N
AU  - Hallett, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Enumeration
KW  - Cortex (premotor)
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Development of a "Split Transcription Factor" System for Refined Spatial Manipulation of Neuronal Activity in Drosophila
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39882818; 4123528
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Luan, H
AU  - Marsh, J
AU  - White, B H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Transcription factors
KW  - Drosophila
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Effect of Antipsychotics on Neural Activation During Reward Anticipation in Schizophrenia
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39882815; 4129776
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Wint, D
AU  - Koch, P
AU  - Dreher, J
AU  - Furman, D
AU  - Kohn, P
AU  - Egan, M
AU  - Weinberger, D
AU  - Berman, K F
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Neuroleptics
KW  - Schizophrenia
KW  - Reinforcement
KW  - Mental disorders
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Percept - Related Fluctuations of MT Local Field Potentials
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39882314; 4127540 DE:
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Maier, A V
AU  - Logothetis, N K
AU  - Leopold, D A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Negative Reinforcers Activates the Neural Reward Circuitry
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39882252; 4120997
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Martin-Soelch, C
AU  - Herdener, M
AU  - Kandzia, W
AU  - Scheffler, K
AU  - Seifritz, E
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Reinforcement
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Prefrontal Mechanisms for Abstract Response Strategies
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39882246; 4120862 DE:
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Genovesio, A
AU  - Brasted, P J
AU  - Mitz, A R
AU  - Wise, S P
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Investigating the Neural Basis of Psychophysiological Interactions in fMRI
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39882155; 4120835
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kim, J
AU  - Horwitz, B
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Functional magnetic resonance imaging
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Depletion of Chromogranin A by Antisense RNAs Leads to Abnormal Chromaffin Granule Biogenesis in Transgenic Mice
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39882016; 4134135
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kim, T
AU  - Zhang, C F
AU  - Sun, Z
AU  - Wu, H.
AU  - Loh, Y P
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mice
KW  - Antisense RNA
KW  - Chromogranins
KW  - Evolution
KW  - Transgenic mice
KW  - Chromaffin granules
KW  - Biogenesis
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Calcium Influx Through Postsynaptic AMPA Receptors Elicits GABA Release at a Reciprocal Synapse of Rat Retina
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39881327; 4127271
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Chavez, A E
AU  - Diamond, J S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Retina
KW  - ^a-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptors
KW  - Calcium influx
KW  - Synapses
KW  - ^g-Aminobutyric acid
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Myelin - Associated Glycoprotein - Activated Signaling in Oligodendrocytes
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39881175; 4134347
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Cheng, S
AU  - Quarles, R H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Signal transduction
KW  - Myelin
KW  - Glycoproteins
KW  - Oligodendrocytes
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39881175?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Dopamine - - Glutamate Interaction Induces Neuronal Avalanches in Superficial Layers of Rat Prefrontal Cortex
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39880894; 4134285
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Stewart, C V
AU  - Gerfen, C
AU  - Plenz, D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Avalanches
KW  - Glutamic acid
KW  - Cortex (prefrontal)
KW  - Dopamine
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39880894?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Neural Correlates of Regional Electroencephalogram Power Change
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39880809; 4134255
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Oishi, N
AU  - Mima, T
AU  - Ishii, K
AU  - Bushara, K O
AU  - Hiraoka, T
AU  - Ueki, Y
AU  - Fukuyama, H
AU  - Hallett, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - EEG
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Kinetic and Metabolic Evaluation of New PET Ligands for Peripheral Benzodiazepine Receptors
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39880363; 4126872
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Imaizumi, M
AU  - Briard, E
AU  - Zoghbi, S S
AU  - Hong, J
AU  - Shah, J
AU  - Musachio, J L
AU  - Pike, V W
AU  - Innis, R B
AU  - Fujita, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Kinetics
KW  - Benzodiazepine receptors
KW  - Ligands
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Further Evidence Supporting Glycogen Synthase Kinase - 3 and b - Catenin as Mediators of the Behavioral Effects of Lithium
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39880289; 4121780
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Gould, T D
AU  - Einat, H
AU  - Picchini, A M
AU  - Bhat, R
AU  - Eberthart, C G
AU  - Schloesser, R J
AU  - Manji, H K
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Lithium
KW  - Catenin
KW  - Glycogen synthase kinase 3
KW  - Glycogen
KW  - U 7000:Multidisciplinary
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Decision - Making Processes During Potential Reward and Punishment: An fMRI Study
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39880285; 4133217
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Hardin, M G
AU  - Pine, D S
AU  - Ernst, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Reinforcement
KW  - Punishment
KW  - Functional magnetic resonance imaging
KW  - Decision making
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39880285?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Nucleotide Sequence Variation Within the Human Tyrosine Kinase B Neurotrophin Receptor Gene ( NTRK2 ) is Associated with Alcohol Dependence and Alcohol Abuse
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39879960; 4133681
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Xu, K.
AU  - Anderson, T R
AU  - Neyer, K M
AU  - Lamparella, N
AU  - Jenkins, G
AU  - Zhou, Z
AU  - Lipsky, R H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Alcohols
KW  - Protein-tyrosine kinase
KW  - Neurotrophin receptors
KW  - Drug abuse
KW  - Drug dependence
KW  - Nucleotide sequence
KW  - Tyrosine
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Two Critical Stages of Late - phase Long - term Potentiation (L - LTP) Mediated by BDNF with Distinct Mechanisms
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39879565; 4130800
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Pang, P T
AU  - Yung, W H
AU  - Lu, B.
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Long-term potentiation
KW  - Brain-derived neurotrophic factor
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Distribution of Scaffolding Molecules at the Postsynaptic Density
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39878913; 4119712
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - DeGiorgis, J A
AU  - Dosemeci, A
AU  - Reese, T S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Postsynaptic density
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Single Nucleotide Polymorphisms ( SNPs ) in NRG1 Affect Nicotinic Acetylcholine Receptor ( nAChR ) a7 Subunit Expression
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39878207; 4130104
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Mathew, S V
AU  - Hyde, T M
AU  - Lipska, B K
AU  - Vakkalanka, R
AU  - Straub, R E
AU  - Weinberger, D R
AU  - Kleinman, J E
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Acetylcholine receptors (nicotinic)
KW  - Single-nucleotide polymorphism
KW  - Neurotransmitters
KW  - Nucleotides
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39878207?accountid=14244
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Dysregulation of the Brain Stress System and Propensity to Relapse in Genetically Selected Alcohol Preferring msP Rats
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39877938; 4130173
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Hansson, A C
AU  - Cippitelli, A
AU  - Sommer, W H
AU  - Fideli, A
AU  - Massi, M
AU  - Heilig, M
AU  - Ciccocioppo, R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Alcohols
KW  - Stress
KW  - Brain
KW  - Rats
KW  - Ethanol
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39877938?accountid=14244
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - The Function of Alternatively Spliced Nonmuscle Myosin II - B Isoforms in Mouse Brain Development
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39877816; 4130444
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Ma, X.
AU  - Kawamoto, S
AU  - Bridgman, P C
AU  - Uribe, J A
AU  - Adelstein, R S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain
KW  - Myosin
KW  - Alternative splicing
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Vanilloid - Evoked Calcium Responses from Embryonic Cortical Neurons in Primary Culture
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39877240; 4125788
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Csermely, T
AU  - Mitchell, K
AU  - Keller, J
AU  - Karai, L
AU  - Iadarola, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Calcium
KW  - Embryos
KW  - Cortex
KW  - Neurons
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Shifting Visual Receptive Fields in the Frontal Eye Field: Do they Use Corollary Discharge from the Thalamus?
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39877221; 4119673
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Sommer, M A
AU  - Wurtz, R H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Eye
KW  - Thalamus
KW  - Receptive field
KW  - U 7000:Multidisciplinary
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Activation of Dopamine D@@d1@, Not D@@d5@, Receptors Facilitates Extinction of Fear Memories in Mice
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39876816; 4128065
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Izquierdo, A
AU  - Cabrera, D M
AU  - Sibley, D R
AU  - Holmes, A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mice
KW  - Dopamine D5 receptors
KW  - Extinction
KW  - Fear
KW  - Dopamine D1 receptors
KW  - Memory
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Additive Effects of Endogenous Cannabinoid Anandamide and Halothane on a7 - Nicotinic Acetylcholine Receptor - Mediated Responses in Xenopus Oocytes
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39876697; 4133972
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Zhang, L
AU  - Oz, M.
AU  - Jackson, S N
AU  - Woods, A S
AU  - Morales, M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Additives
KW  - Anandamide
KW  - Oocytes
KW  - Acetylcholine receptors (nicotinic)
KW  - Halothane
KW  - Neurotransmitters
KW  - Amphibiotic species
KW  - Xenopus
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Novel Patterns of NMDAR 2C Subunit Expression Revealed Using b - Gal Knock - in Mice
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39876550; 4127134
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Karavanova, I
AU  - Vasudevan, K
AU  - Buonanno, A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mice
KW  - Glutamic acid receptors
KW  - N-Methyl-D-aspartic acid receptors
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39876550?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Activity - Dependent Interaction between Axons and Astrocytes Promotes CNS Myelination
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39876080; 4124081
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Ishibashi, T
AU  - Lee, P R
AU  - Fields, R D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Central nervous system
KW  - Myelination
KW  - Astrocytes
KW  - Axons
KW  - Neurons
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Vasopressin Mediates Pituitary Mitogenesis but not Increases in the Number of ACTH Containing Corticotrophs
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39875864; 4129420
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Subburaju, S
AU  - Zeise, M
AU  - Aguilera, G
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Adrenocorticotropic hormone
KW  - Pituitary
KW  - Vasopressin
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Imaging the Effects of Levodopa on Motor Memory Formation with 11 - C - Raclopride PET in Healthy Elderly Subjects
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39874856; 4118998
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Floel, A
AU  - Garraux, G
AU  - Breitenstein, C
AU  - Herscovitch, P
AU  - Knecht, S
AU  - Cohen, L G
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Elderly
KW  - Levodopa
KW  - Raclopride
KW  - Geriatrics
KW  - Memory
KW  - Imaging techniques
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Molecular Modeling Study of the Human P2Y@@d2@ Receptor Agonists
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39873747; 4125435
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Ivanov, A A
AU  - Costanzi, S
AU  - Jacobson, K A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Purine P2Y receptors
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Time - Course Changes of Dopamine D@@d2@ and CB1 Cannabinoid Receptors During Cocaine Self - Administration
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39872810; 4128482
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Thanos, P K
AU  - Soria, L
AU  - Michaelides, M E
AU  - Piyis, Y K
AU  - Pappas, G P
AU  - Maldonado, R
AU  - Valverde, O
AU  - Volkow, N D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Cocaine
KW  - Cannabinoid CB1 receptors
KW  - Dopamine D2 receptors
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - In Vivo and In Vitro Measurement of Brain Phosphodiesterase 4 in Rats after Antidepressant Treatment
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39872242; 4119892
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Fujita, M
AU  - Imaizumi, M
AU  - D'Sa, C
AU  - Zoghbi, S S
AU  - Crescenzo, M S
AU  - Hong, J
AU  - Musachio, J L
AU  - Gee, A D
AU  - Seidel, J
AU  - Green, M V
AU  - Pike, V W
AU  - Duman, R S
AU  - Innis, R B
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Antidepressants
KW  - Brain
KW  - Rats
KW  - Phosphodiesterase IV
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Sulcal Morphometry in Williams Syndrome
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39870781; 4126098
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kippenhan, J S
AU  - Meyer-Lindenberg, A
AU  - Olsen, R K
AU  - Mervis, C B
AU  - Morris, C A
AU  - Kohn, P D
AU  - Berman, K F
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Williams syndrome
KW  - Morphometry
KW  - Animal morphology
KW  - Symptoms
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Shifting Visual Receptive Fields in the Frontal Eye Field: Do they Spread or do they Jump?
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39868971; 4119672
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Wurtz, R H
AU  - Sommer, M A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Eye
KW  - Receptive field
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Menstrual Cycle Phase Modulates the Reward System in Women
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39868730; 4121005
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Dreher, J
AU  - Schmidt, P
AU  - Kohn, P
AU  - Furman, D
AU  - Olsen, R
AU  - Koch, P
AU  - Rubinow, D
AU  - Berman, K
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Menstrual cycle
KW  - Reinforcement
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Respective Contributions of Two Negative Feedback Mechanisms in Neuronal Rhythms
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39867443; 4124004
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Tabak, J
AU  - Rinzel, J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Feedback
KW  - Rhythms
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Early Global Gene Responses to Distinct Activity Patterns
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39864047; 4125865
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Rana, Z A
AU  - Gundersen, K
AU  - Buonanno, A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Activity patterns
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Discovery and Characterization of S100a8 and S100a9 in the Sensory Pathway System: Implications for Nociception
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39863598; 4125789
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Mitchell, K
AU  - Muhly, W T
AU  - Keller, J M
AU  - Yang, H T
AU  - Iadarola, M J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Pain perception
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Prefrontal Cortex Inefficiency During Working Memory in Unaffected Siblings of Patients with Schizophrenia
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39863074; 4128019
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Sust, S
AU  - Tan, H Y
AU  - Mattay, V S
AU  - Buckholtz, J
AU  - Egan, M F
AU  - Weinberger, D R
AU  - Callicott, J H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Schizophrenia
KW  - Mental disorders
KW  - Short term memory
KW  - Cortex (prefrontal)
KW  - Siblings
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39863074?accountid=14244
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TY  - CPAPER
T1  - Comparison of Saccade - Reward Contingency - Modulated Activity in the Primate Frontal Eye Field and Caudate Nucleus
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39862611; 4121011
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Ding, L
AU  - Hikosaka, O
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Eye
KW  - Reinforcement
KW  - Saccadic eye movements
KW  - Contingency
KW  - Caudate nucleus
KW  - Primates
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Lithium Attenuates Smad3/4 Transcriptional Activity: Roles of GSK - 3 and cAMP/PKA Signaling
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39862039; 4119472
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Liang, M H
AU  - Chuang, D M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Lithium
KW  - Signal transduction
KW  - Protein kinase A
KW  - Transcription
KW  - Cyclic AMP
KW  - Smad3 protein
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Parametric Modulation of Cortico - Limbic Structures by Interobject Desirability Distance: An fMRI Investigation
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39861963; 4118910
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Peschardt, K
AU  - Marsh, A
AU  - Morton, J
AU  - Drevets, W C
AU  - Blair, J R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Functional magnetic resonance imaging
KW  - U 7000:Multidisciplinary
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LA  - English
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TY  - CPAPER
T1  - Spatial Working Memory Development During Childhood and Adolescence
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39857182; 4128028
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Ordaz, S J
AU  - Wallace, G L
AU  - Greenstein, D K
AU  - Clasen, L S
AU  - Taylor, K N
AU  - Rosenthal, M A
AU  - Rose, A B
AU  - Giedd, J N
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Short term memory
KW  - Spatial memory
KW  - Adolescence
KW  - Children
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39857182?accountid=14244
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A Selective Intracellular Signaling Pathway in the Anterior Cingulate Cortex Regulates Mania - related Behavior
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39842384; 4131896
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Creson, T K
AU  - Hao, Y
AU  - Engel, S
AU  - Yuan, P
AU  - Manji, H K
AU  - Chen, G
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Affective disorders
KW  - Intracellular signalling
KW  - Cortex (cingulate)
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Requirement of the Forebrain Rap1 for the Expression of Fear
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39840294; 4123051
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Vautier, F
AU  - Ito, W
AU  - Miah, C
AU  - Mirlas, B
AU  - Pan, B
AU  - Kandel, E R
AU  - Morozov, A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Rap1 protein
KW  - Forebrain
KW  - Fear
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Relationship of PSD Thickening and CaMKII Clustering to the Local Availability of a - CaMKII in Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39837264; 4130704
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Brightman, M W
AU  - Gallant, P
AU  - Dosemeci, A
AU  - Reese, T S
AU  - Tao-Cheng, J H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Ca@@u2+@/calmodulin-dependent protein kinase II
KW  - Neurons
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Differential Modulation of A1 Adenosine Receptor - Mediated Adenylyl Cyclase Signaling and Phospholipase C Signaling by PD 81,723
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39837015; 4125424
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Gao, Z
AU  - Mamedova, L K
AU  - Jacobson, K A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Signal transduction
KW  - Adenylate cyclase
KW  - Adenosine receptors
KW  - Phospholipase C
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39837015?accountid=14244
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
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TY  - CPAPER
T1  - Changes in Cortical Interneurons in BDNF Conditional Knock - Out Mice
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39836529; 4125362
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Paletzki, R F
AU  - Morozov, A Y
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mice
KW  - Interneurons
KW  - Brain-derived neurotrophic factor
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A Pilot Study to Determine the Influence of Gastrocnemius Muscle on Knee Movement Sense
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39836279; 4132521
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Brindle, T J
AU  - Mizelle, J C
AU  - McLucas, J L
AU  - Stanhope, S J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Muscles
KW  - Knee
KW  - Gastrocnemius muscle
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39836279?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Identification of an ER - Retention Motif in an Intracellular Loop of the Kainate Receptor KA2 Subunit
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39835985; 4132387
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Nishimura, Y N
AU  - Tang, T.T.T.
AU  - Hurtado, D E
AU  - Isaac, J.T.R.
AU  - Roche, K W
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Glutamic acid receptors
KW  - Kainic acid receptors
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39835985?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Heterogeneity of Dopamine Neuronal Responses in Monkeys during Visually Cued Reward Schedules
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39835136; 4134854
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Ravel, S
AU  - Richmond, B J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Reinforcement
KW  - Dopamine
KW  - U 7000:Multidisciplinary
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Anticipation of Waiting for Reward Degrades Performance in Visual Discrimination
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39835099; 4134851
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Minamimoto, T
AU  - Richmond, B J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Reinforcement
KW  - Visual discrimination
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39835099?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Differential Effects of Hydrocortisone on Amygdala Habituation to Emotional Facial Expressions: An fMRI Study
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39834972; 4122896
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Erickson, K
AU  - Wood, S E
AU  - Furey, M L
AU  - Nugent, A C
AU  - Mah, L
AU  - Schulkin, J
AU  - Drevets, W C
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Amygdala
KW  - Hydrocortisone
KW  - Functional magnetic resonance imaging
KW  - Emotions
KW  - Habituation
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39834972?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Resonance Energy Transfer Imaging of Stargazin - GluR1 Interactions in Living Cells
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39834710; 4133933
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Thaler, C
AU  - Honse, Y
AU  - Lovinger, D M
AU  - Vogel, S S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Imaging techniques
KW  - CACNG2 protein
KW  - Glutamic acid receptors (ionotropic)
KW  - Calcium channels (voltage-gated)
KW  - Energy transfer
KW  - Resonance
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39834710?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Cyclooxygenase ( COX ) - 2 is Required for Muscarinic Receptor - Mediated Brain Signaling Involving Phospholipase A2 Activation and Arachidonic Acid Release From Phospholipid
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39834523; 4132326
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Basselin, M
AU  - Villacreses, N E
AU  - Langerbach, R
AU  - Bell, J M
AU  - Rapoport, S I
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain
KW  - Arachidonic acid
KW  - Phospholipase A2
KW  - Signal transduction
KW  - Prostaglandin-endoperoxide synthase
KW  - Phospholipids
KW  - Acetylcholine receptors (muscarinic)
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Disulfide Crosslinking Studies with Cysteine - Substituted Mutant M3 Muscarinic Receptors: Identification of Agonist - Induced Conformational Changes that Occur Close to the Ligand Binding Pocket 149 G-Protein-Linked Receptors: Muscarinic
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39833376; 4122105
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Han, S
AU  - Hamdan, F F
AU  - Kim, S
AU  - Jacobson, K A
AU  - Bloodworth, L M
AU  - Li, B.
AU  - Wess, J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mutants
KW  - Acetylcholine receptors (muscarinic)
KW  - Cysteine
KW  - Ligands
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Neurogranin and PKC Play a Critical Role in Modulating Affective States Seen in Bipolar Disorder
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39831784; 4131906
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Szabo, S T
AU  - Du, J.
AU  - Einat, H
AU  - Yuan, P
AU  - Wu, J.
AU  - Falke, C
AU  - Wei, Y
AU  - Zhou, R
AU  - Zhang, L
AU  - Huang, F
AU  - Huang, K
AU  - Manji, H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Emotional behavior
KW  - Bipolar disorder
KW  - Protein kinase C
KW  - Neurogranin
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - The Anticonvulsants Lamotrigine, Riluzole, and Valproate Differentially Regulate AMPA Receptor Trafficking: Relationship to Clinical Effects in Mood Disorders
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39831722; 4131904
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Wei, Y
AU  - Du, J.
AU  - Chen, Z
AU  - Falke, C
AU  - Suzuki, K
AU  - Zarate, C
AU  - Manji, H K
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Protein transport
KW  - ^a-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptors
KW  - Mood
KW  - Lamotrigine
KW  - Anticonvulsants
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Effect of Angiotensin II AT1 Receptor Antagonists on White Matter Lesions in the Rat Brain Induced by Cerebral Hypoperfusion
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39831580; 4131858
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Nishioku, T
AU  - Saavedra, J M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain
KW  - Lesions
KW  - Substantia alba
KW  - Angiotensin II
KW  - Antagonists
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - The Role of Substance Abuse in a Postmortem Sample of Schizophrenia
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39830880; 4128354
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Deep-Soboslay, A
AU  - Hyde, T M
AU  - Bigelow, L B
AU  - Herman, M M
AU  - Martin, C E
AU  - Kleinman, J E
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Substance abuse
KW  - Schizophrenia
KW  - Mental disorders
KW  - Drug abuse
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Functional Connectivity of Temporal Cortex during Categorization of Sounds
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39830652; 4134380
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Husain, F T
AU  - McKinney, C M
AU  - Horwitz, B
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Cortex (temporal)
KW  - Sound
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Differential Expression of Glutathione S - Transferase a 4 in a Genetic Model of Alcoholism
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39829861; 4121348
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Bjork, K
AU  - Arlinde, C
AU  - Saarikoski, S T
AU  - Hyytia, P
AU  - Heilig, M
AU  - Sommer, W H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Glutathione
KW  - Drug abuse
KW  - Alcoholism
KW  - Models
KW  - Transferases
KW  - Coenzymes
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - The Neural Substrate of Face and House Perception During Passive Viewing in Williams Syndrome: Additional Evidence for Dorsal Stream Dysfunction
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39829784; 4130169
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Sarpal, D
AU  - Meyer-Lindenberg, A
AU  - Kohn, P D
AU  - Kippenhan, S
AU  - Mervis, C B
AU  - Morris, C A
AU  - Berman, K F
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Residential areas
KW  - Housing
KW  - Perception
KW  - Williams syndrome
KW  - Face
KW  - Streams
KW  - Pattern recognition
KW  - Symptoms
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Low Frequency Priming Facilitates Induction of LTP by Up - regulation of Endocannabinoid Signaling in the Hippocampus
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39829526; 4130565
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Zhu, P
AU  - Lovinger, D M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Signal transduction
KW  - Long-term potentiation
KW  - Cannabinoids
KW  - Hippocampus
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Uncertainty, Likelihood, and Perceptual Decision Making
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39829262; 4120019
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Marrett, S
AU  - Ruff, D A
AU  - Heekeren, H R
AU  - Hwang, G C
AU  - Boemio, A
AU  - Bandettini, P A
AU  - Ungerleider, L G
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Decision making
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39829262?accountid=14244
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Velocity - Dependent Hypertonia of the Rectus Femoris Muscle in Patients with Cerebral Palsy
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39827469; 4135046
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Lebiedowska, M K
AU  - Burns, S R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Muscles
KW  - Velocity
KW  - Paralysis
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Rhythmic Electrical Activity in Developing GnRH - 1 Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39826665; 4131293
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Constantin, S
AU  - Duittoz, A
AU  - Wray, S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Neurons
KW  - Gonadotropin-releasing hormone
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Cdk5 is Essential for Survival in Cortical Neurogenesis: A Study Based on Selective FACS Sorting of Neural Phenotypes
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39826355; 4128758
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Grant, P
AU  - Maric, D
AU  - Takahashi, S
AU  - Pareet, T
AU  - Barker, J L
AU  - Kulkarni, A
AU  - Pant, H C
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Neurogenesis
KW  - Cyclin-dependent kinase 5
KW  - Survival
KW  - Phenotypes
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Effects of Scopolamine, Nicotine, and LY354740 on the 5 - choice Serial Reaction Time Task in the Common Marmoset Monkey
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39826026; 4129550
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Spinelli, S
AU  - Ballard, T M
AU  - Higley, J D
AU  - Higgins, G A
AU  - Feldon, J
AU  - Pryce, C R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Nicotine
KW  - Reaction time task
KW  - Scopolamine
KW  - Callithrix
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Intranuclear Localization of Mre11, Rad50, and Nbs1 Proteins in Bergmann Glia, Purkinje Neurons, and Other Large Neurons of the Human Brain: Implications for the Pathogenesis of Ataxia - Telangiectasia - Like Disorder
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39825554; 4128546
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Brooks, P J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain
KW  - NBS1 protein
KW  - Ataxia
KW  - Glia
KW  - Neurons
KW  - Purkinje cells
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Cyln2 - Deficient Mice Display Reduced Preference for Social Novelty: Relevance to Williams Syndrome
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39825514; 4128539
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Crawley, J N
AU  - Cohen, J J
AU  - Cuasay, K
AU  - Hill, J M
AU  - Sharer, K
AU  - Koretsky, A P
AU  - Galjart, N
AU  - Berman, K F
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mice
KW  - Williams syndrome
KW  - Novelty
KW  - Symptoms
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Expansion of Monkey Superior Colliculus Movement Fields with Saccades to Moving Targets
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39825307; 4122408
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Port, N L
AU  - Wurtz, R H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Superior colliculus
KW  - Saccadic eye movements
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Activity - dependent Regulation of mRNA Stability and Nucleocytoplasmic Shuttling of Ribonucleoproteins in Hippocampal Neurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39824338; 4130799
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Cohen, J E
AU  - Lee, P R
AU  - Fields, R D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - MRNA stability
KW  - Hippocampus
KW  - Ribonucleoproteins
KW  - Neurons
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39824338?accountid=14244
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - D - b - Hydroxyburyrate Reduces Mitochondrial Apoptotic Signaling in Serum - Free Hypoxic Hippocampal Primary Culture
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39823641; 4128249
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kashiwaya, Y
AU  - Masuda, R
AU  - Fukuhara, Y
AU  - Takeshima, T
AU  - Veech, R L
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Signal transduction
KW  - Cell culture
KW  - Hypoxia
KW  - Mitochondria
KW  - Apoptosis
KW  - Hippocampus
KW  - Serum
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Control of BDNF Transcription Through Relief of Basic Helix - Loop - Helix Protein - Mediated Repression and Activation of CREB and NF - kB in NMDA - Mediated Neuroprotection
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39822109; 4119034
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Lipsky, R H
AU  - Jiang, X
AU  - Tian, F
AU  - Wu, X.
AU  - Pan, H
AU  - Xu K.
AU  - Egan, S E
AU  - Marini, A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Cyclic AMP response element-binding protein
KW  - Transcription
KW  - N-Methyl-D-aspartic acid
KW  - Neuroprotection
KW  - Brain-derived neurotrophic factor
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39822109?accountid=14244
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Effect of Dietary N - 3 Fatty Acid Deficiency and Subsequent Reduction of Brain Docosahexaenoic Acid on GABA@@dA@ Receptor Function
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39822075; 4134047
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Kloda, J H
AU  - Fedorova, I
AU  - Majchrzak, S
AU  - Swenby, N
AU  - Salem Jr, N
AU  - Mitchell, D C
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain
KW  - Fatty acids
KW  - ^g-Aminobutyric acid A receptors
KW  - Docosahexaenoic acid
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - A Frequency - Dependent Switch of Synaptic Inhibition Polarity Recruits a Network of Hippocampal Stratum Interneurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39821982; 4134026
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Banke, T G
AU  - McBain, C J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Interneurons
KW  - Recruitment
KW  - Hippocampus
KW  - Polarity
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - An fMRI Study of Simultaneous Practice - Related Changes in Perception and Response Selection
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39821936; 4119545
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Jansma, J M
AU  - van Raalten, T.R.
AU  - Ramsey, N F
AU  - van Gelderen, P
AU  - Duyn, J H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Perception
KW  - Functional magnetic resonance imaging
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Different Neurons in the Inferior Temporal Cortex Reflect where Monkeys will and should Look
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39821726; 4119955
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Messinger, A
AU  - Squire, L R
AU  - Zola, S M
AU  - Albright, T D
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Cortex (temporal)
KW  - Neurons
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - NMDA Receptors Interact with GIPC
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39821703; 4127141
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Yi, Z.
AU  - Petralia, R S
AU  - Sans, N
AU  - Wenthold, R J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Glutamic acid receptors
KW  - N-Methyl-D-aspartic acid receptors
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Molecules Interacting with Disrupted - in - Schizophrenia - 1(DISC1) are Differentially Expressed in Schizophrenia and Regulated by SNPs Associated with the Disease
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39821363; 4119878
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Lipska, B K
AU  - Peters, T
AU  - Halim, N
AU  - Mitkus, S
AU  - Sawa, A
AU  - Hyde, T M
AU  - Weinberger, D R
AU  - Kleinman, J E
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Schizophrenia
KW  - Mental disorders
KW  - Single-nucleotide polymorphism
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Cdk5 Activity is Required to Regulate Pain Signaling
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39821321; 4119383
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Pareek, T K
AU  - Keller, J
AU  - Kesavapany, S
AU  - Pant, H C
AU  - Iadarola, M J
AU  - Kulkarni, A B
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Pain
KW  - Signal transduction
KW  - Cyclin-dependent kinase 5
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Mapping a Cortical - Subcortical Loop in Vivo Using Manganese - Enhanced Magnetic Resonance Imaging in Monkey
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39820512; 4126865
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Simmons, J M
AU  - Lizak, M J
AU  - Ortiz, M
AU  - Koretsky, A P
AU  - Richmond, B J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Mapping
KW  - Manganese
KW  - Magnetic resonance imaging
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Chronic Valproate Does Not Alter the Kinetics of Docosahexaenoic Acid within Brain Phospholipids of the Unanesthetized Rat
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39820005; 4121359
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Lee, H
AU  - Rao, J S
AU  - chang, L
AU  - Rapoport, S I
AU  - Bazinet, R P
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Kinetics
KW  - Brain
KW  - Docosahexaenoic acid
KW  - Phospholipids
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - A Fast, Windows - Based Dynamic Clamp
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39819681; 4128628 DE:
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Mogri, M
AU  - Milescu, L
AU  - Ptak, K
AU  - Smith, J C
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39819681?accountid=14244
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A Family of Adhesion - Like Molecules Associated with the NMDA Receptor Complex
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39819219; 4127142
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Seabold, G K
AU  - Wang, C Y
AU  - Petralia, R S
AU  - Wenthold, R J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Glutamic acid receptors
KW  - N-Methyl-D-aspartic acid receptors
KW  - Adhesion
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39819219?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Activity - dependent Transcription of BDNF Through Promoter 3 Contributes Selectively to Long - term Hippocampal Plasticity and Long - term Memory
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39818634; 4128965
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Sakata, K
AU  - Woo, N
AU  - Wu, J.
AU  - Shen, L
AU  - Lu, B.
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Promoters
KW  - Transcription
KW  - Plasticity (hippocampal)
KW  - Brain-derived neurotrophic factor
KW  - Hippocampus
KW  - Memory
KW  - Plasticity
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39818634?accountid=14244
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LA  - English
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Differential Regulation of mGluR7 Trafficking
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39818529; 4120252 DE:
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Lavezzari, G
AU  - Roche, K W
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39818529?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - m - Calpain Activates Microglia and is Toxic to Dopaminergic Neurons: Mechanisms of Reactive Microgliosis
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39818336; 4129893
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Block, M L
AU  - Wilson, B
AU  - Pang, H
AU  - Qian, L
AU  - Wu, X.
AU  - Gao, X
AU  - Zhang, W
AU  - Mandavilli, B
AU  - Dallas, S
AU  - Miller, D
AU  - Hong, J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Microglia
KW  - Calpain
KW  - Neurons
KW  - Dopamine
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Awareness Modulates MEG Responses to Fearful Faces
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39818130; 4129826 DE:
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Crocker, L D
AU  - Japee, S
AU  - Holroyd, T
AU  - Carver, F W
AU  - Pessoa, L
AU  - Ungerleider, L G
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39818130?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Dendritic Release of Dopamine Modulates GABA Neurotransmission in Substantia Nigra Pars Reticulata: Iontophoresis in Awake Unrestrained Rats
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39815923; 4129331
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Windels, F
AU  - Kiyatkin, E A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Rats
KW  - Neurotransmission
KW  - Substantia nigra pars reticulata
KW  - Iontophoresis
KW  - ^g-Aminobutyric acid
KW  - Dopamine
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Genetic Variations between Normotensive and Hypertensive Rats in Brain Microvessels and Potential Targets of AT1 Receptor Antagonists
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39813760; 4119751
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Zhou, J
AU  - Macova, M
AU  - Ando, H
AU  - Saavedra, J M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Brain
KW  - Rats
KW  - Antagonists
KW  - U 7000:Multidisciplinary
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TY  - CPAPER
T1  - Chondroitin Sulfate Proteoglycan Glycosaminoglycan Chain Synthesis: a Potential Molecular Target
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39811604; 4125636
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Laabs, T L
AU  - Fawcett, J W
AU  - Geller, H M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Sulfate
KW  - Glycosaminoglycans
KW  - Chondroitin sulfate
KW  - Proteoglycans
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Protein Synthesis Inhibitors Prevent Presynaptically Expressed Long - Term Depression in the Sensorimotor Striatum
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39811358; 4125577
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Ronesi, J
AU  - Yin, H H
AU  - Lovinger, D M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Depression
KW  - Protein biosynthesis
KW  - Neostriatum
KW  - Protein synthesis
KW  - Inhibitors
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Studies of Oxytocin Transcription in the Rat Hypothalamus Using an Intron - Specific Probe
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39804145; 4134727
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Yue, C
AU  - Mutsuga, N
AU  - Scordalakes, E M
AU  - Gainer, H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Probes
KW  - Introns
KW  - Transcription
KW  - Oxytocin
KW  - Hypothalamus
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Angiotensin II Receptor Antagonist Reduces Proinflammatory Cytokine Production in Rat Tissues
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39801026; 4134758
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Fernando, L P
AU  - Pavel, J
AU  - Nazarali, A J
AU  - Saavedra, J M
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Cytokines
KW  - Angiotensin II receptors
KW  - Inflammation
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Differential Distribution of KCNQ Channel Subunits in Hippocampal CA1 Interneurons
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39800201; 4132440
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Churchill, J F
AU  - Travis, K A
AU  - Statland, J M
AU  - Saraga, F
AU  - Skinner, F K
AU  - McBain, C J
AU  - Lawrence, J J
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Channels
KW  - Interneurons
KW  - Potassium channels (voltage-gated)
KW  - Hippocampus
KW  - Differential distribution
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39800201?accountid=14244
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - The Quantal Size Variation is Mainly Determined by Transmitter Concentration in Glutamatergic Vesicles
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39791451; 4134137
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Wu, X.
AU  - Wu, L.
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Vesicles
KW  - Glutamatergic transmission
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Amygdala Activation in Affective Priming: An MEG Study
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39785473; 4122895
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Munoz, K E
AU  - Garolera, M
AU  - Goldberg, T E
AU  - Elvevag, B
AU  - Carver, F W
AU  - Zoltick, B J
AU  - Weinberger, D R
AU  - Coppola, R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Amygdala
KW  - U 7000:Multidisciplinary
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Isoflurane Reduces Excitability and Glutamate Release at the Drosophila Neuromuscular Junction: The Role of Leak K@@u+@ Channels
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39778409; 4122184
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Sandstrom, D J
AU  - Nash, H A
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Potassium channels
KW  - Glutamic acid
KW  - Isoflurane
KW  - Neuromuscular junctions
KW  - Excitability
KW  - Drosophila
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Delivery of a Sensory Neuron Specific Promoter Region for the Mouse Scn10a Gene Using an Adenoviral Dual Reporter Construct
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39777456; 4122143
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Puhl, H L
AU  - Chen, H
AU  - Ikeda, S R
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Promoters
KW  - Sensory neurons
KW  - Neurons
KW  - U 7000:Multidisciplinary
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Distribution of a - CaMKII near the Presynaptic Active Zone in Resting and Stimulated Synapses
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39773901; 4118969
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Reese, T S
AU  - Dosemeci, A
AU  - Winters, C A
AU  - Tao-Cheng, J H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Synapses
KW  - Ca@@u2+@/calmodulin-dependent protein kinase II
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39773901?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Sulfation of Astrocyte Chondroitin Sulfate Proteoglycan in Neuronal Growth
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39769540; 4125637
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Wang, H
AU  - Katagiri, Y
AU  - Tan, F
AU  - Geller, H
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Sulfate
KW  - Chondroitin sulfate
KW  - Proteoglycans
KW  - Astrocytes
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39769540?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Mass of the Postsynaptic Density and the Number of Copies of Three Key Molecules
T2  - 35th Annual Meeting of the Society for Neuroscience
AN  - 39767694; 4119711
JF  - 35th Annual Meeting of the Society for Neuroscience
AU  - Chen, X
AU  - Vinade, L
AU  - Leapman, R D
AU  - Petersen, J D
AU  - Nakagawa, T
AU  - Phillips, T M
AU  - Sheng, M
AU  - Reese, T S
Y1  - 2005/11/12/
PY  - 2005
DA  - 2005 Nov 12
KW  - Postsynaptic density
KW  - U 7000:Multidisciplinary
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LA  - English
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - JOUR
T1  - Suppression of hypoxia-inducible factor 1alpha (HIF-1alpha) transcriptional activity by the HIF prolyl hydroxylase EGLN1.
AN  - 68765610; 16157596
AB  - The cellular response to hypoxia is, at least in part, mediated by the transcriptional regulation of hypoxia-responsive genes involved in balancing the intracellular ATP production and consumption. Recent evidence suggests that the transcription factor, HIF-1alpha, functions as a master regulator of oxygen homeostasis by controlling a broad range of cellular events in hypoxia. In normoxia, HIF-1alpha is targeted for destruction via prolyl hydroxylation, an oxygen-dependent modification that signals for recognition by the ubiquitin ligase complex containing the von Hippel-Lindau tumor suppressor. Three HIF prolyl hydroxylases (EGLN1, EGLN2, and EGLN3) have been identified in mammals, among which EGLN1 and EGLN3 are hypoxia-inducible at their mRNA levels in an HIF-1alpha-dependent manner. In this study, we demonstrated that apart from promoting HIF-1alpha proteolysis in normoxia, EGLN1 specifically represses HIF-1alpha transcriptional activity in hypoxia. Ectopic expression of EGLN1 inhibited HIF-1alpha transcriptional activity without altering its protein levels in a von Hippel-Lindau-deficient cell line, indicating a discrete activity of EGLN1 in transcriptional repression. Conversely, silencing of EGLN1 expression augmented HIF-1alpha transcriptional activity and its target gene expression in hypoxia. Thus, we proposed that the accumulated EGLN1 in hypoxia acts as a negative-feedback mechanism to modulate HIF-1alpha target gene expression. Our finding also provided new insight into the pharmacological manipulation of the HIF prolyl hydroxylase for ischemic diseases.
JF  - The Journal of biological chemistry
AU  - To, Kenneth K W
AU  - Huang, L Eric
AD  - Laboratory of Human Carcinogenesis, NCI, National Institutes of Health, Bethesda, MD 20892, USA.
Y1  - 2005/11/11/
PY  - 2005
DA  - 2005 Nov 11
SP  - 38102
EP  - 38107
VL  - 280
IS  - 45
SN  - 0021-9258, 0021-9258
KW  - Hypoxia-Inducible Factor 1, alpha Subunit
KW  - 0
KW  - Immediate-Early Proteins
KW  - EGLN1 protein, human
KW  - EC 1.14.11.2
KW  - Procollagen-Proline Dioxygenase
KW  - Hypoxia-Inducible Factor-Proline Dioxygenases
KW  - EC 1.14.11.29
KW  - Oxygen
KW  - S88TT14065
KW  - Index Medicus
KW  - Animals
KW  - Genes, Reporter -- genetics
KW  - Protein Binding -- drug effects
KW  - Oxygen -- pharmacology
KW  - Oxygen -- metabolism
KW  - Humans
KW  - Cell Line
KW  - Immediate-Early Proteins -- genetics
KW  - Hypoxia-Inducible Factor 1, alpha Subunit -- genetics
KW  - Procollagen-Proline Dioxygenase -- genetics
KW  - Immediate-Early Proteins -- metabolism
KW  - Hypoxia-Inducible Factor 1, alpha Subunit -- antagonists & inhibitors
KW  - Gene Silencing
KW  - Transcription, Genetic
KW  - Procollagen-Proline Dioxygenase -- metabolism
KW  - Hypoxia-Inducible Factor 1, alpha Subunit -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-12
N1  - Date created - 2005-11-07
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
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N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Comparison of protease-resistant prion protein inhibitors in cell cultures infected with two strains of mouse and sheep scrapie
AN  - 20237623; 6535846
AB  - The transmissible spongiform encephalopathies (TSEs) are fatal neurodegenerative diseases. A primary therapeutic target for TSE intervention has been a protease-resistant form of prion protein known as PrP super(Sc) or PrP-res. In vitro testing of mouse scrapie-infected cell cultures has identified many PrP-res inhibitors that also have activity in vivo. Here we identify 32 new inhibitors of two strains of mouse scrapie PrP-res. Furthermore, to investigate the species-specificity of these and other PrP-res inhibitors, we have developed a high-throughput cell culture assay based on Rov9 cells chronically-infected with sheep scrapie. Of 32 inhibitors of murine PrP-res that were also tested in the Rov9 cells, only six showed inhibitory activity against sheep PrP-res. The three most potent inhibitors of both murine and ovine PrP-res formation (with 50% inhibition at less than or equal to 5 mu M) were tannic acid, pentosan polysulfate and Fe(III) deuteroporphyrin 2,4-bisethyleneglycol. The latter two have anti-mouse scrapie activity in vivo. These results identify new inhibitors of murine and ovine PrP-res formation and reinforce the idea that compounds effective against PrP-res from one species or strain cannot be assumed to be active against others.
JF  - Neuroscience Letters
AU  - Kocisko, DA
AU  - Engel, AL
AU  - Harbuck, K
AU  - Arnold, K M
AU  - Olsen, E A
AU  - Raymond, L D
AU  - Vilette, D
AU  - Caughey, B
AD  - Laboratory of Persistent Viral Diseases, Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, National Institutes of Health, 903 S. 4th Street, Hamilton, MT 59840, USA
Y1  - 2005/11/11/
PY  - 2005
DA  - 2005 Nov 11
SP  - 106
EP  - 111
VL  - 388
IS  - 2
SN  - 0304-3940, 0304-3940
KW  - Biotechnology and Bioengineering Abstracts; CSA Neurosciences Abstracts
KW  - Transmissible spongiform encephalopathy
KW  - Neurodegenerative diseases
KW  - Nervous system
KW  - Prion protein
KW  - Cell culture
KW  - Scrapie
KW  - Tannic acid
KW  - pentosan polysulfate
KW  - N3 11028:Neuropharmacology & toxicology
KW  - W 30945:Fermentation & Cell Culture
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20237623?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Neuroscience+Letters&rft.atitle=Comparison+of+protease-resistant+prion+protein+inhibitors+in+cell+cultures+infected+with+two+strains+of+mouse+and+sheep+scrapie&rft.au=Kocisko%2C+DA%3BEngel%2C+AL%3BHarbuck%2C+K%3BArnold%2C+K+M%3BOlsen%2C+E+A%3BRaymond%2C+L+D%3BVilette%2C+D%3BCaughey%2C+B&rft.aulast=Kocisko&rft.aufirst=DA&rft.date=2005-11-11&rft.volume=388&rft.issue=2&rft.spage=106&rft.isbn=&rft.btitle=&rft.title=Neuroscience+Letters&rft.issn=03043940&rft_id=info:doi/10.1016%2Fj.neulet.2005.06.053
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Transmissible spongiform encephalopathy; Neurodegenerative diseases; Nervous system; Prion protein; Cell culture; Tannic acid; Scrapie; pentosan polysulfate
DO  - http://dx.doi.org/10.1016/j.neulet.2005.06.053
ER  - 



TY  - JOUR
T1  - Selection of control genes for quantitative RT-PCR based on microarray data
AN  - 17404665; 6524202
AB  - Use of internal reference gene(s) is necessary for adequate quantification of target gene expression by RT-PCR. Herein, we elaborated a strategy of control gene selection based on microarray data and illustrated it by analyzing endomyocardial biopsies with acute cardiac rejection and infection. Using order statistics and binomial distribution we evaluated the probability of finding low-varying genes by chance. For analysis, the microarray data were divided into two sample subsets. Among the first 10% of genes with the lowest standard deviations, we found 14 genes common to both subsets. After normalization using two selected genes, high correlation was observed between expression of target genes evaluated by microarray and RT-PCR, and in independent dataset by RT-PCR (r=0.9, p<0.001). In conclusion, we showed a simple and reliable strategy of selection and validation of control genes for RT-PCR from microarray data that can be easily applied for different experimental designs and tissues.
JF  - Biochemical and Biophysical Research Communications
AU  - Shulzhenko, N
AU  - Yambartsev, A
AU  - Goncalves-Primo, A
AU  - Gerbase-DeLima, M
AU  - Morgun, A
AD  - Pediatrics Department, Universidade Federal de Sao Paulo-UNIFESP, Sao Paulo, SP, Brazil, morguna@niaid.nih.gov
Y1  - 2005/11/11/
PY  - 2005
DA  - 2005 Nov 11
SP  - 306
EP  - 312
PB  - Elsevier Inc.
VL  - 337
IS  - 1
SN  - 0006-291X, 0006-291X
KW  - Genetics Abstracts; Biochemistry Abstracts 2: Nucleic Acids; Biotechnology and Bioengineering Abstracts
KW  - Heart
KW  - Data processing
KW  - Statistics
KW  - Standard deviation
KW  - Statistical analysis
KW  - Polymerase chain reaction
KW  - Biopsy
KW  - Infection
KW  - N 14025:RNA/DNA role in infection & immune response
KW  - W 30960:Bioinformatics & Computer Applications
KW  - G 07700:Molecular Genetics
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Biochemical+and+Biophysical+Research+Communications&rft.atitle=Selection+of+control+genes+for+quantitative+RT-PCR+based+on+microarray+data&rft.au=Shulzhenko%2C+N%3BYambartsev%2C+A%3BGoncalves-Primo%2C+A%3BGerbase-DeLima%2C+M%3BMorgun%2C+A&rft.aulast=Shulzhenko&rft.aufirst=N&rft.date=2005-11-11&rft.volume=337&rft.issue=1&rft.spage=306&rft.isbn=&rft.btitle=&rft.title=Biochemical+and+Biophysical+Research+Communications&rft.issn=0006291X&rft_id=info:doi/10.1016%2Fj.bbrc.2005.09.048
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-08-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Heart; Standard deviation; Statistics; Data processing; Statistical analysis; Polymerase chain reaction; Biopsy; Infection
DO  - http://dx.doi.org/10.1016/j.bbrc.2005.09.048
ER  - 



TY  - JOUR
T1  - Visualization of the Phosphorylated Active Site Loop of the Cytoplasmic B Domain of the Mannitol Transporter II super(M) super(a) super(n) super(n) super(i) super(t) super(o) super(l) of the Escherichia coli Phosphotransferase System by NMR Spectroscopy and Residual Dipolar Couplings
AN  - 17403643; 6523617
AB  - The solution structure of a stably phosphorylated form of the cytoplasmic B domain of the mannitol-specific transporter (IIB super(M) super(t) super(l)) of the Escherichia coli phosphotransferase system, containing a mutation of the active site Cys384 to Ser, has been solved by NMR. The strategy employed relies principally on backbone residual dipolar couplings recorded in three different alignment media, supplemented by nuclear Overhauser enhancement data and torsion angle restraints related specifically to the active site loop (residues 383-393). As judged from the dipolar coupling data, the remainder of the structure is unchanged upon phosphorylation within the errors of the coordinates of the previously determined solution structure of unphosphorylated wild-type IIB super(M) super(t) super(l). Thus, only the active site loop was refined. Phosphorylation results in a backbone atomic rms shift of } .7A in the active site loop. The resulting conformation is less than 0.5A away from the equivalent P-loop in both the low and high molecular mass eukaryotic tyrosine phosphatases. super(3)J sub(N) sub(P) coupling constant measurements using quantitative J-correlation spectroscopy provide a direct demonstration of a hydrogen bond between the phosphoryl group and the backbone amide of Ser391 at position i+7 from phospho-Ser384, with an approximately linear P-O-H sub(N) bond angle. The structure also reveals additional hydrogen bonding interactions involving the backbone amides of residues at positions i+4 and i+5, and the hydroxyl groups of two serine residues at positions i+6 and i+7 that stabilize the phosphoryl group. respectively, of II super(M) super(t) super(l)
JF  - Journal of Molecular Biology
AU  - Suh, J Y
AU  - Tang, C
AU  - Cai, M
AU  - Clore, G
AD  - Building 5, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892-0520, USA, mariusc@intra.niddk.nih.gov
Y1  - 2005/11/11/
PY  - 2005
DA  - 2005 Nov 11
SP  - 1129
EP  - 1136
VL  - 353
IS  - 5
SN  - 0022-2836, 0022-2836
KW  - Microbiology Abstracts B: Bacteriology
KW  - Wild type
KW  - phosphotransferase
KW  - Spectroscopy
KW  - Protein-tyrosine-phosphatase
KW  - Phosphorylation
KW  - Mannitol
KW  - Hydrogen bonding
KW  - Magnetic resonance spectroscopy
KW  - Escherichia coli
KW  - N.M.R.
KW  - Active sites
KW  - Mutation
KW  - amides
KW  - Conformation
KW  - J 02728:Enzymes
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Molecular+Biology&rft.atitle=Visualization+of+the+Phosphorylated+Active+Site+Loop+of+the+Cytoplasmic+B+Domain+of+the+Mannitol+Transporter+II+super%28M%29+super%28a%29+super%28n%29+super%28n%29+super%28i%29+super%28t%29+super%28o%29+super%28l%29+of+the+Escherichia+coli+Phosphotransferase+System+by+NMR+Spectroscopy+and+Residual+Dipolar+Couplings&rft.au=Suh%2C+J+Y%3BTang%2C+C%3BCai%2C+M%3BClore%2C+G&rft.aulast=Suh&rft.aufirst=J&rft.date=2005-11-11&rft.volume=353&rft.issue=5&rft.spage=1129&rft.isbn=&rft.btitle=&rft.title=Journal+of+Molecular+Biology&rft.issn=00222836&rft_id=info:doi/10.1016%2Fj.jmb.2005.09.033
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-05-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Wild type; phosphotransferase; Spectroscopy; Protein-tyrosine-phosphatase; Phosphorylation; Hydrogen bonding; Mannitol; Magnetic resonance spectroscopy; N.M.R.; Active sites; amides; Mutation; Conformation; Escherichia coli
DO  - http://dx.doi.org/10.1016/j.jmb.2005.09.033
ER  - 



TY  - CPAPER
T1  - Inflammatory Protein Profile During Systemic High Dose Interleukin-2 Administration
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39814967; 4074306
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Rossi, Leonardo
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Interleukin 2
KW  - Inflammation
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39814967?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Inflammatory+Protein+Profile+During+Systemic+High+Dose+Interleukin-2+Administration&rft.au=Rossi%2C+Leonardo&rft.aulast=Rossi&rft.aufirst=Leonardo&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Factors that Influence Responses to Adoptive Cancer Immunotherapy
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39809602; 4074291
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Robbins, Paul F
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Cancer
KW  - Immunotherapy
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39809602?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Factors+that+Influence+Responses+to+Adoptive+Cancer+Immunotherapy&rft.au=Robbins%2C+Paul+F&rft.aulast=Robbins&rft.aufirst=Paul&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Hematopoietic Stem Cell Transplant with Lymphodepletion Augments T Cell-Based Adoptive Immunotherapy
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39796400; 4074317
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Wrzesinski, Claudia
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Adoptive immunotherapy
KW  - Transplants
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39796400?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Hematopoietic+Stem+Cell+Transplant+with+Lymphodepletion+Augments+T+Cell-Based+Adoptive+Immunotherapy&rft.au=Wrzesinski%2C+Claudia&rft.aulast=Wrzesinski&rft.aufirst=Claudia&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Gene Profiling of BCC Treated with the Immunomodifier Imiquimod (ALDARA @@uTM@) Reveals Key Signatures of Tumor Rejection
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39796273; 4074304
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Panelli, Monica
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Imiquimod
KW  - Profiling
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39796273?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Gene+Profiling+of+BCC+Treated+with+the+Immunomodifier+Imiquimod+%28ALDARA+%40%40uTM%40%29+Reveals+Key+Signatures+of+Tumor+Rejection&rft.au=Panelli%2C+Monica&rft.aulast=Panelli&rft.aufirst=Monica&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Cytokines and Tumor Immunology
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39789372; 4074327
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Wigginton, Jon M
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Immunology
KW  - Cytokines
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39789372?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Cytokines+and+Tumor+Immunology&rft.au=Wigginton%2C+Jon+M&rft.aulast=Wigginton&rft.aufirst=Jon&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - IL-2 Paradoxically Controls Tolerance and Immunity to a Tumor/Self-Antigen
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39774790; 4074278
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Antony, Paul A
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Interleukin 2
KW  - Immunity
KW  - Autoantigens
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39774790?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=IL-2+Paradoxically+Controls+Tolerance+and+Immunity+to+a+Tumor%2FSelf-Antigen&rft.au=Antony%2C+Paul+A&rft.aulast=Antony&rft.aufirst=Paul&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Treatment of Patients with Metastatic Melanoma by Infusion of Anti-MART-1 TCR-Gene Engineered Lymphocytes
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39763201; 4074315
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Morgan, Richard
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Lymphocytes
KW  - T-cell receptor
KW  - Melanoma
KW  - Metastases
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39763201?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Treatment+of+Patients+with+Metastatic+Melanoma+by+Infusion+of+Anti-MART-1+TCR-Gene+Engineered+Lymphocytes&rft.au=Morgan%2C+Richard&rft.aulast=Morgan&rft.aufirst=Richard&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Proteasome Inhibition Upregulates the Cell Surface Expression of Receptors for IFN-a and TNF-a on Murine Neuroblastoma Cells and Enhances the Proapoptotic and Overall Antitumor Activity of Systemic Cytokine Therapy in Murine Neuroblastoma Tumors
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39755259; 4074286
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Khan, Tahira
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Cytokines
KW  - Antitumor activity
KW  - Proteasomes
KW  - Neuroblastoma cells
KW  - Cell surface
KW  - Neuroblastoma
KW  - Therapy
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39755259?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Proteasome+Inhibition+Upregulates+the+Cell+Surface+Expression+of+Receptors+for+IFN-a+and+TNF-a+on+Murine+Neuroblastoma+Cells+and+Enhances+the+Proapoptotic+and+Overall+Antitumor+Activity+of+Systemic+Cytokine+Therapy+in+Murine+Neuroblastoma+Tumors&rft.au=Khan%2C+Tahira&rft.aulast=Khan&rft.aufirst=Tahira&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - CD4 Cells can be More Efficient at Tumor Rejection than CD8 Cells
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39752385; 4074311
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Perez-Diez, Ainhoa
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - CD8 antigen
KW  - CD4 antigen
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39752385?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=CD4+Cells+can+be+More+Efficient+at+Tumor+Rejection+than+CD8+Cells&rft.au=Perez-Diez%2C+Ainhoa&rft.aulast=Perez-Diez&rft.aufirst=Ainhoa&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Phase I Trial of Siplizumab in CD2-Positive Lymphoproliferative Disease
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39752336; 4074300
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Janik, John
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Immunoproliferative diseases
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39752336?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Phase+I+Trial+of+Siplizumab+in+CD2-Positive+Lymphoproliferative+Disease&rft.au=Janik%2C+John&rft.aulast=Janik&rft.aufirst=John&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Expansion of CD4 + CD25 + Regulatory T Cells During Lymphopenia and Following IL2 Therapy
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39752290; 4074298
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Mackall, Crystal
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Interleukin 2
KW  - Lymphocytes T
KW  - Immunoregulation
KW  - CD25 antigen
KW  - CD4 antigen
KW  - Lymphopenia
KW  - Therapy
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39752290?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Expansion+of+CD4+%2B+CD25+%2B+Regulatory+T+Cells+During+Lymphopenia+and+Following+IL2+Therapy&rft.au=Mackall%2C+Crystal&rft.aulast=Mackall&rft.aufirst=Crystal&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Tumor Therapy with Proteasome Inhibitor Bortezomib (Velcade, PS- 341) Plus Death Receptor (DR5) Agonist Antibody MD5.1
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39741274; 4074283
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Shanker, Anil
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Mortality
KW  - Antibodies
KW  - Proteasome inhibitors
KW  - Death receptors
KW  - Therapy
KW  - Inhibitors
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39741274?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Tumor+Therapy+with+Proteasome+Inhibitor+Bortezomib+%28Velcade%2C+PS-+341%29+Plus+Death+Receptor+%28DR5%29+Agonist+Antibody+MD5.1&rft.au=Shanker%2C+Anil&rft.aulast=Shanker&rft.aufirst=Anil&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - How Host Cells Sink Anti-Tumor Responses by Competing for Activating Cytokines
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39741169; 4074277
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Restifo, Nicholas P
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Cytokines
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39741169?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=How+Host+Cells+Sink+Anti-Tumor+Responses+by+Competing+for+Activating+Cytokines&rft.au=Restifo%2C+Nicholas+P&rft.aulast=Restifo&rft.aufirst=Nicholas&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Making Vaccines Work: Translating Basic and Preclinical Immunology into Human Immunotherapies
T2  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AN  - 39695322; 4074334
JF  - 20th Annual Meeting of the International Society for Biological Therapy of Cancer
AU  - Restifo, Nicholas P
Y1  - 2005/11/10/
PY  - 2005
DA  - 2005 Nov 10
KW  - Vaccines
KW  - Immunology
KW  - Immunotherapy
KW  - Disease control
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39695322?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.atitle=Making+Vaccines+Work%3A+Translating+Basic+and+Preclinical+Immunology+into+Human+Immunotherapies&rft.au=Restifo%2C+Nicholas+P&rft.aulast=Restifo&rft.aufirst=Nicholas&rft.date=2005-11-10&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=20th+Annual+Meeting+of+the+International+Society+for+Biological+Therapy+of+Cancer&rft.issn=&rft_id=info:doi/
L2  - http://www.isbtc.org/meetings/am05/presentations.html
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Epigenetic mechanisms and gene networks in the nervous system.
AN  - 68786583; 16280577
JF  - The Journal of neuroscience : the official journal of the Society for Neuroscience
AU  - Colvis, Christine M
AU  - Pollock, Jonathan D
AU  - Goodman, Richard H
AU  - Impey, Soren
AU  - Dunn, John
AU  - Mandel, Gail
AU  - Champagne, Frances A
AU  - Mayford, Mark
AU  - Korzus, Edward
AU  - Kumar, Arvind
AU  - Renthal, William
AU  - Theobald, David E H
AU  - Nestler, Eric J
AD  - Division of Basic Neurosciences and Behavioral Research, National Institute on Drug Abuse, Bethesda, Maryland 20892, USA. ccolvis@nida.nih.gov
Y1  - 2005/11/09/
PY  - 2005
DA  - 2005 Nov 09
SP  - 10379
EP  - 10389
VL  - 25
IS  - 45
KW  - Histones
KW  - 0
KW  - Transcription Factors
KW  - Index Medicus
KW  - Environment
KW  - Animals
KW  - DNA Methylation
KW  - Models, Molecular
KW  - Gene Silencing
KW  - Neurons
KW  - Histones -- metabolism
KW  - Genome
KW  - Substance-Related Disorders -- genetics
KW  - Epigenesis, Genetic -- physiology
KW  - Transcription Factors -- metabolism
KW  - Chromatin Assembly and Disassembly -- physiology
KW  - Nervous System
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68786583?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=The+Journal+of+neuroscience+%3A+the+official+journal+of+the+Society+for+Neuroscience&rft.atitle=Epigenetic+mechanisms+and+gene+networks+in+the+nervous+system.&rft.au=Colvis%2C+Christine+M%3BPollock%2C+Jonathan+D%3BGoodman%2C+Richard+H%3BImpey%2C+Soren%3BDunn%2C+John%3BMandel%2C+Gail%3BChampagne%2C+Frances+A%3BMayford%2C+Mark%3BKorzus%2C+Edward%3BKumar%2C+Arvind%3BRenthal%2C+William%3BTheobald%2C+David+E+H%3BNestler%2C+Eric+J&rft.aulast=Colvis&rft.aufirst=Christine&rft.date=2005-11-09&rft.volume=25&rft.issue=45&rft.spage=10379&rft.isbn=&rft.btitle=&rft.title=The+Journal+of+neuroscience+%3A+the+official+journal+of+the+Society+for+Neuroscience&rft.issn=1529-2401&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-25
N1  - Date created - 2005-11-10
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Thyroid hormone receptor beta mutants: Dominant negative regulators of peroxisome proliferator-activated receptor gamma action.
AN  - 68778117; 16260719
AB  - Thyroid hormone (T3) and peroxisome proliferators have overlapping metabolic effects in the maintenance of lipid homeostasis. Their actions are mediated by their respective receptors: thyroid hormone receptors (TR) and peroxisome proliferator-activated receptors (PPAR). We recently found that a dominantly negative TRbeta mutant (PV) that causes a genetic disease, resistance to thyroid hormone, acts to repress the ligand (troglitazone)-mediated transcriptional activity of PPARgamma in cultured thyroid cells. This finding suggests that TRbeta mutants could crosstalk with PPARgamma-signaling pathways. The present study explored the molecular mechanisms by which PV represses the PPARgamma transcriptional activity. Gel-shift assays show that the PV, similar to wild-type TRbeta, bound to the peroxisome proliferator response element (PPRE) as homodimers and heterodimers with PPARgamma or the retinoid X receptor (RXR), thereby competing with PPARgamma for binding to PPRE and for sequestering RXR. Association of PPRE-bound PV with corepressors [e.g., nuclear receptor corepressor (NCoR)] that led to transcriptional repression was independent of T3 and troglitazone. Chromatin immunoprecipitation assay further demonstrated that, despite the presence of ligands, NCoR was recruited to PPRE-bound PV on a PPARgamma-target gene, the lipoprotein lipase, in vivo, suggesting the dominant action of PV on PPARgamma-mediated transcriptional activity. Thus, the dominant negative action of PV is not limited on the wild-type TRs. The findings that TRbeta mutants affect PPARgamma functions through dominant negative action provide insights into the molecular mechanisms by which TR regulates the PPARgamma-target genes involved in metabolic pathways, lipid homeostasis, and carcinogenesis.
JF  - Proceedings of the National Academy of Sciences of the United States of America
AU  - Araki, Osamu
AU  - Ying, Hao
AU  - Furuya, Fumihiko
AU  - Zhu, Xuguang
AU  - Cheng, Sheue-Yann
AD  - Laboratory of Molecular Biology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892-4264, USA.
Y1  - 2005/11/08/
PY  - 2005
DA  - 2005 Nov 08
SP  - 16251
EP  - 16256
VL  - 102
IS  - 45
SN  - 0027-8424, 0027-8424
KW  - Chromans
KW  - 0
KW  - PPAR gamma
KW  - Retinoid X Receptors
KW  - Thiazolidinediones
KW  - Thyroid Hormone Receptors beta
KW  - Transcription Factors
KW  - Histone Acetyltransferases
KW  - EC 2.3.1.48
KW  - Ncoa1 protein, mouse
KW  - Nuclear Receptor Coactivator 1
KW  - troglitazone
KW  - I66ZZ0ZN0E
KW  - Index Medicus
KW  - Transcription Factors -- physiology
KW  - Animals
KW  - Dimerization
KW  - Mice
KW  - Retinoid X Receptors -- chemistry
KW  - Transcriptional Activation
KW  - Promoter Regions, Genetic
KW  - Chromans -- pharmacology
KW  - Cells, Cultured
KW  - Thiazolidinediones -- pharmacology
KW  - Response Elements
KW  - Mutation
KW  - Signal Transduction
KW  - Retinoid X Receptors -- metabolism
KW  - Thyroid Hormone Receptors beta -- physiology
KW  - Thyroid Hormone Receptors beta -- genetics
KW  - PPAR gamma -- physiology
KW  - PPAR gamma -- chemistry
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68778117?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Proceedings+of+the+National+Academy+of+Sciences+of+the+United+States+of+America&rft.atitle=Thyroid+hormone+receptor+beta+mutants%3A+Dominant+negative+regulators+of+peroxisome+proliferator-activated+receptor+gamma+action.&rft.au=Araki%2C+Osamu%3BYing%2C+Hao%3BFuruya%2C+Fumihiko%3BZhu%2C+Xuguang%3BCheng%2C+Sheue-Yann&rft.aulast=Araki&rft.aufirst=Osamu&rft.date=2005-11-08&rft.volume=102&rft.issue=45&rft.spage=16251&rft.isbn=&rft.btitle=&rft.title=Proceedings+of+the+National+Academy+of+Sciences+of+the+United+States+of+America&rft.issn=00278424&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-12
N1  - Date created - 2005-11-09
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Endocr Rev. 1993 Jun;14(3):348-99 [8319599]
Trends Endocrinol Metab. 2005 May-Jun;16(4):176-82 [15860414]
Dev Biol. 1994 Oct;165(2):654-69 [7958429]
J Biol Chem. 1995 Jul 28;270(30):18117-22 [7629123]
Biochemistry. 1995 Aug 22;34(33):10591-9 [7544615]
Cell. 1995 Dec 15;83(6):841-50 [8521508]
Mol Pharmacol. 1996 Feb;49(2):276-87 [8632760]
Mol Cell Endocrinol. 1996 Feb 5;116(2):213-21 [8647322]
EMBO J. 1996 Oct 1;15(19):5336-48 [8895578]
Annu Rev Cell Dev Biol. 1996;12:335-63 [8970730]
J Biol Chem. 1997 Apr 4;272(14):9048-54 [9083030]
Proc Natl Acad Sci U S A. 2000 Nov 21;97(24):13209-14 [11069286]
Rev Endocr Metab Disord. 2000 Jan;1(1-2):9-18 [11704997]
J Biol Chem. 2002 Jul 26;277(30):26821-30 [12015306]
Mol Endocrinol. 2002 Sep;16(9):2077-92 [12198244]
Thyroid. 2002 Nov;12(11):963-9 [12490073]
Carcinogenesis. 2003 Sep;24(9):1467-79 [12869418]
Cancer Res. 2003 Sep 1;63(17):5274-80 [14500358]
Endocr Rev. 2004 Feb;25(1):45-71 [14769827]
Cell. 1987 Nov 6;51(3):445-53 [3664642]
J Clin Endocrinol Metab. 1991 Nov;73(5):990-4 [1682340]
J Clin Invest. 1991 Dec;88(6):2123-30 [1661299]
Mol Endocrinol. 1992 Feb;6(2):248-58 [1569968]
Mol Endocrinol. 1997 Apr;11(4):470-80 [9092799]
J Biol Chem. 1997 Aug 8;272(32):20108-17 [9242684]
Endocrinology. 1998 Feb;139(2):640-50 [9449636]
Endocr Rev. 1999 Oct;20(5):649-88 [10529898]
Genes Dev. 2005 Feb 15;19(4):453-61 [15681609]
J Biol Chem. 1994 Apr 22;269(16):11683-6 [8163464]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The ETV6-NTRK3 chimeric tyrosine kinase suppresses TGF-beta signaling by inactivating the TGF-beta type II receptor.
AN  - 68776049; 16258068
AB  - An emerging theme in cancer biology is that although some malignancies occur through the sequential acquisition of different genetic alterations, certain dominantly acting oncoproteins such as those associated with chromosomal translocations have multiple functions and do not require additional mutations for cell transformation. The ETV6-NTRK3 (EN) chimeric tyrosine kinase, a potent oncoprotein expressed in tumors derived from multiple cell lineages, functions as a constitutively active protein tyrosine kinase. Here, we show that EN suppresses TGF-beta signaling by directly binding to the type II TGF-beta receptor, thereby preventing it from interacting with the type I TGF-beta receptor. This activity requires a functional EN protein tyrosine kinase, and type II TGF-beta receptor appears to be a direct target of EN. Our findings provide evidence for a previously undescribed mechanism by which oncogenic tyrosine kinases can block TGF-beta tumor suppressor activity.
JF  - Proceedings of the National Academy of Sciences of the United States of America
AU  - Jin, Wook
AU  - Kim, Byung-Chul
AU  - Tognon, Cristina
AU  - Lee, Ho-Jae
AU  - Patel, Sejal
AU  - Lannon, Chris L
AU  - Maris, John M
AU  - Triche, Timothy J
AU  - Sorensen, Poul H B
AU  - Kim, Seong-Jin
AD  - Laboratory of Cell Regulation and Carcinogenesis, National Cancer Institute, Bethesda, MD 20892-5055, USA.
Y1  - 2005/11/08/
PY  - 2005
DA  - 2005 Nov 08
SP  - 16239
EP  - 16244
VL  - 102
IS  - 45
SN  - 0027-8424, 0027-8424
KW  - ETV6-NTRK3 fusion protein, human
KW  - 0
KW  - Oncogene Proteins, Fusion
KW  - Receptors, Transforming Growth Factor beta
KW  - Smad2 Protein
KW  - Smad3 Protein
KW  - Transforming Growth Factor beta
KW  - TGF-beta type I receptor
KW  - EC 2.7.1.11
KW  - Protein-Serine-Threonine Kinases
KW  - EC 2.7.11.1
KW  - Activin Receptors, Type I
KW  - EC 2.7.11.30
KW  - transforming growth factor-beta type II receptor
KW  - Index Medicus
KW  - Animals
KW  - Smad2 Protein -- metabolism
KW  - Phosphorylation
KW  - Activin Receptors, Type I -- physiology
KW  - Humans
KW  - Smad3 Protein -- metabolism
KW  - Molecular Sequence Data
KW  - Mice
KW  - Amino Acid Sequence
KW  - NIH 3T3 Cells
KW  - Cell Transformation, Neoplastic
KW  - Signal Transduction -- physiology
KW  - Oncogene Proteins, Fusion -- physiology
KW  - Receptors, Transforming Growth Factor beta -- physiology
KW  - Receptors, Transforming Growth Factor beta -- antagonists & inhibitors
KW  - Transforming Growth Factor beta -- antagonists & inhibitors
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68776049?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Proceedings+of+the+National+Academy+of+Sciences+of+the+United+States+of+America&rft.atitle=The+ETV6-NTRK3+chimeric+tyrosine+kinase+suppresses+TGF-beta+signaling+by+inactivating+the+TGF-beta+type+II+receptor.&rft.au=Jin%2C+Wook%3BKim%2C+Byung-Chul%3BTognon%2C+Cristina%3BLee%2C+Ho-Jae%3BPatel%2C+Sejal%3BLannon%2C+Chris+L%3BMaris%2C+John+M%3BTriche%2C+Timothy+J%3BSorensen%2C+Poul+H+B%3BKim%2C+Seong-Jin&rft.aulast=Jin&rft.aufirst=Wook&rft.date=2005-11-08&rft.volume=102&rft.issue=45&rft.spage=16239&rft.isbn=&rft.btitle=&rft.title=Proceedings+of+the+National+Academy+of+Sciences+of+the+United+States+of+America&rft.issn=00278424&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-12
N1  - Date created - 2005-11-09
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Cell. 1992 Dec 11;71(6):1003-14 [1333888]
Cell. 1992 Feb 21;68(4):775-85 [1310899]
EMBO J. 1995 May 15;14(10):2199-208 [7774578]
Nat Genet. 1998 Feb;18(2):184-7 [9462753]
Mol Cell. 1998 Mar;1(4):611-7 [9660945]
J Biol Chem. 1998 Aug 14;273(33):21145-52 [9694870]
Mol Cell. 1998 Jul;2(1):109-20 [9702197]
Am J Pathol. 1998 Nov;153(5):1451-8 [9811336]
Cancer Res. 1998 Nov 15;58(22):5046-8 [9823307]
Blood. 1999 Feb 15;93(4):1355-63 [9949179]
BJU Int. 1999 Sep;84(4):495-502 [10468769]
Clin Cancer Res. 1999 Aug;5(8):2205-12 [10473107]
Oncogene. 2000 Feb 17;19(7):906-15 [10702799]
EMBO J. 2000 Apr 17;19(8):1827-38 [10775267]
J Natl Cancer Inst. 2000 Sep 6;92(17):1388-402 [10974075]
Cancer Res. 2001 Dec 15;61(24):8909-16 [11751416]
Cytokine Growth Factor Rev. 2002 Feb;13(1):11-7 [11750876]
Cancer Cell. 2002 Mar;1(2):117-23 [12086869]
Oncogene. 2002 Aug 22;21(37):5684-95 [12173038]
Cancer Cell. 2002 Nov;2(5):367-76 [12450792]
Science. 2003 May 9;300(5621):949 [12738854]
Cell. 2003 Jun 13;113(6):685-700 [12809600]
Leukemia. 2003 Sep;17(9):1731-7 [12970772]
Nature. 2003 Oct 9;425(6958):577-84 [14534577]
J Biol Chem. 2004 Feb 20;279(8):6225-34 [14668342]
Mol Cell Biol. 2004 Jun;24(11):4636-50 [15143160]
Proc Natl Acad Sci U S A. 1994 Dec 20;91(26):12867-71 [7809137]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Nucleoid remodeling by an altered HU protein: Reorganization of the transcription program
AN  - 19395313; 7144985
AB  - Bacterial nucleoid organization is believed to have minimal influence on the global transcription program. Using an altered bacterial histone-like protein, HU alpha , we show that reorganization of the nucleoid configuration can dynamically modulate the cellular transcription pattern. The mutant protein transformed the loosely packed nucleoid into a densely condensed structure. The nucleoid compaction, coupled with increased global DNA supercoiling, generated radical changes in the morphology, physiology, and metabolism of wild-type K-12 Escherichia coli. Many constitutive housekeeping genes involved in nutrient utilization were repressed, whereas many quiescent genes associated with virulence were activated in the mutant. We propose that, as in eukaryotes, the nucleoid architecture dictates the global transcription profile and, consequently, the behavior pattern in bacteria.
JF  - Proceedings of the National Academy of Sciences, USA
AU  - Kar, Sudeshna
AU  - Edgar, Rotem
AU  - Adhya, Sankar
AD  - Laboratory of Molecular Biology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892-4264
Y1  - 2005/11/08/
PY  - 2005
DA  - 2005 Nov 08
SP  - 16397
EP  - 16402
PB  - National Academy of Sciences, 2101 Constitution Ave. Washington DC 20418 USA
VL  - 102
IS  - 45
SN  - 0027-8424, 0027-8424
KW  - Microbiology Abstracts B: Bacteriology; Biochemistry Abstracts 2: Nucleic Acids
KW  - Virulence
KW  - Supercoiling
KW  - Escherichia coli
KW  - DNA
KW  - Transcription
KW  - Nucleoids
KW  - double prime HU protein
KW  - Nutrient utilization
KW  - Compaction
KW  - Metabolism
KW  - Radicals
KW  - J 02330:Biochemistry
KW  - N 14835:Protein-Nucleic Acids Association
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19395313?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Proceedings+of+the+National+Academy+of+Sciences%2C+USA&rft.atitle=Nucleoid+remodeling+by+an+altered+HU+protein%3A+Reorganization+of+the+transcription+program&rft.au=Kar%2C+Sudeshna%3BEdgar%2C+Rotem%3BAdhya%2C+Sankar&rft.aulast=Kar&rft.aufirst=Sudeshna&rft.date=2005-11-08&rft.volume=102&rft.issue=45&rft.spage=16397&rft.isbn=&rft.btitle=&rft.title=Proceedings+of+the+National+Academy+of+Sciences%2C+USA&rft.issn=00278424&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Virulence; Supercoiling; DNA; Transcription; Nucleoids; Nutrient utilization; double prime HU protein; Compaction; Metabolism; Radicals; Escherichia coli
ER  - 



TY  - JOUR
T1  - Inhibition of mitochondrial aldehyde dehydrogenase by nitric oxide-mediated S-nitrosylation.
AN  - 68763885; 16242127
AB  - Mitochondrial aldehyde dehydrogenase (ALDH2) is responsible for the metabolism of acetaldehyde and other toxic lipid aldehydes. Despite many reports about the inhibition of ALDH2 by toxic chemicals, it is unknown whether nitric oxide (NO) can alter the ALDH2 activity in intact cells or in vivo animals. The aim of this study was to investigate the effects of NO on ALDH2 activity in H4IIE-C3 rat hepatoma cells. NO donors such as S-nitrosoglutathione (GSNO), S-nitroso-N-acetylpenicillamine, and 3-morpholinosydnonimine significantly increased the nitrite concentration while they inhibited the ALDH2 activity. Addition of GSH-ethylester (GSH-EE) completely blocked the GSNO-mediated ALDH2 inhibition and increased nitrite concentration. To directly demonstrate the NO-mediated S-nitrosylation and inactivation, ALDH2 was immunopurified from control or GSNO-treated cells and subjected to immunoblot analysis. The anti-nitrosocysteine antibody recognized the immunopurified ALDH2 only from the GSNO-treated samples. All these results indicate that S-nitrosylation of ALDH2 in intact cells leads to reversible inhibition of ALDH2 activity.
JF  - FEBS letters
AU  - Moon, Kwan-Hoon
AU  - Kim, Bong-Jo
AU  - Song, Byoung J
AD  - Laboratory of Membrane Biochemistry and Biophysics, National Institute on Alcohol Abuse and Alcoholism, Bethesda, MD 20892-9410, USA.
Y1  - 2005/11/07/
PY  - 2005
DA  - 2005 Nov 07
SP  - 6115
EP  - 6120
VL  - 579
IS  - 27
SN  - 0014-5793, 0014-5793
KW  - Antibodies
KW  - 0
KW  - Mitochondrial Proteins
KW  - Nitric Oxide Donors
KW  - Nitrites
KW  - Nitric Oxide
KW  - 31C4KY9ESH
KW  - S-Nitrosoglutathione
KW  - 57564-91-7
KW  - linsidomine
KW  - 5O5U71P6VQ
KW  - S-Nitroso-N-Acetylpenicillamine
KW  - 79032-48-7
KW  - Molsidomine
KW  - D46583G77X
KW  - Aldehyde Dehydrogenase
KW  - EC 1.2.1.3
KW  - Aldehyde Dehydrogenase, Mitochondrial
KW  - Aldh2 protein, rat
KW  - Cysteine
KW  - K848JZ4886
KW  - Index Medicus
KW  - Rats
KW  - S-Nitroso-N-Acetylpenicillamine -- pharmacology
KW  - Nitrites -- analysis
KW  - Antibodies -- immunology
KW  - Animals
KW  - Cysteine -- metabolism
KW  - Tumor Cells, Cultured
KW  - S-Nitrosoglutathione -- pharmacology
KW  - Molsidomine -- analogs & derivatives
KW  - Molsidomine -- pharmacology
KW  - Nitric Oxide Donors -- pharmacology
KW  - Mitochondria -- enzymology
KW  - Aldehyde Dehydrogenase -- immunology
KW  - Mitochondria -- drug effects
KW  - Mitochondrial Proteins -- antagonists & inhibitors
KW  - Nitric Oxide -- metabolism
KW  - Aldehyde Dehydrogenase -- antagonists & inhibitors
KW  - Aldehyde Dehydrogenase -- analysis
KW  - Mitochondrial Proteins -- analysis
KW  - Mitochondrial Proteins -- immunology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68763885?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=FEBS+letters&rft.atitle=Inhibition+of+mitochondrial+aldehyde+dehydrogenase+by+nitric+oxide-mediated+S-nitrosylation.&rft.au=Moon%2C+Kwan-Hoon%3BKim%2C+Bong-Jo%3BSong%2C+Byoung+J&rft.aulast=Moon&rft.aufirst=Kwan-Hoon&rft.date=2005-11-07&rft.volume=579&rft.issue=27&rft.spage=6115&rft.isbn=&rft.btitle=&rft.title=FEBS+letters&rft.issn=00145793&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-23
N1  - Date created - 2005-11-04
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Biochem Pharmacol. 2001 Mar 1;61(5):537-45 [11239496]
Sci STKE. 2001 Jun 12;2001(86):re1 [11752656]
Int J Cancer. 2002 Jan 10;97(2):261-5 [11774273]
Free Radic Biol Med. 2002 Feb 15;32(4):350-9 [11841925]
Mol Pharmacol. 2003 Feb;63(2):401-8 [12527812]
Toxicol Lett. 2003 Oct 15;144(3):279-88 [12927346]
Alcohol. 2003 Aug-Oct;31(1-2):19-24 [14615007]
J Clin Invest. 2004 Feb;113(3):352-4 [14755331]
J Clin Invest. 2004 Feb;113(3):482-9 [14755345]
Biochem Pharmacol. 2004 Jun 1;67(11):2167-74 [15135311]
J Biol Chem. 2004 May 21;279(21):21749-58 [15031298]
Biochem Pharmacol. 1981 Dec 15;30(24):3265-75 [7034733]
Anal Biochem. 1982 Oct;126(1):131-8 [7181105]
Toxicol Appl Pharmacol. 1983 Feb;67(2):159-65 [6836571]
Arch Biochem Biophys. 1985 Jan;236(1):36-46 [3966800]
Hepatology. 1985 Mar-Apr;5(2):260-3 [3979959]
Alcohol. 1987 Sep-Oct;4(5):413-8 [3675864]
J Biol Chem. 1989 Feb 25;264(6):3568-72 [2914964]
Hepatology. 1991 Apr;13(4):728-34 [2010168]
Free Radic Biol Med. 1991;11(1):81-128 [1937131]
Hepatology. 1991 Nov;14(5):798-801 [1937384]
J Biol Chem. 1993 Aug 25;268(24):17878-82 [8349672]
Arch Biochem Biophys. 1995 Jan 10;316(1):197-205 [7840616]
Biochemistry. 1995 Feb 28;34(8):2592-8 [7873540]
J Biol Chem. 1995 Jul 14;270(28):16487-90 [7622447]
Biochemistry. 1995 Sep 12;34(36):11494-9 [7547878]
Alcohol Clin Exp Res. 1995 Dec;19(6):1414-9 [8749803]
Toxicol Appl Pharmacol. 1996 Nov;141(1):299-307 [8917703]
Alcohol. 1997 Mar-Apr;14(2):181-9 [9085720]
Hepatology. 1997 Jun;25(6):1418-24 [9185762]
Hepatology. 1997 Dec;26(6):1386-92 [9397975]
Carcinogenesis. 1998 Aug;19(8):1383-7 [9744533]
J Biol Chem. 1999 Apr 2;274(14):9427-30 [10092623]
Proteomics. 2004 Nov;4(11):3401-12 [15449375]
Nat Rev Mol Cell Biol. 2005 Feb;6(2):150-66 [15688001]
J Biol Chem. 2005 Feb 4;280(5):3125-8 [15590625]
Proc Natl Acad Sci U S A. 2005 Aug 23;102(34):12159-64 [16103363]
J Hepatol. 1999 Nov;31(5):887-94 [10580587]
Mol Pharmacol. 2000 Sep;58(3):535-41 [10953046]
Arch Biochem Biophys. 2000 Dec 1;384(1):81-7 [11147839]
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Ultrasound, a Tool for Detection of Cardiotoxicity
T2  - 2005 Annual Meeting of the American College of Toxicology
AN  - 39693341; 4038894
JF  - 2005 Annual Meeting of the American College of Toxicology
AU  - Johnson, Kennita
Y1  - 2005/11/06/
PY  - 2005
DA  - 2005 Nov 06
KW  - Ultrasound
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39693341?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+American+College+of+Toxicology&rft.atitle=Ultrasound%2C+a+Tool+for+Detection+of+Cardiotoxicity&rft.au=Johnson%2C+Kennita&rft.aulast=Johnson&rft.aufirst=Kennita&rft.date=2005-11-06&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+American+College+of+Toxicology&rft.issn=&rft_id=info:doi/
L2  - http://www.actox.org/attmtg/PROGRAM05a.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Calindol, a positive allosteric modulator of the human Ca(2+) receptor, activates an extracellular ligand-binding domain-deleted rhodopsin-like seven-transmembrane structure in the absence of Ca(2+).
AN  - 68740969; 16135510
AB  - The extracellular calcium-sensing human Ca(2+) receptor (hCaR),2 a member of the family-3 G-protein-coupled receptors (GPCR) possesses a large amino-terminal extracellular ligand-binding domain (ECD) in addition to a seven-transmembrane helical domain (7TMD) characteristic of all GPCRs. Two calcimimetic allosteric modulators, NPS R-568 and Calindol ((R)-2-{1-(1-naphthyl)ethyl-aminom-ethyl}indole), that bind the 7TMD of the hCaR have been reported to potentiate Ca(2+) activation without independently activating the wild type receptor. Because agonists activate rhodopsin-like family-1 GPCRs by binding within the 7TMD, we examined the ability of Calindol, a novel chemically distinct calcimimetic, to activate a Ca(2+) receptor construct (T903-Rhoc) in which the ECD and carboxyl-terminal tail have been deleted to produce a rhodopsin-like 7TMD. Here we report that although Calindol has little or no agonist activity in the absence of extracellular Ca(2+) for the ECD-containing wild type or carboxyl-terminal deleted receptors, it acts as a strong agonist of the T903-Rhoc. In addition, Ca(2+) alone displays little or no agonist activity for the hCaR 7TMD, but potentiates the activation by Calindol. We confirm that activation of Ca(2+) T903-Rhoc by Calindol truly the is independent using in vitro reconstitution with purified G(q). These findings demonstrate distinct allosteric linkages between Ca(2+) site(s) in the ECD and 7TMD and the 7TMD site(s) for calcimimetics.
JF  - The Journal of biological chemistry
AU  - Ray, Kausik
AU  - Tisdale, Justin
AU  - Dodd, Robert H
AU  - Dauban, Philippe
AU  - Ruat, Martial
AU  - Northup, John K
AD  - Laboratory of Cellular Biology, NIDCD, National Institutes of Health, Bethesda, Maryland 20892, USA. rayk@nidcd.nih.gov
Y1  - 2005/11/04/
PY  - 2005
DA  - 2005 Nov 04
SP  - 37013
EP  - 37020
VL  - 280
IS  - 44
SN  - 0021-9258, 0021-9258
KW  - (R)-2-(1-(1-naphthyl)ethyl-aminom-ethyl)indole
KW  - 0
KW  - Aniline Compounds
KW  - Indoles
KW  - Ligands
KW  - Membrane Proteins
KW  - N-(2-chlorophenylpropyl)-1-(3-methoxyphenyl)ethylamine
KW  - Naphthalenes
KW  - Phenethylamines
KW  - Propylamines
KW  - RHOC protein, human
KW  - Receptors, Calcium-Sensing
KW  - Rhodopsin
KW  - 9009-81-8
KW  - rho GTP-Binding Proteins
KW  - EC 3.6.5.2
KW  - Calcium
KW  - SY7Q814VUP
KW  - Index Medicus
KW  - Kidney -- metabolism
KW  - Aniline Compounds -- pharmacology
KW  - Membrane Proteins -- chemistry
KW  - Humans
KW  - Membrane Proteins -- metabolism
KW  - Calcium -- pharmacology
KW  - Mutagenesis, Site-Directed
KW  - Calcium -- agonists
KW  - Cells, Cultured
KW  - Protein Structure, Tertiary
KW  - rho GTP-Binding Proteins -- metabolism
KW  - Sequence Deletion
KW  - Naphthalenes -- pharmacology
KW  - Receptors, Calcium-Sensing -- chemistry
KW  - Receptors, Calcium-Sensing -- genetics
KW  - Receptors, Calcium-Sensing -- metabolism
KW  - Indoles -- pharmacology
KW  - Allosteric Regulation
KW  - Rhodopsin -- chemistry
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-28
N1  - Date created - 2005-10-31
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Binding of Escherichia coli Hemolysin and Activation of the Target Cells Is Not Receptor-dependent
AN  - 17660554; 6503661
AB  - Production of a single cysteine substitution mutant, S177C, allowed Escherichia coli hemolysin (HlyA) to be radioactively labeled with tritiated N-ethylmaleimide without affecting biological activity. It thus became possible to study the binding characteristics of HlyA as well as of toxin mutants in which one or both acylation sites were deleted. All toxins bound to erythrocytes and granulocytes in a nonsaturable manner. Only wild-type toxin and the lytic monoacylated mutant stimulated production of superoxide anions in granulocytes. An oxidative burst coincided with elevation of intracellular Ca super(2+), which was likely because of passive influx of Ca super(2+) through the toxin pores. Competition experiments showed that binding to the cells was receptor-independent, and preloading of cells with a nonlytic HlyA mutant did not abrogate the respiratory burst provoked by a subsequent application of wild-type HlyA. In contrast to a previous report, expression or activation of the beta sub(2) integrin lymphocyte function-associated antigen-1 did not affect binding of HlyA. We conclude that HlyA binds nonspecifically to target cells and a receptor is involved neither in causing hemolysis nor in triggering cellular reactions.
JF  - Journal of Biological Chemistry
AU  - Valeva, Angela
AU  - Walev, Ivan
AU  - Kemmer, Helene
AU  - Weis, Silvia
AU  - Siegel, Isabel
AU  - Boukhallouk, Fatima
AU  - Wassenaar, Trudy M
AU  - Chavakis, Triantafyllos
AU  - Bhakdi, Sucharit
AD  - Institute of Medical Microbiology and Hygiene, University of Mainz, D-55101 Mainz, Germany, Molecular Microbiology and Genomics Consultants 55576, Zotzenheim, Germany, and Experimental Immunology Branch, NCI, National Institutes of Health, Bethesda, Maryland 20892
Y1  - 2005/11/04/
PY  - 2005
DA  - 2005 Nov 04
SP  - 36657
EP  - 36663
PB  - American Society for Biochemistry and Molecular Biology, 9650 Rockville Pike Bethesda MD 20814-3996 USA, [mailto:asbmb@asbmb.faseb.org], [URL:http://www.jbc.org]
VL  - 280
IS  - 44
SN  - 0021-9258, 0021-9258
KW  - Genetics Abstracts; Microbiology Abstracts B: Bacteriology
KW  - G 07240:Immunogenetics
KW  - J 02727:Amino acids, peptides and proteins
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
ER  - 



TY  - JOUR
T1  - Quantitative Lingual, Pharyngeal and Laryngeal Ultrasonography in Swallowing Research: A Technical Review
AN  - 85624069; 200513279
AB  - Because of its distinct advantage in radiation-free soft tissue imaging, ultrasonography has been widely used to study lingual, pharyngeal, hyoid, laryngeal, & even esophageal action during swallowing in individuals of all ages. Qualitative ultrasonographic observations have made considerable contributions to our understanding of deglutition. Quantitative ultrasonographic swallowing research has also grown by leaps & bounds over the years with advances in imaging technologies & analytical methodologies. As a technical primer for new investigators, this paper reviews the modern methods for quantitative analysis in ultrasonographic swallowing research. The intended outcome is a basic understanding of the application of ultrasonography with various analysis options to the quantitative study of the deglutitive action of selected upper aerodigestive structures. Though proven useful for swallowing research, ultrasonography has inherent limitations & methodological issues. Future technological advancement & sophisticated image processing & analysis algorithms will resolve some of these issues. Figures, References. Adapted from the source document
JF  - Clinical Linguistics & Phonetics
AU  - Chi-Fishman, Gloria
AD  - National Instit Health, Bethesda, MD gcf@nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 589
EP  - 604
VL  - 19
IS  - 6-7
SN  - 0269-9206, 0269-9206
KW  - Articulatory Measurement Techniques (04730)
KW  - Oral Cavity (61200)
KW  - Vocal Tract (94900)
KW  - Phonation Structures (64550)
KW  - Research Design (72950)
KW  - article
KW  - 6210: hearing and speech physiology; hearing and speech physiology
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LA  - English
DB  - Linguistics and Language Behavior Abstracts (LLBA)
N1  - Date revised - 2012-03-01
N1  - Last updated - 2016-09-27
N1  - CODEN - CLLPEZ
N1  - SubjectsTermNotLitGenreText - Phonation Structures (64550); Oral Cavity (61200); Articulatory Measurement Techniques (04730); Research Design (72950); Vocal Tract (94900)
ER  - 



TY  - JOUR
T1  - Clinical prognostic factors in malignant parotid gland tumors.
AN  - 85391989; pmid-16274796
AB  - To analyze the factors in parotid malignant epithelial tumors influencing recurrences and disease-specific survival.We retrospectively reviewed the files of 150 patients treated at our institution, from 1974 to 1998. Twenty-four patients were not treated by surgery and were excluded from this study. The remaining 126 patients were treated with surgery and 74 patients had postoperative radiotherapy. Thirty-three patients were treated with parotidectomy plus neck dissection. Neck lymph node metastasis was found in 22 patients, 5 patients had occult neck metastasis, and 4 periparotid lymph nodes metastasis. The mean age was 49 years old. According to the UICC/1997 TNM Classification, 49 patients were stage I, 27 stage II, 22 stage III, and 28 stage IV. The influence of selected factors on the 10 year disease-specific survival was analyzed using the Kaplan-Meier actuarial method and the log-rank test.Forty patients had mucoepidermoid carcinoma, 18 patients adenocarcinoma NOS, 18 patients acinic cell carcinoma, 15 patients adenoid cystic carcinoma, 11 patients malignant mixed tumor, 11 patients salivary duct carcinoma, and 13 patients other pathology. Twenty-five patients had recurrences: 17 had local recurrences, 4 patients had neck recurrences, and 4 were loco-regional recurrences. Five factors influenced negatively the prognosis: 1) T stage (p.00001), 2) grade (p.00001), 3) + lymph nodes (p.0007), 4) facial nerve dysfunction (p.0001), and 5) age (p.004). Patients with high-grade tumors and high-stage tumors had the worst prognosis according to the multivariate analysis. The 10-year disease-specific survival was 97% for stage I, 81% for stage II, 56% for stage III, and 20% for stage IV.The grade of the tumor and stage were the most important prognostic factor.C.
JF  - Otolaryngology--head and neck surgery : official journal of American Academy of Otolaryngology-Head and Neck Surgery
AU  - Lima, Roberto A
AU  - Tavares, Marcos R
AU  - Dias, Fernando L
AU  - Kligerman, Jacob
AU  - Nascimento, Marilene F
AU  - Barbosa, Mauro M
AU  - Cernea, Claudio R
AU  - Soares, Jose R
AU  - Santos, Izabella C
AU  - Salviano, Scheylla
AD  - Department of Head and Neck Surgery, Brazilian National Cancer Institute/INCA, Rio de Janeiro, Brazil. rlimamd@globo.com
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 702
EP  - 708
VL  - 133
IS  - 5
SN  - 0194-5998, 0194-5998
KW  - Index Medicus
KW  - National Library of Medicine
KW  - *Adenocarcinoma: mortality
KW  - Adenocarcinoma: pathology
KW  - *Adenocarcinoma: therapy
KW  - Adolescent
KW  - Adult
KW  - Age Factors
KW  - Aged
KW  - Aged, 80 and over
KW  - Child
KW  - Child, Preschool
KW  - Cohort Studies
KW  - Combined Modality Therapy
KW  - Female
KW  - Follow-Up Studies
KW  - Humans
KW  - Male
KW  - Middle Aged
KW  - Multivariate Analysis
KW  - Neck Dissection: methods
KW  - *Neoplasm Invasiveness: pathology
KW  - Neoplasm Staging
KW  - Parotid Gland: radiation effects
KW  - Parotid Gland: surgery
KW  - *Parotid Neoplasms: mortality
KW  - Parotid Neoplasms: pathology
KW  - *Parotid Neoplasms: therapy
KW  - Probability
KW  - Proportional Hazards Models
KW  - Radiotherapy, Adjuvant
KW  - Retrospective Studies
KW  - Risk Assessment
KW  - Sex Factors
KW  - Survival Analysis
KW  - Time Factors
KW  - Treatment Outcome
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LA  - English (eng)
DB  - ComDisDome
N1  - Date revised - 2011-12-15
N1  - Last updated - 2012-07-13
ER  - 



TY  - JOUR
T1  - Inhibition of core histones acetylation by carcinogenic nickel(II)
AN  - 839694232; 13863789
AB  - Nickel, a well-established human carcinogen, was shown to decrease acetylation of histones H4 and H3 in cultured cells. Such a decrease is expected to suppress gene expression. However, nickel is known to not only suppress but also enhance the expression of many genes. So, perhaps, nickel can alter histone acetylation in a more complex way? In a first step of testing this presumption, we examined acetylation status of histones H2A, H2B, H3 and H4, in human (HAE) and rat (NRK) cells exposed to nickel(II) under various conditions. In both cell lines, acetylation of all four histones was down-regulated by nickel(II) in a concentration- and time-dependent manner. Acetylation of histone H2B was suppressed to greater extent than that of the others, with histone H3 being relatively least affected. The analysis of acetylation status of each of the four lysine sites at the N-terminal tail of histone H2B revealed decreases consistent with those observed in the total acetylation patterns, with the K12 and K20 residues being markedly more affected than K5 and K15 residues. Thus, the decrease in acetylation was to some degree site specific. In NRK cells, the observed uniform down-regulation of histone acetylation was consistent with a marked suppression of global gene transcription measured as [ super(3)H]-uridine incorporation into mRNA. However, in HAE cells, global RNA expression was transiently increased (in 24 h) before dropping below control after longer exposure (3 days). In conclusion, the effects of Ni(II) on histone acetylation are inhibitory, with their extent depending on the dose and exposure time. This uniform inhibition, however, is not consistently reflected in global RNA expression that in HAE cells may include both increase and decrease of the expression, clearly indicating the involvement of factors other than histone acetylation. The observed effects may contribute to neoplastic transformation of Ni(II)-exposed cells.
JF  - Molecular and Cellular Biochemistry
AU  - Golebiowski, Filip
AU  - Kasprzak, Kazimierz S
AD  - Laboratory of Comparative Carcinogenesis, NCI at Frederick, Frederick, MD, 21702-1201, USA, filip@ncifcrf.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 133
EP  - 139
PB  - Springer-Verlag, Tiergartenstrasse 17 Heidelberg 69121 Germany
VL  - 279
IS  - 1-2
SN  - 0300-8177, 0300-8177
KW  - Biochemistry Abstracts 2: Nucleic Acids; Toxicology Abstracts
KW  - Gene expression
KW  - Transformation
KW  - Acetylation
KW  - Histone H4
KW  - Nickel
KW  - Lysine
KW  - Transcription
KW  - Histone H2B
KW  - Carcinogens
KW  - Histone H3
KW  - Histone H2A
KW  - N 14820:DNA Metabolism & Structure
KW  - X 24360:Metals
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2011-01-01
N1  - Last updated - 2012-03-29
N1  - SubjectsTermNotLitGenreText - Transformation; Gene expression; Acetylation; Histone H4; Nickel; Transcription; Lysine; Histone H2B; Carcinogens; Histone H3; Histone H2A
DO  - http://dx.doi.org/10.1007/s11010-005-8285-1
ER  - 



TY  - JOUR
T1  - The role of copper in development of drug resistance in murine carcinoma.
AN  - 70163261; 16787340
AB  - Multidrug resistance (MDR) is a major obstacle to successful application of cancer chemotherapy and also a basic problem in cancer biology. Studies on the molecular basis of MDR have revealed that a number of proteins over express in multidrug resistant cells viz., multidrug resistant MDR1 gene product P-glycoprotein, the multidrug resistance-associated protein (MRP) and enzymes associated with the glutathione (GSH) metabolism. Decreased expression or altered activity of topoisomerase II has also been implicated in MDR. In the present investigation a number of changes in phase II detoxification parameters have been noticed in drug resistant cells but the novel aspect of the present report is the observation that the metal copper is involved in drug resistance. Although copper plays important roles in many human and other biological systems and even in the treatment of cancer but the relation of Cu and drug resistance has not so far been studied in detailed. The present report describes the novel findings that the level of copper increases with the development of drug resistance in Ehrlich ascites carcinoma and in Lewis lung carcinoma cells and also in serum of mice bearing drug resistant cancer cells compared to mice bearing drug sensitive cells; the work indicates the important aspect of treating drug resistant cancer patients by lowering Cu level in the cancerous cells and serum prior to treatment.
JF  - Medicinal chemistry (Shariqah (United Arab Emirates))
AU  - Majumder, S
AU  - Dutta, P
AU  - Choudhuri, S K
AD  - Department of Environmental Carcinogenesis and Toxicology (ECT), Chittaranjan National Cancer Institute, CNCI, Calcutta-700026, India.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 563
EP  - 573
VL  - 1
IS  - 6
SN  - 1573-4064, 1573-4064
KW  - Copper
KW  - 789U1901C5
KW  - Catalase
KW  - EC 1.11.1.6
KW  - Superoxide Dismutase
KW  - EC 1.15.1.1
KW  - Index Medicus
KW  - Superoxide Dismutase -- analysis
KW  - Animals
KW  - Disease Progression
KW  - Kidney -- enzymology
KW  - Superoxide Dismutase -- metabolism
KW  - Liver -- metabolism
KW  - Cell Line, Tumor
KW  - Mice
KW  - Kidney -- chemistry
KW  - Liver -- chemistry
KW  - Catalase -- analysis
KW  - Structure-Activity Relationship
KW  - Catalase -- metabolism
KW  - Male
KW  - Carcinoma, Lewis Lung -- drug therapy
KW  - Carcinoma, Lewis Lung -- blood
KW  - Carcinoma, Ehrlich Tumor -- drug therapy
KW  - Carcinoma, Lewis Lung -- chemistry
KW  - Carcinoma, Ehrlich Tumor -- chemistry
KW  - Drug Resistance, Neoplasm
KW  - Carcinoma, Ehrlich Tumor -- blood
KW  - Copper -- blood
KW  - Copper -- chemistry
KW  - Drug Resistance, Multiple
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-07-24
N1  - Date created - 2006-06-21
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The epidemiology of social anxiety disorder in the United States: results from the National Epidemiologic Survey on Alcohol and Related Conditions.
AN  - 69072266; 16420070
AB  - To present nationally representative data on 12-month and lifetime prevalence, correlates and comorbidity of social anxiety disorder (SAD) among adults in the United States as determined by the 2001-2002 National Epidemiologic Survey on Alcohol and Related Conditions.
          Face-to-face survey. The United States.
          Adults (aged 18 and over) residing in households and group quarters (N = 43,093). Prevalence and associations of SAD with sociodemographic and psychiatric correlates and Axis I and II disorders.
          The prevalence of 12-month and lifetime DSM-IV SAD was 2.8% (95% CI = 2.5 to 3.1) and 5.0% (95% CI = 4.6 to 5.4), respectively. Being Native American, being young, or having low income increased risk, while being male, being of Asian, Hispanic, or black race/ethnicity, or living in urban or more populated regions reduced risk. Mean age at onset of SAD was 15.1 years, with a mean duration of 16.3 years. Over 80% of individuals with SAD received no treatment, and the mean age at first treatment was 27.2 years. Current and lifetime SAD were significantly related to other specific psychiatric disorders, most notably generalized anxiety, bipolar I, and avoidant and dependent personality disorders. The mean number of feared social situations among individuals with SAD was 7.0, with the majority reporting anxiety in performance situations. Social anxiety disorder was associated with substantial unremitting course and extremely early age at onset. Social anxiety disorder often goes untreated, underscoring the need for health care initiatives geared toward increasing recognition and treatment. Comprehensive evaluation of patients with SAD should include a systematic assessment of comorbid disorders, and novel approaches to the treatment of comorbid SAD are needed.
JF  - The Journal of clinical psychiatry
AU  - Grant, Bridget F
AU  - Hasin, Deborah S
AU  - Blanco, Carlos
AU  - Stinson, Frederick S
AU  - Chou, S Patricia
AU  - Goldstein, Rise B
AU  - Dawson, Deborah A
AU  - Smith, Sharon
AU  - Saha, Tulshi D
AU  - Huang, Boji
AD  - Laboratory of Epidemiology and Biometry, Division of Intramural Clinical and Biological Research, National Institute on Alcohol Abuse and Alcoholism (NIAAA), NIH/DHHS, 5635 Fishers Lane, Bethesda, MD 20892-9304, USA. bgrant@willco.niaaa.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1351
EP  - 1361
VL  - 66
IS  - 11
SN  - 0160-6689, 0160-6689
KW  - Index Medicus
KW  - Mental Disorders -- therapy
KW  - Age of Onset
KW  - Humans
KW  - Mental Disorders -- epidemiology
KW  - Aged
KW  - Mental Disorders -- etiology
KW  - Comorbidity
KW  - Ethnic Groups -- statistics & numerical data
KW  - Mental Disorders -- diagnosis
KW  - Psychiatric Status Rating Scales
KW  - Adult
KW  - Middle Aged
KW  - Adolescent
KW  - United States -- epidemiology
KW  - Female
KW  - Male
KW  - Prevalence
KW  - Alcohol-Related Disorders -- epidemiology
KW  - Phobic Disorders -- therapy
KW  - Health Surveys
KW  - Phobic Disorders -- epidemiology
KW  - Phobic Disorders -- diagnosis
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-30
N1  - Date created - 2006-01-19
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment In:
Evid Based Ment Health. 2006 Aug;9(3):88 [16868207]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Immunotherapeutic approaches in ocular inflammatory diseases.
AN  - 69068467; 16407781
AB  - This comprehensive review discusses immunotherapeutic approaches to ocular inflammatory diseases, updates information provided in the literature, and presents clinical experiences with an emphasis on autoimmune uveitis at the National Eye Institute, United States. Current medical and surgical therapeutic approaches, including medications such as corticosteroids, anti-metabolites, alkylating agents, calcineurin and purine synthesis inhibitors, biologics as well as some anti-infectious agents, are reviewed along with new modalities and experimental approaches. Most immunosuppressive therapies have significant adverse effects. Physicians must be familiar with the pharmacology of the available drugs and aware of the philosophies behind the treatment.
JF  - Archivum immunologiae et therapiae experimentalis
AU  - Kurup, Shree K
AU  - Chan, Chi-Chao
AD  - National Eye Institute, National Institutes of Health, 10 Center Drive, Bethesda, MD 20892-1857, USA.
PY  - 2005
SP  - 484
EP  - 496
VL  - 53
IS  - 6
SN  - 0004-069X, 0004-069X
KW  - Anti-Inflammatory Agents
KW  - 0
KW  - Antimetabolites
KW  - Calcineurin Inhibitors
KW  - Glucocorticoids
KW  - Purines
KW  - Index Medicus
KW  - Purines -- metabolism
KW  - Humans
KW  - Antimetabolites -- therapeutic use
KW  - Glucocorticoids -- therapeutic use
KW  - Plasmapheresis
KW  - Stem Cell Transplantation
KW  - Uveitis -- therapy
KW  - Anti-Inflammatory Agents -- therapeutic use
KW  - Uveitis -- diagnosis
KW  - Uveitis -- physiopathology
KW  - Uveitis -- immunology
KW  - Immunotherapy -- methods
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-02
N1  - Date created - 2006-01-12
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Development of novel anticancer agents in older patients: pharmacokinetic, pharmacodynamic, and other considerations.
AN  - 69065744; 16393482
AB  - The development of novel anticancer agents in older patients presents both challenges and unique opportunities. Intrapatient variability due to comorbid conditions and the use of multiple concomitant medications may overshadow other age-related differences in pharmacokinetics. The increasing interest in oral agents may be especially problematic in older patients who have difficulty with adherence, particularly if the oral agents are given in combination or according to complex schedules. Polypharmacy, chronic comorbid conditions, and impaired organ reserve in the elderly can lead to pharmacodynamic differences such as increased toxicity and, possibly, reduced efficacy. Hampered immune responsiveness is an important area warranting further research. The development of novel agents to treat older patients with cancer cannot be successfully accomplished without increasing the proportion of elderly patients entered into clinical trials. Furthermore, data obtained from studies in older patients may provide valuable information applicable to the development of novel agents in younger patients and to a better understanding of cancer biology and treatment in general.
JF  - Cancer journal (Sudbury, Mass.)
AU  - Murgo, Anthony J
AU  - Espinoza-Delgado, Igor
AD  - National Cancer Institute, National Institutes of Health, Rockville, Maryland 20852, USA. murgoa@mail.nih.gov
PY  - 2005
SP  - 481
EP  - 487
VL  - 11
IS  - 6
SN  - 1528-9117, 1528-9117
KW  - Antineoplastic Agents
KW  - 0
KW  - Drugs, Investigational
KW  - Index Medicus
KW  - Aged -- physiology
KW  - Immune System -- drug effects
KW  - Humans
KW  - Clinical Trials as Topic
KW  - Comorbidity
KW  - Drugs, Investigational -- pharmacokinetics
KW  - Neoplasms -- drug therapy
KW  - Drugs, Investigational -- pharmacology
KW  - Drug Evaluation
KW  - Antineoplastic Agents -- pharmacokinetics
KW  - Neoplasms -- epidemiology
KW  - Drugs, Investigational -- adverse effects
KW  - Antineoplastic Agents -- pharmacology
KW  - Neoplasms -- immunology
KW  - Antineoplastic Agents -- adverse effects
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cancer+journal+%28Sudbury%2C+Mass.%29&rft.atitle=Development+of+novel+anticancer+agents+in+older+patients%3A+pharmacokinetic%2C+pharmacodynamic%2C+and+other+considerations.&rft.au=Murgo%2C+Anthony+J%3BEspinoza-Delgado%2C+Igor&rft.aulast=Murgo&rft.aufirst=Anthony&rft.date=2005-11-01&rft.volume=11&rft.issue=6&rft.spage=481&rft.isbn=&rft.btitle=&rft.title=Cancer+journal+%28Sudbury%2C+Mass.%29&rft.issn=15289117&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-30
N1  - Date created - 2006-01-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Stability regulation of mRNA and the control of gene expression.
AN  - 69062758; 16394137
AB  - Microarray technology has become highly valuable for identifying complex global changes in gene expression patterns. Standard techniques measure changes in total cellular poly(A) mRNA levels. The assumption that changes in gene expression as measured by these techniques are directly and well correlated with changes in rates of new gene synthesis form the basis of attempts to connect coordinated changes in gene expression with shared transcription regulatory elements. Yet systematic attempts at this approach remain difficult to demonstrate convincingly. One reason for this difficulty may result from the intricate convergence of both transcriptional and mRNA turnover events which, together, directly influence steady-state mRNA levels. Recent technical advances have led to the successful scale-up and application of nuclear run-on procedures directly to microarrays. This development has allowed a gene-by-gene comparison between new gene synthesis in the nucleus and measured changes in total cellular polyA mRNA. Results from these studies have begun to challenge the strict interpretation of changes in gene expression measured by conventional microarrays as being closely correlated with changes in mRNA transcription rate, but rather they tend to support the significant expansion of the role played by changes in mRNA stability regulation to standard analyses of gene expression. Gene expression profiles obtained from both polyA mRNA (whole-cell) and nuclear run-on (newly transcribed) RNA across a time course of one hour following the activation of human Jurkat T cells with PMA plus ionomycin revealed that regulation of mRNA stability may account for as much as 50% of all measurements of changes in total cellular polyA mRNA in this system. Stability regulation was inferred by the absence of corresponding regulation of nuclear gene transcription activity for groups of genes strongly regulated at the whole cell level and which were also resistant to inhibition by Actinomycin D pre-treatment. Consistent patterns across the time course were observed for both transcribed and stability-regulated genes. It is proposed that the regulation of mRNA stability in response to external stimuli contributes significantly to observed changes in gene expression as measured by high throughput systems.
JF  - Annals of the New York Academy of Sciences
AU  - Cheadle, Chris
AU  - Fan, Jinshui
AU  - Cho-Chung, Yoon S
AU  - Werner, Thomas
AU  - Ray, Jill
AU  - Do, Lana
AU  - Gorospe, Myriam
AU  - Becker, Kevin G
AD  - Cellular Biochemistry Section, Basic Research Laboratory, Center for Cancer Research, National Cancer Institute, NIH, Bethesda, Maryland 20892, USA. cheadlec@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 196
EP  - 204
VL  - 1058
SN  - 0077-8923, 0077-8923
KW  - Phorbol Esters
KW  - 0
KW  - RNA, Messenger
KW  - Dactinomycin
KW  - 1CC1JFE158
KW  - phorbol-12-myristate
KW  - 20839-06-9
KW  - Ionomycin
KW  - 56092-81-0
KW  - RNA
KW  - 63231-63-0
KW  - Index Medicus
KW  - Phorbol Esters -- chemistry
KW  - Dactinomycin -- pharmacology
KW  - Oligonucleotide Array Sequence Analysis
KW  - RNA -- metabolism
KW  - Cell Nucleus -- metabolism
KW  - Humans
KW  - Jurkat Cells
KW  - Gene Expression
KW  - Transcription, Genetic
KW  - Ionomycin -- pharmacology
KW  - Cell Line, Tumor
KW  - Time Factors
KW  - RNA, Messenger -- metabolism
KW  - Gene Expression Regulation
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Annals+of+the+New+York+Academy+of+Sciences&rft.atitle=Stability+regulation+of+mRNA+and+the+control+of+gene+expression.&rft.au=Cheadle%2C+Chris%3BFan%2C+Jinshui%3BCho-Chung%2C+Yoon+S%3BWerner%2C+Thomas%3BRay%2C+Jill%3BDo%2C+Lana%3BGorospe%2C+Myriam%3BBecker%2C+Kevin+G&rft.aulast=Cheadle&rft.aufirst=Chris&rft.date=2005-11-01&rft.volume=1058&rft.issue=&rft.spage=196&rft.isbn=&rft.btitle=&rft.title=Annals+of+the+New+York+Academy+of+Sciences&rft.issn=00778923&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-26
N1  - Date created - 2006-01-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Methamphetamine-induced neuronal apoptosis involves the activation of multiple death pathways. Review.
AN  - 68917057; 16371314
AB  - The abuse of the illicit drug methamphetamine (METH) is a major concern because it can cause terminal degeneration and neuronal cell death in the brain. METH-induced cell death occurs via processes that resemble apoptosis. In the present review, we discuss the role of various apoptotic events in the causation of METH-induced neuronal apoptosis in vitro and in vivo. Studies using comprehensive approaches to gene expression profiling have allowed for the identification of several genes that are up-regulated or down-regulated after an apoptosis-inducing dose of the drug. Further experiments have also documented the fact that the drug can cause demise of striatal enkephalinergic neurons by cross-talks between mitochondria-, endoplasmic reticulum- and receptor-mediated apoptotic events. These neuropathological observations have also been reported in models of drug-induced neuroplastic alterations used to mimic drug addiction (Nestler, 2001).
JF  - Neurotoxicity research
AU  - Cadet, Jean Lud
AU  - Jayanthi, Subramaniam
AU  - Deng, Xiaolin
AD  - Molecular Neuropsychiatry Branch, NIH/NIDA, Intramural Research Program, Department of Health and Human Services, 5500 Nathan Shock Drive, Baltimore, MD 21224, USA. JCADET@intra.nida.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 199
EP  - 206
VL  - 8
IS  - 3-4
SN  - 1029-8428, 1029-8428
KW  - Central Nervous System Stimulants
KW  - 0
KW  - Transcription Factors
KW  - Methamphetamine
KW  - 44RAL3456C
KW  - Index Medicus
KW  - Models, Animal
KW  - Animals
KW  - Transcription Factors -- metabolism
KW  - Humans
KW  - Mitochondria -- drug effects
KW  - Enzyme Activation -- drug effects
KW  - Models, Biological
KW  - Endoplasmic Reticulum -- drug effects
KW  - Central Nervous System Stimulants -- toxicity
KW  - Neurons -- drug effects
KW  - Signal Transduction -- drug effects
KW  - Neurons -- cytology
KW  - Apoptosis -- drug effects
KW  - Methamphetamine -- toxicity
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68917057?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Neurotoxicity+research&rft.atitle=Methamphetamine-induced+neuronal+apoptosis+involves+the+activation+of+multiple+death+pathways.+Review.&rft.au=Cadet%2C+Jean+Lud%3BJayanthi%2C+Subramaniam%3BDeng%2C+Xiaolin&rft.aulast=Cadet&rft.aufirst=Jean&rft.date=2005-11-01&rft.volume=8&rft.issue=3-4&rft.spage=199&rft.isbn=&rft.btitle=&rft.title=Neurotoxicity+research&rft.issn=10298428&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-04-27
N1  - Date created - 2005-12-22
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The husbandry and care of dendrobatid frogs.
AN  - 68911237; 16370573
AB  - Dendrobatid frogs are studied primarily for the bioactive alkaloids found in their skin. Also known as poison-dart frogs, these animals accumulate toxic alkaloids from dietary sources. The function and uses of the many alkaloids, the alkaloid accumulation system, and the basic biology and physiology of the frogs themselves are of research interest. Here we overview the taxonomy of these frogs and some of the unique aspects of their natural biology and reproduction. We also describe the components of a successful laboratory housing system, including temperature, lighting, humidity, ventilation, nutrition, health considerations, and handling. A brief summary of dendrobatid research highlights is provided.
JF  - Contemporary topics in laboratory animal science
AU  - St Claire, Mark B
AU  - Kennett, Mary J
AU  - Thomas, Marvin L
AU  - Daly, John W
AD  - Laboratory Animal Science Section and Laboratory of Bioorganic Chemistry, NIDDK, DHHS, NIH, Bethesda, Maryland, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 8
EP  - 14
VL  - 44
IS  - 6
SN  - 1060-0558, 1060-0558
KW  - Index Medicus
KW  - Animals
KW  - Male
KW  - Larva -- growth & development
KW  - Female
KW  - Environment
KW  - Animal Nutritional Physiological Phenomena
KW  - Reproduction -- physiology
KW  - Animal Husbandry -- methods
KW  - Housing, Animal
KW  - Anura -- genetics
KW  - Anura -- physiology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-22
N1  - Date created - 2005-12-22
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Animal models of melanoma.
AN  - 68907429; 16358815
JF  - The journal of investigative dermatology. Symposium proceedings
AU  - Ha, Linan
AU  - Noonan, Frances P
AU  - De Fabo, Edward C
AU  - Merlino, Glenn
AD  - Laboratory of Cell Regulation and Carcinogenesis, National Cancer Institute, Bethesda, Maryland 20892, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 86
EP  - 88
VL  - 10
IS  - 2
SN  - 1087-0024, 1087-0024
KW  - Hepatocyte Growth Factor
KW  - 67256-21-7
KW  - Index Medicus
KW  - Animals
KW  - Humans
KW  - Mice
KW  - Mice, Transgenic
KW  - Hepatocyte Growth Factor -- physiology
KW  - Ultraviolet Rays
KW  - Melanoma -- pathology
KW  - Skin Neoplasms -- etiology
KW  - Melanoma -- etiology
KW  - Hepatocyte Growth Factor -- genetics
KW  - Disease Models, Animal
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68907429?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-28
N1  - Date created - 2005-12-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - CLIC4, an intracellular chloride channel protein, is a novel molecular target for cancer therapy.
AN  - 68905779; 16358817
AB  - Chloride intracellular channel (CLIC)4 is a p53- and tumor necrosis factor alpha (TNFalpha)-regulated chloride channel protein that is localized to the mitochondria and cytoplasm of mouse and human keratinocytes. CLIC4 protein increases in differentiating keratinocytes and in keratinocytes exposed to DNA-damaging agents and metabolic inhibitors. Increasing CLIC4 levels by transduction of recombinant CLIC4 causes apoptosis. CLIC4 translocates to the nucleus under a variety of conditions of cell stress, and nuclear CLIC4 is associated with cell cycle arrest and accelerated apoptosis. Reduction of CLIC4 and several other CLIC family members by expressing a doxycycline-regulated CLIC4 antisense also causes apoptosis in squamous cancer cell lines. Expressing antisense CLIC4 in tumors derived from transplanting these cells into nude mice inhibits tumor growth, increases tumor apoptosis, and reduces tumor cell proliferation. Co-administration of TNFalpha intraperitoneally enhances the tumor-inhibitory influence of CLIC4 antisense expression. Together, these results suggest that CLIC4 is important for keratinocyte viability and may be a novel target for anti-cancer therapy.
JF  - The journal of investigative dermatology. Symposium proceedings
AU  - Suh, Kwang S
AU  - Mutoh, Michihiro
AU  - Gerdes, Michael
AU  - Yuspa, Stuart H
AD  - Laboratory of Cellular Carcinogenesis and Tumor Promotion, Center for Cancer Research, National Cancer Institute, Bethesda, Maryland 20892-4255, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 105
EP  - 109
VL  - 10
IS  - 2
SN  - 1087-0024, 1087-0024
KW  - CLIC4 protein, human
KW  - 0
KW  - Chloride Channels
KW  - Oligonucleotides, Antisense
KW  - Index Medicus
KW  - Animals
KW  - Humans
KW  - Keratinocytes -- cytology
KW  - Cell Differentiation
KW  - Oligonucleotides, Antisense -- pharmacology
KW  - Mice
KW  - Chloride Channels -- physiology
KW  - Neoplasms -- therapy
KW  - Chloride Channels -- antagonists & inhibitors
KW  - Chloride Channels -- genetics
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=The+journal+of+investigative+dermatology.+Symposium+proceedings&rft.atitle=CLIC4%2C+an+intracellular+chloride+channel+protein%2C+is+a+novel+molecular+target+for+cancer+therapy.&rft.au=Suh%2C+Kwang+S%3BMutoh%2C+Michihiro%3BGerdes%2C+Michael%3BYuspa%2C+Stuart+H&rft.aulast=Suh&rft.aufirst=Kwang&rft.date=2005-11-01&rft.volume=10&rft.issue=2&rft.spage=105&rft.isbn=&rft.btitle=&rft.title=The+journal+of+investigative+dermatology.+Symposium+proceedings&rft.issn=10870024&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-28
N1  - Date created - 2005-12-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Paclitaxel pharmacokinetics and response to chemotherapy in patients with advanced cancer treated with a weekly regimen.
AN  - 68873709; 16334120
AB  - Paclitaxel pharmacokinetics were shown to be related to toxicity and survival.
          We evaluated the effects of time above paclitaxel concentrations of 0.05 micromol/l (T(>0.05) and systemic exposures (AUC) to total and unbound paclitaxel (tPAC, uPAC) on response in patients with advanced cancer treated with weekly 1-h or 3-h infusions.
          After 6 weeks of therapy (WOT), 13 out of 21 assessable patients showed either partial response (PR) or stable disease (SD), while 8 had progressive disease (PD). As compared to patients with PD, those with PR or SD showed similar AUCs to uPAC and tPAC but higher (p 0.05). Patients with T(>0.05) > or = 20.7 hours had lower probability (p < 0.05) to progress within 12 WOT.
          Taking the heterogeneity of the studied tumor types into account, we found T(>0.05) to be associated with response to treatment. This emphasizes the value of threshold models for the investigation of paclitaxel pharmacodynamics.
JF  - Anticancer research
AU  - Mielke, Stephan
AU  - Sparreboom, Alex
AU  - Behringer, Dirk
AU  - Mross, Klaus
AD  - Department of Hematology and Oncology, University of Freiburg Medical Center, Freiburg i. Br., Germany. mielkes@nhlbi.nih.gov
PY  - 2005
SP  - 4423
EP  - 4427
VL  - 25
IS  - 6C
SN  - 0250-7005, 0250-7005
KW  - Antineoplastic Agents, Phytogenic
KW  - 0
KW  - Paclitaxel
KW  - P88XT4IS4D
KW  - Index Medicus
KW  - Drug Administration Schedule
KW  - Prospective Studies
KW  - Infusions, Intravenous
KW  - Humans
KW  - Adult
KW  - Aged
KW  - Middle Aged
KW  - Peripheral Nervous System Diseases -- chemically induced
KW  - Male
KW  - Female
KW  - Paclitaxel -- administration & dosage
KW  - Antineoplastic Agents, Phytogenic -- pharmacokinetics
KW  - Neoplasms -- drug therapy
KW  - Paclitaxel -- adverse effects
KW  - Antineoplastic Agents, Phytogenic -- adverse effects
KW  - Paclitaxel -- pharmacokinetics
KW  - Antineoplastic Agents, Phytogenic -- administration & dosage
KW  - Neoplasms -- metabolism
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68873709?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-25
N1  - Date created - 2005-12-07
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Loading and unloading: orchestrating centrosome duplication and spindle assembly by Ran/Crm1.
AN  - 68830100; 16294017
AB  - The cell cycle is an intricate process of DNA replication and cell division that concludes with the formation of two genetically equivalent daughter cells. In this progression, the centrosome is duplicated once and only once during the G1/S transition to produce the bipolar spindle and ensure proper chromosome segregation. The presence of multiple centrosomes in cancer cells suggests that this process is mis-regulated during carcinogenesis. This suggests that certain factors exist that license the progression of centrosome duplication and serve to inhibit further duplications during a single cell cycle. Recent studies suggest that the Ran/Crm1 complex not only regulates nucleocytoplasmic transport but is also independently involved in mitotic spindle assembly. Factors that are capable of interacting with Ran/Crm1 through their nuclear export sequences, such as cyclins/cdks, p53 and Brca1/2, may potentially function as centrosome checkpoints akin to the G1/S and G2/M checkpoints of the cell cycle. Our recent findings indicate that nucleophosmin, a protein whose trafficking is mediated by the Ran/Crm1 network, is one of such checkpoint factors for maintaining proper centrosome duplication. We propose that Ran/Crm1 may act as a 'loading dock' to coordinate various checkpoint factors in regulating the fidelity of centrosome duplication during cell cycle progression, and the disruption of these processes may lead to genomic instability and an acceleration of oncogenesis.
JF  - Cell cycle (Georgetown, Tex.)
AU  - Budhu, Anuradha S
AU  - Wang, Xin W
AD  - Laboratory of Human Carcinogenesis, Center for Cancer Research, NCI, NIH, Bethesda, Maryland 20892-4255, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1510
EP  - 1514
VL  - 4
IS  - 11
KW  - Cell Cycle Proteins
KW  - 0
KW  - Karyopherins
KW  - Receptors, Cytoplasmic and Nuclear
KW  - exportin 1 protein
KW  - ran GTP-Binding Protein
KW  - EC 3.6.5.2
KW  - Index Medicus
KW  - Animals
KW  - Humans
KW  - Protein Transport -- physiology
KW  - Cell Cycle Proteins -- physiology
KW  - Receptors, Cytoplasmic and Nuclear -- physiology
KW  - Karyopherins -- metabolism
KW  - Karyopherins -- chemistry
KW  - ran GTP-Binding Protein -- chemistry
KW  - ran GTP-Binding Protein -- physiology
KW  - Cell Cycle Proteins -- metabolism
KW  - ran GTP-Binding Protein -- metabolism
KW  - Cell Cycle Proteins -- chemistry
KW  - Karyopherins -- physiology
KW  - Receptors, Cytoplasmic and Nuclear -- chemistry
KW  - Receptors, Cytoplasmic and Nuclear -- metabolism
KW  - Centrosome -- physiology
KW  - Spindle Apparatus -- metabolism
KW  - Centrosome -- chemistry
KW  - Spindle Apparatus -- physiology
KW  - Spindle Apparatus -- chemistry
KW  - Centrosome -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2007-02-12
N1  - Date created - 2005-11-24
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
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J Cell Sci. 2003 Aug 15;116(Pt 16):3399-411 [12840069]
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Mol Cell. 1999 Mar;3(3):389-95 [10198641]
Oncogene. 1999 May 6;18(18):2892-900 [10362260]
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Cell. 1999 May 28;97(5):575-86 [10367887]
Nat Genet. 1999 Oct;23(2):176-84 [10508513]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Modulating molecular chaperone Hsp90 functions through reversible acetylation.
AN  - 68817977; 16199163
AB  - The molecular chaperone protein Hsp90 is a key regulator of approximately 100 'client' proteins crucial for numerous cell signaling processes. Consequently, understanding the molecular underpinnings that regulate Hsp90 activity is an important biological endeavor. Exciting new results now suggest that, at least for nuclear receptor activity, Hsp90 function is directly regulated by histone deacetylase 6 (HDAC6). These observations have consequences for various biological processes and potentially important implications for the development of cancer therapeutics.
JF  - Trends in cell biology
AU  - Aoyagi, Sayura
AU  - Archer, Trevor K
AD  - Chromatin and Gene Expression Section, Laboratory of Molecular Carcinogenesis, National Institute of Environmental Health Sciences, National Institutes of Health, 111 Alexander Drive, P.O. Box 12233, Research Triangle Park, NC 27709, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 565
EP  - 567
VL  - 15
IS  - 11
SN  - 0962-8924, 0962-8924
KW  - HSP90 Heat-Shock Proteins
KW  - 0
KW  - Receptors, Glucocorticoid
KW  - HDAC6 protein, human
KW  - EC 3.5.1.98
KW  - Hdac6 protein, mouse
KW  - Histone Deacetylases
KW  - Index Medicus
KW  - Animals
KW  - Acetylation
KW  - Humans
KW  - Protein Processing, Post-Translational
KW  - Mice
KW  - Receptors, Glucocorticoid -- metabolism
KW  - Models, Biological
KW  - Histone Deacetylases -- metabolism
KW  - HSP90 Heat-Shock Proteins -- metabolism
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68817977?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Trends+in+cell+biology&rft.atitle=Modulating+molecular+chaperone+Hsp90+functions+through+reversible+acetylation.&rft.au=Aoyagi%2C+Sayura%3BArcher%2C+Trevor+K&rft.aulast=Aoyagi&rft.aufirst=Sayura&rft.date=2005-11-01&rft.volume=15&rft.issue=11&rft.spage=565&rft.isbn=&rft.btitle=&rft.title=Trends+in+cell+biology&rft.issn=09628924&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-27
N1  - Date created - 2005-11-21
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Characteristics of metals in nano/ultrafine/fine/coarse particles collected beside a heavily trafficked road.
AN  - 68804532; 16294844
AB  - Fine particles emitted from vehicles have adverse health effects because of their sizes and chemical compositions. Therefore, this study attempted to characterize the metals in nano (0.010 < Dp < 0.056 microm), ultrafine (Dp < 0.1 microm), fine (Dp < 2.5 microm), and coarse (2.5 < Dp < 10 microm) particles collected near a busy road using a microorifice uniform deposition impactor (MOUDI) and a Nano-MOUDI. The nano particles were found to contain more of traffic-related metals (Pb, Cd, Cu, Zn, Ba, and Ni) than particles of other sizes, although crustal metals accounted for over 90% of all the particulate metals. Most crustal metals, Ba, Ni, Pb, and Zn in ultrafine particles displayed Aitken modes due to their local origins. The Ag, Cd, Cr, Ni, Pb, Sb, V, and Zn were 37, 50, 28, 30, 24, 64, 38, and 22% by mass, respectively, in < 0.1-microm particles, with submicron mass median diameters (MMDs) in PM(0.01-18) (except Zn) (particularly the < 0.1-microm MMDs for Cd and Sb). These levels raise potential health issues. Particle-bound Zn was more abundant in the accumulation mode than in the nucleation/condensation mode, but the opposite was true for Ag, Cd, and Sb. The Ag, Ba, Cd, Pb, Sb, V, and Zn contents in nano particles were strongly associated with diesel fuel, while the Cu, Mn, and Sr in particles < 0.1 microm were more strongly associated with gasoline. The high content of Si in nano particles, more associated with diesel soot than with gasoline exhaust, is another health concern.
JF  - Environmental science & technology
AU  - Lin, Chih-Chung
AU  - Chen, Shui-Jen
AU  - Huang, Kuo-Lin
AU  - Hwang, Wen-Ing
AU  - Chang-Chien, Guo-Ping
AU  - Lin, Wen-Yinn
AD  - Department of Environmental Engineering and Science, National Pingtung University of Science and Technology, Nei Pu, PingTung 91201, Taiwan.
Y1  - 2005/11/01/
PY  - 2005
DA  - 2005 Nov 01
SP  - 8113
EP  - 8122
VL  - 39
IS  - 21
SN  - 0013-936X, 0013-936X
KW  - Air Pollutants
KW  - 0
KW  - Metals
KW  - Vehicle Emissions
KW  - Index Medicus
KW  - Particle Size
KW  - Air Pollutants -- analysis
KW  - Air Pollutants -- toxicity
KW  - Italy
KW  - Nanotechnology
KW  - Metals -- chemistry
KW  - Vehicle Emissions -- analysis
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68804532?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Environmental+science+%26+technology&rft.atitle=Characteristics+of+metals+in+nano%2Fultrafine%2Ffine%2Fcoarse+particles+collected+beside+a+heavily+trafficked+road.&rft.au=Lin%2C+Chih-Chung%3BChen%2C+Shui-Jen%3BHuang%2C+Kuo-Lin%3BHwang%2C+Wen-Ing%3BChang-Chien%2C+Guo-Ping%3BLin%2C+Wen-Yinn&rft.aulast=Lin&rft.aufirst=Chih-Chung&rft.date=2005-11-01&rft.volume=39&rft.issue=21&rft.spage=8113&rft.isbn=&rft.btitle=&rft.title=Environmental+science+%26+technology&rft.issn=0013936X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2005-11-18
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Interindividual variation in nucleotide excision repair genes and risk of endometrial cancer.
AN  - 68796140; 16284373
AB  - Exposure to estrogens is a likely cause of endometrial cancer, but the means by which estrogens exert this effect are not entirely clear. One hypothesis is that certain estrogen metabolites bind to the DNA, forming bulky adducts that damage the DNA and initiate carcinogenesis. A woman's reduced capacity to repair such damage may increase her risk of endometrial cancer. We conducted a population-based case-control study in western Washington State to address the role of variation in nucleotide excision repair genes on the risk of endometrial cancer. Case women (n = 371), ages 50 to 69 years, were diagnosed with invasive endometrial cancer between 1994 and 1999. Control women (n = 420) were selected using random-digit dialing (ages 50-65 years) and by random selection from Health Care Financing Administration data files (ages 66-69 years). Genotyping assays were done for ERCC1, ERCC2 (XPD), ERCC4 (XPF), ERCC5 (XPG), XPA, and XPC. No appreciable differences between cases and controls were observed in the genotype distributions of ERCC1 (c8092a and c19007t), ERCC2 (D312N, K751Q, and c22541a), ERCC4 (R415Q and t30028c), or ERCC5 (D1104H). Carriage of at least one variant allele for XPA G23A was associated with decreased risk of endometrial cancer [odds ratio (OR), 0.70; 95% confidence interval (95% CI), 0.53-0.93]. Carriage of at least one XPC A499V variant allele was associated with a modest decrease in risk (OR, 0.79; 95% CI, 0.59-1.05). Women with variant alleles at both XPC A499V and K939Q had 58% of the risk of women with no XPC variant alleles (OR, 0.58; 95% CI, 0.35-0.96). Our data suggest that interindividual variation in XPA and XPC influences a woman's risk of endometrial cancer.
JF  - Cancer epidemiology, biomarkers & prevention : a publication of the American Association for Cancer Research, cosponsored by the American Society of Preventive Oncology
AU  - Weiss, Jocelyn M
AU  - Weiss, Noel S
AU  - Ulrich, Cornelia M
AU  - Doherty, Jennifer A
AU  - Voigt, Lynda F
AU  - Chen, Chu
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, Occupational and Environmental Epidemiology Branch, 6120 Executive Boulevard, EPS 8123, MSC 7240, Rockville, MD 20852, USA. weissjoc@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 2524
EP  - 2530
VL  - 14
IS  - 11 Pt 1
SN  - 1055-9965, 1055-9965
KW  - DNA Adducts
KW  - 0
KW  - DNA-Binding Proteins
KW  - Index Medicus
KW  - Genetic Variation
KW  - DNA Damage
KW  - Humans
KW  - Aged
KW  - Genotype
KW  - Polymorphism, Restriction Fragment Length
KW  - Risk Factors
KW  - Case-Control Studies
KW  - Middle Aged
KW  - Genetic Predisposition to Disease
KW  - Cell Transformation, Neoplastic
KW  - Female
KW  - DNA Repair -- genetics
KW  - DNA-Binding Proteins -- genetics
KW  - Endometrial Neoplasms -- genetics
KW  - Endometrial Neoplasms -- etiology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cancer+epidemiology%2C+biomarkers+%26+prevention+%3A+a+publication+of+the+American+Association+for+Cancer+Research%2C+cosponsored+by+the+American+Society+of+Preventive+Oncology&rft.atitle=Interindividual+variation+in+nucleotide+excision+repair+genes+and+risk+of+endometrial+cancer.&rft.au=Weiss%2C+Jocelyn+M%3BWeiss%2C+Noel+S%3BUlrich%2C+Cornelia+M%3BDoherty%2C+Jennifer+A%3BVoigt%2C+Lynda+F%3BChen%2C+Chu&rft.aulast=Weiss&rft.aufirst=Jocelyn&rft.date=2005-11-01&rft.volume=14&rft.issue=11+Pt+1&rft.spage=2524&rft.isbn=&rft.btitle=&rft.title=Cancer+epidemiology%2C+biomarkers+%26+prevention+%3A+a+publication+of+the+American+Association+for+Cancer+Research%2C+cosponsored+by+the+American+Society+of+Preventive+Oncology&rft.issn=10559965&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-10
N1  - Date created - 2005-11-14
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Erratum In:
Cancer Epidemiol Biomarkers Prev. 2008 Jan;17(1):261
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The AUDIT-C: screening for alcohol use disorders and risk drinking in the presence of other psychiatric disorders.
AN  - 68776638; 16275207
AB  - This article examines the performance of the AUDIT-C, as embedded in a large national survey, as a screener for alcohol use disorders (AUDs) and risk drinking among individuals with past-year psychopathology. The analysis is based on data collected in personal interviews from a representative population sample of US adults. The study population consisted of past-year drinkers with any past-year mood disorder (n = 2818), any past-year anxiety disorder (n = 3173), or any personality disorder (n = 4389). Screening performance was evaluated by means of sensitivity, specificity, and areas under receiver operating characteristic curves (AUCs). The AUCs for the AUDIT-C were from 0.888 to 0.893 for alcohol dependence, from 0.864 to 0.876 for any AUD, and from 0.941 to 0.951 for any AUD or risk drinking-all on a par with those observed in the general population. Among men, cut points of either > or =5 or > or =6 points (the former favoring sensitivity and the latter favoring specificity) were optimal for detecting dependence, and cut points of > or =5 points were optimal for any AUD and for any AUD or risk drinking. Among women, a cut point of > or =4 points was optimal for the outcomes of both alcohol dependence and any AUD, whereas a cut point of > or =3 points was preferable for detecting any AUD or risk drinking.
JF  - Comprehensive psychiatry
AU  - Dawson, Deborah A
AU  - Grant, Bridget F
AU  - Stinson, Frederick S
AD  - Laboratory of Epidemiology and Biometry, Division of Intramural Clinical and Biological Research, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Bethesda, MD 20892-9304, USA. ddawson@mail.nih.gov
PY  - 2005
SP  - 405
EP  - 416
VL  - 46
IS  - 6
SN  - 0010-440X, 0010-440X
KW  - Index Medicus
KW  - United States
KW  - Sensitivity and Specificity
KW  - Risk-Taking
KW  - Humans
KW  - Aged
KW  - Adult
KW  - Health Surveys
KW  - Alcohol Drinking -- psychology
KW  - Middle Aged
KW  - Adolescent
KW  - Sex Distribution
KW  - Female
KW  - Male
KW  - Alcoholism -- diagnosis
KW  - Surveys and Questionnaires
KW  - Mass Screening -- instrumentation
KW  - Mental Disorders -- complications
KW  - Alcoholism -- complications
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-16
N1  - Date created - 2005-11-08
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Evaluation of (76)Br-FBAU as a PET reporter probe for HSV1-tk gene expression imaging using mouse models of human glioma.
AN  - 68766432; 16269608
AB  - The utility of 5-(76)Br-bromo-2'-fluoro-2'-deoxyuridine ((76)Br-FBAU), a uracil analog, as a PET reporter probe for use with the herpes simplex virus type 1 thymidine kinase (HSV1-tk) reporter gene system for gene expression imaging was evaluated in vivo and in vitro using human and rat glioma cells.
          Human glioma cell lines U87 and U251 were transduced with replication-defective adenovirus constitutively expressing HSV1-tk (Ad.TK) or a control expressing green fluorescent protein (Ad.GFP). These cells were incubated with (76)Br-FBAU for 20-120 min to determine the percentage of total dose uptake. In vitro uptake of equimolar concentrations (1.8 x 10(-8) mol/L) of (76)Br-FBAU and 2'-fluoro-2'-deoxy-5-iodouracil-beta-d-arabinofuranoside ((14)C-FIAU) was also determined in RG2-TK rat glioma cells stably expressing HSV1-tk and in control RG2 cells at 30-120 min. In vivo uptake of (76)Br-FBAU was determined in subcutaneous U87 tumor intratumorally transduced with Ad.TK by ex vivo biodistribution. Uptake in intracranial U87 tumors transduced with Ad.TK expressing HSV1-tk was measured by brain autoradiography. In vivo PET was performed on subcutaneous and intracranial U87 tumors transduced with Ad.TK and on subcutaneous and intracranial stably expressing RG2-TK tumors. U87 and U251 cells transduced with Ad.TK had significantly increased uptake of (76)Br-FBAU compared with cells transduced with Ad.GFP over 20-120 min. In stably expressing cells at 120 min, (14)C-FIAU uptake in RG2-TK tumor cells was 11.3 %ID (percentage injected dose) and in RG2 control cells was 1.7 %ID, and (76)Br-FBAU uptake in RG2-TK tumor cells was 14.2 %ID and in RG2 control cells was 1.5 %ID. Ex vivo biodistribution of subcutaneous U87 tumors transduced with Ad.TK accumulated (76)Br-FBAU significantly more than in the control Ad.GFP transduced tumor and normal tissue, with the lowest uptake in brain. Autoradiography showed localized uptake in intracranial U87 and U251 cells transduced with Ad.TK. PET image analyses of mice with RG2-TK tumors resulted in an increased tumor-to-background ratio of 13 and 26 from 2 to 6 h after injection, respectively, in intracranial tumors.
          (76)Br-FBAU accumulates in glioma cells constitutively expressing HSV1-tk by either adenoviral transduction or in stably expressing cell lines both in vitro and in vivo. (76)Br-FBAU shows promise as a PET reporter probe for use with the HSV1-tk in vivo gene expression imaging system.
JF  - Journal of nuclear medicine : official publication, Society of Nuclear Medicine
AU  - Cho, Steve Y
AU  - Ravasi, Laura
AU  - Szajek, Lawrence P
AU  - Seidel, Jurgen
AU  - Green, Michael V
AU  - Fine, Howard A
AU  - Eckelman, William C
AD  - NeuroOncology Branch, National Cancer Institute and National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1923
EP  - 1930
VL  - 46
IS  - 11
SN  - 0161-5505, 0161-5505
KW  - 1-(2-fluoro-2-deoxyarabinofuranosyl)-5-bromouracil
KW  - 0
KW  - Radiopharmaceuticals
KW  - Recombinant Proteins
KW  - Viral Proteins
KW  - Bromouracil
KW  - 4HK400G5UO
KW  - thymidine kinase, Canid herpesvirus 1
KW  - EC 2.7.1.-
KW  - Thymidine Kinase
KW  - EC 2.7.1.21
KW  - Index Medicus
KW  - Radiopharmaceuticals -- pharmacokinetics
KW  - Animals
KW  - Humans
KW  - Disease Models, Animal
KW  - Metabolic Clearance Rate
KW  - Mice
KW  - Mice, Nude
KW  - Organ Specificity
KW  - Tissue Distribution
KW  - Recombinant Proteins -- genetics
KW  - Radionuclide Imaging
KW  - Gene Expression Regulation, Neoplastic
KW  - Recombinant Proteins -- metabolism
KW  - Genes, Reporter
KW  - Drug Evaluation, Preclinical
KW  - Molecular Probe Techniques
KW  - Viral Proteins -- genetics
KW  - Transfection -- methods
KW  - Glioma -- diagnostic imaging
KW  - Viral Proteins -- metabolism
KW  - Thymidine Kinase -- metabolism
KW  - Gene Expression Profiling -- methods
KW  - Bromouracil -- analogs & derivatives
KW  - Thymidine Kinase -- genetics
KW  - Bromouracil -- pharmacokinetics
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+nuclear+medicine+%3A+official+publication%2C+Society+of+Nuclear+Medicine&rft.atitle=Evaluation+of+%2876%29Br-FBAU+as+a+PET+reporter+probe+for+HSV1-tk+gene+expression+imaging+using+mouse+models+of+human+glioma.&rft.au=Cho%2C+Steve+Y%3BRavasi%2C+Laura%3BSzajek%2C+Lawrence+P%3BSeidel%2C+Jurgen%3BGreen%2C+Michael+V%3BFine%2C+Howard+A%3BEckelman%2C+William+C&rft.aulast=Cho&rft.aufirst=Steve&rft.date=2005-11-01&rft.volume=46&rft.issue=11&rft.spage=1923&rft.isbn=&rft.btitle=&rft.title=Journal+of+nuclear+medicine+%3A+official+publication%2C+Society+of+Nuclear+Medicine&rft.issn=01615505&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2005-11-04
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Cardiac and extracardiac sympathetic denervation in Parkinson's disease with orthostatic hypotension and in pure autonomic failure.
AN  - 68765353; 16269589
AB  - The uptake of 6-(18)F-fluorodopamine by cardiac noradrenergic nerves enables visualization of the sympathetic innervation of the left ventricular myocardium by PET. Patients with Parkinson's disease (PD) and orthostatic hypotension (OH) (PD+OH) or with pure autonomic failure (PAF) have markedly decreased myocardial 6-(18)F-fluorodopamine-derived radioactivity, consistent with cardiac sympathetic denervation, a phenomenon that neurochemical, neuropharmacologic, and, most recently, postmortem neuropathologic studies have confirmed. In this study, we examined whether 6-(18)F-fluorodopamine can visualize sympathetic innervation in extracardiac organs and, if so, whether patients with PD+OH or PAF have neuroimaging evidence of extracardiac noradrenergic denervation.
          To validate the method, healthy volunteers underwent 6-(18)F-fluorodopamine scanning of the head, thorax, and abdomen, with or without treatment with desipramine to block sympathoneural uptake of catecholamines. (13)N-Ammonia scanning was used to address possible group differences in 6-(18)F-fluorodopamine delivery by blood perfusion. Desipramine treatment was associated with decreased 6-(18)F-fluorodopamine-derived radioactivity in the heart, renal cortex, and thyroid gland but not in the liver, spleen, renal pelvis, or salivary glands. Both the PD+OH group and the PAF group had decreased 6-(18)F-fluorodopamine-derived radioactivity in the heart (P < 0.0001) and renal cortex (P = 0.02 and P = 0.005, respectively). The PD+OH group also had decreased radioactivity in the thyroid gland (P = 0.01). Neither group had decreased radioactivity in the other organs, after correction for (13)N-ammonia-derived radioactivity.
          6-(18)F-Fluorodopamine scanning visualizes sympathetic innervation in the heart, renal cortex, and thyroid gland. Both PD+OH and PAF involve decreased noradrenergic innervation that is most prominent in the heart but is also detectable in extracardiac organs.
JF  - Journal of nuclear medicine : official publication, Society of Nuclear Medicine
AU  - Tipre, Dnyanesh N
AU  - Goldstein, David S
AD  - Clinical Neurocardiology Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892, USA. dnyanesht@yahoo.com
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1775
EP  - 1781
VL  - 46
IS  - 11
SN  - 0161-5505, 0161-5505
KW  - Fluorine Radioisotopes
KW  - 0
KW  - Radiopharmaceuticals
KW  - 6-fluorodopamine
KW  - 59043-70-8
KW  - Desipramine
KW  - TG537D343B
KW  - Dopamine
KW  - VTD58H1Z2X
KW  - Index Medicus
KW  - Sensitivity and Specificity
KW  - Reproducibility of Results
KW  - Heart Ventricles -- diagnostic imaging
KW  - Humans
KW  - Heart Ventricles -- drug effects
KW  - Heart Ventricles -- innervation
KW  - Adult
KW  - Aged
KW  - Middle Aged
KW  - Radionuclide Imaging
KW  - Dopamine -- analogs & derivatives
KW  - Autonomic Nervous System -- drug effects
KW  - Autonomic Nervous System -- diagnostic imaging
KW  - Sympathetic Nervous System -- drug effects
KW  - Shy-Drager Syndrome -- diagnostic imaging
KW  - Parkinsonian Disorders -- chemically induced
KW  - Shy-Drager Syndrome -- chemically induced
KW  - Parkinsonian Disorders -- diagnostic imaging
KW  - Autonomic Nervous System Diseases -- diagnostic imaging
KW  - Autonomic Nervous System Diseases -- chemically induced
KW  - Sympathetic Nervous System -- diagnostic imaging
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2005-11-04
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Lymphopenia and interleukin-2 therapy alter homeostasis of CD4+CD25+ regulatory T cells.
AN  - 68764596; 16227988
AB  - CD4(+)CD25(+) regulatory T (T(reg)) cells have a crucial role in maintaining immune tolerance. Mice and humans born lacking T(reg) cells develop severe autoimmune disease, and depletion of T(reg) cells in lymphopenic mice induces autoimmunity. Interleukin (IL)-2 signaling is required for thymic development, peripheral expansion and suppressive activity of T(reg) cells. Animals lacking IL-2 die of autoimmunity, which is prevented by administration of IL-2-responsive T(reg) cells. In light of the emerging evidence that one of the primary physiologic roles of IL-2 is to generate and maintain T(reg) cells, the question arises as to the effects of IL-2 therapy on them. We monitored T(reg) cells during immune reconstitution in individuals with cancer who did or did not receive IL-2 therapy. CD4(+)CD25(hi) cells underwent homeostatic peripheral expansion during immune reconstitution, and in lymphopenic individuals receiving IL-2, the T(reg) cell compartment was markedly increased. Mouse studies showed that IL-2 therapy induced expansion of existent T(reg) cells in normal hosts, and IL-2-induced T(reg) cell expansion was further augmented by lymphopenia. On a per-cell basis, T(reg) cells generated by IL-2 therapy expressed similar levels of FOXP3 and had similar potency for suppression compared to T(reg) cells present in normal hosts. These studies suggest that IL-2 and lymphopenia are primary modulators of CD4(+)CD25(+) T(reg) cell homeostasis.
JF  - Nature medicine
AU  - Zhang, Hua
AU  - Chua, Kevin S
AU  - Guimond, Martin
AU  - Kapoor, Veena
AU  - Brown, Margaret V
AU  - Fleisher, Thomas A
AU  - Long, Lauren M
AU  - Bernstein, Donna
AU  - Hill, Brenna J
AU  - Douek, Daniel C
AU  - Berzofsky, Jay A
AU  - Carter, Charles S
AU  - Read, E J
AU  - Helman, Lee J
AU  - Mackall, Crystal L
AD  - Pediatric Oncology Branch, National Institutes of Health, 10 Center Drive, Bethesda, Maryland 20892, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1238
EP  - 1243
VL  - 11
IS  - 11
SN  - 1078-8956, 1078-8956
KW  - Forkhead Transcription Factors
KW  - 0
KW  - Foxp3 protein, mouse
KW  - Interleukin-2
KW  - Receptors, Interleukin-2
KW  - Recombinant Proteins
KW  - Index Medicus
KW  - Animals
KW  - Homeostasis -- immunology
KW  - Humans
KW  - Child
KW  - Mice
KW  - Sarcoma -- drug therapy
KW  - Mice, Knockout
KW  - Lymphocyte Transfusion
KW  - Adult
KW  - Mice, Inbred C57BL
KW  - Sarcoma -- complications
KW  - Middle Aged
KW  - Adolescent
KW  - Recombinant Proteins -- therapeutic use
KW  - Female
KW  - Forkhead Transcription Factors -- analysis
KW  - Receptors, Interleukin-2 -- metabolism
KW  - Interleukin-2 -- administration & dosage
KW  - T-Lymphocytes, Regulatory -- drug effects
KW  - Lymphopenia -- chemically induced
KW  - Interleukin-2 -- therapeutic use
KW  - CD4-Positive T-Lymphocytes -- immunology
KW  - Lymphopenia -- immunology
KW  - Interleukin-2 -- immunology
KW  - CD4-Positive T-Lymphocytes -- drug effects
KW  - Lymphopenia -- drug therapy
KW  - Receptors, Interleukin-2 -- immunology
KW  - T-Lymphocytes, Regulatory -- immunology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-28
N1  - Date created - 2005-11-04
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Opposing effects of amygdala and orbital prefrontal cortex lesions on the extinction of instrumental responding in macaque monkeys.
AN  - 68756769; 16262672
AB  - Extinction is a well-known behavioural phenomenon that allows organisms to respond flexibly to a changing environment. Although recent work implicates the amygdala and orbital prefrontal cortex (PFo) in extinction of Pavlovian conditioned fear and aversion, much less is known about the neural bases of instrumental extinction. To explore the contribution of the macaque amygdala to flexible responding in the face of changing reward contingency, we tested the effects of selective, excitotoxic lesions of the amygdala on extinction of an instrumental response. For comparison, we evaluated the effects of ablation of PFo on the same task. Amygdala lesions facilitated the extinction of instrumental responses, whereas lesions of PFo had the opposite effect.
JF  - The European journal of neuroscience
AU  - Izquierdo, Alicia
AU  - Murray, Elisabeth A
AD  - Section on the Neurobiology of Learning and Memory, Laboratory of Neuropsychology, National Institute of Mental Health, NIH, Bethesda, MD 20892, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 2341
EP  - 2346
VL  - 22
IS  - 9
SN  - 0953-816X, 0953-816X
KW  - Excitatory Amino Acid Agonists
KW  - 0
KW  - Ibotenic Acid
KW  - 2552-55-8
KW  - Index Medicus
KW  - Animals
KW  - Suction -- methods
KW  - Reward
KW  - Macaca mulatta
KW  - Ibotenic Acid -- toxicity
KW  - Excitatory Amino Acid Agonists -- toxicity
KW  - Male
KW  - Behavior, Animal
KW  - Prefrontal Cortex -- injuries
KW  - Conditioning, Classical -- physiology
KW  - Prefrontal Cortex -- physiology
KW  - Amygdala -- physiology
KW  - Extinction, Psychological -- physiology
KW  - Amygdala -- injuries
KW  - Amygdala -- drug effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-17
N1  - Date created - 2005-11-02
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The role of IL-6 and STAT3 in inflammation and cancer.
AN  - 68755428; 16199153
AB  - The defense of the host from foreign pathogens is the commonly accepted function of the vertebrate immune system. A complex system consisting of many differing cells and structures communicating by both soluble and cell bound ligands, serves to protect the host from infection, and plays a role in preventing the development of certain types of tumours. Numerous signalling pathways are involved in the coordination of the immune system, serving both to activate and attenuate its responses to attack. The ability of the immune system, specifically those cells involved in acute inflammatory responses, to mediate the directed (and sometimes indirect) killing of cells and pathogens, make it a potential threat to host survival. Furthermore, the production and release of various survival factors such as the pleiotropic cytokine IL-6, a major mediator of inflammation and activator of signal transducer and activator of transcription 3, serves to block apoptosis in cells during the inflammatory process, keeping them alive in very toxic environments. Unfortunately, these same pathways serve also to maintain cells progressing towards neoplastic growth, protecting them from cellular apoptotic deletion and chemotherapeutic drugs. Here, we discuss the relationships between cancer and inflammation, and some of the molecular mechanisms involved in mediating the unintended consequences of host defense and tumour survival.
JF  - European journal of cancer (Oxford, England : 1990)
AU  - Hodge, David R
AU  - Hurt, Elaine M
AU  - Farrar, William L
AD  - Laboratory of Molecular Immunoregulation, Cytokine Molecular Mechanisms Section, Center for Cancer Research, The National Cancer Institute at Frederick, Frederick, MD 21702, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 2502
EP  - 2512
VL  - 41
IS  - 16
SN  - 0959-8049, 0959-8049
KW  - Interleukin-6
KW  - 0
KW  - STAT Transcription Factors
KW  - STAT3 Transcription Factor
KW  - Protein-Tyrosine Kinases
KW  - EC 2.7.10.1
KW  - Index Medicus
KW  - Humans
KW  - Signal Transduction -- genetics
KW  - Signal Transduction -- immunology
KW  - Drug Resistance, Neoplasm -- immunology
KW  - STAT Transcription Factors -- physiology
KW  - Immunotherapy -- methods
KW  - STAT3 Transcription Factor -- physiology
KW  - Interleukin-6 -- physiology
KW  - Inflammation -- genetics
KW  - Inflammation -- immunology
KW  - Neoplasms -- therapy
KW  - Protein-Tyrosine Kinases -- physiology
KW  - Neoplasms -- genetics
KW  - Neoplasms -- immunology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-15
N1  - Date created - 2005-11-02
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Meeting report: Structural determination of environmentally responsive proteins.
AN  - 68751564; 16263521
AB  - The three-dimensional structure of gene products continues to be a missing lynchpin between linear genome sequences and our understanding of the normal and abnormal function of proteins and pathways. Enhanced activity in this area is likely to lead to better understanding of how discrete changes in molecular patterns and conformation underlie functional changes in protein complexes and, with it, sensitivity of an individual to an exposure. The National Institute of Environmental Health Sciences convened a workshop of experts in structural determination and environmental health to solicit advice for future research in structural resolution relative to environmentally responsive proteins and pathways. The highest priorities recommended by the workshop were to support studies of structure, analysis, control, and design of conformational and functional states at molecular resolution for environmentally responsive molecules and complexes; promote understanding of dynamics, kinetics, and ligand responses; investigate the mechanisms and steps in posttranslational modifications, protein partnering, impact of genetic polymorphisms on structure/function, and ligand interactions; and encourage integrated experimental and computational approaches. The workshop participants also saw value in improving the throughput and purity of protein samples and macromolecular assemblies; developing optimal processes for design, production, and assembly of macromolecular complexes; encouraging studies on protein-protein and macromolecular interactions; and examining assemblies of individual proteins and their functions in pathways of interest for environmental health.
JF  - Environmental health perspectives
AU  - Reinlib, Leslie
AD  - Division of Extramural Research and Training, National Institute of Environmental Health Sciences, National Institutes of Health, U.S. Department of Health and Human Services, Research Triangle Park, North Carolina 27709-2233, USA. reinlib@niehs.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1622
EP  - 1626
VL  - 113
IS  - 11
SN  - 0091-6765, 0091-6765
KW  - Ligands
KW  - 0
KW  - Macromolecular Substances
KW  - Proteins
KW  - Index Medicus
KW  - Environmental Health
KW  - Protein Processing, Post-Translational
KW  - Toxicogenetics
KW  - Protein Binding
KW  - Proteins -- chemistry
KW  - Proteins -- metabolism
KW  - Protein Conformation
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Environmental+health+perspectives&rft.atitle=Meeting+report%3A+Structural+determination+of+environmentally+responsive+proteins.&rft.au=Reinlib%2C+Leslie&rft.aulast=Reinlib&rft.aufirst=Leslie&rft.date=2005-11-01&rft.volume=113&rft.issue=11&rft.spage=1622&rft.isbn=&rft.btitle=&rft.title=Environmental+health+perspectives&rft.issn=00916765&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-26
N1  - Date created - 2005-11-02
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Nat Struct Biol. 2001 Oct;8(10):822-4 [11573079]
Bioinformatics. 2005 Jun 15;21(12):2814-20 [15827081]
Annu Rev Genomics Hum Genet. 2002;3:243-62 [12194989]
Nature. 2003 Jan 23;421(6921):431-5 [12540917]
Curr Opin Struct Biol. 2003 Dec;13(6):748-57 [14675554]
Nucleic Acids Res. 2004 Jan 1;32(Database issue):D217-22 [14681398]
Biochemistry. 2004 Feb 24;43(7):1950-62 [14967035]
Curr Med Chem. 2004 Mar;11(5):525-38 [15032601]
Curr Top Med Chem. 2004;4(7):687-700 [15032682]
Curr Med Chem. 2004 Apr;11(8):1065-84 [15078166]
Mol Interv. 2004 Jun;4(3):147-56 [15210868]
Nature. 2004 Oct 21;431(7011):931-45 [15496913]
Genomics Proteomics Bioinformatics. 2004 Feb;2(1):1-5 [15629037]
FEBS J. 2005 Jan;272(2):293-312 [15654870]
Curr Opin Struct Biol. 2005 Feb;15(1):15-22 [15718128]
Bioinformatics. 2005 May 1;21(9):1901-7 [15657096]
Proc Natl Acad Sci U S A. 2001 Dec 4;98(25):14274-9 [11724958]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Recovery of erection after pelvic urologic surgery: our experience.
AN  - 68744912; 15889123
AB  - The incidence of erectile dysfunction (ED) in patients undergoing pelvic urologic surgery, the efficacy and tolerability of vardenafil-based rehabilitative treatment as first option in these patients, the role of spontaneous erection (SE) as a possible positive predictive factor to erection recovery after such treatment, and the role of second-line therapies in those nonresponders are evaluated. All the patients undergoing pelvic urologic surgery at our Institution between November 2002 and December 2003 were considered. Preoperative erectile function (EF) was evaluated by using the abridged five-item version of the International Index of Erectile Function (IIEF5) questionnaire. Study population was divided into separate groups considering grade of preoperative EF, nerve sparing (NS) surgery and type of procedure (radical prostatectomy, radical cystectomy (RC) or nerve and seminal sparing cystectomy). In total, 86 patients were evaluated. After 6 months, an increase in mean IIEF5 score of 12.9 points was found in those who had undergone a bilateral NSRP after vardenafil therapy, of 8.0 points in those who had undergone unilateral NSRP, of 11.3 in those who had undergone NSRC and of 11.5 in nerve and seminal sparing cistectomies. A better vardenafil response was found in patients with SE+(P<0.001). Among those vardenafil notresponders, 13 were treated by using intracavernous injections, one by vacuum device and three with penile prosthesis implant. In conclusion, in our experience, vardenafil showed to be well tolerated and effective for recovery of EF in patients undergoing pelvic urologic surgery. This drug was particularly effective for those with a normal preoperative EF undergoing an NS procedure. Of course, it should be recognized that the absence of a control group in the study represents an important limitation. However, based on the data from the literature, there is a strong belief that such an approach will lead to an earlier recovery of EF than without rehabilitative treatment.
JF  - International journal of impotence research
AU  - Gallo, L
AU  - Perdonã, S
AU  - Autorino, R
AU  - Celentano, E
AU  - Menna, L
AU  - Di Lorenzo, G
AU  - Gallo, A
AD  - Division of Urology, National Cancer Institute, Fondazione Pascale, Naples, Italy. gigginogallo@tin.it
PY  - 2005
SP  - 484
EP  - 493
VL  - 17
IS  - 6
SN  - 0955-9930, 0955-9930
KW  - Imidazoles
KW  - 0
KW  - Phosphodiesterase Inhibitors
KW  - Piperazines
KW  - Sulfones
KW  - Triazines
KW  - Vardenafil Dihydrochloride
KW  - 5O8R96XMH7
KW  - Index Medicus
KW  - Cystectomy -- adverse effects
KW  - Humans
KW  - Piperazines -- therapeutic use
KW  - Urinary Bladder Neoplasms -- surgery
KW  - Aged
KW  - Piperazines -- adverse effects
KW  - Phosphodiesterase Inhibitors -- therapeutic use
KW  - Phosphodiesterase Inhibitors -- adverse effects
KW  - Cystectomy -- methods
KW  - Sulfones -- adverse effects
KW  - Prostatectomy -- methods
KW  - Prostatectomy -- adverse effects
KW  - Sulfones -- therapeutic use
KW  - Prostatic Neoplasms -- surgery
KW  - Surveys and Questionnaires
KW  - Imidazoles -- therapeutic use
KW  - Middle Aged
KW  - Triazines -- adverse effects
KW  - Triazines -- therapeutic use
KW  - Imidazoles -- adverse effects
KW  - Male
KW  - Urologic Surgical Procedures, Male -- adverse effects
KW  - Erectile Dysfunction -- drug therapy
KW  - Erectile Dysfunction -- etiology
KW  - Erectile Dysfunction -- epidemiology
KW  - Penile Erection
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68744912?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=International+journal+of+impotence+research&rft.atitle=Recovery+of+erection+after+pelvic+urologic+surgery%3A+our+experience.&rft.au=Gallo%2C+L%3BPerdon%C3%A3%2C+S%3BAutorino%2C+R%3BCelentano%2C+E%3BMenna%2C+L%3BDi+Lorenzo%2C+G%3BGallo%2C+A&rft.aulast=Gallo&rft.aufirst=L&rft.date=2005-11-01&rft.volume=17&rft.issue=6&rft.spage=484&rft.isbn=&rft.btitle=&rft.title=International+journal+of+impotence+research&rft.issn=09559930&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-31
N1  - Date created - 2005-11-02
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Redundant roles for nucleocapsid and matrix RNA-binding sequences in human immunodeficiency virus type 1 assembly.
AN  - 68740344; 16254319
AB  - RNA appears to be required for the assembly of retroviruses. This is likely due to binding of RNA by multiple Gags, which in turn organizes and stabilizes the Gag-Gag interactions that form the virion. While the nucleocapsid (NC) domain is the most conspicuous RNA-binding region of the human immunodeficiency virus type 1 (HIV-1) Gag polyprotein, we have previously shown that NC is not strictly required for efficient particle production. To determine if an RNA requirement for HIV-1 assembly exists, we analyzed virions produced by an NC deletion mutant for the presence of RNA. The results revealed that virions without NC still contained significant amounts of RNA. Since these packaged RNAs are probably incorporated by other RNA-binding sequences in Gag, an RNA-binding site in the matrix protein (MA) of Gag was mutated. While this mutation did not interfere with HIV-1 replication, a construct with both MA and NC mutations (MX/NX) failed to produce particles. The MX/NX mutant was rescued in trans by coassembly with several forms of Gag: wild-type Gag, either of the single-mutant Gags, or Gag truncations that contain MA or NC sequences. Addition of basic sequences to the MX/NX mutant partially restored particle production, consistent with a requirement for Gag-RNA binding in addition to Gag-Gag interactions. Together, these results support an RNA-binding requirement for Gag assembly, which relies on binding of RNA by MA or NC sequences to condense, organize, and stabilize the HIV-1 Gag-Gag interactions that form the virion.
JF  - Journal of virology
AU  - Ott, David E
AU  - Coren, Lori V
AU  - Gagliardi, Tracy D
AD  - Basic Research Program, SAIC-Frederick, Inc., National Cancer Institute at Frederick, Frederick, MD 21702-1201, USA. ott@ncifcrf.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 13839
EP  - 13847
VL  - 79
IS  - 22
SN  - 0022-538X, 0022-538X
KW  - Gene Products, gag
KW  - 0
KW  - RNA, Viral
KW  - Index Medicus
KW  - Mutagenesis, Site-Directed
KW  - Gene Products, gag -- genetics
KW  - Virion -- genetics
KW  - Transfection
KW  - Proviruses -- genetics
KW  - Molecular Sequence Data
KW  - Genetic Complementation Test
KW  - Amino Acid Sequence
KW  - Cloning, Molecular
KW  - HIV-1 -- genetics
KW  - Nucleocapsid -- genetics
KW  - RNA, Viral -- genetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-27
N1  - Date created - 2005-10-28
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Science. 1993 Nov 26;262(5138):1401-7 [8248779]
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J Virol. 2000 Aug;74(16):7238-49 [10906178]
Virology. 2000 Dec 5;278(1):111-21 [11112487]
Proc Natl Acad Sci U S A. 2001 Apr 24;98(9):5246-51 [11320254]
RNA. 2001 Apr;7(4):576-84 [11345436]
Virology. 2002 Feb 15;293(2):368-78 [11886257]
J Virol. 2002 Apr;76(8):4131-7 [11907255]
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J Virol. 2002 Nov;76(22):11177-85 [12388677]
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J Virol. 2003 May;77(10):5547-56 [12719547]
J Virol. 2004 Jan;78(1):52-60 [14671087]
J Virol. 2004 Jan;78(2):716-23 [14694103]
J Virol. 2004 Aug;78(16):8486-95 [15280457]
J Biol Chem. 2004 Aug 20;279(34):35822-8 [15210704]
J Virol. 2004 Nov;78(22):12378-85 [15507624]
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Virology. 1973 Apr;52(2):456-67 [4705382]
J Virol. 1979 Jan;29(1):328-35 [219227]
Nature. 1981 Oct 15-21;293(5833):543-8 [6169994]
J Gen Virol. 1992 Dec;73 ( Pt 12):3079-86 [1469349]
J Virol. 1993 Nov;67(11):6487-98 [8411352]
J Virol. 1987 Jan;61(1):209-13 [3640832]
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J Virol. 1989 Apr;63(4):1558-68 [2926863]
J Virol. 1990 Jul;64(7):3207-11 [2191147]
Biotechniques. 1990 May;8(5):528-35 [2357375]
Curr Top Microbiol Immunol. 1990;157:125-52 [2394131]
J Virol. 1991 Jan;65(1):71-80 [1985218]
Proc Natl Acad Sci U S A. 1991 Apr 15;88(8):3213-7 [2014242]
Virology. 1995 Feb 1;206(2):854-65 [7856098]
J Virol. 1995 Oct;69(10):6487-97 [7666550]
J Virol. 1996 Aug;70(8):5106-14 [8764018]
Curr Top Microbiol Immunol. 1996;214:177-218 [8791728]
J Virol. 1996 Oct;70(10):6607-16 [8794295]
J Virol. 1996 Oct;70(10):6820-5 [8794322]
Virology. 1996 Dec 15;226(2):294-305 [8955049]
J Virol. 1997 Feb;71(2):1443-52 [8995670]
Virology. 1997 Mar 31;230(1):125-33 [9126268]
Virology. 1997 Mar 31;230(1):134-44 [9126269]
J Virol. 1997 Jun;71(6):4425-35 [9151833]
Nucleic Acids Res. 1997 Jul 15;25(14):2902-10 [9207041]
Eur J Biochem. 1997 Oct 15;249(2):592-600 [9370371]
J Virol. 1998 Mar;72(3):1782-9 [9499028]
J Virol. 1998 Mar;72(3):1902-9 [9499042]
Trends Biochem Sci. 1998 Aug;23(8):297-301 [9757830]
Virology. 1998 Nov 10;251(1):1-15 [9813197]
J Mol Biol. 1999 Jan 8;285(1):1-32 [9878383]
Science. 1999 Jan 1;283(5398):80-3 [9872746]
J Virol. 1999 Mar;73(3):2270-9 [9971810]
J Virol. 1999 Jul;73(7):5388-401 [10364286]
J Virol. 1999 Oct;73(10):8527-40 [10482606]
Mol Cell. 2005 Jan 7;17(1):137-43 [15629724]
J Virol. 2005 Apr;79(7):4055-65 [15767407]
J Virol. 2005 Jul;79(14):9038-45 [15994797]
J Virol. 1994 Oct;68(10):6782-6 [8084015]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Drosophila melanogaster homolog of Down syndrome critical region 1 is critical for mitochondrial function.
AN  - 68737641; 16222229
AB  - Mitochondrial dysfunction has emerged as a common theme that underlies numerous neurological disorders, including Down syndrome. Down syndrome cultures and tissues show mitochondrial damage such as impaired mitochondrial enzyme activities, defective mitochondrial DNA repairs and accumulation of toxic free radicals, but the cause of mitochondrial dysfunction remains elusive. Here we demonstrate that the Drosophila melanogaster homolog of human Down syndrome critical region gene 1 (DSCR1), nebula (also known as sarah, sra), has a crucial role in the maintenance of mitochondrial function and integrity. We report that nebula protein is located in the mitochondria. An alteration in the abundance of nebula affects mitochondrial enzyme activities, mitochondrial DNA content, and the number and size of mitochondria. Furthermore, nebula interacts with the ADP/ATP translocator and influences its activity. These results identify nebula/DSCR1 as a regulator of mitochondrial function and integrity and further suggest that an increased level of DSCR1 may contribute to the mitochondrial dysfunction seen in Down syndrome.
JF  - Nature neuroscience
AU  - Chang, Karen T
AU  - Min, Kyung-Tai
AD  - Neurogenetics Branch, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1577
EP  - 1585
VL  - 8
IS  - 11
SN  - 1097-6256, 1097-6256
KW  - DNA, Mitochondrial
KW  - 0
KW  - DSC1 protein, human
KW  - Desmocollins
KW  - Drosophila Proteins
KW  - Membrane Glycoproteins
KW  - Reactive Oxygen Species
KW  - Adenosine Triphosphate
KW  - 8L70Q75FXE
KW  - Mitochondrial ADP, ATP Translocases
KW  - 9068-80-8
KW  - Prostaglandin-Endoperoxide Synthases
KW  - EC 1.14.99.1
KW  - Succinate Dehydrogenase
KW  - EC 1.3.99.1
KW  - Calcineurin
KW  - EC 3.1.3.16
KW  - Index Medicus
KW  - Reactive Oxygen Species -- metabolism
KW  - Animals
KW  - Age Factors
KW  - Calcineurin -- metabolism
KW  - Drosophila melanogaster -- chemistry
KW  - Larva
KW  - Humans
KW  - Blotting, Western -- methods
KW  - Brain -- metabolism
KW  - Immunohistochemistry -- methods
KW  - Animals, Genetically Modified
KW  - Neuropil -- metabolism
KW  - Neuropil -- ultrastructure
KW  - Mitochondrial ADP, ATP Translocases -- metabolism
KW  - Microscopy, Electron, Transmission -- methods
KW  - Prostaglandin-Endoperoxide Synthases -- metabolism
KW  - Photoreceptor Cells, Invertebrate -- ultrastructure
KW  - Microscopy, Immunoelectron -- methods
KW  - Adenosine Triphosphate -- metabolism
KW  - DNA, Mitochondrial -- metabolism
KW  - Immunoprecipitation -- methods
KW  - Subcellular Fractions -- metabolism
KW  - Succinate Dehydrogenase -- metabolism
KW  - Mutation
KW  - Mitochondria -- physiology
KW  - Drosophila Proteins -- chemistry
KW  - Mitochondria -- ultrastructure
KW  - Membrane Glycoproteins -- physiology
KW  - Drosophila Proteins -- genetics
KW  - Membrane Glycoproteins -- genetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-25
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The role of neuroadaptations in relapse to drug seeking.
AN  - 68737607; 16251983
AB  - One of the most difficult problems in treating addiction is not withdrawing addicts from drugs, but preventing relapse. Persistent neuroadaptations are thought to underlie aspects of addiction, including relapse. This commentary assesses the degree to which these neuroadaptations, primarily identified in preclinical studies on cocaine, induce relapse.
JF  - Nature neuroscience
AU  - Shaham, Yavin
AU  - Hope, Bruce T
AD  - Behavioral Neuroscience Branch, Intramural Research Program, National Institute on Drug Abuse, National Institutes of Health, Department of Health and Human Services, 5500 Nathan Shock Drive, Baltimore, Maryland 21224, USA. yshaham@intra.nida.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1437
EP  - 1439
VL  - 8
IS  - 11
SN  - 1097-6256, 1097-6256
KW  - Index Medicus
KW  - Animals
KW  - Amygdala -- physiopathology
KW  - Humans
KW  - Time Factors
KW  - Recurrence
KW  - Cocaine-Related Disorders -- psychology
KW  - Cocaine-Related Disorders -- physiopathology
KW  - Adaptation, Physiological
KW  - Cocaine-Related Disorders -- prevention & control
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Nature+neuroscience&rft.atitle=The+role+of+neuroadaptations+in+relapse+to+drug+seeking.&rft.au=Shaham%2C+Yavin%3BHope%2C+Bruce+T&rft.aulast=Shaham&rft.aufirst=Yavin&rft.date=2005-11-01&rft.volume=8&rft.issue=11&rft.spage=1437&rft.isbn=&rft.btitle=&rft.title=Nature+neuroscience&rft.issn=10976256&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-25
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Laboratory models of alcoholism: treatment target identification and insight into mechanisms.
AN  - 68737436; 16251990
AB  - Laboratory models, including animal tissues and live animals, have proven useful for discovery of molecular targets of alcohol action as well as for characterization of genetic and environmental factors that influence alcohol's neural actions. Here we consider strengths and weaknesses of laboratory models used in alcohol research and analyze the limitations of using animals to model a complex human disease. We describe targets for the neural actions of alcohol, and we review studies in which animal models were used to examine excessive alcohol drinking and to discover genes that may contribute to risk for alcoholism. Despite some limitations of the laboratory models used in alcohol research, these experimental approaches are likely to contribute to the development of new therapies for alcohol abuse and alcoholism.
JF  - Nature neuroscience
AU  - Lovinger, David M
AU  - Crabbe, John C
AD  - Laboratory for Integrative Neuroscience, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Rockville, Maryland 20852, USA. lovindav@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1471
EP  - 1480
VL  - 8
IS  - 11
SN  - 1097-6256, 1097-6256
KW  - Index Medicus
KW  - Environment
KW  - Animals
KW  - Models, Genetic
KW  - Humans
KW  - Genetic Predisposition to Disease
KW  - Models, Biological
KW  - Alcoholism -- therapy
KW  - Disease Models, Animal
KW  - Alcoholism -- metabolism
KW  - Alcoholism -- physiopathology
KW  - Alcoholism -- genetics
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Nature+neuroscience&rft.atitle=Laboratory+models+of+alcoholism%3A+treatment+target+identification+and+insight+into+mechanisms.&rft.au=Lovinger%2C+David+M%3BCrabbe%2C+John+C&rft.aulast=Lovinger&rft.aufirst=David&rft.date=2005-11-01&rft.volume=8&rft.issue=11&rft.spage=1471&rft.isbn=&rft.btitle=&rft.title=Nature+neuroscience&rft.issn=10976256&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-25
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The neuroscience of addiction.
AN  - 68735315; 16251981
JF  - Nature neuroscience
AU  - Volkow, Nora
AU  - Li, Ting-Kai
AD  - National Institute on Drug Abuse, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1429
EP  - 1430
VL  - 8
IS  - 11
SN  - 1097-6256, 1097-6256
KW  - Index Medicus
KW  - Humans
KW  - Neurobiology
KW  - Substance-Related Disorders
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-25
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Bacillus anthracis edema toxin causes extensive tissue lesions and rapid lethality in mice.
AN  - 68733801; 16251415
AB  - Bacillus anthracis edema toxin (ET), an adenylyl cyclase, is an important virulence factor that contributes to anthrax disease. The role of ET in anthrax pathogenesis is, however, poorly understood. Previous studies using crude toxin preparations associated ET with subcutaneous edema, and ET-deficient strains of B. anthracis showed a reduction in virulence. We report the first comprehensive study of ET-induced pathology in an animal model. Highly purified ET caused death in BALB/cJ mice at lower doses and more rapidly than previously seen with the other major B. anthracis virulence factor, lethal toxin. Observations of gross pathology showed intestinal intralumenal fluid accumulation followed by focal hemorrhaging of the ileum and adrenal glands. Histopathological analyses of timed tissue harvests revealed lesions in several tissues including adrenal glands, lymphoid organs, bone, bone marrow, gastrointestinal mucosa, heart, and kidneys. Concomitant blood chemistry analyses supported the induction of tissue damage. Several cytokines increased after ET administration, including granulocyte colony-stimulating factor, eotaxin, keratinocyte-derived cytokine, MCP-1/JE, interleukin-6, interleukin-10, and interleukin-1beta. Physiological measurements also revealed a concurrent hypotension and bradycardia. These studies detail the extensive pathological lesions caused by ET and suggest that it causes death due to multiorgan failure.
JF  - The American journal of pathology
AU  - Firoved, Aaron M
AU  - Miller, Georgina F
AU  - Moayeri, Mahtab
AU  - Kakkar, Rahul
AU  - Shen, Yuequan
AU  - Wiggins, Jason F
AU  - McNally, Elizabeth M
AU  - Tang, Wei-Jen
AU  - Leppla, Stephen H
AD  - National Institute of Allergy and Infectious Diseases, Office of Research Services, National Institutes of Health, 30 Convent Dr., Building 30, Room 303, Bethesda, MD 20892-4349, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1309
EP  - 1320
VL  - 167
IS  - 5
SN  - 0002-9440, 0002-9440
KW  - Antigens, Bacterial
KW  - 0
KW  - Bacterial Toxins
KW  - Cytokines
KW  - Virulence Factors
KW  - anthrax toxin
KW  - Adenylyl Cyclases
KW  - EC 4.6.1.1
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Animals
KW  - Bone Marrow -- pathology
KW  - Kidney -- pathology
KW  - Lymphoid Tissue -- pathology
KW  - Myocardium -- pathology
KW  - Virulence Factors -- toxicity
KW  - Cytokines -- biosynthesis
KW  - Mice
KW  - Ileum -- pathology
KW  - Mice, Inbred BALB C
KW  - Hemorrhage
KW  - Adrenal Glands -- pathology
KW  - Gastric Mucosa -- pathology
KW  - Bone and Bones -- pathology
KW  - Multiple Organ Failure
KW  - Adenylyl Cyclases -- toxicity
KW  - Intestinal Mucosa -- pathology
KW  - Antigens, Bacterial -- toxicity
KW  - Bacillus anthracis -- pathogenicity
KW  - Bacterial Toxins -- toxicity
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-26
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Chest. 1999 Nov;116(5):1369-76 [10559102]
Rev Physiol Biochem Pharmacol. 2004;152:135-64 [15549606]
Hypertension. 2000 Nov;36(5):912-6 [11082166]
Biochem J. 2000 Dec 15;352 Pt 3:739-45 [11104681]
J Leukoc Biol. 2001 Apr;69(4):513-21 [11310836]
Mod Pathol. 2001 May;14(5):482-95 [11353060]
AJR Am J Roentgenol. 2001 Aug;177(2):357-8 [11461861]
Am J Physiol Endocrinol Metab. 2001 Dec;281(6):E1122-7 [11701424]
Emerg Infect Dis. 2001 Nov-Dec;7(6):933-44 [11747719]
Nature. 2002 Jan 24;415(6870):396-402 [11807546]
JAMA. 2002 Feb 20;287(7):863-8 [11851578]
Annu Rev Immunol. 2002;20:125-63 [11861600]
Int J Mol Med. 2002 Jul;10(1):3-10 [12060844]
J Clin Invest. 2002 Jul;110(2):203-8 [12122112]
Curr Top Microbiol Immunol. 2002;271:1-19 [12224519]
FEBS Lett. 2002 Nov 20;531(3):384-8 [12435580]
Clin Infect Dis. 2003 Feb 1;36(3):328-36 [12539075]
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N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Pharmacokinetics, safety, and tolerability of caspofungin in children and adolescents.
AN  - 68733470; 16251293
AB  - Caspofungin is a parenteral antifungal that inhibits beta-1,3-D-glucan synthesis. Although licensed for adult use, the appropriate caspofungin dosing regimen in pediatric patients is not yet known. We therefore investigated the pharmacokinetics and safety of caspofungin in pediatric patients. Thirty-nine children (ages 2 to 11 years) and adolescents (ages 12 to 17 years) with neutropenia were administered caspofungin using either a weight-based regimen (1 mg/kg of body weight/day) or a body surface area regimen (50 mg/m2/day or 70 mg/m2/day). Plasma samples for caspofungin profiles were collected on days 1 and 4. These results were compared to those from adults treated with either 50 or 70 mg/day for mucosal candidiasis. In children receiving 1 mg/kg/day (maximum, 50 mg/day), the area under the concentration-time curve over 24 h (AUC(0-24)) was significantly smaller (46% after multiple doses) than that observed in adults receiving 50 mg/day (P < 0.001). In children and adolescents receiving 50 mg/m2/day (maximum, 70 mg/day), the AUC(0-24) following multiple doses was similar to that for the exposure in adults receiving 50 mg/day. The AUC(0-24) and concentration trough (at 24 h) in pediatric patients receiving the 50-mg/m2 daily regimen were consistent across the range of ages. Caspofungin was generally well tolerated in this study. None of the patients developed a serious drug-related adverse event or were discontinued for toxicity. These results demonstrate that caspofungin at 1 mg/kg/day in pediatric patients is suboptimal. Caspofungin administration at 50 mg/m2/day provides a comparable exposure to that of adult patients treated with 50 mg/day.
JF  - Antimicrobial agents and chemotherapy
AU  - Walsh, Thomas J
AU  - Adamson, Peter C
AU  - Seibel, Nita L
AU  - Flynn, Patricia M
AU  - Neely, Michael N
AU  - Schwartz, Cindy
AU  - Shad, Aziza
AU  - Kaplan, Sheldon L
AU  - Roden, Maureen M
AU  - Stone, Julie A
AU  - Miller, Alisha
AU  - Bradshaw, Susan K
AU  - Li, Susan X
AU  - Sable, Carole A
AU  - Kartsonis, Nicholas A
AD  - Immunocompromised Host Section, Pediatric Oncology Branch, National Cancer Institute, Bldg. 10-CRC, Room 1W-5750, 10 Center Drive, Bethesda, Maryland 20892, USA. walsht@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 4536
EP  - 4545
VL  - 49
IS  - 11
SN  - 0066-4804, 0066-4804
KW  - Antifungal Agents
KW  - 0
KW  - Echinocandins
KW  - Lipopeptides
KW  - Peptides, Cyclic
KW  - caspofungin
KW  - F0XDI6ZL63
KW  - Index Medicus
KW  - Humans
KW  - Body Surface Area
KW  - Adult
KW  - Child
KW  - Adolescent
KW  - Male
KW  - Female
KW  - Child, Preschool
KW  - Peptides, Cyclic -- administration & dosage
KW  - Antifungal Agents -- pharmacokinetics
KW  - Peptides, Cyclic -- adverse effects
KW  - Peptides, Cyclic -- pharmacokinetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-18
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Antimicrob Agents Chemother. 1996 May;40(5):1277-9 [8723483]
Leuk Lymphoma. 1993 Jul;10(4-5):369-76 [8220136]
J Med Vet Mycol. 1997 Jul-Aug;35(4):285-7 [9292427]
Antimicrob Agents Chemother. 1997 Nov;41(11):2326-32 [9371328]
Antimicrob Agents Chemother. 1997 Nov;41(11):2333-8 [9371329]
Bone Marrow Transplant. 1998 Apr;21 Suppl 2:S78-80 [9630334]
Pediatr Infect Dis J. 1998 Nov;17(11):1007-11 [9849983]
Eur J Clin Microbiol Infect Dis. 1999 Apr;18(4):302-4 [10385023]
Clin Infect Dis. 2004 Dec 1;39(11):1563-71 [15578352]
Bone Marrow Transplant. 1996 Dec;18 Suppl 3:S15-20 [8971401]
Clin Infect Dis. 2001 Nov 1;33(9):1529-35 [11588698]
Clin Infect Dis. 2002 Jan 1;34(1):7-14 [11731939]
Antimicrob Agents Chemother. 2002 Jan;46(1):12-23 [11751105]
Antimicrob Agents Chemother. 2002 Feb;46(2):451-7 [11796357]
J Antimicrob Chemother. 2002 Feb;49 Suppl 1:69-73 [11801585]
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Am J Med. 2002 Sep;113(4):294-9 [12361815]
J Acquir Immune Defic Syndr. 2002 Oct 1;31(2):183-7 [12394797]
Eur J Clin Microbiol Infect Dis. 2002 Nov;21(11):767-74 [12461585]
N Engl J Med. 2002 Dec 19;347(25):2020-9 [12490683]
Antimicrob Agents Chemother. 2003 Apr;47(4):1187-92 [12654645]
Pediatr Infect Dis J. 2003 Aug;22(8):747-9 [12938676]
Pediatrics. 2003 Sep;112(3 Pt 1):634-40 [12949295]
Antimicrob Agents Chemother. 2004 Mar;48(3):815-23 [14982770]
J Infect Dis. 2004 Oct 15;190(8):1464-71 [15378439]
N Engl J Med. 2004 Sep 30;351(14):1391-402 [15459300]
N Engl J Med. 1987 Oct 22;317(17):1098 [3657876]
J Clin Oncol. 1990 Feb;8(2):280-6 [2299371]
Clin Infect Dis. 1992 Feb;14(2):485-91 [1554835]
Adv Pediatr Infect Dis. 1996;11:187-290 [8718464]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Dynamic structure of the SPANX gene cluster mapped to the prostate cancer susceptibility locus HPCX at Xq27.
AN  - 68732380; 16251457
AB  - Genetic linkage studies indicate that germline variations in a gene or genes on chromosome Xq27-28 are implicated in prostate carcinogenesis. The linkage peak of prostate cancer overlies a region of approximately 750 kb containing five SPANX genes (SPANX-A1, -A2, -B, -C, and -D) encoding sperm proteins associated with the nucleus; their expression was also detected in a variety of cancers. SPANX genes are >95% identical and reside within large segmental duplications (SDs) with a high level of similarity, which confounds mutational analysis of this gene family by routine PCR methods. In this work, we applied transformation-associated recombination cloning (TAR) in yeast to characterize individual SPANX genes from prostate cancer patients showing linkage to Xq27-28 and unaffected controls. Analysis of genomic TAR clones revealed a dynamic nature of the replicated region of linkage. Both frequent gene deletion/duplication and homology-based sequence transfer events were identified within the region and were presumably caused by recombinational interactions between SDs harboring the SPANX genes. These interactions contribute to diversity of the SPANX coding regions in humans. We speculate that the predisposition to prostate cancer in X-linked families is an example of a genomic disease caused by a specific architecture of the SPANX gene cluster.
JF  - Genome research
AU  - Kouprina, Natalay
AU  - Pavlicek, Adam
AU  - Noskov, Vladimir N
AU  - Solomon, Greg
AU  - Otstot, John
AU  - Isaacs, William
AU  - Carpten, John D
AU  - Trent, Jeffrey M
AU  - Schleutker, Joanna
AU  - Barrett, J Carl
AU  - Jurka, Jerzy
AU  - Larionov, Vladimir
AD  - Laboratory of Biosystems and Cancer, National Cancer Institute, Bethesda, Maryland 20892, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1477
EP  - 1486
VL  - 15
IS  - 11
SN  - 1088-9051, 1088-9051
KW  - Nuclear Proteins
KW  - 0
KW  - SPANXA1 protein, human
KW  - SPANXA2 protein, human
KW  - SPANXD protein, human
KW  - Index Medicus
KW  - Yeasts
KW  - Base Sequence
KW  - Gene Components
KW  - Genomics -- methods
KW  - Recombination, Genetic -- genetics
KW  - Humans
KW  - Molecular Sequence Data
KW  - Sequence Analysis, DNA
KW  - Male
KW  - Cloning, Molecular
KW  - Gene Duplication
KW  - Nuclear Proteins -- genetics
KW  - Genetic Linkage -- genetics
KW  - Chromosomes, Human, X -- genetics
KW  - Prostatic Neoplasms -- genetics
KW  - Genetic Predisposition to Disease
KW  - Chromosome Mapping
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68732380?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Genome+research&rft.atitle=Dynamic+structure+of+the+SPANX+gene+cluster+mapped+to+the+prostate+cancer+susceptibility+locus+HPCX+at+Xq27.&rft.au=Kouprina%2C+Natalay%3BPavlicek%2C+Adam%3BNoskov%2C+Vladimir+N%3BSolomon%2C+Greg%3BOtstot%2C+John%3BIsaacs%2C+William%3BCarpten%2C+John+D%3BTrent%2C+Jeffrey+M%3BSchleutker%2C+Joanna%3BBarrett%2C+J+Carl%3BJurka%2C+Jerzy%3BLarionov%2C+Vladimir&rft.aulast=Kouprina&rft.aufirst=Natalay&rft.date=2005-11-01&rft.volume=15&rft.issue=11&rft.spage=1477&rft.isbn=&rft.btitle=&rft.title=Genome+research&rft.issn=10889051&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-05-02
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Gene. 2003 May 8;309(2):125-33 [12758128]
Genome Res. 2003 May;13(5):781-93 [12727898]
Nature. 2003 Jun 19;423(6942):825-37 [12815422]
J Theor Biol. 2003 Sep 7;224(1):27-42 [12900202]
Mod Pathol. 2004 Mar;17(3):380-8 [14752525]
Int J Androl. 2004 Jun;27(3):134-9 [15139967]
Nucleic Acids Res. 2004 Jul 1;32(Web Server issue):W48-9 [15215348]
Virchows Arch. 2004 Jun;444(6):503-8 [15045584]
Science. 2004 Jul 23;305(5683):525-8 [15273396]
J Natl Cancer Inst. 2004 Aug 18;96(16):1240-7 [15316059]
Genome Res. 2004 Oct;14(10A):1861-9 [15466286]
Mol Biol Evol. 1989 Sep;6(5):526-38 [2677599]
J Mol Biol. 1990 Oct 5;215(3):403-10 [2231712]
Comput Chem. 1996 Mar;20(1):119-21 [8867843]
Prostate. 2003 Dec 1;57(4):320-5 [14601028]
Eur J Epidemiol. 2003;18(11):1027-36 [14620936]
FEMS Microbiol Rev. 2003 Dec;27(5):629-49 [14638416]
Genome Res. 2003 Dec;13(12):2519-32 [14656960]
Br J Cancer. 2004 Jan 26;90(2):510-4 [14735201]
Clin Cancer Res. 2004 Jan 1;10(1 Pt 1):101-12 [14734458]
Cancer Immun. 2004 Jan 23;4:1 [14738373]
Hum Mol Genet. 2004 Apr 1;13 Spec No 1:R103-21 [14749351]
Hum Mol Genet. 2004 Apr 1;13 Spec No 1:R57-64 [14764619]
Proc Natl Acad Sci U S A. 2004 Mar 2;101(9):3077-82 [14973187]
Genome Res. 2004 Apr;14(4):693-9 [15060012]
Proc Natl Acad Sci U S A. 1998 Apr 14;95(8):4469-74 [9539761]
Nat Genet. 1998 Oct;20(2):175-9 [9771711]
Genes Dev. 1998 Dec 15;12(24):3831-42 [9869637]
Cancer Lett. 1999 Jun 1;140(1-2):227-34 [10403563]
Hum Genet. 2005 Feb;116(3):179-85 [15592687]
FEBS Lett. 2005 Jan 31;579(3):604-8 [15670815]
Nature. 2005 Mar 17;434(7031):325-37 [15772651]
Hum Genet. 2005 Aug;117(4):307-16 [15906096]
Mol Cell Biol. 2000 Jan;20(1):54-60 [10594008]
Cancer Res. 1999 Dec 15;59(24):6223-9 [10626816]
Clin Cancer Res. 1999 Dec;5(12):4013-20 [10632333]
Biol Reprod. 2000 Aug;63(2):469-81 [10906052]
Trends Genet. 2000 Sep;16(9):418-20 [10973072]
Mol Cell Biol. 2000 Dec;20(23):9068-75 [11074004]
Mol Genet Metab. 2000 Nov;71(3):463-9 [11073713]
Biol Reprod. 2001 Jan;64(1):345-58 [11133693]
J Surg Res. 2001 Jun 15;98(2):76-80 [11397121]
Genomics. 2002 Jan;79(1):41-50 [11827456]
Genome Res. 2002 Apr;12(4):656-64 [11932250]
Nat Rev Genet. 2002 Apr;3(4):262-73 [11967551]
Prostate. 2002 Jun 1;52(1):12-9 [11992616]
Science. 2002 Aug 9;297(5583):1003-7 [12169732]
Blood. 2003 Feb 1;101(3):955-60 [12393489]
Nucleic Acids Res. 2003 Mar 15;31(6):e29 [12626728]
Int J Cancer. 2003 Jul 1;105(4):454-8 [12712434]
Genes Chromosomes Cancer. 2003 Aug;37(4):381-8 [12800149]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Hepatitis C virus-NS3P in relation to p53, p21waf, mdm2, p21-ras and c-erbB2 in hepatocarcinogenesis.
AN  - 68730908; 16246194
AB  - The non-structural protein 3 (NS3P) of hepatitis C virus (HCV) genome was linked to the neoplastic transformation of normal hepatocytes in chronically infected patients. However, the exact mechanisms involved in this process are unidentified yet, especially in the Egyptian population where the commonest type is genotype 4.
          We investigated 32 HCV reverse transcriptase-polymerase chain reaction (RT-PCR) positive hepatocellular carcinoma (HCC) cases and 18 morphologically normal hepatic tissues distant to tumors (MNT) for the correlation between HCV-NS3P, p53, p21(waf), mdm2, p21ras and c-erbB2 and DNA content by immunohistochemistry and image analysis. The NS3P expression was lower in HCC (65.6%) than in MNT (94.4%) patients. The expression level of studied genes in HCC was: p53 (56.25%), p21(waf) (43.7%), mdm2 (59.4%), p21-ras (73.3%) and c-erbB2 (75%). Whereas in MNT, it was 22.2, 61.1, 44.4, 41.2 and 77.8%, respectively. The NS3P expression showed a significant correlation with the presence of cirrhosis, chronic active hepatitis (CAH) and tumor grade (P < 0.05). c-erbB2 overexpression and p21(waf) loss were higher in MNT than in HCC patients, however, this did not reach a statistically significant level. There was a statistically significant correlation between NS3P, c-erbB2 and p21(waf) (P < 0.01). There was also a significant correlation between p21(waf) loss and CAH (P = 0.01) as well as between mdm2, c-erbB2 and cirrhosis (P = 0.025 and 0.001) in HCC cases. There was a statistically significant difference in the ploidy status between HCC and MNT, but there was no significant relationship between the ploidy status and other clinicopathological features.
          The carcinogenic effect of NS3P is probably exerted at an early stage of HCC possibly through a pathway involving c-erbB2 and p21(waf) alterations. In contrast, p53, p21ras and mdm2 alterations are late events in hepatocarcinogenesis and are usually associated with an aggressive phenotype.
JF  - Journal of gastroenterology and hepatology
AU  - Bahnassi, Abeer A
AU  - Zekri, Abdel-Rahman N
AU  - El-Houssini, Soumaya
AU  - Mokhtar, Nadia M
AU  - Abdel-Aziz, Asraf O
AU  - Sherif, Ghada M
AU  - El-Mishad, Abla M
AU  - Khaled, Hussein M
AD  - Pathology Department, National Cancer Institute, Cairo University, Cairo, Egypt.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1731
EP  - 1740
VL  - 20
IS  - 11
SN  - 0815-9319, 0815-9319
KW  - CDKN1A protein, human
KW  - 0
KW  - Cyclin-Dependent Kinase Inhibitor p21
KW  - DNA, Neoplasm
KW  - NS3 protein, hepatitis C virus
KW  - Proto-Oncogene Proteins
KW  - Tumor Suppressor Protein p53
KW  - Viral Nonstructural Proteins
KW  - MDM2 protein, human
KW  - EC 2.3.2.27
KW  - Proto-Oncogene Proteins c-mdm2
KW  - Receptor, ErbB-2
KW  - EC 2.7.10.1
KW  - Serine Endopeptidases
KW  - EC 3.4.21.-
KW  - Proto-Oncogene Proteins p21(ras)
KW  - EC 3.6.5.2
KW  - Index Medicus
KW  - Proto-Oncogene Proteins p21(ras) -- metabolism
KW  - Receptor, ErbB-2 -- metabolism
KW  - Humans
KW  - Aged
KW  - Child
KW  - Tumor Suppressor Protein p53 -- metabolism
KW  - Adult
KW  - Cyclin-Dependent Kinase Inhibitor p21 -- metabolism
KW  - DNA, Neoplasm -- genetics
KW  - Middle Aged
KW  - Proto-Oncogene Proteins c-mdm2 -- metabolism
KW  - Adolescent
KW  - Ploidies
KW  - Female
KW  - Male
KW  - Viral Nonstructural Proteins -- genetics
KW  - Serine Endopeptidases -- metabolism
KW  - Carcinoma, Hepatocellular -- etiology
KW  - Serine Endopeptidases -- genetics
KW  - Carcinoma, Hepatocellular -- genetics
KW  - Hepatitis C, Chronic -- complications
KW  - Proto-Oncogene Proteins -- metabolism
KW  - Liver Neoplasms -- etiology
KW  - Viral Nonstructural Proteins -- metabolism
KW  - Liver Neoplasms -- genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68730908?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+gastroenterology+and+hepatology&rft.atitle=Hepatitis+C+virus-NS3P+in+relation+to+p53%2C+p21waf%2C+mdm2%2C+p21-ras+and+c-erbB2+in+hepatocarcinogenesis.&rft.au=Bahnassi%2C+Abeer+A%3BZekri%2C+Abdel-Rahman+N%3BEl-Houssini%2C+Soumaya%3BMokhtar%2C+Nadia+M%3BAbdel-Aziz%2C+Asraf+O%3BSherif%2C+Ghada+M%3BEl-Mishad%2C+Abla+M%3BKhaled%2C+Hussein+M&rft.aulast=Bahnassi&rft.aufirst=Abeer&rft.date=2005-11-01&rft.volume=20&rft.issue=11&rft.spage=1731&rft.isbn=&rft.btitle=&rft.title=Journal+of+gastroenterology+and+hepatology&rft.issn=08159319&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-23
N1  - Date created - 2005-10-25
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Phenotype of ENAM mutations is dosage-dependent.
AN  - 68728777; 16246937
AB  - Five mutations in the ENAM gene have been found to cause hypoplastic amelogenesis imperfecta (AI), with phenotypes ranging from localized enamel pitting in carriers to severe hypoplastic AI. To determine the generality of ENAM mutations in hypoplastic AI, we sequenced the ENAM gene in ten Turkish families segregating autosomal hypoplastic AI. In two families, ENAM mutations were found. A novel nonsense mutation (g.12663C>A; p.S246X) was identified in one family segregating local hypoplastic AI as a dominant trait. Affected individuals in a second family segregating autosomal-recessive AI were compound heterozygotes for a novel insertion mutation (g.12946_12947insAGTCAGTACCAGTACTGTGTC) and a previously described insertion (g.13185_13186insAG) mutation. Heterozygous carriers of either insertion had a localized enamel-pitting phenotype. These findings substantiate that enamel phenotypes of ENAM mutations may be dose-dependent, with generalized hypoplastic AI segregating as a recessive trait and localized enamel pitting segregating as a dominant trait.
JF  - Journal of dental research
AU  - Ozdemir, D
AU  - Hart, P S
AU  - Firatli, E
AU  - Aren, G
AU  - Ryu, O H
AU  - Hart, T C
AD  - Clinical Research Core, NIDCR/National Institutes of Health, 10 Center Drive, Building 10, Room 5-2531, Bethesda, MD 20892-1432, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1036
EP  - 1041
VL  - 84
IS  - 11
SN  - 0022-0345, 0022-0345
KW  - Codon, Nonsense
KW  - 0
KW  - Dental Enamel Proteins
KW  - tuftelin
KW  - Cytosine
KW  - 8J337D1HZY
KW  - Adenine
KW  - JAC85A2161
KW  - Dentistry
KW  - Index Medicus
KW  - Pedigree
KW  - Genes, Dominant -- genetics
KW  - Genes, Recessive -- genetics
KW  - Humans
KW  - Child
KW  - Sequence Analysis, Protein
KW  - Phenotype
KW  - Heterozygote
KW  - Adolescent
KW  - Female
KW  - Mutagenesis, Insertional -- genetics
KW  - Codon, Nonsense -- genetics
KW  - Amelogenesis Imperfecta -- genetics
KW  - Dental Enamel Proteins -- genetics
KW  - Mutation -- genetics
KW  - Gene Dosage -- genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68728777?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+dental+research&rft.atitle=Phenotype+of+ENAM+mutations+is+dosage-dependent.&rft.au=Ozdemir%2C+D%3BHart%2C+P+S%3BFiratli%2C+E%3BAren%2C+G%3BRyu%2C+O+H%3BHart%2C+T+C&rft.aulast=Ozdemir&rft.aufirst=D&rft.date=2005-11-01&rft.volume=84&rft.issue=11&rft.spage=1036&rft.isbn=&rft.btitle=&rft.title=Journal+of+dental+research&rft.issn=00220345&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-15
N1  - Date created - 2005-10-25
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Arch Oral Biol. 2003 Aug;48(8):589-96 [12828988]
Oral Dis. 2003 Jan;9(1):19-23 [12617253]
Crit Rev Oral Biol Med. 2003;14(6):387-98 [14656895]
J Med Genet. 2003 Dec;40(12):900-6 [14684688]
Oral Surg Oral Med Oral Pathol Oral Radiol Endod. 2004 Feb;97(2):220-30 [14970781]
J Dent Res. 2004 May;83(5):378-83 [15111628]
J Med Genet. 2004 Jul;41(7):545-9 [15235027]
Acta Odontol Scand. 1982;40(3):135-44 [6957136]
Community Dent Oral Epidemiol. 1986 Aug;14(4):211-6 [3461907]
J Oral Pathol. 1988 Nov;17(9-10):547-53 [3150442]
Ciba Found Symp. 1997;205:175-82; discussion 183-6 [9189624]
Adv Dent Res. 1996 Nov;10(2):111-8 [9206327]
J Dent Res. 2005 Mar;84(3):278-82 [15723871]
J Med Genet. 2005 Mar;42(3):271-5 [15744043]
Arch Oral Biol. 2005 Jul;50(7):611-23 [15892947]
J Craniofac Genet Dev Biol. 1999 Jul-Sep;19(3):148-56 [10589396]
Hum Mol Genet. 2001 Aug 1;10(16):1673-7 [11487571]
Arch Oral Biol. 2002 Apr;47(4):255-60 [11922868]
Arch Oral Biol. 2002 Apr;47(4):261-5 [11922869]
Hum Mol Genet. 2002 May 1;11(9):1069-74 [11978766]
J Dent Res. 2002 Nov;81(11):738-42 [12407086]
Connect Tissue Res. 2003;44 Suppl 1:72-8 [12952177]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - In situ expression of brain-derived neurotrophic factor or neurotrophin-3 promotes sprouting of cortical serotonergic axons following a neurotoxic lesion.
AN  - 68713819; 16206279
AB  - Neurotrophins promote sprouting and elongation of central nervous system (CNS) axons following injury. Consequently, it has been suggested that neurotrophins could be used to repair the CNS by inducing axonal sprouting from nearby intact axons, thereby compensating for the loss of recently injured axons. We tested whether long-term overexpression of neurotrophins in the rat cortex would induce sprouting of cortical serotonergic axons following a neurotoxic injury. After a single subcutaneous injection of para-chloroamphetamine (PCA; 9 mg/ml) that lesions the majority of serotonergic axons in the rat cortex, we injected adenoviral vectors containing cDNAs for brain-derived neurotrophic factor (Adv.BDNF), neurotrophin-3 (Adv.NT-3), or nerve growth factor (Adv.NGF) into the rat frontal cortex. Nine days later, we measured significant increases in the concentration of the respective neurotrophins surrounding the vector injection sites, as measured by ELISA. Immunohistochemical localization of serotonin revealed a fourfold increase in the density of serotonergic fibers surrounding the injection sites of Adv.BDNF and Adv.NT-3, corresponding to a 50% increase in cortical serotonin concentration, compared with a control vector containing the cDNA for enhanced green fluorescent protein (Adv.EGFP). In contrast, there was no difference in serotonergic fiber density or cortical serotonin concentration surrounding the injection of Adv.NGF compared with Adv.EGFP. These data demonstrate that localized overexpression of BDNF or NT-3, but not NGF, is sufficient to promote sprouting of serotonergic axons in the cortex following an experimental neurotoxic injury.
          Copyright (c) 2005 Wiley-Liss, Inc.
JF  - Journal of neuroscience research
AU  - Grider, M H
AU  - Mamounas, L A
AU  - Le, W
AU  - Shine, H D
AD  - Department of Neuroscience, Baylor College of Medicine, Houston, Texas 77030, and NINDS, NIH, Bethesda, MD, USA.
Y1  - 2005/11/01/
PY  - 2005
DA  - 2005 Nov 01
SP  - 404
EP  - 412
VL  - 82
IS  - 3
SN  - 0360-4012, 0360-4012
KW  - Brain-Derived Neurotrophic Factor
KW  - 0
KW  - Neurotoxins
KW  - Neurotrophin 3
KW  - enhanced green fluorescent protein
KW  - Green Fluorescent Proteins
KW  - 147336-22-9
KW  - Serotonin
KW  - 333DO1RDJY
KW  - p-Chloroamphetamine
KW  - 64-12-0
KW  - Nerve Growth Factor
KW  - 9061-61-4
KW  - Index Medicus
KW  - Animals
KW  - Neural Pathways -- physiopathology
KW  - Neuronal Plasticity -- genetics
KW  - Neural Pathways -- metabolism
KW  - Disease Models, Animal
KW  - Up-Regulation -- genetics
KW  - Brain Diseases -- drug therapy
KW  - Brain Diseases -- metabolism
KW  - Green Fluorescent Proteins -- genetics
KW  - Rats
KW  - Transfection
KW  - Brain Diseases -- chemically induced
KW  - Genetic Vectors -- genetics
KW  - Serotonin -- metabolism
KW  - Green Fluorescent Proteins -- metabolism
KW  - Nerve Growth Factor -- genetics
KW  - Female
KW  - Neurotrophin 3 -- genetics
KW  - Brain-Derived Neurotrophic Factor -- metabolism
KW  - Growth Cones -- metabolism
KW  - Neurotrophin 3 -- metabolism
KW  - Cerebral Cortex -- metabolism
KW  - Raphe Nuclei -- physiopathology
KW  - Raphe Nuclei -- metabolism
KW  - Nerve Regeneration -- genetics
KW  - Cerebral Cortex -- physiopathology
KW  - Brain-Derived Neurotrophic Factor -- genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68713819?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+neuroscience+research&rft.atitle=In+situ+expression+of+brain-derived+neurotrophic+factor+or+neurotrophin-3+promotes+sprouting+of+cortical+serotonergic+axons+following+a+neurotoxic+lesion.&rft.au=Grider%2C+M+H%3BMamounas%2C+L+A%3BLe%2C+W%3BShine%2C+H+D&rft.aulast=Grider&rft.aufirst=M&rft.date=2005-11-01&rft.volume=82&rft.issue=3&rft.spage=404&rft.isbn=&rft.btitle=&rft.title=Journal+of+neuroscience+research&rft.issn=03604012&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-24
N1  - Date created - 2005-10-24
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Motivational effects of cannabinoids and opioids on food reinforcement depend on simultaneous activation of cannabinoid and opioid systems.
AN  - 68711071; 15812567
AB  - Strong functional interactions exist between endogenous cannabinoid and opioid systems. Here, we investigated whether cannabinoid-opioid interactions modulate motivational effects of food reinforcement. In rats responding for food under a progressive-ratio schedule, the maximal effort (break point) expended to obtain 45 mg pellets depended on the level of food deprivation, with free-feeding reducing break points and food-deprivation increasing break points. Delta-9-tetrahydrocannabinol (THC; 0.3-5.6 mg/kg intrapeitoneally (i.p.)) and morphine (1-10 mg/kg i.p.) dose-dependently increased break points for food reinforcement, while the cannabinoid CB1 receptor antagonist rimonabant (SR-141716A; 0.3-3 mg/kg i.p.) and the preferential mu-opioid receptor antagonist naloxone (0.3-3 mg/kg i.p.) dose-dependently decreased break points. THC and morphine only increased break points when food was delivered during testing, suggesting that these treatments directly influenced reinforcing effects of food, rather than increasing behavior in a nonspecific manner. Effects of THC were blocked by rimonabant and effects of morphine were blocked by naloxone, demonstrating that THC's effects depended on cannabinoid CB1 receptor activation and morphine's effects depended on opioid-receptor activation. Furthermore, THC's effects were blocked by naloxone and morphine's effects were blocked by rimonabant, demonstrating that mu-opioid receptors were involved in the effects of THC and cannabinoid CB1 receptors were involved in the effects of morphine on food-reinforced behavior. Thus, activation of both endogenous cannabinoid and opioid systems appears to jointly facilitate motivational effects of food measured under progressive-ratio schedules of reinforcement and this facilitatory modulation appears to critically depend on interactions between these two systems. These findings support the proposed therapeutic utility of cannabinoid agonists and antagonists in eating disorders.
JF  - Neuropsychopharmacology : official publication of the American College of Neuropsychopharmacology
AU  - Solinas, Marcello
AU  - Goldberg, Steven R
AD  - Preclinical Pharmacology Section, Behavioral Neuroscience Branch, National Institute on Drug Abuse, Intramural Research Program, National Institutes of Health, Department of Health and Human Services, Baltimore, MD, USA. msolinas@intra.nida.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 2035
EP  - 2045
VL  - 30
IS  - 11
SN  - 0893-133X, 0893-133X
KW  - Analgesics, Non-Narcotic
KW  - 0
KW  - Analgesics, Opioid
KW  - Cannabinoid Receptor Agonists
KW  - Cannabinoid Receptor Antagonists
KW  - Cannabinoids
KW  - Central Nervous System Stimulants
KW  - Drug Combinations
KW  - Narcotics
KW  - Piperidines
KW  - Pyrazoles
KW  - Receptors, Cannabinoid
KW  - Receptors, Opioid
KW  - Methamphetamine
KW  - 44RAL3456C
KW  - Morphine
KW  - 76I7G6D29C
KW  - Dronabinol
KW  - 7J8897W37S
KW  - rimonabant
KW  - RML78EN3XE
KW  - Index Medicus
KW  - Eating -- drug effects
KW  - Conditioning, Operant -- drug effects
KW  - Animals
KW  - Drug Interactions
KW  - Analgesics, Non-Narcotic -- pharmacology
KW  - Analysis of Variance
KW  - Central Nervous System Stimulants -- pharmacology
KW  - Reinforcement Schedule
KW  - Dose-Response Relationship, Drug
KW  - Food Deprivation -- physiology
KW  - Dronabinol -- pharmacology
KW  - Behavior, Animal
KW  - Morphine -- pharmacology
KW  - Rats
KW  - Piperidines -- pharmacology
KW  - Pyrazoles -- pharmacology
KW  - Rats, Sprague-Dawley
KW  - Analgesics, Opioid -- pharmacology
KW  - Methamphetamine -- pharmacology
KW  - Time Factors
KW  - Male
KW  - Receptors, Cannabinoid -- physiology
KW  - Motivation
KW  - Food
KW  - Reinforcement (Psychology)
KW  - Narcotics -- pharmacology
KW  - Cannabinoids -- pharmacology
KW  - Receptors, Opioid -- physiology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68711071?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Neuropsychopharmacology+%3A+official+publication+of+the+American+College+of+Neuropsychopharmacology&rft.atitle=Motivational+effects+of+cannabinoids+and+opioids+on+food+reinforcement+depend+on+simultaneous+activation+of+cannabinoid+and+opioid+systems.&rft.au=Solinas%2C+Marcello%3BGoldberg%2C+Steven+R&rft.aulast=Solinas&rft.aufirst=Marcello&rft.date=2005-11-01&rft.volume=30&rft.issue=11&rft.spage=2035&rft.isbn=&rft.btitle=&rft.title=Neuropsychopharmacology+%3A+official+publication+of+the+American+College+of+Neuropsychopharmacology&rft.issn=0893133X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-24
N1  - Date created - 2005-10-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Curcumin suppresses interleukin 1beta-mediated microsomal prostaglandin E synthase 1 by altering early growth response gene 1 and other signaling pathways.
AN  - 68709211; 16081677
AB  - Curcumin (diferuloylmethane) is one of the phytophenolic compounds found in the turmeric plant with anti-inflammatory and anticarcinogenic activities. One possible mechanism for these activities is the inhibition of prostaglandin (PG) E(2) formation. In this study and other reports, curcumin suppresses interleukin-1beta-induced formation of prostaglandin E(2) in a concentration-dependent manner. Interleukin-1beta-induced microsomal prostaglandin E synthase 1 (mPGES-1) and cyclooxygenase-2 were attenuated by curcumin at the protein and mRNA levels, but a more dramatic inhibition of mPGES-1 expression was observed at lower concentrations of curcumin in A549 human lung epithelial cells. The inhibition of mPGES-1 expression by curcumin shifted the arachidonic acid profile from PGE(2) to PGF(2alpha) and 6-keto-PGF(1alpha) as major metabolites. The expression of early growth response gene 1 (EGR-1), a key transcription factor of cytokine-induced mPGES-1, was inhibited by curcumin. Incubation with siRNA for EGR-1 inhibited interleukin (IL)-1beta-induced mPGES-1, and the controlled expression of EGR-1 increased the mPGES-1 expression. Several proinflammatory signaling molecules, such as nuclear factor kappaB (NF-kappaB) and mitogen-activated protein kinases, are also known to affect curcumin-regulated gene expression. Curcumin inhibited IkappaBalpha phosphorylation and degradation and thus reduced the expression of mPGES-1. Curcumin suppressed cytokine-induced mPGES-1 by inhibiting phosphorylation of Jun N-terminal kinase (JNK)1/2. However, EGR-1 expression was suppressed by lower concentrations of curcumin, as compared with JNK1/2 and IkappaBalpha. These results indicate that curcumin inhibits IL-1beta-induced PGE(2) formation by inhibiting the expression of mPGES-1 that is mediated by suppression of EGR-1 expression as well as NF-kappaB and JNK1/2.
JF  - The Journal of pharmacology and experimental therapeutics
AU  - Moon, Yuseok
AU  - Glasgow, Wayne C
AU  - Eling, Thomas E
AD  - Eicosanoid Biochemistry Section, Laboratory of Molecular Carcinogenesis, National Institute of Environmental Health Sciences, National Institutes of Health, Research Triangle Park, NC 27709, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 788
EP  - 795
VL  - 315
IS  - 2
SN  - 0022-3565, 0022-3565
KW  - Anti-Inflammatory Agents, Non-Steroidal
KW  - 0
KW  - Anticarcinogenic Agents
KW  - Early Growth Response Protein 1
KW  - Interleukin-1
KW  - NF-kappa B
KW  - RNA, Small Interfering
KW  - Arachidonic Acid
KW  - 27YG812J1I
KW  - Luciferases
KW  - EC 1.13.12.-
KW  - Cyclooxygenase 2
KW  - EC 1.14.99.1
KW  - Mitogen-Activated Protein Kinase 9
KW  - EC 2.7.1.24
KW  - Mitogen-Activated Protein Kinase 8
KW  - EC 2.7.11.24
KW  - Intramolecular Oxidoreductases
KW  - EC 5.3.-
KW  - PTGES protein, human
KW  - EC 5.3.99.3
KW  - Prostaglandin-E Synthases
KW  - Curcumin
KW  - IT942ZTH98
KW  - Index Medicus
KW  - Plasmids -- genetics
KW  - Cyclooxygenase 2 -- genetics
KW  - Humans
KW  - Cyclooxygenase 2 -- biosynthesis
KW  - Cell Line, Tumor
KW  - Mitogen-Activated Protein Kinase 8 -- metabolism
KW  - Mitogen-Activated Protein Kinase 9 -- metabolism
KW  - Reverse Transcriptase Polymerase Chain Reaction
KW  - Arachidonic Acid -- metabolism
KW  - Luciferases -- biosynthesis
KW  - Blotting, Western
KW  - Cell Survival -- drug effects
KW  - Transfection
KW  - RNA, Small Interfering -- pharmacology
KW  - Luciferases -- genetics
KW  - NF-kappa B -- metabolism
KW  - Interleukin-1 -- physiology
KW  - Intramolecular Oxidoreductases -- metabolism
KW  - Signal Transduction -- drug effects
KW  - Microsomes, Liver -- enzymology
KW  - Anticarcinogenic Agents -- pharmacology
KW  - Microsomes, Liver -- drug effects
KW  - Early Growth Response Protein 1 -- genetics
KW  - Curcumin -- pharmacology
KW  - Anti-Inflammatory Agents, Non-Steroidal -- pharmacology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=The+Journal+of+pharmacology+and+experimental+therapeutics&rft.atitle=Curcumin+suppresses+interleukin+1beta-mediated+microsomal+prostaglandin+E+synthase+1+by+altering+early+growth+response+gene+1+and+other+signaling+pathways.&rft.au=Moon%2C+Yuseok%3BGlasgow%2C+Wayne+C%3BEling%2C+Thomas+E&rft.aulast=Moon&rft.aufirst=Yuseok&rft.date=2005-11-01&rft.volume=315&rft.issue=2&rft.spage=788&rft.isbn=&rft.btitle=&rft.title=The+Journal+of+pharmacology+and+experimental+therapeutics&rft.issn=00223565&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-12
N1  - Date created - 2005-10-20
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Transcriptional regulation of activating transcription factor 3 involves the early growth response-1 gene.
AN  - 68707748; 16079301
AB  - Previously, our laboratory identified activating transcription factor 3 (ATF3) as up-regulated by nonsteroidal anti-inflammatory drugs using microarray analysis of mRNA from human colorectal cancer cells treated with sulindac sulfide. ATF3 is a transcription factor involved in cell growth, apoptosis, and invasion and is induced by a variety of anticancer and dietary compounds. However, the regulation of ATF3 by anticancer agents is not known. The promoter of ATF3 contains several transcription factor binding sites. We identified three putative Egr-1 binding sites in the promoter of ATF3 and report for the first time that the molecular mechanism responsible for the transcriptional regulation of ATF3 by two divergent pharmaceutical compounds, sulindac sulfide and troglitazone, involved the early growth response gene-1 (Egr-1). For example, overexpression of Egr-1 protein induced ATF3 mRNA 3.5-fold and transcriptional activity of an ATF3 promoter construct more than 20-fold. ATF3 and Egr-1 mRNA and protein and ATF3 promoter activity were induced by these compounds, whereas induction of ATF3 by these compounds was blocked by Egr-1 small interfering RNA. Sulindac sulfide and troglitazone regulated ATF3 promoter activity, which was suppressed when the two Egr-1 sites were mutated. These compounds induced phosphorylation of extracellular signal-regulated kinase1/2 (Erk1/2), whereas a dominant-negative inhibitor of mitogen-activate protein kinase kinase (MEK) 1 blocked the induction of ATF3. The MEK1/2 inhibitor PD98059 (2'-amino-3'-methoxyflavone) blocked the induction of ATF3 and Egr-1 mRNA expression and ATF3 promoter activity by these compounds. Therefore, this is a novel first report demonstrating that the expression of ATF3 occurs via Egr-1 downstream of Erk1/2.
JF  - The Journal of pharmacology and experimental therapeutics
AU  - Bottone, Frank G
AU  - Moon, Yuseok
AU  - Alston-Mills, Brenda
AU  - Eling, Thomas E
AD  - Laboratory of Molecular Carcinogenesis, National Institute of Environmental Health Sciences, National Institutes of Health, Research Triangle Park, North Carolina, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 668
EP  - 677
VL  - 315
IS  - 2
SN  - 0022-3565, 0022-3565
KW  - Activating Transcription Factor 3
KW  - 0
KW  - Anti-Inflammatory Agents, Non-Steroidal
KW  - Chromans
KW  - Early Growth Response Protein 1
KW  - Thiazolidinediones
KW  - Sulindac
KW  - 184SNS8VUH
KW  - RNA
KW  - 63231-63-0
KW  - Luciferases
KW  - EC 1.13.12.-
KW  - Mitogen-Activated Protein Kinases
KW  - EC 2.7.11.24
KW  - MAP Kinase Kinase 1
KW  - EC 2.7.12.2
KW  - troglitazone
KW  - I66ZZ0ZN0E
KW  - Index Medicus
KW  - MAP Kinase Kinase 1 -- genetics
KW  - Mitogen-Activated Protein Kinases -- metabolism
KW  - Humans
KW  - Reverse Transcriptase Polymerase Chain Reaction
KW  - Autoradiography
KW  - RNA -- biosynthesis
KW  - Blotting, Western
KW  - Gene Expression Regulation -- physiology
KW  - Chromans -- pharmacology
KW  - Signal Transduction -- drug effects
KW  - Thiazolidinediones -- pharmacology
KW  - Sulindac -- pharmacology
KW  - RNA -- isolation & purification
KW  - Genes, Reporter
KW  - Promoter Regions, Genetic -- genetics
KW  - Luciferases -- genetics
KW  - Cell Line
KW  - Anti-Inflammatory Agents, Non-Steroidal -- pharmacology
KW  - Densitometry
KW  - Early Growth Response Protein 1 -- physiology
KW  - Early Growth Response Protein 1 -- genetics
KW  - Activating Transcription Factor 3 -- genetics
KW  - Activating Transcription Factor 3 -- biosynthesis
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-12
N1  - Date created - 2005-10-20
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Cannabinoid agonists but not inhibitors of endogenous cannabinoid transport or metabolism enhance the reinforcing efficacy of heroin in rats.
AN  - 68698420; 15870833
AB  - Accumulating evidence suggests that the endogenous cannabinoid system is involved in the reinforcing effects of heroin. In rats intravenously self-administering heroin, we investigated effects of cannabinoid CB1 receptor agonists and compounds that block transport or metabolism of the endogenous cannabinoid anandamide. The natural cannnabinoid CB1 receptor agonist delta-9-tetrahydrocannabinol (THC, 0.3-3 mg/kg i.p.) did not alter self-administration of heroin under a fixed-ratio one (FR1) schedule, except at a high 3 mg/kg dose which decreased heroin self-administration. Under a progressive-ratio schedule, however, THC dose-dependently increased the number of 50 mug/kg heroin injections self-administered per session and the maximal ratio completed (break-point), with peak increases at 1 mg/kg THC. In addition, 1 mg/kg THC increased break-points and injections self-administered over a wide range of heroin injection doses (25-100 microg/kg), indicating an increase in heroin's reinforcing efficacy and not its potency. The synthetic cannabinoid CB1 receptor agonist WIN55,212-2 (0.3-3 mg/kg i.p.) had effects similar to THC under the progressive-ratio schedule. In contrast, AM-404 (1-10 mg/kg i.p.), an inhibitor of transport of anandamide, and URB-597 (0.01-0.3 mg/kg i.p.), an inhibitor of the enzyme fatty acid amide hydrolase (FAAH) that degrades anandamide, or their combination, did not increase reinforcing efficacy of heroin at any dose tested. Thus, activation of cannabinoid CB1 receptors facilitates the reinforcing efficacy of heroin and this appears to be mediated by interactions between cannabinoid CB1 receptors and mu-opioid receptors and their signaling pathways, rather than by an opioid-induced release of endogenous cannabinoids.
JF  - Neuropsychopharmacology : official publication of the American College of Neuropsychopharmacology
AU  - Solinas, Marcello
AU  - Panlilio, Leigh V
AU  - Tanda, Gianluigi
AU  - Makriyannis, Alexandros
AU  - Matthews, Stephanie A
AU  - Goldberg, Steven R
AD  - Preclinical Pharmacology Section, Behavioral Neuroscience Branch, Intramural Research Program, National Institute on Drug Abuse, National Institutes of Health, Department of Health and Human Services, Baltimore, MD 21224, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 2046
EP  - 2057
VL  - 30
IS  - 11
SN  - 0893-133X, 0893-133X
KW  - Arachidonic Acids
KW  - 0
KW  - Benzamides
KW  - Benzoxazines
KW  - Cannabinoid Receptor Modulators
KW  - Cannabinoids
KW  - Carbamates
KW  - Morpholines
KW  - N-(4-hydroxyphenyl)arachidonylamide
KW  - Naphthalenes
KW  - Narcotics
KW  - cyclohexyl carbamic acid 3'-carbamoylbiphenyl-3-yl ester
KW  - Win 55212-2
KW  - 5H31GI9502
KW  - Heroin
KW  - 70D95007SX
KW  - Dronabinol
KW  - 7J8897W37S
KW  - Index Medicus
KW  - Carbamates -- pharmacology
KW  - Naphthalenes -- pharmacology
KW  - Reaction Time -- drug effects
KW  - Animals
KW  - Drug Interactions
KW  - Reinforcement Schedule
KW  - Dose-Response Relationship, Drug
KW  - Dronabinol -- pharmacology
KW  - Morpholines -- pharmacology
KW  - Self Administration -- psychology
KW  - Behavior, Animal
KW  - Arachidonic Acids -- pharmacology
KW  - Rats
KW  - Rats, Sprague-Dawley
KW  - Benzamides -- pharmacology
KW  - Time Factors
KW  - Male
KW  - Conditioning, Operant -- drug effects
KW  - Cannabinoid Receptor Modulators -- agonists
KW  - Cannabinoids -- agonists
KW  - Reinforcement (Psychology)
KW  - Narcotics -- administration & dosage
KW  - Cannabinoid Receptor Modulators -- antagonists & inhibitors
KW  - Heroin -- administration & dosage
KW  - Cannabinoids -- antagonists & inhibitors
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68698420?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Neuropsychopharmacology+%3A+official+publication+of+the+American+College+of+Neuropsychopharmacology&rft.atitle=Cannabinoid+agonists+but+not+inhibitors+of+endogenous+cannabinoid+transport+or+metabolism+enhance+the+reinforcing+efficacy+of+heroin+in+rats.&rft.au=Solinas%2C+Marcello%3BPanlilio%2C+Leigh+V%3BTanda%2C+Gianluigi%3BMakriyannis%2C+Alexandros%3BMatthews%2C+Stephanie+A%3BGoldberg%2C+Steven+R&rft.aulast=Solinas&rft.aufirst=Marcello&rft.date=2005-11-01&rft.volume=30&rft.issue=11&rft.spage=2046&rft.isbn=&rft.btitle=&rft.title=Neuropsychopharmacology+%3A+official+publication+of+the+American+College+of+Neuropsychopharmacology&rft.issn=0893133X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-24
N1  - Date created - 2005-10-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Historical limitations of determinant based exposure groupings in the rubber manufacturing industry.
AN  - 68697214; 16234406
AB  - To study the validity of using a cross-sectional industry-wide exposure survey to develop exposure groupings for epidemiological purposes that extend beyond the time period in which the exposure data were collected.
          Exposure determinants were used to group workers into high, medium, and low exposure groups. The contrast of this grouping and other commonly used grouping schemes based on plant and department within this exposure survey and a previously conducted survey within the same industry (and factories) were estimated and compared. Grouping of inhalable and dermal exposure based on exposure determinants resulted in the highest, but still modest, contrast (epsilon approximately 0.3). Classifying subjects based on a combination of plant and department resulted in a slightly lower contrast (epsilon approximately 0.2). If the determinant based grouping derived from the 1997 exposure survey was used to classify workers in the 1988 survey the average contrast decreased significantly for both exposures (epsilon approximately 0.1). On the contrary, the exposure classification based on plant and department increased in contrast (from epsilon approximately 0.2 to epsilon approximately 0.3) and retained its relative ranking overtime.
          Although determinant based groupings seem to result in more efficient groupings within a cross-sectional survey, they have to be used with caution as they might result in significant less contrast beyond the studied population or time period. It is concluded that a classification based on plant and department might be more desirable for retrospective studies in the rubber manufacturing industry, as they seem to have more historical relevance and are most likely more accurately recorded historically than information on exposure determinants in a particular industry.
JF  - Occupational and environmental medicine
AU  - Vermeulen, R
AU  - Kromhout, H
AD  - Occupational and Environmental Epidemiology Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, NIH, DHHS, Rockville, MD 20892, USA. vermeulr@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 793
EP  - 799
VL  - 62
IS  - 11
KW  - Air Pollutants, Occupational
KW  - 0
KW  - Dust
KW  - Rubber
KW  - 9006-04-6
KW  - Index Medicus
KW  - Inhalation Exposure -- analysis
KW  - Epidemiologic Methods
KW  - Air Pollutants, Occupational -- analysis
KW  - Skin Absorption
KW  - Humans
KW  - Epidemiological Monitoring
KW  - Environmental Monitoring -- methods
KW  - Industry
KW  - Occupational Exposure -- analysis
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Occupational+and+environmental+medicine&rft.atitle=Historical+limitations+of+determinant+based+exposure+groupings+in+the+rubber+manufacturing+industry.&rft.au=Vermeulen%2C+R%3BKromhout%2C+H&rft.aulast=Vermeulen&rft.aufirst=R&rft.date=2005-11-01&rft.volume=62&rft.issue=11&rft.spage=793&rft.isbn=&rft.btitle=&rft.title=Occupational+and+environmental+medicine&rft.issn=1470-7926&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-15
N1  - Date created - 2005-10-19
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Ann Occup Hyg. 2000 Jan;44(1):43-56 [10689758]
Occup Environ Med. 1997 Oct;54(10):714-9 [9404318]
Mutat Res. 2000 Jul 10;468(2):165-71 [10882893]
Ann Occup Hyg. 2000 Aug;44(5):325-7 [10930496]
Ann Occup Hyg. 2000 Aug;44(5):343-54 [10930498]
Risk Anal. 2000 Oct;20(5):653-63 [11110212]
Mutat Res. 2001 Jan 25;490(1):27-34 [11152969]
Ann Occup Hyg. 2002 Jan;46(1):69-77 [12005135]
Ann Occup Hyg. 1993 Apr;37(2):117-34 [8317851]
Am Ind Hyg Assoc J. 1993 Nov;54(11):654-62 [8256689]
Ann Occup Hyg. 1994 Feb;38(1):3-22 [8161092]
Am J Ind Med. 1995 Feb;27(2):171-85 [7755008]
Scand J Work Environ Health. 1996 Apr;22(2):94-101 [8738886]
Ann Occup Hyg. 1997 Apr;41(2):135-53 [9155236]
Ann Occup Hyg. 1997 Jun;41(3):287-96 [9204756]
Epidemiology. 1997 Mar;8(2):218-9 [9229220]
Ann Occup Hyg. 2000 Jan;44(1):57-66 [10689759]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Inability of a fusion protein of IL-2 and diphtheria toxin (Denileukin Diftitox, DAB389IL-2, ONTAK) to eliminate regulatory T lymphocytes in patients with melanoma.
AN  - 68689235; 16224276
AB  - Elimination of regulatory T lymphocytes may provide a way to break self-tolerance and unleash the anti-tumor properties of circulating lymphocytes. The use of fusion proteins, which link cytotoxic molecules to receptor targets, provides one approach to this problem. This study examined the ability of a fusion protein of interleukin-2 (IL-2) and diphtheria toxin (Denileukin Diftitox, DAB389IL-2, ONTAK) to eliminate regulatory T lymphocytes based on their expression of high-affinity IL-2 receptors. Thirteen patients (12 with metastatic melanoma, 1 with metastatic renal cell carcinoma) were treated at one of the two Food and Drug Administration-approved doses of Denileukin Diftitox (seven patients at 9 microg/kg, six patients at 18 microg/kg). None of the patients experienced an objective clinical response. Foxp3 expression did not decrease significantly overall, although it did decrease minimally among patients receiving 18 microg/kg (-2.01+/-0.618 copies of Foxp3/10(3) copies of beta-actin; P=0.031). Denileukin Diftitox did not decrease the suppressive ability of CD4CD25 cells as quantified by an in vitro co-culture suppression assay. Furthermore, the increased numbers of lymphocytes in patients resulting from treatment with IL-2 were not susceptible to Denileukin Diftitox. Administration of Denileukin Diftitox does not appear to eliminate regulatory T lymphocytes or cause regression of metastatic melanoma.
JF  - Journal of immunotherapy (Hagerstown, Md. : 1997)
AU  - Attia, Peter
AU  - Maker, Ajay V
AU  - Haworth, Leah R
AU  - Rogers-Freezer, Linda
AU  - Rosenberg, Steven A
AD  - Surgery Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892-1201, USA.
PY  - 2005
SP  - 582
EP  - 592
VL  - 28
IS  - 6
SN  - 1524-9557, 1524-9557
KW  - Antineoplastic Agents
KW  - 0
KW  - Diphtheria Toxin
KW  - FOXP3 protein, human
KW  - Forkhead Transcription Factors
KW  - Interleukin-2
KW  - RNA, Messenger
KW  - Receptors, Interleukin-2
KW  - Recombinant Fusion Proteins
KW  - denileukin diftitox
KW  - 25E79B5CTM
KW  - Index Medicus
KW  - Kidney Neoplasms -- pathology
KW  - Kidney Neoplasms -- drug therapy
KW  - CD8-Positive T-Lymphocytes -- drug effects
KW  - Humans
KW  - Carcinoma, Renal Cell -- drug therapy
KW  - Cell Line, Tumor
KW  - Receptors, Interleukin-2 -- immunology
KW  - Gene Expression Regulation, Neoplastic
KW  - Forkhead Transcription Factors -- genetics
KW  - RNA, Messenger -- metabolism
KW  - CD8-Positive T-Lymphocytes -- immunology
KW  - Adult
KW  - Carcinoma, Renal Cell -- secondary
KW  - Neoplasm Metastasis
KW  - Middle Aged
KW  - Forkhead Transcription Factors -- metabolism
KW  - Recombinant Fusion Proteins -- therapeutic use
KW  - Carcinoma, Renal Cell -- immunology
KW  - Male
KW  - Female
KW  - Kidney Neoplasms -- immunology
KW  - Skin Neoplasms -- drug therapy
KW  - T-Lymphocytes, Regulatory -- drug effects
KW  - Antineoplastic Agents -- administration & dosage
KW  - Skin Neoplasms -- immunology
KW  - Melanoma -- secondary
KW  - Interleukin-2 -- therapeutic use
KW  - Melanoma -- drug therapy
KW  - Diphtheria Toxin -- therapeutic use
KW  - Melanoma -- immunology
KW  - Antineoplastic Agents -- therapeutic use
KW  - Skin Neoplasms -- secondary
KW  - T-Lymphocytes, Regulatory -- immunology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+immunotherapy+%28Hagerstown%2C+Md.+%3A+1997%29&rft.atitle=Inability+of+a+fusion+protein+of+IL-2+and+diphtheria+toxin+%28Denileukin+Diftitox%2C+DAB389IL-2%2C+ONTAK%29+to+eliminate+regulatory+T+lymphocytes+in+patients+with+melanoma.&rft.au=Attia%2C+Peter%3BMaker%2C+Ajay+V%3BHaworth%2C+Leah+R%3BRogers-Freezer%2C+Linda%3BRosenberg%2C+Steven+A&rft.aulast=Attia&rft.aufirst=Peter&rft.date=2005-11-01&rft.volume=28&rft.issue=6&rft.spage=582&rft.isbn=&rft.btitle=&rft.title=Journal+of+immunotherapy+%28Hagerstown%2C+Md.+%3A+1997%29&rft.issn=15249557&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-04-28
N1  - Date created - 2005-10-14
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
J Immunol. 2004 Feb 1;172(3):1531-9 [14734731]
Am J Health Syst Pharm. 2005 Feb 15;62(4):391-6 [15745891]
Novartis Found Symp. 2004;256:149-52; discussion 152-7, 259-69 [15027488]
Annu Rev Immunol. 2004;22:531-62 [15032588]
Semin Immunol. 2004 Apr;16(2):73-80 [15036230]
Semin Immunol. 2004 Apr;16(2):135-43 [15036237]
J Immunol. 2004 May 1;172(9):5213-21 [15100259]
Br J Haematol. 2004 Jul;126(1):81-4 [15198736]
Int Immunol. 2004 Aug;16(8):1189-201 [15237110]
Blood. 2004 Aug 15;104(4):1224-6 [15113758]
J Clin Oncol. 2004 Oct 15;22(20):4095-102 [15353540]
Fed Proc. 1976 Jul;35(9):2067-72 [1084293]
Immunogenetics. 1981;14(1-2):15-27 [7035348]
J Exp Med. 1988 Feb 1;167(2):612-22 [3126255]
J Immunol. 1989 Jan 15;142(2):471-80 [2783437]
J Natl Cancer Inst. 2000 Feb 2;92(3):205-16 [10655437]
J Exp Med. 2000 Jul 17;192(2):303-10 [10899917]
Nat Genet. 2001 Jan;27(1):20-1 [11137993]
J Clin Oncol. 2001 Jan 15;19(2):376-88 [11208829]
J Immunol. 2001 Aug 1;167(3):1245-53 [11466340]
J Clin Oncol. 2001 Aug 1;19(15):3477-82 [11481353]
Immunogenetics. 2001 Aug;53(6):435-9 [11685453]
Clin Lymphoma. 2000 Sep;1(2):110-6; discussion 117 [11707818]
Clin Lymphoma. 2000 Nov;1 Suppl 1:S27-31 [11707860]
Curr Opin Pediatr. 2001 Dec;13(6):533-8 [11753102]
Arthritis Res. 2002;4(4):241-6 [12106494]
J Clin Invest. 2002 Jul;110(2):185-92 [12122110]
J Immunol. 2002 Sep 1;169(5):2756-61 [12193750]
J Immunol. 2002 Oct 15;169(8):4183-9 [12370347]
Science. 2002 Oct 25;298(5594):850-4 [12242449]
J Immunol. 2002 Dec 1;169(11):6210-7 [12444126]
J Immunother. 2003 Jan-Feb;26(1):85-93 [12514432]
Adv Dermatol. 2002;18:29-43 [12528401]
Eur J Immunol. 2002 Nov;32(11):3267-75 [12555672]
Nat Immunol. 2003 Apr;4(4):330-6 [12612578]
Cancer Chemother Biol Response Modif. 2002;20:301-13 [12703211]
Expert Opin Biol Ther. 2003 Feb;3(1):179-86 [12718740]
Cancer Immun. 2002 Feb 22;2:1 [12747746]
Leuk Lymphoma. 2003 Apr;44(4):731-3 [12769354]
Proc Natl Acad Sci U S A. 2003 Jul 8;100(14):8372-7 [12826605]
Nat Rev Cancer. 2003 Sep;3(9):666-75 [12951585]
Clin Cancer Res. 2003 Sep 1;9(10 Pt 1):3555-61 [14506141]
J Leukoc Biol. 2003 Oct;74(4):471-8 [14519757]
Protein Eng. 1987 Dec;1(6):493-8 [3334101]
Ann Surg. 1989 Oct;210(4):474-84; discussion 484-5 [2679456]
Proc Natl Acad Sci U S A. 1989 Dec;86(23):9485-8 [2594781]
Nature. 1992 May 21;357(6375):216-22 [1589020]
J Exp Med. 1996 Aug 1;184(2):387-96 [8760792]
Essays Biochem. 1995;30:119-31 [8822152]
Blood. 1998 Jan 15;91(2):399-405 [9427692]
J Immunol. 1998 Feb 1;160(3):1212-8 [9570536]
Am J Hematol. 1998 May;58(1):87-90 [9590158]
Curr Top Microbiol Immunol. 1998;234:63-81 [9670613]
Ann Surg. 1998 Sep;228(3):307-19 [9742914]
Methods Mol Med. 2005;109:285-96 [15585928]
J Immunol. 2005 Jan 1;174(1):90-8 [15611231]
Infect Immun. 2005 Jan;73(1):523-31 [15618192]
J Immunother. 2005 Mar-Apr;28(2):120-8 [15725955]
J Immunol. 2005 Mar 1;174(5):2591-601 [15728465]
J Surg Res. 2005 Mar;124(1):151-7 [15734494]
Immunity. 2004 Jan;20(1):107-18 [14738769]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Cytotoxic T-lymphocyte-associated antigen-4 blockage can induce autoimmune hypophysitis in patients with metastatic melanoma and renal cancer.
AN  - 68688511; 16224277
AB  - Cytotoxic T-lymphocyte-associated antigen-4 (CTLA-4) is an immunoregulatory molecule expressed by activated T cells and resting CD4CD25 T cells. In patients with advanced melanoma, our group reported that administration of anti-CTLA-4 antibody mediated objective cancer regression in 13% of patients. This study also established that the blockade of CTLA-4 was associated with grade III/IV autoimmune manifestations that included dermatitis, enterocolitis, hepatitis, uveitis, and a single case of hypophysitis. Since this initial report, 7 additional patients with anti-CTLA-4 antibody-induced autoimmune hypophysitis have been accumulated. The characteristics, clinical course, laboratory values, radiographic findings, and treatment of these 8 patients are the focus of this report.
JF  - Journal of immunotherapy (Hagerstown, Md. : 1997)
AU  - Blansfield, Joseph A
AU  - Beck, Kimberly E
AU  - Tran, Khoi
AU  - Yang, James C
AU  - Hughes, Marybeth S
AU  - Kammula, Udai S
AU  - Royal, Richard E
AU  - Topalian, Suzanne L
AU  - Haworth, Leah R
AU  - Levy, Catherine
AU  - Rosenberg, Steven A
AU  - Sherry, Richard M
AD  - Surgery Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892-1201, USA.
PY  - 2005
SP  - 593
EP  - 598
VL  - 28
IS  - 6
SN  - 1524-9557, 1524-9557
KW  - Antibodies, Monoclonal
KW  - 0
KW  - Antigens, CD
KW  - Antigens, Differentiation
KW  - CTLA-4 Antigen
KW  - CTLA4 protein, human
KW  - Index Medicus
KW  - Magnetic Resonance Imaging
KW  - Kidney Neoplasms -- drug therapy
KW  - Kidney Neoplasms -- pathology
KW  - Humans
KW  - Melanoma -- secondary
KW  - Skin Neoplasms -- pathology
KW  - Carcinoma, Renal Cell -- drug therapy
KW  - Skin Neoplasms -- drug therapy
KW  - Adult
KW  - Carcinoma, Renal Cell -- secondary
KW  - Melanoma -- drug therapy
KW  - Neoplasm Metastasis
KW  - Middle Aged
KW  - Male
KW  - Pituitary Gland -- pathology
KW  - Antigens, Differentiation -- immunology
KW  - Autoimmune Diseases -- pathology
KW  - Autoimmune Diseases -- therapy
KW  - Autoimmune Diseases -- chemically induced
KW  - Autoimmune Diseases -- blood
KW  - Antibodies, Monoclonal -- adverse effects
KW  - Antibodies, Monoclonal -- administration & dosage
KW  - Pituitary Gland -- drug effects
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68688511?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+immunotherapy+%28Hagerstown%2C+Md.+%3A+1997%29&rft.atitle=Cytotoxic+T-lymphocyte-associated+antigen-4+blockage+can+induce+autoimmune+hypophysitis+in+patients+with+metastatic+melanoma+and+renal+cancer.&rft.au=Blansfield%2C+Joseph+A%3BBeck%2C+Kimberly+E%3BTran%2C+Khoi%3BYang%2C+James+C%3BHughes%2C+Marybeth+S%3BKammula%2C+Udai+S%3BRoyal%2C+Richard+E%3BTopalian%2C+Suzanne+L%3BHaworth%2C+Leah+R%3BLevy%2C+Catherine%3BRosenberg%2C+Steven+A%3BSherry%2C+Richard+M&rft.aulast=Blansfield&rft.aufirst=Joseph&rft.date=2005-11-01&rft.volume=28&rft.issue=6&rft.spage=593&rft.isbn=&rft.btitle=&rft.title=Journal+of+immunotherapy+%28Hagerstown%2C+Md.+%3A+1997%29&rft.issn=15249557&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-04-28
N1  - Date created - 2005-10-14
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Proc Natl Acad Sci U S A. 2003 Apr 15;100(8):4712-7 [12682289]
Nature. 2003 May 29;423(6939):506-11 [12724780]
Proc Natl Acad Sci U S A. 2003 Jul 8;100(14):8372-7 [12826605]
Singapore Med J. 2004 Feb;45(2):93-4 [14985851]
Neurosurgery. 1995 May;36(5):1016-9 [7791966]
J Clin Endocrinol Metab. 1995 Aug;80(8):2302-11 [7629223]
J Clin Oncol. 2005 Sep 1;23(25):6043-53 [16087944]
Science. 1995 Nov 10;270(5238):985-8 [7481803]
Immunity. 1995 Nov;3(5):541-7 [7584144]
Immunity. 1997 Dec;7(6):885-95 [9430233]
J Clin Endocrinol Metab. 1999 Mar;84(3):844-52 [10084559]
J Neurol Neurosurg Psychiatry. 1999 Sep;67(3):398-402 [10449568]
J Clin Oncol. 2005 Feb 1;23(4):741-50 [15613700]
Immunol Today. 1995 Jun;16(6):289-94 [7662098]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Conversion of Fas-resistant to Fas-sensitive MCF-7 breast cancer cells by the synergistic interaction of interferon-gamma and all-trans retinoic acid.
AN  - 68670557; 16136269
AB  - The membrane receptor Fas (Apo-1/CD95) is an important initiator of programmed cell death induced by anti-Fas antibody or Fas ligand. MCF-7 human breast cancer cells have low levels of Fas receptor (FasR) and are resistant to anti-FasR antibody mediated apoptosis, however two naturally occurring substances, interferon and all-trans retinoic acid (AT), act synergistically to enhance antiproliferative processes in these cells, suggesting this combination may also be an effective means for enhancing FasR expression. When this was studied, it was found that IFN-gamma and AT in combination acted synergistically to induce expression of FasR mRNA and FasR protein in a time-dependent and dose-dependent manner. This induction required continuous protein synthesis, and STAT1 protein, but not PKR or TR1 protein, was induced in a manner quantitatively and temporally related to FasR protein induction, and consistent with STAT1 mediation of the synergistic effect of IFN-gamma and AT on FasR expression. FasR-induced cells were resistant to stimulation of apoptosis by anti-FasR antibody, however treatment with cycloheximide rendered these cells sensitive to antibody-induced apoptosis, suggesting endogenous blockade to signaling. These cells did not express caspase 3, or FLIP(L), but strongly expressed the endogenous inhibitor of apoptosis Bcl-2, indicating a type II Fas signaling pathway. Expression of these proteins was not modulated by IFN/AT, however treatment of Fas-induced cells with Bcl-2 specific small interfering RNA (SiRNA) downregulated Bcl-2 protein expression and rendered these cells sensitive to the cytotoxic effects of anti-Fas antibody. These findings indicate that IFN-gamma+AT in combination modulate Fas signaling and provide a novel mechanism for the promotion of cell death in breast cancer cells.
JF  - Breast cancer research and treatment
AU  - Danforth, David N
AU  - Zhu, Yuelin
AD  - Surgery Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA. David_Danforth@nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 81
EP  - 91
VL  - 94
IS  - 1
SN  - 0167-6806, 0167-6806
KW  - Antigens, CD95
KW  - 0
KW  - Proto-Oncogene Proteins c-bcl-2
KW  - Tretinoin
KW  - 5688UTC01R
KW  - Interferon-gamma
KW  - 82115-62-6
KW  - Index Medicus
KW  - Dose-Response Relationship, Drug
KW  - Proto-Oncogene Proteins c-bcl-2 -- drug effects
KW  - Humans
KW  - Signal Transduction -- drug effects
KW  - Apoptosis -- drug effects
KW  - Cell Line, Tumor
KW  - Drug Synergism
KW  - Time Factors
KW  - Statistics, Nonparametric
KW  - Breast Neoplasms -- drug therapy
KW  - Tretinoin -- pharmacology
KW  - Interferon-gamma -- pharmacology
KW  - Antigens, CD95 -- drug effects
KW  - Drug Resistance, Neoplasm -- drug effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-27
N1  - Date created - 2005-10-10
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Induction of suppressors of cytokine signaling (SOCS) in the retina during experimental autoimmune uveitis (EAU): potential neuroprotective role of SOCS proteins.
AN  - 68666909; 16154209
AB  - Suppressors of cytokine signaling (SOCS) are implicated in immunopathogenic mechanisms of autoimmune diseases. We show here that SOCS expression in retina is temporarily correlated with progression of experimental autoimmune uveitis (EAU), an organ-specific autoimmune disease that serves as model of human uveitis. Peak of EAU correlates with highest SOCS genes expression while disease resolution coincides with their down-regulation. Surprisingly, SOCS5 is constitutively expressed in retina. SOCS5 expression increases significantly during EAU and remains elevated even after disease resolution. Our data suggest that cytokine-inducible SOCS members may be involved in negative regulation of inflammatory cytokines activities during EAU, while constitutively expressed SOCS5 may have neuroprotective functions.
JF  - Journal of neuroimmunology
AU  - Takase, H
AU  - Yu, C-R
AU  - Liu, X
AU  - Fujimoto, C
AU  - Gery, I
AU  - Egwuagu, C E
AD  - Experimental Immunology Section, Laboratory of Immunology, National Eye Institute, National Institutes of Health, Building 10, Room 10N116, 10 Center Drive, Bethesda, Maryland 20892-1857, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 118
EP  - 127
VL  - 168
IS  - 1-2
SN  - 0165-5728, 0165-5728
KW  - Antigens, CD4
KW  - 0
KW  - Cytokines
KW  - Neuroprotective Agents
KW  - RNA, Messenger
KW  - Retinol-Binding Proteins
KW  - Suppressor of Cytokine Signaling Proteins
KW  - interphotoreceptor retinoid binding protein, rat
KW  - Index Medicus
KW  - Gene Expression -- drug effects
KW  - Animals
KW  - Disease Models, Animal
KW  - Blotting, Western -- methods
KW  - Mice
KW  - Reverse Transcriptase Polymerase Chain Reaction -- methods
KW  - Cell Proliferation
KW  - RNA, Messenger -- biosynthesis
KW  - Antigens, CD4 -- metabolism
KW  - Enzyme-Linked Immunosorbent Assay -- methods
KW  - T-Lymphocytes -- metabolism
KW  - Electrophoretic Mobility Shift Assay -- methods
KW  - Time Factors
KW  - Uveitis -- prevention & control
KW  - Retina -- metabolism
KW  - Cytokines -- genetics
KW  - Retina -- physiology
KW  - Retina -- drug effects
KW  - Cytokines -- metabolism
KW  - Neuroprotective Agents -- pharmacology
KW  - Suppressor of Cytokine Signaling Proteins -- pharmacology
KW  - Signal Transduction -- physiology
KW  - Suppressor of Cytokine Signaling Proteins -- therapeutic use
KW  - Uveitis -- metabolism
KW  - Neuroprotective Agents -- therapeutic use
KW  - Uveitis -- chemically induced
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-17
N1  - Date created - 2005-10-07
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Differential expression of CYP1A, 2B, and 3A genes in the F344 rat following exposure to a polybrominated diphenyl ether mixture or individual components.
AN  - 68658074; 16107549
AB  - Polybrominated diphenyl ethers (PBDEs), used as flame retardants, have been detected in the environment and in mammalian tissues and fluids. Evidence indicates that PBDE mixtures induce CYPs through aryl hydrocarbon receptor (AhR)-dependent and -independent pathways. The present work has investigated the effects of individual components of a commercial PBDE mixture (DE71) on expression of CYP1A1, a biomarker for activation of the AhR (dioxin-like), and CYP2B and CYP3A, biomarkers for activation of the constitutive androstane and pregnanexreceptors (CAR and PXR), respectively, in the rat. Male F344 rats were dosed orally on three consecutive days with either DE71, PBDE components, 2,2',4,4'-tetraBDE (BDE47), 2,2',4,4',5-pentaBDE (BDE99), 2,2',4,4',5,5'-hexaBDE (BDE153), representative polybrominated dibenzofurans (PBDFs) present in DE71, or reference PCBs. Differential expression of target genes was determined in liver 24 h after the last dose. Quantitative PCR analysis indicated up-regulation of CYP1A1 by DE71; however, the response was weak compared to that for dioxin-like PCB126. Individual PBDE components of DE71 up-regulated CYP1A1 only at the highest administered dose (100 micromol/kg/day). Representative PBDFs efficiently up-regulated CYP1A1; therefore, they, along with other PBDFs and polybrominated dibenzodioxins detected in DE71 and individual PBDE components, may be responsible for most, if not all, dioxin-like properties previously observed for PBDEs. Conversely, PBDEs appear capable of up-regulating CYP2B and CYP3A in rats at doses similar to that for non-dioxin-like PCB153. These results indicate that in vivo PBDE-mediated toxicity would be better categorized by AhR-independent mechanisms, rather than the well-characterized AhR-dependent mechanism associated with exposure to dioxin-like chemicals.
JF  - Toxicological sciences : an official journal of the Society of Toxicology
AU  - Sanders, J M
AU  - Burka, L T
AU  - Smith, C S
AU  - Black, W
AU  - James, R
AU  - Cunningham, M L
AD  - Laboratory of Pharmacology and Chemistry, National Institute of Environmental Health Sciences (NIEHS), Research Triangle Park, North Carolina 27709, USA. sander10@niehs.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 127
EP  - 133
VL  - 88
IS  - 1
SN  - 1096-6080, 1096-6080
KW  - Complex Mixtures
KW  - 0
KW  - Flame Retardants
KW  - Halogenated Diphenyl Ethers
KW  - Phenyl Ethers
KW  - Polybrominated Biphenyls
KW  - RNA, Messenger
KW  - pentabromodiphenyl ether
KW  - 7REL09ZX35
KW  - Aryl Hydrocarbon Hydroxylases
KW  - EC 1.14.14.1
KW  - Cytochrome P-450 CYP1A1
KW  - Cytochrome P-450 CYP2B1
KW  - Cytochrome P-450 CYP3A
KW  - Oxidoreductases, N-Demethylating
KW  - EC 1.5.-
KW  - Index Medicus
KW  - Rats
KW  - Administration, Oral
KW  - Animals
KW  - Rats, Inbred F344
KW  - RNA, Messenger -- metabolism
KW  - Up-Regulation
KW  - Reverse Transcriptase Polymerase Chain Reaction
KW  - Male
KW  - Oxidoreductases, N-Demethylating -- genetics
KW  - Cytochrome P-450 CYP2B1 -- genetics
KW  - Cytochrome P-450 CYP1A1 -- genetics
KW  - Aryl Hydrocarbon Hydroxylases -- metabolism
KW  - Phenyl Ethers -- toxicity
KW  - Gene Expression Regulation, Enzymologic -- drug effects
KW  - Cytochrome P-450 CYP2B1 -- metabolism
KW  - Cytochrome P-450 CYP1A1 -- metabolism
KW  - Aryl Hydrocarbon Hydroxylases -- genetics
KW  - Polybrominated Biphenyls -- toxicity
KW  - Oxidoreductases, N-Demethylating -- metabolism
KW  - Flame Retardants -- toxicity
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-15
N1  - Date created - 2005-10-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - A comparison of a prototype PCR assay and hybrid capture 2 for detection of carcinogenic human papillomavirus DNA in women with equivocal or mildly abnormal papanicolaou smears.
AN  - 68649093; 16203281
AB  - We evaluated Hybrid Capture 2 (HC2) and polymerase chain reaction (PCR) results for paired specimens collected at 19,187 visits from 5,026 of 5,060 women participating in the Atypical Squamous Cells of Undetermined Significance/Low-Grade Squamous Intraepithelial Lesion Triage Study (ALTS). We examined the test agreement between HC2 and PCR detection for any of 13 carcinogenic human papillomavirus types targeted by HC2 and compared clinical performance of the 2 tests for detecting concurrent and follow-up cervical intraepithelial neoplasia (CIN) 3 or cancer. The k value for the 2 assays was 0.65 (95% confidence interval, 0.64-0.66), with 82.7% crude agreement. HC2 was more sensitive (93.6% vs 89.3%; P < .0005) but less specific (41.2% vs 48.5%; P < .0005) than PCR for detecting 2-year cumulative CIN 3 or cancer (n = 503). The presence of multiple types as detected by PCR and/or cytologic abnormality increased the likelihood of an HC2+ result. Increased sensitivity of HC2 compared with PCR was surprising, given the theoretical advantages of PCR-based methods for analytic sensitivity. Smaller amounts of material used in PCR could have limited its sensitivity, but our results demonstrate the importance of optimization and standardization of PCR-based assays for clinical applications.
JF  - American journal of clinical pathology
AU  - Schiffman, Mark
AU  - Wheeler, Cosette M
AU  - Dasgupta, Abhijit
AU  - Solomon, Diane
AU  - Castle, Philip E
AU  - ALTS Group
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Department of Health and Human Services, Bethesda, MD 20892-7234, USA. ; ALTS Group
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 722
EP  - 732
VL  - 124
IS  - 5
SN  - 0002-9173, 0002-9173
KW  - DNA, Viral
KW  - 0
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Aged, 80 and over
KW  - Humans
KW  - Adult
KW  - Aged
KW  - Middle Aged
KW  - Adolescent
KW  - Female
KW  - Papillomavirus Infections -- diagnosis
KW  - DNA, Viral -- analysis
KW  - Papillomaviridae -- isolation & purification
KW  - Polymerase Chain Reaction -- methods
KW  - Uterine Cervical Neoplasms -- diagnosis
KW  - Vaginal Smears
KW  - Papillomaviridae -- genetics
KW  - Cervical Intraepithelial Neoplasia -- diagnosis
KW  - Papanicolaou Test
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-22
N1  - Date created - 2005-10-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Antitumor activity and distribution of pyrroloiminoquinones in the sponge genus Zyzzya.
AN  - 68623094; 16009557
AB  - A detailed analysis of four different collections of the sponge genus Zyzzya yielded nine pyrroloiminoquinones of the makaluvamine, batzelline, and isobatzelline/damirone classes. Dereplication analyses of additional Zyzzya extracts did not disclose more potent or additional new compounds. Comparative testing of these compounds in the National Cancer Institute's 60 cell line human tumor screen revealed varying levels of potency and differential cytotoxicity, apparently related to the unsaturation levels in and substitution patterns on the core ring system. Further studies on the topoisomerase II-mediated DNA cleavage were conducted. Reductive activation of the pyrroloiminoquinones led to DNA damage in vitro, which correlated with half wave potentials and reversibility parameters. DNA damage could be abrogated by ascorbate. Fluorescence displacement was used to measure intercalation with DNA; intercalation efficiency did not correlate with DNA-damaging proficiency. Makaluvamine H (5) emerged as the most potent and differential of our isolates, roughly comparable to makaluvamines C (in vitro) and I (in vivo). 3,7-Dimethyl guanine was isolated from one of the Zyzzya collections and from the sponge Latrunculia purpurea.
JF  - Bioorganic & medicinal chemistry
AU  - Dijoux, Marie-Geneviève
AU  - Schnabel, Peter C
AU  - Hallock, Yali F
AU  - Boswell, Jamie L
AU  - Johnson, Tanya R
AU  - Wilson, Jennifer A
AU  - Ireland, Chris M
AU  - van Soest, Rob
AU  - Boyd, Michael R
AU  - Barrows, Louis R
AU  - Cardellina, John H
AD  - Laboratory of Drug Discovery Research and Development, Developmental Therapeutics Program, Division of Cancer Treatment and Diagnosis, National Cancer Institute-Frederick Cancer Research & Development Center, Frederick, MD 21702-1201, USA.
Y1  - 2005/11/01/
PY  - 2005
DA  - 2005 Nov 01
SP  - 6035
EP  - 6044
VL  - 13
IS  - 21
SN  - 0968-0896, 0968-0896
KW  - Antineoplastic Agents
KW  - 0
KW  - Pyrroloiminoquinones
KW  - DNA
KW  - 9007-49-2
KW  - Index Medicus
KW  - Molecular Structure
KW  - Animals
KW  - Spectrometry, Fluorescence
KW  - Humans
KW  - DNA -- metabolism
KW  - DNA -- chemistry
KW  - Cell Line, Tumor
KW  - Inhibitory Concentration 50
KW  - Magnetic Resonance Spectroscopy
KW  - DNA -- drug effects
KW  - Pyrroloiminoquinones -- isolation & purification
KW  - Antineoplastic Agents -- isolation & purification
KW  - Porifera -- chemistry
KW  - Antineoplastic Agents -- chemistry
KW  - Pyrroloiminoquinones -- chemistry
KW  - Antineoplastic Agents -- pharmacology
KW  - Pyrroloiminoquinones -- pharmacology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-23
N1  - Date created - 2005-09-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Twelve-Month Prevalence and Changes in Driving after Drinking: United States, 1991-1992 and 2001-2002
AN  - 59984061; 200605891
AB  - Background: Drinking & driving has been identified as one of the most important contributors of motor vehicle fatalities. This paper addressed the existing gap in our public health knowledge regarding the current prevalence of driving after drinking & how this has changed over the past decade. Methods: Prevalence rates of drinking & driving in 2001-2002, & changes in those prevalence rates between 1991-1992 & 2001-2002 were examined in two large nationally representative surveys of the U.S. population. Results: Overall, the prevalence of driving after drinking was 2.9% in 2001-2002 representing approximately six million U.S. adults. This rate was about three quarters of the rate observed in 1991-1992 (3.7%), reflecting a 22% reduction. Generally, the male-female differentials in the rate of driving after drinking decreased over the past decade. However, the sex ratios increased substantially for underaged youth over the past decade, reflecting the sharp decrease in prevalence of driving after drinking among 18-20-year-old women. Constant & emerging subgroups at high risk for drinking & driving included Whites, Native Americans, males, underaged young adults & 21-25-year-olds. Conclusions: The results of this study highlighted the need to continue to monitor prevalence & changes in driving after drinking. Results are discussed in the context of strengthening existing prevention & intervention efforts & developing new programs with the sociodemographic differentials observed in this study in mind. Tables, References. [Copyright 2006 Elsevier Ireland Ltd.]
JF  - Drug and Alcohol Dependence
AU  - Chou, S Patricia
AU  - Grant, Bridget F
AU  - Dawson, Deborah A
AU  - Stinson, Frederick S
AU  - Saha, Tulshi
AU  - Pickering, Roger P
AD  - Laboratory Epidemiology & Biometry, Division Intramural Clnical & Biological Research, National Instit Alcohol Abuse & Alcoholism, National Instit Health, Dept Health & Human Services, Bethesda, MD pchou@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 223
EP  - 230
PB  - Elsevier Ireland, Amsterdam The Netherlands
VL  - 80
IS  - 2
SN  - 0376-8716, 0376-8716
KW  - Alcohol-impaired driving
KW  - Drinking and driving
KW  - Sociodemographic characteristics
KW  - High-risk subgroups
KW  - Changes in Drinking and Driving
KW  - Fatalities
KW  - Drinking Behavior
KW  - United States of America
KW  - Young Adults
KW  - Automobiles
KW  - Sociodemographic Characteristics
KW  - article
KW  - 2079: sociology of health and medicine; substance use/abuse & compulsive behaviors (drug abuse, addiction, alcoholism, gambling, eating disorders, etc.)
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LA  - English
DB  - Sociological Abstracts
N1  - Date revised - 2007-04-01
N1  - Last updated - 2016-09-28
N1  - CODEN - DADEDV
N1  - SubjectsTermNotLitGenreText - Automobiles; Drinking Behavior; Sociodemographic Characteristics; United States of America; Young Adults; Fatalities
DO  - http://dx.doi.org/10.1016/j.drugalcdep.2005.03.013
ER  - 



TY  - JOUR
T1  - Reducing HIV/AIDS and Criminal Justice Involvement in African Americans as a Consequence of Drug Abuse
AN  - 57147708; 200602337
AB  - Despite a similarity in drug use across ethnic groups in the United States, there are differences in the impact of drug involvement on the health and well being of racial/ethnic minority groups. For instance, minority and ethnic groups are at higher risk for addiction than their white counterparts. African Americans have disproportionately experienced the negative impacts of substance use, including high addiction rates, HIV/AIDS infection rates and criminal justice involvement. D. Miller
JF  - Journal of Health Care for the Poor and Underserved
AU  - Beatty, Lula
AU  - Jones, Dionne
AU  - Doctor, LeKhessa
AD  - Special Populations Office, National Instit Drug Abuse, National Instits Health, Bethesda, MD lbeatty@nida.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1
EP  - 5
VL  - 16
IS  - supp B
SN  - 1049-2089, 1049-2089
KW  - Black American people
KW  - Criminal justice
KW  - AIDS
KW  - HIV
KW  - Drug addiction
KW  - Drug abuse
KW  - article
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aassia&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Health+Care+for+the+Poor+and+Underserved&rft.atitle=Reducing+HIV%2FAIDS+and+Criminal+Justice+Involvement+in+African+Americans+as+a+Consequence+of+Drug+Abuse&rft.au=Beatty%2C+Lula%3BJones%2C+Dionne%3BDoctor%2C+LeKhessa&rft.aulast=Beatty&rft.aufirst=Lula&rft.date=2005-11-01&rft.volume=16&rft.issue=supp+B&rft.spage=1&rft.isbn=&rft.btitle=&rft.title=Journal+of+Health+Care+for+the+Poor+and+Underserved&rft.issn=10492089&rft_id=info:doi/
LA  - English
DB  - Applied Social Sciences Index & Abstracts (ASSIA)
N1  - Date revised - 2006-04-07
N1  - Last updated - 2016-09-27
N1  - CODEN - JHCUEK
N1  - SubjectsTermNotLitGenreText - Black American people; Drug abuse; Drug addiction; HIV; AIDS; Criminal justice
ER  - 



TY  - JOUR
T1  - Oral Language and Reading: Reply to Bracken (2005)
AN  - 57147221; 200604056
AB  - Early language competence in preschool relates both directly & indirectly to elementary school reading in both 1st & 3rd grades. Further, comprehensive language skills are more strongly related to early reading than are vocabulary scores alone. In response to a challenge by S. A. Bracken (2005), the current article reaffirms the National Institute of Child Health & Human Development Early Child Care Research Network's (2005) findings. 9 References. [Copyright 2005 American Psychological Association]
JF  - Developmental Psychology
AU  - Steering Committee
AD  - Steering Committee; National Instit of Child Health & Human Development Early Child Care Research Network, NICHD Rockville, MD
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 1000
EP  - 1002
VL  - 41
IS  - 6
SN  - 0012-1649, 0012-1649
KW  - emergent literacy, language, literacy
KW  - Young children
KW  - Language skills
KW  - Preschool children
KW  - Early childhood education
KW  - Literacy skills
KW  - article
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/57147221?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aassia&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Developmental+Psychology&rft.atitle=Oral+Language+and+Reading%3A+Reply+to+Bracken+%282005%29&rft.au=Steering+Committee&rft.aulast=Steering+Committee&rft.aufirst=&rft.date=2005-11-01&rft.volume=41&rft.issue=6&rft.spage=1000&rft.isbn=&rft.btitle=&rft.title=Developmental+Psychology&rft.issn=00121649&rft_id=info:doi/
LA  - English
DB  - Applied Social Sciences Index & Abstracts (ASSIA)
N1  - Date revised - 2006-04-07
N1  - Last updated - 2016-09-27
N1  - CODEN - DEVPA9
N1  - SubjectsTermNotLitGenreText - Preschool children; Young children; Language skills; Literacy skills; Early childhood education
ER  - 



TY  - JOUR
T1  - Validation of Scales Measuring Attitudes and Norms Related to Mammography Screening in Women Veterans
AN  - 57143080; 200605812
AB  - Validation of psychosocial measures for use in mammography screening research has been given inadequate attention in the literature. The authors report on the validation of 5 measures examining 4 attitudinal constructs (i.e., pros, cons, outcome expectations, & cancer worries) & 1 social influence construct (i.e., subjective norms) in a 22-item inventory. The study participants consisted of a national, randomly sampled population of women veterans (n = 2,910). After minor revision of scales, the authors found independent measures for 4 constructs: pros, cons, cancer worries, & subjective norms. The authors concluded that these scales have acceptable psychometric properties; support construct validity; & provide brief, reliable, & valid measures of attitudes toward & norms regarding mammography screening. These scales may be useful for intervention research. 5 Tables, 1 Figure, 1 Appendix, 79 References. [Copyright 2005 The American Psychological Association.]
JF  - Health Psychology
AU  - Tiro, Jasmin A
AU  - Diamond, Pamela M
AU  - Perz, Catherine A
AU  - Fernandez, Maria
AU  - Rakowski, William
AU  - DiClemente, Carlo C
AU  - Vernon, Sally W
AD  - Division Cancer Control & Population Sciences, National Cancer Instit, Bethesda, MD tiroj@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 555
EP  - 566
PB  - American Psychological Association, Washington DC
VL  - 24
IS  - 6
SN  - 0278-6133, 0278-6133
KW  - mammography, attitudes, subjective norms, construct validation
KW  - Norms
KW  - Attitudes
KW  - Mammography
KW  - Women
KW  - Construct validity
KW  - Psychometrics
KW  - article
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/57143080?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aassia&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Health+Psychology&rft.atitle=Validation+of+Scales+Measuring+Attitudes+and+Norms+Related+to+Mammography+Screening+in+Women+Veterans&rft.au=Tiro%2C+Jasmin+A%3BDiamond%2C+Pamela+M%3BPerz%2C+Catherine+A%3BFernandez%2C+Maria%3BRakowski%2C+William%3BDiClemente%2C+Carlo+C%3BVernon%2C+Sally+W&rft.aulast=Tiro&rft.aufirst=Jasmin&rft.date=2005-11-01&rft.volume=24&rft.issue=6&rft.spage=555&rft.isbn=&rft.btitle=&rft.title=Health+Psychology&rft.issn=02786133&rft_id=info:doi/10.1037%2F0278-6133.24.6.555
LA  - English
DB  - Applied Social Sciences Index & Abstracts (ASSIA)
N1  - Date revised - 2006-05-02
N1  - Last updated - 2016-09-27
N1  - SubjectsTermNotLitGenreText - Mammography; Attitudes; Psychometrics; Women; Construct validity; Norms
DO  - http://dx.doi.org/10.1037/0278-6133.24.6.555
ER  - 



TY  - JOUR
T1  - Unraveling Health Disparities: Examining the Dimensions of Hypertension and Diabetes through Community Engagement
AN  - 57119655; 200602254
AB  - The contexts of people's lives can perpetuate racial & ethnic health disparities. In this work, community members from four racial/ethnic groups (Hispanic, Native American, African American, Asian) engaged in an investigative process to analyze their own life conditions, & to explore dimensions of their health behaviors & lifestyles when managing diabetes &/or hypertension. Principal conclusions of the researchers: (1) Respondents were knowledgeable about their health conditions, but had no knowledge of health disparities. (2) Respondents felt the media portrays members of racial/ethnic minorities as hopeless & helpless; this discourages them from believing they can live healthier or better lives. (3) The over-abundance of fast food & unhealthy food eateries in minority communities contradicts the advice of the public health industry. (4) The majority of all respondents were in one of two stages relative to their willingness to change unhealthy behaviors: not interested or already doing it. 9 Figures, 1 Appendix. [Reprinted by permission of Sage Publications Inc., copyright 2005.]
JF  - Journal of Health Care for the Poor and Underserved
AU  - Anderson, Julia B
AD  - National Instit Child Health & Human Development, National Instits Health, Bethesda, MD Andersju@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 91
EP  - 117
VL  - 16
IS  - supplement A
SN  - 1049-2089, 1049-2089
KW  - Health disparities, community-based participatory research, stages of change, health attitudes and beliefs
KW  - Health inequalities
KW  - Health beliefs
KW  - Community participation
KW  - Ethnic groups
KW  - Hypertension
KW  - Diabetes
KW  - article
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/57119655?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aassia&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Health+Care+for+the+Poor+and+Underserved&rft.atitle=Unraveling+Health+Disparities%3A+Examining+the+Dimensions+of+Hypertension+and+Diabetes+through+Community+Engagement&rft.au=Anderson%2C+Julia+B&rft.aulast=Anderson&rft.aufirst=Julia&rft.date=2005-11-01&rft.volume=16&rft.issue=supplement+A&rft.spage=91&rft.isbn=&rft.btitle=&rft.title=Journal+of+Health+Care+for+the+Poor+and+Underserved&rft.issn=10492089&rft_id=info:doi/
LA  - English
DB  - Applied Social Sciences Index & Abstracts (ASSIA)
N1  - Date revised - 2006-04-07
N1  - Last updated - 2016-09-27
N1  - CODEN - JHCUEK
N1  - SubjectsTermNotLitGenreText - Ethnic groups; Community participation; Health inequalities; Health beliefs; Diabetes; Hypertension
ER  - 



TY  - JOUR
T1  - Oral language and reading: reply to Bracken (2005)
AN  - 38200459; 2988851
AB  - Early language competence in preschool relates both directly and indirectly to elementary school reading in both 1st and 3rd grades. Further, comprehensive language skills are more strongly related to early reading than are vocabulary scores alone. In response to a challenge by S. A. Bracken (2005), the current article reaffirms the National Institute of Child Health and Human Development Early Child Care Research Network's (2005) findings. Reprinted by permission of the American Psychological Association
JF  - Developmental psychology
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1000
EP  - 1002
VL  - 41
IS  - 6
SN  - 0012-1649, 0012-1649
KW  - Sociology
KW  - Reading
KW  - Oral tradition
KW  - Psychology
KW  - Language
KW  - Literacy
KW  - Public policy
KW  - Developmental psychology
KW  - Child development
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/38200459?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Developmental+psychology&rft.atitle=Oral+language+and+reading%3A+reply+to+Bracken+%282005%29&rft.au=&rft.aulast=&rft.aufirst=&rft.date=2005-11-01&rft.volume=41&rft.issue=6&rft.spage=1000&rft.isbn=&rft.btitle=&rft.title=Developmental+psychology&rft.issn=00121649&rft_id=info:doi/10.1037%2F0012-1649.41.6.1000
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 8978 12867; 7226; 10627 11713; 2197 2212 6075 3483; 7454 7353 4049; 3518 10404; 10472; 10404
DO  - http://dx.doi.org/10.1037/0012-1649.41.6.1000
ER  - 



TY  - JOUR
T1  - Theoretical and methodological issues in studying families
AN  - 38195231; 2986068
JF  - Journal of marriage and the family
AU  - White, Lynn
AU  - Matthews, Sarah H
AU  - Furstenberg, Frank F
AU  - Voydanoff, Patricia
AU  - LaRossa, Ralph
AU  - MacMillan, Ross
AU  - Copher, Ronda
AU  - O'Brien, Marion
AU  - Hofferth, Sandra L
AU  - Seltzer, Judith A
AU  - Bachrach, Christine A
AU  - Bianchi, Suzanne M
AU  - Bledsoe, Caroline H
AU  - Casper, Lynne M
AU  - Chase-Lansdale, P Lindsay
AU  - DiPrete, Thomas A
AU  - Hotz, V Joseph
AU  - Morgan, S Philip
AU  - Sanders, Seth G
AU  - Thomas, Duncan
AU  - Cheng, Simon
AU  - Powell, Brian
AU  - Small, Stephen A
AU  - Uttal, Lynet
AU  - Dodson, Lisa
AU  - Schmalzbauer, Leah
AU  - Saltzman, Linda E
AU  - Mahendra, Reshma R
AU  - Ikeda, Robin M
AU  - Ingram, Eben M
AU  - Roosa, Mark W
AU  - Deng, Shiying
AU  - Nair, Rajni L
AU  - Burrell, Ginger Lockhart
AU  - Manning, Wendy D
AU  - Smock, Pamela J
AU  - Ganong, Lawrence
AU  - Coleman, Marilyn
AU  - Acock, Alan C
AU  - Wu, Zheng
AU  - Lyons, Karen S
AU  - Sayer, Aline G
AU  - Johnson, David
AU  - Stolz, Heidi E
AU  - Barber, Brian K
AU  - Olsen, Joseph A
AD  - University of Nebraska ; Cleveland State University ; University of Pennsylvania ; University of Dayton ; Georgia State University ; University of Minnesota ; University of North Carolina ; University of Maryland ; University of California ; National Institute of Child Health and Human Development ; Northwestern University ; University of Southern California ; Columbia University ; Duke University ; University of Connecticut ; Indiana University ; University of Wisconsin ; Boston College ; Montana State University ; Centers for Disease Control and Prevention ; Arizona State University ; Bowling Green State University ; University of Michigan ; University of Missouri ; Oregon State University ; University of Victoria
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 791
EP  - 1092
VL  - 67
IS  - 4
SN  - 0022-2445, 0022-2445
KW  - Sociology
KW  - Anthropology
KW  - Longitudinal studies
KW  - Qualitative analysis
KW  - Measurement
KW  - Parent-child relations
KW  - Statistical analysis
KW  - Interracial marriages
KW  - Linear models
KW  - Sociological theory
KW  - Research methods
KW  - Regression analysis
KW  - Family relations
KW  - Applied research
KW  - Data collection
KW  - Intergenerational relations
KW  - Action research
KW  - U.S.A.
KW  - Data analysis
KW  - Error
KW  - Methodology
KW  - Family studies
KW  - Social science research
KW  - Cohabitation
KW  - Poverty
KW  - Demographic change
KW  - Domestic violence
KW  - Dyad
KW  - Bias
KW  - Homosexuals
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/38195231?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+marriage+and+the+family&rft.atitle=Theoretical+and+methodological+issues+in+studying+families&rft.au=White%2C+Lynn%3BMatthews%2C+Sarah+H%3BFurstenberg%2C+Frank+F%3BVoydanoff%2C+Patricia%3BLaRossa%2C+Ralph%3BMacMillan%2C+Ross%3BCopher%2C+Ronda%3BO%27Brien%2C+Marion%3BHofferth%2C+Sandra+L%3BSeltzer%2C+Judith+A%3BBachrach%2C+Christine+A%3BBianchi%2C+Suzanne+M%3BBledsoe%2C+Caroline+H%3BCasper%2C+Lynne+M%3BChase-Lansdale%2C+P+Lindsay%3BDiPrete%2C+Thomas+A%3BHotz%2C+V+Joseph%3BMorgan%2C+S+Philip%3BSanders%2C+Seth+G%3BThomas%2C+Duncan%3BCheng%2C+Simon%3BPowell%2C+Brian%3BSmall%2C+Stephen+A%3BUttal%2C+Lynet%3BDodson%2C+Lisa%3BSchmalzbauer%2C+Leah%3BSaltzman%2C+Linda+E%3BMahendra%2C+Reshma+R%3BIkeda%2C+Robin+M%3BIngram%2C+Eben+M%3BRoosa%2C+Mark+W%3BDeng%2C+Shiying%3BNair%2C+Rajni+L%3BBurrell%2C+Ginger+Lockhart%3BManning%2C+Wendy+D%3BSmock%2C+Pamela+J%3BGanong%2C+Lawrence%3BColeman%2C+Marilyn%3BAcock%2C+Alan+C%3BWu%2C+Zheng%3BLyons%2C+Karen+S%3BSayer%2C+Aline+G%3BJohnson%2C+David%3BStolz%2C+Heidi+E%3BBarber%2C+Brian+K%3BOlsen%2C+Joseph+A&rft.aulast=White&rft.aufirst=Lynn&rft.date=2005-11-01&rft.volume=67&rft.issue=4&rft.spage=791&rft.isbn=&rft.btitle=&rft.title=Journal+of+marriage+and+the+family&rft.issn=00222445&rft_id=info:doi/
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - SuppNotes - Collection of 21 articles
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 4783; 548 10902; 1168 10902; 10519 3279 971 3286; 10739 12228 10919; 12224 971; 3279 971 3286; 3286; 7419 8163; 7541 7537 971; 7854; 7994; 10919; 3782 5636 5676 971; 1565 1362 2688 2449 10404; 4387; 12004 12008; 11919 10902; 3407 3412 9859; 4777 6093; 9178 4777 6093 6823; 3708 13325; 9962; 5971; 6826 7748 6823; 6645 6823; 2454 6823 6040 5676; 433 293 14
ER  - 



TY  - JOUR
T1  - Explaining family change and variation: challenges for family demographers
AN  - 38193431; 2985883
AB  - Twenty years ago, the National Institute of Child Health and Human Development (NICHD) issued a request for proposals that resulted in the National Survey of Families and Households (NSFH), a unique survey valuable to a wide range of family scholars. This paper describes the efforts of an interdisciplinary group of family demographers to build on the progress enabled by the NSFH and many other theoretical and methodological innovations. Our work, also supported by NICHD, will develop plans for research and data collection to address the central question of what causes family change and variation. We outline the group's initial assessments of orienting frameworks, key aspects of family life to study, and theoretical and methodological challenges for research on family change. Finally, we invite family scholars to follow our progress and to help develop this shared public good. Reprinted by permission of National Council on Family Relations
JF  - Journal of marriage and the family
AU  - Seltzer, Judith A
AU  - Bachrach, Christine A
AU  - Bianchi, Suzanne M
AU  - Bledsoe, Caroline H
AU  - Casper, Lynne M
AU  - Chase-Lansdale, P Lindsay
AU  - DiPrete, Thomas A
AU  - Hotz, V Joseph
AU  - Morgan, S Philip
AU  - Sanders, Seth G
AU  - Thomas, Duncan
AD  - University of California ; National Institute of Child Health and Human Development ; University of Maryland ; Northwestern University ; University of Southern California ; Columbia University ; Duke University
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 908
EP  - 925
VL  - 67
IS  - 4
SN  - 0022-2445, 0022-2445
KW  - Sociology
KW  - Anthropology
KW  - Social science research
KW  - Data collection
KW  - Interdisciplinary research
KW  - Research methods
KW  - Demographic change
KW  - Methodology
KW  - Family studies
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/38193431?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+marriage+and+the+family&rft.atitle=Explaining+family+change+and+variation%3A+challenges+for+family+demographers&rft.au=Seltzer%2C+Judith+A%3BBachrach%2C+Christine+A%3BBianchi%2C+Suzanne+M%3BBledsoe%2C+Caroline+H%3BCasper%2C+Lynne+M%3BChase-Lansdale%2C+P+Lindsay%3BDiPrete%2C+Thomas+A%3BHotz%2C+V+Joseph%3BMorgan%2C+S+Philip%3BSanders%2C+Seth+G%3BThomas%2C+Duncan&rft.aulast=Seltzer&rft.aufirst=Judith&rft.date=2005-11-01&rft.volume=67&rft.issue=4&rft.spage=908&rft.isbn=&rft.btitle=&rft.title=Journal+of+marriage+and+the+family&rft.issn=00222445&rft_id=info:doi/
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 3407 3412 9859; 4783; 6631 10902; 7994; 3286; 10919; 11919 10902
ER  - 



TY  - JOUR
T1  - High frequency transformation of Cryptococcus neoformans and Cryptococcus gattii by Agrobacterium tumefaciens
AN  - 20789821; 6633990
AB  - Cryptococcus neoformans and Cryptococcus gattii are the caus-ative agents of cryptococcal meningoencephalitis and are amenable to genetic manipulations, making them important models of pathogenic fungi. To improve the efficiency of Agrobacterium tumefaciens mediated transformation (ATMT) in C. neoformans, we optimized various co-cultivation conditions including incubation time and temperature, and bacteria to yeast ratio. ATMT was also applied to both serotypes (B and C) of C. gattii. Transformation efficiency by ATMT in C. neoformans was comparable to either electroporation or biolistic transformation and gave superior efficiencies in serotypes B and C, but unlike Saccharomyces cerevisiae, adenine auxotrophy did not increase ATMT efficiency in C. neoformans or C. gattii. All transformants tested were stable, with a majority containing only a single T-DNA insertion; however, homologous recombination was not observed. Additionally, we isolated adenine auxotrophs containing a single T-DNA insertion in the ADE2 gene for representative serotype B and C strains.
JF  - Fungal Genetics and Biology
AU  - McClelland, C M
AU  - Chang, Y C
AU  - Kwon-Chung, K J
AD  - National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892, USA, june_kwon-chung@nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 904
EP  - 913
VL  - 42
IS  - 11
SN  - 1087-1845, 1087-1845
KW  - budding yeast
KW  - Microbiology Abstracts B: Bacteriology; Microbiology Abstracts C: Algology, Mycology & Protozoology; Genetics Abstracts
KW  - Temperature effects
KW  - Transformation
KW  - Serotypes
KW  - Electroporation
KW  - Auxotrophs
KW  - ADE2 gene
KW  - Fungi
KW  - Meningoencephalitis
KW  - Auxotrophy
KW  - Saccharomyces cerevisiae
KW  - Models
KW  - Agrobacterium tumefaciens
KW  - Cryptococcus neoformans
KW  - Insertion
KW  - Adenine
KW  - T-DNA
KW  - homologous recombination
KW  - J 02310:Genetics & Taxonomy
KW  - G 07330:Fungal genetics
KW  - K 03079:Fungi
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20789821?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Fungal+Genetics+and+Biology&rft.atitle=High+frequency+transformation+of+Cryptococcus+neoformans+and+Cryptococcus+gattii+by+Agrobacterium+tumefaciens&rft.au=McClelland%2C+C+M%3BChang%2C+Y+C%3BKwon-Chung%2C+K+J&rft.aulast=McClelland&rft.aufirst=C&rft.date=2005-11-01&rft.volume=42&rft.issue=11&rft.spage=904&rft.isbn=&rft.btitle=&rft.title=Fungal+Genetics+and+Biology&rft.issn=10871845&rft_id=info:doi/10.1016%2Fj.fgb.2005.07.003
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Transformation; Temperature effects; Serotypes; Electroporation; Auxotrophs; Fungi; ADE2 gene; Meningoencephalitis; Auxotrophy; Models; Insertion; Adenine; T-DNA; homologous recombination; Agrobacterium tumefaciens; Cryptococcus neoformans; Saccharomyces cerevisiae
DO  - http://dx.doi.org/10.1016/j.fgb.2005.07.003
ER  - 



TY  - JOUR
T1  - Essential Role of the MyD88 Pathway, but Nonessential Roles of TLRs 2, 4, and 9, in the Adjuvant Effect Promoting Th1-Mediated Autoimmunity
AN  - 20726475; 7143892
AB  - Induction of tissue-specific experimental autoimmune diseases involves an obligatory adjuvant effect to trigger an innate response of a type that will drive a Th1-biased adaptive response. This is achieved by use of CFA containing mycobacteria (Mycobacterium tuberculosis), whose recognition by cells of the innate immune system depends on TLRs that signal through the adaptor molecule MyD88. We examined the role of selected components of the MyD88 pathway in promoting experimental autoimmune uveitis (EAU). Mice deficient in MyD88, TLR2, TLR4, or TLR9 were immunized with the retinal Ag interphotoreceptor retinoid-binding protein in CFA, and their EAU scores and associated immunological responses were examined. MyD88 super(-/-) mice were completely resistant to EAU and had a profound defect in Th1, but not Th2, responses to autoantigen challenge. Surprisingly, TLR2 super(-/-), TLR4 super(-/-), and TLR9 super(-/-) mice were fully susceptible to EAU and had unaltered adaptive responses to interphotoreceptor retinoid-binding protein. Examination of IL-1R family members, which share the common adaptor MyD88 with the TLR family, revealed that IL-1R-deficient mice, but not IL-18-deficient mice, are resistant to EAU and have profoundly reduced Th1 and Th2 responses. These data are compatible with the interpretation that TLR9, TLR4, and TLR2 signaling is either not needed, or, more likely, redundant in the adjuvant effect needed to induce EAU. In contrast, signaling through the IL-1R plays a necessary and nonredundant role in EAU and can by itself account for the lack of EAU development in MyD88 mice.
JF  - Journal of Immunology
AU  - Su, Shao Bo
AU  - Silver, Phyllis B
AU  - Grajewski, Rafael S
AU  - Agarwal, Rajeev K
AU  - Tang, Jun
AU  - Chan, Chi-Chao
AU  - Caspi, Rachel R
AD  - Laboratory of Immunology, National Eye Institute, National Institutes of Health, Bethesda, MD 20892
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 6303
EP  - 6310
PB  - American Association of Immunologists, 9650 Rockville Pike Bethesda MD 20814-3998 USA, [URL:http://www.jimmunol.org/]
VL  - 175
IS  - 10
SN  - 0022-1767, 0022-1767
KW  - Microbiology Abstracts B: Bacteriology; Immunology Abstracts
KW  - Data processing
KW  - Retina
KW  - MyD88 protein
KW  - TLR9 protein
KW  - Helper cells
KW  - Immune system
KW  - TLR2 protein
KW  - Autoimmune diseases
KW  - Adjuvants
KW  - Autoantigens
KW  - adaptor proteins
KW  - interphotoreceptor retinoid-binding protein
KW  - experimental autoimmune uveitis
KW  - Lymphocytes T
KW  - Interleukin 1 receptors
KW  - Experimental autoimmune uveoretinitis
KW  - TLR4 protein
KW  - Toll-like receptors
KW  - Mycobacterium tuberculosis
KW  - Signal transduction
KW  - J 02350:Immunology
KW  - F 06930:Autoimmunity
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Data processing; Retina; MyD88 protein; Immune system; Helper cells; TLR9 protein; Autoimmune diseases; TLR2 protein; Adjuvants; Autoantigens; adaptor proteins; interphotoreceptor retinoid-binding protein; experimental autoimmune uveitis; Lymphocytes T; Interleukin 1 receptors; Experimental autoimmune uveoretinitis; TLR4 protein; Toll-like receptors; Signal transduction; Mycobacterium tuberculosis
ER  - 



TY  - JOUR
T1  - Estimated Urine pH and Bladder Cancer Risk in a Cohort of Male Smokers (Finland)*
AN  - 20718660; 6871954
AB  - Objective:Low urine pH may be an important risk factor for bladder cancer, although few studies have evaluated this association. We examined the relationship between estimated renal net acid excretion (NAE), an indirect measure of urine pH based on nutrient intake and anthropometry, and bladder cancer risk in the Alpha-Tocopherol, Beta-Carotene Cancer Prevention (ATBC) Study.Methods: At baseline, 27,096 male smokers 50-69 years old completed a dietary questionnaire that assessed usual frequency of consumption and portion sizes for the previous 12 months, had height and weight measured, and provided a history of smoking. A total of 446 incident bladder cancer cases were identified during up to 17.4 years of follow-up.Results: In multivariate proportional hazards models, the relative risk (RR) for bladder cancer was 1.15 (95% confidence interval (CI)=0.86-1.55) for individuals in the highest (i.e., most acidic) versus the lowest (i.e., least acidic) NAE quintile (p=0.38). Among men who smoked for more than 45 years, there was a suggestion of increased risk with higher NAE levels (RR=1.72, 95% CI=0.96-3.10, p=0.08).Conclusions: These findings do not indicate that urine pH is a major risk factor for bladder cancer, although certain subsets of individuals may be at increased risk.
JF  - Cancer Causes & Control
AU  - Wright, Margaret E
AU  - Michaud, Dominique S
AU  - Pietinen, Pirjo
AU  - Taylor, Philip R
AU  - Virtamo, Jarmo
AU  - Albanes, Demetrius
AD  - National Cancer Institute, NIH, DHHS, 6120 Executive Blvd., EPS 212D, Rockville, MD, 20852, USA, wrighmar@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1117
EP  - 1123
PB  - Springer-Verlag (Heidelberg), Tiergartenstrasse 17 Heidelberg 69121 Germany, [mailto:subscriptions@springer.de], [URL:http://www.springer.de/]
VL  - 16
IS  - 9
SN  - 0957-5243, 0957-5243
KW  - Risk Abstracts
KW  - Diets
KW  - urinary bladder
KW  - Historical account
KW  - Smoking
KW  - Finland
KW  - Urine
KW  - prevention
KW  - males
KW  - Excretion
KW  - Cancer
KW  - pH
KW  - R2 23060:Medical and environmental health
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-10-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Diets; Smoking; Historical account; urinary bladder; Urine; prevention; males; Excretion; pH; Cancer; Finland
DO  - http://dx.doi.org/10.1007/s10552-005-0348-9
ER  - 



TY  - JOUR
T1  - Prevalence of Impaired Fasting Glucose and Its Relationship With Cardiovascular Disease Risk Factors in US Adolescents, 1999-2000
AN  - 20717855; 6505410
AB  - OBJECTIVE: PEDIATRICS (ISSN 0031 4005). Published in the public domain by the American Academy of Pediatrics.Several studies have reported increases in the occurrence of type 2 diabetes in youths. People with prediabetic states such as impaired fasting glucose (IFG) are at increased risk for developing diabetes and cardiovascular disease (CVD). The objective of this study was to examine the prevalence of IFG and its relationship with overweight and CVD risk factors in a nationally representative sample of US adolescents who were aged 12 to 19 years. METHODS: We used data from the 1999-2000 National Health and Nutrition Examination Survey (NHANES). Adolescents who had fasted for 8 hours or more were included in the study (n = 915). IFG was defined as a fasting glucose of 100 to 125 mg/dL. Participants were classified as overweight when their age- and gender-specific BMI was greater than or equal to 95th percentile and as at-risk for overweight when their BMI was greater than or equal to 85th and <95th percentile. RESULTS: In 1999-2000, the prevalence of IFG in US adolescents was 7.0% and was higher in boys than in girls (10.0% vs 4.0%). Prevalence of IFG was higher in overweight adolescents (17.8%) but was similar in those with normal weight and those who were at risk for overweight (5.4% vs 2.8%). The prevalence of IFG was significantly different across racial/ethnic groups (13.0%, 4.2%, and 7% in Mexican Americans, non-Hispanic black individuals, and non-Hispanic white individuals, respectively). Adolescents with IFG had significantly higher mean hemoglobin A1c, fasting insulin, total and low-density lipoprotein cholesterol, triglycerides, and systolic blood pressure and lower high-density lipoprotein cholesterol than those with normal fasting glucose concentrations. CONCLUSIONS: These data, representing 27 million US adolescents, reveal a very high prevalence of IFG (1 in 10 boys and 1 in 25 girls) among adolescents; the condition affects 1 in every 6 overweight adolescents. Adolescents with IFG have features of insulin resistance and worsened CVD risk factors. Evidence for prevention is still forthcoming in this age group.
JF  - Pediatrics
AU  - Williams, Desmond E
AU  - Cadwell, Betsy L
AU  - Cheng, Yiling J
AU  - Cowie, Catherine C
AU  - Gregg, Edward W
AU  - Geiss, Linda S
AU  - Engelgau, Michael M
AU  - Narayan, KMVenkat
AU  - Imperatore, Giuseppina
AD  - Division of Diabetes Translation, National Center for Chronic Disease Prevention and Health Promotion, Centers for Disease Control and Prevention, Atlanta, Georgia. National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1122
EP  - 1126
PB  - American Academy of Pediatrics, 141 Northwest Point Blvd. Elk Grove Village IL 60007-1098 USA, [mailto:journals@aap.org], [URL:http://www.aap.org]
VL  - 116
IS  - 5
SN  - 0031-4005, 0031-4005
KW  - Risk Abstracts
KW  - Age
KW  - insulin
KW  - obesity
KW  - cholesterol
KW  - Nutrition
KW  - USA
KW  - diabetes mellitus
KW  - Gender
KW  - prevention
KW  - Cardiovascular diseases
KW  - Adolescents
KW  - Ethnic groups
KW  - R2 23060:Medical and environmental health
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-10-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Age; diabetes mellitus; insulin; Gender; prevention; obesity; Cardiovascular diseases; Nutrition; cholesterol; Ethnic groups; Adolescents; USA
ER  - 



TY  - JOUR
T1  - Immunodeficiency in the Absence of High Viral Load in Pig-Tailed Macaques Infected with Simian Immunodeficiency Virus SIVsun or SIVlhoest
AN  - 20717842; 6504757
AB  - Simian immunodeficiency virus (SIV) is known to result in an asymptomatic infection of its natural African monkey host. However, some SIV strains are capable of inducing AIDS-like symptoms and death upon experimental infection of Asian macaques. To further investigate the virulence of natural SIV isolates from African monkeys, pig-tailed (PT) macaques were inoculated intravenously with either of two recently discovered novel lentiviruses, SIVlhoest and SIVsun. Both viruses were apparently apathogenic in their natural hosts but caused immunodeficiency in PT macaques. Infection was characterized by a progressive loss of CD4 super(+) lymphocytes in the peripheral blood and lymph nodes, generalized lymphoid depletion, a wasting syndrome, and opportunistic infections, such as Mycobacterium avium or Pneumocystis carinii infections. However, unlike SIVsm/mac infection of macaques, SIVlhoest and SIVsun infections in PT macaques were not accompanied by high viral loads during the chronic disease stage. In addition, no significant correlation between the viral load at set point (12 weeks postinfection) and survival could be found. Five out of eight SIVlhoest-infected and three out of four SIVsun-infected macaques succumbed to AIDS during the first 5 years of infection. Thus, the survival of SIVsun- and SIVlhoest-infected animals was significantly longer than that of SIVagm- or SIVsm-infected macaques. All PT macaques maintained strong SIV antibody responses despite progression to SIV-induced AIDS. The development of immunodeficiency in the face of low viremia suggests that SIVlhoest and SIVsun infections of macaques may model unique aspects of the pathogenesis of human immunodeficiency virus infection in humans.
JF  - Journal of Virology
AU  - Beer, Brigitte E
AU  - Brown, Charles R
AU  - Whitted, Sonya
AU  - Goldstein, Simoy
AU  - Goeken, Robert
AU  - Plishka, Ronald
AU  - Buckler-White, Alicia
AU  - Hirsch, Vanessa M
AD  - Laboratory of Molecular Microbiology, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rockville, Maryland 20852
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 14044
EP  - 14056
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 79
IS  - 22
SN  - 0022-538X, 0022-538X
KW  - HIV
KW  - Macaques
KW  - SIV
KW  - Microbiology Abstracts B: Bacteriology; Immunology Abstracts; Virology & AIDS Abstracts
KW  - Experimental infection
KW  - Acquired immune deficiency syndrome
KW  - Mycobacterium avium
KW  - Pneumocystis carinii
KW  - Macaca
KW  - Animal models
KW  - Immunodeficiency
KW  - Survival
KW  - Peripheral blood
KW  - Asymptomatic infection
KW  - Lymphocytes
KW  - Lymph nodes
KW  - Opportunist infection
KW  - Virulence
KW  - CD4 antigen
KW  - Antibodies
KW  - Lentivirus
KW  - Human immunodeficiency virus
KW  - Chronic infection
KW  - Viremia
KW  - Simian immunodeficiency virus
KW  - F 06308:Clinical: AIDS
KW  - V 22005:AIDS: Epidemiological aspects
KW  - J 02350:Immunology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Acquired immune deficiency syndrome; Experimental infection; Immunodeficiency; Animal models; Survival; Asymptomatic infection; Peripheral blood; Lymphocytes; Lymph nodes; Opportunist infection; Virulence; Antibodies; CD4 antigen; Chronic infection; Viremia; Pneumocystis carinii; Mycobacterium avium; Lentivirus; Human immunodeficiency virus; Macaca; Simian immunodeficiency virus
ER  - 



TY  - JOUR
T1  - Drinking-Water Nitrate and Health-Recent Findings and Research Needs
AN  - 20582130; 6737368
AB  - Human alteration of the nitrogen cycle has resulted in steadily accumulating nitrate in our water resources. The U.S. maximum contaminant level and World Health Organization guidelines for nitrate in drinking water were promulgated to protect infants from developing methemoglobine-mia, an acute condition. Some scientists have recently suggested that the regulatory limit for nitrate is overly conservative; however, they have not thoroughly considered chronic health outcomes. In August 2004, a symposium on drinking-water nitrate and health was held at the International Society for Environmental Epidemiology meeting to evaluate nitrate exposures and associated health effects in relation to the current regulatory limit. The contribution of drinking-water nitrate toward endogenous formation of N-nitroso compounds was evaluated with a focus toward identifying subpopulations with increased rates of nitrosation. Adverse health effects may be the result of a complex interaction of the amount of nitrate ingested, the concomitant ingestion of nitrosation cofactors and precursors, and specific medical conditions that increase nitrosation. Workshop participants concluded that more experimental studies are needed and that a particularly fruitful approach may be to conduct epidemiologic studies among susceptible subgroups with increased endogenous nitrosation. The few epidemiologic studies that have evaluated intake of nitrosation precursors and/or nitrosation inhibitors have observed elevated risks for colon cancer and neural tube defects associated with drinking-water nitrate concentrations below the regulatory limit. The role of drinking-water nitrate exposure as a risk factor for specific cancers, reproductive outcomes, and other chronic health effects must be studied more thoroughly before changes to the regulatory level for nitrate in drinking water can be considered.
JF  - Environmental Health Perspectives
AU  - Ward, M H
AU  - deKok, TM
AU  - Levallois, P
AU  - Brender, J
AU  - Gulis, G
AU  - Nolan, B T
AU  - VanDerslice, J
AD  - Occupational and Environmental Epidemiology Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, 6120 Executive Blvd., EPS 8104, Bethesda, MD 20892 USA, wardm@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1607
EP  - 1614
VL  - 113
IS  - 11
SN  - 0091-6765, 0091-6765
KW  - Pollution Abstracts; Risk Abstracts; Toxicology Abstracts; Aqualine Abstracts; Water Resources Abstracts; Health & Safety Science Abstracts
KW  - Intakes
KW  - Water resources
KW  - Neural tube defects
KW  - Research Priorities
KW  - Exposure
KW  - Subpopulations
KW  - Nitrogen Cycle
KW  - Colon cancer
KW  - Ingestion
KW  - N-Nitroso compounds
KW  - Cofactors
KW  - Epidemiology
KW  - Water Pollution Effects
KW  - Nitrogen cycle
KW  - Standards
KW  - Nitrosation
KW  - Contaminants
KW  - Water Resources
KW  - Infants
KW  - Nitrate
KW  - Organizations
KW  - Tubes
KW  - Drinking Water
KW  - Pollutants
KW  - Risk factors
KW  - Inhibitors
KW  - Nitrates
KW  - Cancer
KW  - Risk
KW  - USA
KW  - Drinking water
KW  - Symposium
KW  - X 24120:Food, additives & contaminants
KW  - P 2000:FRESHWATER POLLUTION
KW  - AQ 00008:Effects of Pollution
KW  - SW 3030:Effects of pollution
KW  - H 12000:Epidemiology and Public Health
KW  - R2 23050:Environment
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Nitrate; Subpopulations; Water resources; Colon cancer; Neural tube defects; N-Nitroso compounds; Cofactors; Epidemiology; Risk factors; Nitrogen cycle; Nitrosation; Drinking water; Contaminants; Infants; Nitrates; Ingestion; Cancer; Organizations; Intakes; Nitrogen Cycle; Tubes; Risk; Research Priorities; Drinking Water; Pollutants; Exposure; Water Pollution Effects; Inhibitors; Standards; Symposium; Water Resources; USA
DO  - http://dx.doi.org/10.1289/ehp.8043
ER  - 



TY  - JOUR
T1  - Mutant Brca2/p53 mice exhibit altered radiation responses in the developing mammary gland
AN  - 20466071; 7911784
AB  - Appropriate balance between proliferation and apoptosis is critical for mammary gland development and is often altered during tumorigenesis. Carcinogens like radiation induce DNA damage and activate protective responses such as cell cycle arrest and apoptosis. We used mice carrying Brca2-/- and/or p53-/- mutations to evaluate the individual and combined effects of these genes on cell proliferation and apoptosis in the developing mammary gland. Mice were exposed to 5Gy of radiation or chamber exposure (controls) followed by injection with BrdU. Mammary glands were collected 6h post-radiation exposure and evaluated for proliferation (BrdU) and apoptosis (TUNEL) in terminal end buds (TEB) and ducts. Under control conditions, the Brca2 mutation reduced proliferation and apoptosis in TEB but not ducts, whereas the p53 mutation reduced apoptosis in TEB and ducts but did not influence proliferation. Despite these alterations in proliferation and/or apoptosis, neither mutation, either individually or combined, significantly altered the overall balance between the two as measured by the proliferation to apoptosis ratio (growth index). Following irradiation, the Brca2 mutation had no significant effect on proliferation or apoptosis, whereas the p53 mutation resulted in reduced apoptosis in TEB and ducts but did not significantly influence proliferation. Neither mutation by itself altered the growth index in the TEB after irradiation although combined Brca2/p53 mutation caused significantly increased proliferation, reduced apoptosis, and an elevated growth index in TEB and ducts. These results reveal both independent and collaborative growth regulatory roles for Brca2 and p53 under normal and adverse environmental conditions. Additionally, we demonstrate the importance of gene-environment interactions by showing that Brca2- and p53-deficient mice can compensate for their genetic deficiencies under control conditions but not after exposure to radiation. We also demonstrate distinct spatial differences in the cellular functions of Brca2 and p53 and show that combined mutation of both genes is more detrimental than loss of either gene alone.
JF  - Experimental and Toxicologic Pathology
AU  - Houle, Christopher D
AU  - Peddada, Shyamal D
AU  - McAllister, Kimberly A
AU  - Ward, Toni
AU  - Malphurs, Jason
AU  - Gersch, William D
AU  - Davis, Barbara J
AD  - Laboratory of Women's Health, National Institute of Environmental Health Sciences, NIH, P.O. Box 12233, Research Triangle Park, NC 27709, USA, choule@epl-inc.com
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 105
EP  - 115
PB  - Elsevier GmbH, Office Jena, P.O. Box 100537 Jena D-07705 Germany, [mailto:journals@elsevier.com], [URL:http://www.elsevier.de/]
VL  - 57
IS  - 2
SN  - 0940-2993, 0940-2993
KW  - Toxicology Abstracts
KW  - Brca2
KW  - p53
KW  - Apoptosis
KW  - Proliferation
KW  - Radiation
KW  - Mammary gland
KW  - Post-radiation
KW  - Tumorigenesis
KW  - Cell cycle
KW  - Carcinogens
KW  - BRCA2 protein
KW  - Buds
KW  - p53 protein
KW  - DNA damage
KW  - Environmental conditions
KW  - Cell proliferation
KW  - Mutation
KW  - X 24390:Radioactive Materials
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-01-01
N1  - Last updated - 2015-03-27
N1  - SubjectsTermNotLitGenreText - Apoptosis; Post-radiation; Mammary gland; Cell cycle; Tumorigenesis; BRCA2 protein; Carcinogens; p53 protein; Buds; DNA damage; Radiation; Cell proliferation; Environmental conditions; Mutation
DO  - http://dx.doi.org/10.1016/j.etp.2005.06.001
ER  - 



TY  - JOUR
T1  - Nanoparticle Formulation Increases Oral Bioavailability of Poorly Soluble Drugs: Approaches, Experimental Evidences and Theory
AN  - 20368787; 7729187
AB  - The increasing frequency at which poorly soluble new chemical entities are being discovered raises concerns in the pharmaceutical industry about drugability associated with erratic dissolution and low bioavailability of these hydrophobic compounds. Nanonization provides a plausible pharmaceutical basis for enhancing oral bioavailability and therapeutic effectiveness of these compounds by increasing their surface area. This paper surveys methods available to pharmaceutical manufacturing nanoparticles, including wet chemical processes, media milling, high pressure homogenization, gas-phase synthesis, and form-in-place processes, and elaborates physicochemical rational and gastrointestinal physiological basis upon which nano-drugs can be readily absorbed. Relevant examples are illustrated to show that nano- drugs permeate Caco-2 cell monolayer fast and are well absorbed into animal systemic circulation with high Tmax and AUC, resulting in oral bioavailability higher than their counterpart micro-drugs. The size-dependent permeability and bioavailability should be given particular consideration in the development of potent and selective drug candidates with poor aqueous solubility.
JF  - Current Nanoscience
AU  - Jia, Lee
AD  - EPN, Rm 8042, 6130 Executive Blvd., National Cancer Institute, NIH, Rockville, MD 20852, USA.
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 237
EP  - 243
PB  - Bentham Science Publishers B.V., P.O. Box 1673 Hilversum 1200 BR The Netherlands, [mailto:shidding@worldonline.nl], [URL:http://www.bentham.org]
VL  - 1
IS  - 3
SN  - 1573-4137, 1573-4137
KW  - Biotechnology and Bioengineering Abstracts
KW  - Permeability
KW  - Solubility
KW  - Surface area
KW  - Dissolution
KW  - Pharmaceuticals
KW  - Hydrophobicity
KW  - Drug development
KW  - Pressure
KW  - Media (selective)
KW  - nanoparticles
KW  - W 30915:Pharmaceuticals & Vaccines
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20368787?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Current+Nanoscience&rft.atitle=Nanoparticle+Formulation+Increases+Oral+Bioavailability+of+Poorly+Soluble+Drugs%3A+Approaches%2C+Experimental+Evidences+and+Theory&rft.au=Jia%2C+Lee&rft.aulast=Jia&rft.aufirst=Lee&rft.date=2005-11-01&rft.volume=1&rft.issue=3&rft.spage=237&rft.isbn=&rft.btitle=&rft.title=Current+Nanoscience&rft.issn=15734137&rft_id=info:doi/10.2174%2F157341305774642939
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-12-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Pharmaceuticals; Drug development; Hydrophobicity; nanoparticles; Solubility; Surface area; Media (selective); Permeability; Dissolution; Pressure
DO  - http://dx.doi.org/10.2174/157341305774642939
ER  - 



TY  - JOUR
T1  - Novel Phase I Dose De-escalation Design Trial to Determine the Biological Modulatory Dose of the Antiangiogenic Agent SU5416
AN  - 20241799; 7142102
AB  - PURPOSE: To determine the biological modulatory dose of SU5416, we employed a novel trial design, where "dose de-escalation" was based on demonstrable biological changes observed at the maximum tolerated dose. If such an effect was shown, dose de-escalation to a predefined dose level would occur to determine if the lower dose exhibited the same amount of pharmacodynamic effect as the higher dose. Experimental Design: Ten patients with advanced solid tumors were enrolled at each dose level. One of the following pharmacodynamic effects was considered significant: (a) a 35% decrease in microvessel density in sequential tumor biopsies and (b) a 35% decrease in blood flow within tumor as assessed by dynamic contrast-enhanced magnetic resonance imaging. In addition, soluble E-selectin, soluble intercellular adhesion molecule, soluble vascular cell adhesion molecule, and plasma vascular endothelial growth factor were measured sequentially. RESULTS: Nineteen patients were enrolled. Sequential tumor biopsies in all evaluable patients showed an increase in microvessel density. Only one patient met the intended pharmacodynamic end point of >35% reduction in blood flow. There was a significant increase in both soluble E-selectin and soluble intercellular adhesion molecule levels pretreatment versus levels at the time of removal of patients from study (P = 0.04 and P = 0.0007, respectively). Levels of serum fibrinogen rose with therapy. There was a trend toward increase in plasma vascular endothelial growth factor levels. CONCLUSION: SU5416 does not result in decreased blood flow in tumors or a decrease in microvessel density. This corresponds to the lack of clinical activity seen with this agent. Our clinical trial design termed dose de-escalation is a novel approach to determine the in vivo biological effects of targeted therapies in cancer patients.
JF  - Clinical Cancer Research
AU  - Dowlati, Afshin
AU  - Robertson, Kelly
AU  - Radivoyevitch, Tomas
AU  - Waas, John
AU  - Ziats, Nicholas P
AU  - Hartman, Paul
AU  - Abdul-Karim, Fadi W
AU  - Wasman, Jay K
AU  - Jesberger, Jack
AU  - Lewin, Jonathan
AU  - McCrae, Keith
AU  - Ivy, Percy
AU  - Remick, Scot C
AD  - Authors' Affiliations: Developmental Therapeutics Program, Case Comprehensive Cancer Center and Division of Hematology/Oncology, Department of Pathology and Radiology, Case Western Reserve University and University Hospitals of Cleveland, Cleveland, Ohio and National Cancer Institute, Bethesda, Maryland
Y1  - 2005/11/01/
PY  - 2005
DA  - 2005 Nov 01
SP  - 7938
EP  - 7944
PB  - American Association for Cancer Research, 615 Chestnut St., 17th Floor Philadelphia PA 19106-4404 USA, [URL:http://www.aacr.org/]
VL  - 11
IS  - 21
SN  - 1078-0432, 1078-0432
KW  - Biotechnology and Bioengineering Abstracts
KW  - Vascular endothelial growth factor
KW  - antiangiogenic agents
KW  - Solid tumors
KW  - Fibrinogen
KW  - Magnetic resonance imaging
KW  - Biopsy
KW  - Tumors
KW  - Clinical trials
KW  - Cell adhesion molecules
KW  - Pharmacodynamics
KW  - E-selectin
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20241799?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+Cancer+Research&rft.atitle=Novel+Phase+I+Dose+De-escalation+Design+Trial+to+Determine+the+Biological+Modulatory+Dose+of+the+Antiangiogenic+Agent+SU5416&rft.au=Dowlati%2C+Afshin%3BRobertson%2C+Kelly%3BRadivoyevitch%2C+Tomas%3BWaas%2C+John%3BZiats%2C+Nicholas+P%3BHartman%2C+Paul%3BAbdul-Karim%2C+Fadi+W%3BWasman%2C+Jay+K%3BJesberger%2C+Jack%3BLewin%2C+Jonathan%3BMcCrae%2C+Keith%3BIvy%2C+Percy%3BRemick%2C+Scot+C&rft.aulast=Dowlati&rft.aufirst=Afshin&rft.date=2005-11-01&rft.volume=11&rft.issue=21&rft.spage=7938&rft.isbn=&rft.btitle=&rft.title=Clinical+Cancer+Research&rft.issn=10780432&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-09-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Vascular endothelial growth factor; antiangiogenic agents; Solid tumors; Magnetic resonance imaging; Fibrinogen; Biopsy; Tumors; Clinical trials; E-selectin; Pharmacodynamics; Cell adhesion molecules
ER  - 



TY  - JOUR
T1  - Development of Resistance to RNAi in Mammalian Cells
AN  - 20239992; 6663369
AB  - The discovery of RNA interference (RNAi) in C. elegans and in plants has revolutionized current approaches to biology and medicine. RNAi silences genes in a sequence-specific manner through the actions of small pieces of double-stranded RNAs (siRNAs and miRNAs). RNAi has been found as a widespread natural phenomenon in eukaryotic cells and is also being used as a powerful experimental tool to explore gene function. Most importantly, it has many potential therapeutic applications. Viral gene-specific siRNAs are theoretically very promising antiviral inhibitors and have been examined in a broad range of medically important viruses. However, many RNA viruses escape RNAi-mediated suppression by counteracting the RNAi machinery through mutation of the targeted region, by encoding viral suppressors, or both. DNA viruses also counteract the RNAi machinery, preferentially using viral suppressors. Cellular factors may also contribute to RNAi resistance; ADAR1 was the first cellular factor found to be responsible for editing-mediated RNAi resistance. Because siRNAs can be used as potent small-molecule inhibitors of any cellular gene, the best way for a cell to maintain expression of essential genes for its long-term survival is to develop a program to resist the detrimental effects of RNAi.
JF  - Annals of the New York Academy of Sciences
AU  - Zheng, Zhi-Ming
AU  - Tang, Shuang
AU  - Tao, Mingfang
AD  - HIV and AIDS Malignancy Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892, USA
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 105
EP  - 118
PB  - New York Academy of Sciences, 2 East 63rd Street New York NY 10021 USA, [mailto:publications@nyas.org], [URL:http://www.nyas.org]
VL  - 1058
SN  - 0077-8923, 0077-8923
KW  - Virology & AIDS Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Cell survival
KW  - Double-stranded RNA
KW  - Medicinal plants
KW  - miRNA
KW  - Therapeutic applications
KW  - RNA viruses
KW  - DNA viruses
KW  - siRNA
KW  - Mammalian cells
KW  - RNA-mediated interference
KW  - Mutation
KW  - Gene silencing
KW  - W 30940:Products
KW  - V 22340:Antiviral Agents
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Annals+of+the+New+York+Academy+of+Sciences&rft.atitle=Development+of+Resistance+to+RNAi+in+Mammalian+Cells&rft.au=Zheng%2C+Zhi-Ming%3BTang%2C+Shuang%3BTao%2C+Mingfang&rft.aulast=Zheng&rft.aufirst=Zhi-Ming&rft.date=2005-11-01&rft.volume=1058&rft.issue=&rft.spage=105&rft.isbn=&rft.btitle=&rft.title=Annals+of+the+New+York+Academy+of+Sciences&rft.issn=00778923&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-07-01
N1  - Last updated - 2015-03-27
N1  - SubjectsTermNotLitGenreText - Cell survival; Mammalian cells; siRNA; Double-stranded RNA; miRNA; Medicinal plants; Therapeutic applications; RNA-mediated interference; RNA viruses; Mutation; DNA viruses; Gene silencing
ER  - 



TY  - JOUR
T1  - Chemoprevention with Protein Kinase A RI alpha Antisense in DMBA-Mammary Carcinogenesis
AN  - 20223282; 6663382
AB  - Cancer is potentially preventable disease. A surprising variety of intracellular pathways can be a target for chemoprevention. Earlier it was discovered that cAMP-mediated system can play important role in prevention of DMBA-mammary carcinogenesis. There are two types of cAMP-dependent protein kinases (PKA), type I (PKA-I) and type II (PKA-II), which share a common catalytic (C) subunits, but contain distinct regulatory (R) ones, RI versus RII, respectively. Evidence suggests that increased expression of PKA-I and its regulatory subunit (RI alpha ) correlates with tumorogenesis and tumor growth. It was found that downregulation of RI alpha by 21-mer antisense oligonucleotide led to growth arrest of cancer cells. The effect of RI alpha antisense oligonucleotide correlated with a decrease in RI alpha protein and a concomitant increase in RII beta protein level. It was shown that antisense RI alpha can protect in a sequence-specific manner from 7,12-dimethylbenz(a)anthracene (DMBA)-induced mammary carcinogenesis. At 90 days after DMBA intubation, RI alpha -antisense-treated rats exhibited significantly lower number of tumors per rat, than untreated control animals. The antisense also delayed the first tumor appearance. An increase in RI alpha and PKA-I levels in the mammary gland and liver preceded tumor production, and antisense downregulation of RI alpha restored normal levels of PKA-I and PKA-II in these tissues. Antisense RI alpha in the liver induced the phase II enzymes, glutathione S-transferase and quinone oxidoreductase, c-fos protein, and activator protein-1 (AP-1)- and cAMP response element (CRE)-directed transcription. In the mammary gland, antisense RI alpha promoted DNA repair processes. In contrast, the CRE transcription-factor decoy could not mimic these effects of antisense RI alpha . The results demonstrate that RI alpha antisense produces dual anticarcinogenic effects : (a) increasing DMBA detoxification in the liver by increasing phase II enzyme activities, increasing CRE-binding-protein phosphorylation and enhancing CRE- and AP-1 directed transcription; and (b) activating DNA repair processes in the mammary gland by downregulating of PKA-1.
JF  - Annals of the New York Academy of Sciences
AU  - Nesterova, Maria V
AU  - Cho-Chung, Yoon S
AD  - Cellular Biochemistry Section, Basic Research Laboratory, CCR, National Cancer Institute, Bethesda, Maryland 20892, USA
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 255
EP  - 264
PB  - New York Academy of Sciences, 2 East 63rd Street New York NY 10021 USA, [mailto:publications@nyas.org], [URL:http://www.nyas.org]
VL  - 1058
SN  - 0077-8923, 0077-8923
KW  - Toxicology Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Detoxification
KW  - Protein kinase A
KW  - Mammary gland
KW  - Regulatory sequences
KW  - Activator protein 1
KW  - Cyclic AMP
KW  - Enzymes
KW  - Transcription
KW  - Antisense DNA
KW  - Tumors
KW  - c-Fos protein
KW  - DNA repair
KW  - Intubation
KW  - Glutathione transferase
KW  - Cancer
KW  - Antisense oligonucleotides
KW  - Phosphorylation
KW  - Regulatory subunits
KW  - 9,10-Dimethyl-1,2-benzanthracene
KW  - Transcription factors
KW  - Carcinogenesis
KW  - Liver
KW  - quinone oxidoreductase
KW  - X 24310:Pharmaceuticals
KW  - W 30940:Products
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Annals+of+the+New+York+Academy+of+Sciences&rft.atitle=Chemoprevention+with+Protein+Kinase+A+RI+alpha+Antisense+in+DMBA-Mammary+Carcinogenesis&rft.au=Nesterova%2C+Maria+V%3BCho-Chung%2C+Yoon+S&rft.aulast=Nesterova&rft.aufirst=Maria&rft.date=2005-11-01&rft.volume=1058&rft.issue=&rft.spage=255&rft.isbn=&rft.btitle=&rft.title=Annals+of+the+New+York+Academy+of+Sciences&rft.issn=00778923&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-05-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Detoxification; Protein kinase A; Mammary gland; Regulatory sequences; Cyclic AMP; Activator protein 1; Antisense DNA; Transcription; Enzymes; c-Fos protein; Tumors; Glutathione transferase; Intubation; DNA repair; Cancer; Antisense oligonucleotides; Phosphorylation; Transcription factors; 9,10-Dimethyl-1,2-benzanthracene; Regulatory subunits; Carcinogenesis; Liver; quinone oxidoreductase
ER  - 



TY  - JOUR
T1  - Human beta -Defensins Suppress Human Immunodeficiency Virus Infection: Potential Role in Mucosal Protection
AN  - 20118744; 6504784
AB  - beta -Defensins are small (3 to 5 kDa in size) secreted antimicrobial and antiviral proteins that are components of innate immunity. beta -Defensins are secreted by epithelial cells, and they are expressed at high levels in several mucosae, including the mouth, where the concentration of these proteins can reach 100 mu g/ml. Because of these properties, we wondered whether they could be part of the defenses that lower oral transmission of human immunodeficiency virus (HIV) compared to other mucosal sites. Our data show that select beta -defensins, especially human beta -defensin 2 (hBD2) and hBD3, inhibit R5 and X4 HIV infection in a dose-dependent manner at doses that are compatible with or below those measured in the oral cavity. We observed that beta -defensin treatment inhibited accumulation of early products of reverse transcription, as detected by PCR. We could not, however, detect any reproducible inhibition of env-mediated fusion, and we did not observe any modulation of HIV coreceptors following treatment with hBD1 and hBD2, in both resting and phytohemagglutinin-activated cells. Our data instead suggest that, besides a direct inactivation of HIV virions, hBD2 inhibits HIV replication in the intracellular environment. Therefore, we speculate that beta -defensins mediate a novel antiretroviral mechanism that contributes to prevention of oral HIV transmission in the oral cavity. Immunohistochemical data on hBD2 expression in oral mucosal tissue shows that hBD2 is constitutively expressed, forming a barrier layer across the epithelium in healthy subjects, while in HIV-positive subjects levels of hBD2 expression are dramatically diminished. This may predispose HIV-positive subjects to increased incidence of oral complications associated with HIV infection.
JF  - Journal of Virology
AU  - Sun, Lingling
AU  - Finnegan, Catherine M
AU  - Kish-Catalone, Tina
AU  - Blumenthal, Robert
AU  - Garzino-Demo, Paolo
AU  - La Terra Maggiore, Gian M
AU  - Berrone, Sid
AU  - Kleinman, Carol
AU  - Wu, Zhibin
AU  - Abdelwahab, Sayed
AU  - Lu, Wuyuan
AU  - Garzino-Demo, Alfredo
AD  - Division of Basic Science, Institute of Human Virology, University of Maryland Biotechnology Institute, 725 West Lombard Street, Baltimore, Maryland 21201. Center for Cancer Research Nanobiology Program, National Cancer Institute, National Institutes of Health, Frederick, Maryland 21702. Department of Maxillofacial Surgery, S. Giovanni Battista Hospital, University of Torino, Turin, Italy
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 14318
EP  - 14329
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 79
IS  - 22
SN  - 0022-538X, 0022-538X
KW  - HIV
KW  - Microbiology Abstracts A: Industrial & Applied Microbiology; Immunology Abstracts; Virology & AIDS Abstracts
KW  - Virions
KW  - Epithelial cells
KW  - Data processing
KW  - Mucosal immunity
KW  - Replication
KW  - Mucosa
KW  - Immunity
KW  - Infection
KW  - Oral cavity
KW  - Reverse transcription
KW  - Disease transmission
KW  - Antimicrobial agents
KW  - Defensins
KW  - Antiviral agents
KW  - Human immunodeficiency virus
KW  - Polymerase chain reaction
KW  - Epithelium
KW  - Mouth
KW  - A 01340:Antibiotics & Antimicrobials
KW  - V 22003:AIDS: Immunological aspects
KW  - F 06104:Virus
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologya&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Virology&rft.atitle=Human+beta+-Defensins+Suppress+Human+Immunodeficiency+Virus+Infection%3A+Potential+Role+in+Mucosal+Protection&rft.au=Sun%2C+Lingling%3BFinnegan%2C+Catherine+M%3BKish-Catalone%2C+Tina%3BBlumenthal%2C+Robert%3BGarzino-Demo%2C+Paolo%3BLa+Terra+Maggiore%2C+Gian+M%3BBerrone%2C+Sid%3BKleinman%2C+Carol%3BWu%2C+Zhibin%3BAbdelwahab%2C+Sayed%3BLu%2C+Wuyuan%3BGarzino-Demo%2C+Alfredo&rft.aulast=Sun&rft.aufirst=Lingling&rft.date=2005-11-01&rft.volume=79&rft.issue=22&rft.spage=14318&rft.isbn=&rft.btitle=&rft.title=Journal+of+Virology&rft.issn=0022538X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Virions; Epithelial cells; Data processing; Mucosal immunity; Replication; Mucosa; Immunity; Infection; Oral cavity; Antimicrobial agents; Disease transmission; Reverse transcription; Defensins; Antiviral agents; Polymerase chain reaction; Epithelium; Mouth; Human immunodeficiency virus
ER  - 



TY  - JOUR
T1  - Dietary Determinants of One-Carbon Metabolism and the Risk of Non-Hodgkin's Lymphoma: NCI-SEER Case-Control Study, 1998-2000
AN  - 19998216; 7140970
AB  - The role of dietary one-carbon determinants remains largely unexplored for non-Hodgkin's lymphoma (NHL). In a population-based case-control study of non-African-American adult (aged 20-74 years) women and men from four US Surveillance, Epidemiology, and End Results study centers (Detroit, Michigan; Iowa; Los Angeles, California; and Seattle, Washington; 1998-2000), the authors examined folate; vitamins B sub(2), B sub(6), and B sub(12); methionine; and a one-carbon antagonist, alcohol, in 425 incident NHL cases and 359 controls who completed a detailed food frequency questionnaire. Adjusted odds ratios and 95% confidence intervals were estimated by using unconditional logistic regression. Higher intake of one-carbon determinants from food was associated with a lower risk of NHL, but that for only vitamin B sub(6) (highest vs. lowest quartile: odds ratio = 0.57, 95% confidence interval: 0.34, 0.95; p trend = 0.01) and methionine (odds ratio = 0.49, 95% confidence interval: 0.31, 0.76; p trend = 0.002) reached statistical significance. Folate from food was inversely associated with diffuse subtype (odds ratio = 0.47, 95% confidence interval: 0.23, 0.94; p trend = 0.03). The authors found no association between total (food plus supplement) vitamins and NHL. Nonusers of alcohol had an elevated NHL risk compared with users, and alcohol did not modify other nutrient-NHL associations. Findings suggest that one-carbon nutrients, particularly vitamin B sub(6) and methionine, may be protective against NHL.
JF  - American Journal of Epidemiology
AU  - Lim, U
AU  - Schenk, M
AU  - Kelemen, LE
AU  - Davis, S
AU  - Cozen, W
AU  - Hartge, P
AU  - Ward, M H
AU  - Stolzenberg-Solomon, R
AD  - Nutritional Epidemiology Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Department of Health and Human Services, Rockville, MD
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 953
EP  - 964
PB  - Oxford University Press, Oxford Journals Health, Great Clarendon Street Oxford OX2 6DP UK, [mailto:jnl.samples@oup.co.uk], [URL:http://www3.oup.co.uk/jnls/]
VL  - 162
IS  - 10
SN  - 0002-9262, 0002-9262
KW  - Immunology Abstracts; Risk Abstracts
KW  - Statistics
KW  - Food
KW  - Vitamin B6
KW  - Nutrients
KW  - Methionine
KW  - Non-Hodgkin's lymphoma
KW  - Risk factors
KW  - alcohols
KW  - Folic acid
KW  - Lymphoma
KW  - Ethanol
KW  - Diets
KW  - USA, California, Los Angeles
KW  - Alcohol
KW  - Inventories
KW  - USA, Michigan, Detroit
KW  - Vitamin B12
KW  - Epidemiology
KW  - USA, Iowa
KW  - Dietary supplements
KW  - INE, USA, Washington, Seattle
KW  - Metabolism
KW  - F 06915:Cancer Immunology
KW  - R2 23060:Medical and environmental health
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ariskabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=American+Journal+of+Epidemiology&rft.atitle=Dietary+Determinants+of+One-Carbon+Metabolism+and+the+Risk+of+Non-Hodgkin%27s+Lymphoma%3A+NCI-SEER+Case-Control+Study%2C+1998-2000&rft.au=Lim%2C+U%3BSchenk%2C+M%3BKelemen%2C+LE%3BDavis%2C+S%3BCozen%2C+W%3BHartge%2C+P%3BWard%2C+M+H%3BStolzenberg-Solomon%2C+R&rft.aulast=Lim&rft.aufirst=U&rft.date=2005-11-01&rft.volume=162&rft.issue=10&rft.spage=953&rft.isbn=&rft.btitle=&rft.title=American+Journal+of+Epidemiology&rft.issn=00029262&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Inventories; Statistics; Food; Vitamin B6; Nutrients; Methionine; Non-Hodgkin's lymphoma; Epidemiology; Vitamin B12; Dietary supplements; Risk factors; alcohols; Folic acid; Metabolism; Ethanol; Diets; Alcohol; Lymphoma; USA, California, Los Angeles; USA, Michigan, Detroit; USA, Iowa; INE, USA, Washington, Seattle
ER  - 



TY  - JOUR
T1  - Molecular genetics of Staphylococcus epidermidis biofilms on indwelling medical devices
AN  - 19974084; 7051720
AB  - Staphylococcus epidermidis is an opportunistic pathogen associated with foreign body infections and nosocomial sepsis. The pathogenicity of S. epidermidis is mostly due to its ability to colonize indwelling polymeric devices and form a thick, multilayered biofilm. Biofilm formation is a major problem in treating S. epidermidis infection as biofilms provide significant resistance to antibiotics and to components of the innate host defenses. Various cell surface associated bacterial factors play a role in adherence and accumulation of the biofilm such as the polysaccharide Intercellular adhesin and the autolysin AtlE. Furthermore, recent studies have shown that global regulators such as the agr quorum sensing system, the transcriptional regulator sarA and the alternative sigma factor sigB have an important function in the regulation of biofilm formation. Understanding the many complex mechanisms involved in biofilm formation is a key factor in the search for new anti-staphyiococcal therapeutics.
JF  - International Journal of Artificial Organs
AU  - Vadyvaloo, V
AU  - Otto, M
AD  - Rocky Mountain Laboratories, NIAID/NIH, Hamilton, MT - USA
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1069
EP  - 1078
VL  - 28
IS  - 11
SN  - 0391-3988, 0391-3988
KW  - Genetics Abstracts; Microbiology Abstracts B: Bacteriology; Biotechnology and Bioengineering Abstracts
KW  - Adhesins
KW  - Cell surface
KW  - quorum sensing
KW  - Transcription
KW  - Antibiotics
KW  - Pathogens
KW  - Polysaccharides
KW  - Infection
KW  - Opportunist infection
KW  - Autolysins
KW  - Sepsis
KW  - Pathogenicity
KW  - Biofilms
KW  - Sigma factor
KW  - Staphylococcus epidermidis
KW  - Foreign bodies
KW  - Hospitals
KW  - J 02320:Cell Biology
KW  - W 30920:Tissue Engineering
KW  - G 07770:Bacteria
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Cell surface; Adhesins; quorum sensing; Transcription; Antibiotics; Pathogens; Infection; Polysaccharides; Opportunist infection; Autolysins; Sepsis; Pathogenicity; Biofilms; Sigma factor; Foreign bodies; Hospitals; Staphylococcus epidermidis
ER  - 



TY  - JOUR
T1  - Microbial Risk Indicators of Early Childhood Caries
AN  - 19967071; 7143721
AB  - The aim of this study was to use molecular identification methods, such as 16S RNA gene sequence and reverse-capture checkerboard hybridization, for identification of the bacteria associated with dental caries and with dental health in a subset of 204 twins aged 1.5 to 7 years old. A total of 448 plaque samples (118 collected from caries-free subjects and 330 from caries-active subjects) were used for analysis. We compared the bacteria found in biofilms of children exhibiting severe dental caries, with different degrees of lesion severity, with those found in biofilms of caries-free children. A panel of 82 bacterial species was selected, and a PCR-based reverse-capture checkerboard method was used for detection. A simple univariate test was used to determine the overabundance and underabundance of bacterial species in the diseased and in the healthy groups. Features identified with this univariate test were used to construct a probabilistic disease prediction model. Furthermore, a method for the analysis of global patterns of gene expression was performed to permit simultaneous analysis of the abundance of significant species by allowing cross-bacterial comparisons of abundance profiles between caries-active and caries-free subjects. Our results suggested that global patterns of microbial abundance in this population are very distinctive. The top bacterial species found to be overabundant in the caries-active group were Actinomyces sp. strain B19SC, Streptococcus mutans, and Lactobacillus spp., which exhibited an inverse relationship to beneficial bacterial species, such as Streptococcus parasanguinis, Abiotrophia defectiva, Streptococcus mitis, Streptococcus oralis, and Streptococcus sanguinis.
JF  - Journal of Clinical Microbiology
AU  - Corby, P M
AU  - Lyons-Weiler, J
AU  - Bretz, WA
AU  - Hart, T C
AU  - Aas, JA
AU  - Boumenna, T
AU  - Goss, J
AU  - Corby, AL
AU  - Junior, H M
AU  - Weyant, R J
AU  - Paster, B J
AD  - University of Pittsburgh, School of Dental Medicine, Pittsburgh, Pennsylvania. Harvard University, School of Dental Medicine, Boston, Massachusetts. University of Pittsburgh, Hillman Cancer Center, Pittsburgh, Pennsylvania. National Institute of Dental and Craniofacial Research, NIH, Division of Intramural Clinical Research, Bethesda, Maryland. Forsyth Institute, Boston, Massachusetts. University of Oslo, Institute of Oral Biology, Oslo, Norway. Twins Institute for Genetics Research, Montes Claros, Brazil. UNIMONTES, Montes Claros, Brazil
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 5753
EP  - 5759
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 43
IS  - 11
SN  - 0095-1137, 0095-1137
KW  - Microbiology Abstracts A: Industrial & Applied Microbiology; Microbiology Abstracts B: Bacteriology; Calcium & Calcified Tissue Abstracts
KW  - Nucleotide sequence
KW  - Abundance
KW  - Streptococcus parasanguinis
KW  - Children
KW  - Abiotrophia defectiva
KW  - Models
KW  - Gene expression
KW  - Dental caries
KW  - Lactobacillus
KW  - Twins
KW  - RNA
KW  - Streptococcus sanguinis
KW  - Plaques
KW  - Biofilms
KW  - Streptococcus mutans
KW  - Streptococcus mitis
KW  - Actinomyces
KW  - Streptococcus oralis
KW  - T 2045:Teeth
KW  - J 02400:Human Diseases
KW  - A 01300:Methods
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Gene expression; Dental caries; Twins; RNA; Nucleotide sequence; Abundance; Plaques; Biofilms; Children; Models; Lactobacillus; Streptococcus sanguinis; Streptococcus parasanguinis; Streptococcus mutans; Streptococcus mitis; Abiotrophia defectiva; Actinomyces; Streptococcus oralis
ER  - 



TY  - JOUR
T1  - Moraxella catarrhalis Bacterium without Endotoxin, a Potential Vaccine Candidate
AN  - 19941422; 6503148
AB  - Lipooligosaccharide (LOS) is a major surface component of Moraxella catarrhalis and a possible virulence factor in the pathogenesis of human infections caused by this organism. The presence of LOS on the bacterium is an obstacle to the development of vaccines derived from whole cells or outer membrane components of the bacterium. An lpxA gene encoding UDP-N-acetylglucosamine acyltransferase responsible for the first step of lipid A biosynthesis was identified by the construction and characterization of an isogenic M. catarrhalis lpxA mutant in strain O35E. The resulting mutant was viable despite the complete loss of LOS. The mutant strain showed significantly decreased toxicity by the Limulus amebocyte lysate assay, reduced resistance to normal human serum, reduced adherence to human epithelial cells, and enhanced clearance in lungs and nasopharynx in a mouse aerosol challenge model. Importantly, the mutant elicited high levels of antibodies with bactericidal activity and provided protection against a challenge with the wild-type strain. These data suggest that the null LOS mutant is attenuated and may be a potential vaccine candidate against M. catarrhalis.
JF  - Infection and Immunity
AU  - Peng, Daxin
AU  - Hong, Wenzhou
AU  - Choudhury, Biswa P
AU  - Carlson, Russell W
AU  - Gu, Xin-Xing
AD  - Vaccine Research Section, National Institute on Deafness and Other Communication Disorders, Rockville, Maryland 20850. Complex Carbohydrate Research Center, University of Georgia, Athens, Georgia 30602
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 7569
EP  - 7577
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 73
IS  - 11
SN  - 0019-9567, 0019-9567
KW  - Microbiology Abstracts A: Industrial & Applied Microbiology; Genetics Abstracts; Immunology Abstracts; Microbiology Abstracts B: Bacteriology
KW  - Endotoxins
KW  - Amebocytes
KW  - Epithelial cells
KW  - Bacteria
KW  - Aerosols
KW  - Data processing
KW  - virulence factors
KW  - Outer membranes
KW  - Moraxella catarrhalis
KW  - Animal models
KW  - Nasopharynx
KW  - Toxicity
KW  - Infection
KW  - Lipooligosaccharides
KW  - Antibodies
KW  - Limulus
KW  - Acyltransferase
KW  - Lung
KW  - Lipid A
KW  - Vaccines
KW  - Bactericidal activity
KW  - J 02834:Vaccination and immunization
KW  - A 01340:Antibiotics & Antimicrobials
KW  - G 07320:Bacterial genetics
KW  - F 06100:Vaccines - active immunity
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Amebocytes; Endotoxins; Bacteria; Epithelial cells; Aerosols; Data processing; virulence factors; Outer membranes; Animal models; Nasopharynx; Toxicity; Infection; Lipooligosaccharides; Antibodies; Lung; Acyltransferase; Lipid A; Vaccines; Bactericidal activity; Limulus; Moraxella catarrhalis
ER  - 



TY  - JOUR
T1  - Detection of Lymph Node Involvement in Hematologic Malignancies Using Micromagnetic Resonance Lymphangiography with a Gadolinum-Labeled Dendrimer Nanoparticle
AN  - 19936045; 7076548
AB  - Animal models of lymphoma should reflect their counterparts in humans; however, it can be difficult to ascertain whether an induced disease is intralymphatic or extralymphatic based on direct visualization. Current imaging methods are insufficient for identifying lymphatic and intralymphatic involvement. To differentiate intralymphatic from extralymphatic involvement, we have developed a magnetic resonance imaging-based lymphangiography method and tested it on two animal models of lymphoma. A gadolinium (Gd)-labeled dendrimer nanoparticle (generation-6; similar to 220 kDa/ similar to 10 nm) was injected interstitially into mice bearing hematologic malignancies to perform dynamic micromagnetic resonance lymphangiography (micro-MRL). Both a standard T1-weighted 3D fast spoiled gradient echo and a T2/Tl-weighted 3D fast imaging employing steady-state acquisition (3D-FIESTA-C) were compared in an imaging study to differentiate intralymphatic from extralymphatic involvement of tumors. The lymphatics and lymph nodes were visualized with both methods in all cases. In addition, 3D-FIESTA-C depicted both the lymphatic system and the extralymphatic tumor. In an animal model, 3D-FIESTA-C demonstrated that the bulk of the tumor thought to be intralymphatic was actually extralymphatic. In conclusion, micro-MRL, using Gd-labeled dendrimer nanoparticles with the combined method, can define both the normal and abnormal lymphatics and can distinguish intralymphatic from extralymphatic diseases in mouse models of malignant lymphoma.
JF  - Neoplasia
AU  - Kobayashi, H
AU  - Kawamoto, S
AU  - Brechbiel, M W
AU  - Bernardo, M
AU  - Sato, N
AU  - Waldmann, T A
AU  - Tagaya, Y
AU  - Choyke, P L
AD  - Molecular Imaging Program, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 984
EP  - 991
VL  - 7
IS  - 11
SN  - 1522-8002, 1522-8002
KW  - Immunology Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Malignancy
KW  - Gadolinium
KW  - Magnetic resonance imaging
KW  - Animal models
KW  - Tumors
KW  - imaging
KW  - Lymphoma
KW  - nanoparticles
KW  - Lymph nodes
KW  - Lymphatic system
KW  - Lymphangiography
KW  - W 30905:Medical Applications
KW  - F 06915:Cancer Immunology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Malignancy; Magnetic resonance imaging; Gadolinium; Animal models; Tumors; nanoparticles; Lymphoma; imaging; Lymphatic system; Lymph nodes; Lymphangiography
DO  - http://dx.doi.org/10.1593/neo.05454
ER  - 



TY  - JOUR
T1  - Modeling genome evolution with a diffusion approximation of a birth-and-death process
AN  - 19883459; 7873098
AB  - Motivation: In our previous studies, we developed discrete-space birth, death and innovation models (BDIMs) of genome evolution. These models explain the origin of the characteristic Pareto distribution of paralogous gene family sizes in genomes, and model parameters that provide for the evolution of these distributions within a realistic time frame have been identified. However, extracting the temporal dynamics of genome evolution from discrete-space BDIM was not technically feasible. We were interested in obtaining dynamic portraits of the genome evolution process by developing a diffusion approximation of BDIM. Results: The diffusion version of BDIM belongs to a class of continuous-state models whose dynamics is described by the Fokker-Plank equation and the stationary solution could be any specified Pareto function. The diffusion models have time-dependent solutions of a special kind, namely, generalized self-similar solutions, which describe the transition from one stationary distribution of the system to another; this provides for the possibility of examining the temporal dynamics of genome evolution. Analysis of the generalized self-similar solutions of the diffusion BDIM reveals a biphasic curve of genome growth in which the initial, relatively short, self-accelerating phase is followed by a prolonged phase of slow deceleration. This evolutionary dynamics was observed both when genome growth started from zero and proceeded via innovation (a potential model of primordial evolution), and when evolution proceeded from one stationary state to another. In biological terms, this regime of evolution can be tentatively interpreted as a punctuated-equilibrium-like phenomenon whereby evolutionary transitions are accompanied by rapid gene amplification and innovation, followed by slow relaxation to a new stationary state.
JF  - Bioinformatics
AU  - Karev, Georgy P
AU  - Berezovskaya, Faina S
AU  - Koonin, Eugene V
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1
PB  - Oxford University Press, Oxford Journals, Great Clarendon Street
VL  - 21
IS  - S3
SN  - 1367-4803, 1367-4803
KW  - Genetics Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Genomes
KW  - Birth
KW  - Mathematical models
KW  - Gene amplification
KW  - Diffusion
KW  - Bioinformatics
KW  - Gene families
KW  - Models
KW  - G 07740:Evolution
KW  - W 30960:Bioinformatics & Computer Applications
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-01-01
N1  - Last updated - 2015-03-27
N1  - SubjectsTermNotLitGenreText - Birth; Genomes; Mathematical models; Gene amplification; Diffusion; Bioinformatics; Gene families; Models
ER  - 



TY  - JOUR
T1  - Pooled ORF Expression Technology (POET): Using Proteomics to Screen Pools of Open Reading Frames for Protein Expression
AN  - 19770431; 7144614
AB  - We have developed a pooled ORF expression technology, POET, that uses recombinational cloning and proteomic methods (two-dimensional gel electrophoresis and mass spectrometry) to identify ORFs that when expressed are likely to yield high levels of soluble, purified protein. Because the method works on pools of ORFs, the procedures needed to subclone, express, purify, and assay protein expression for hundreds of clones are greatly simplified. Small scale expression and purification of 12 positive clones identified by POET from a pool of 688 Caenorhabditis elegans ORFs expressed in Escherichia coli yielded on average 6 times as much protein as 12 negative clones. Larger scale expression and purification of six of the positive clones yielded 47-374 mg of purified protein/liter. Using POET, pools of ORFs can be constructed, and the pools of the resulting proteins can be analyzed and manipulated to rapidly acquire information about the attributes of hundreds of proteins simultaneously.
JF  - Molecular and Cellular Proteomics
AU  - Gillette, William K
AU  - Esposito, Dominic
AU  - Frank, Peter H
AU  - Zhou, Ming
AU  - Yu, Li-Rong
AU  - Jozwik, Catherine
AU  - Zhang, Xiuying
AU  - McGowan, Brighid
AU  - Jacobowitz, David M
AU  - Pollard, Harvey B
AU  - Hao, Tong
AU  - Hill, David E
AU  - Vidal, Marc
AU  - Conrads, Thomas P
AU  - Veenstra, Timothy D
AU  - Hartley, James L
AD  - Protein Expression Laboratory and Laboratory of Proteomics and Analytical Technologies, Research Technology Program, SAIC-Frederick, Inc./NCI, National Institutes of Health, Frederick, Maryland 21702, Department of Anatomy, Physiology, and Genetics, Uniformed Services University, Bethesda, Maryland 20814, Center for Cancer Systems Biology and Department of Cancer Biology, Dana-Farber Cancer Institute, and Department of Genetics, Harvard Medical School, Boston, Massachusetts 02115, and Laboratory of Clinical Science, National Institute of Mental Health, Bethesda, Maryland 20892
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1647
EP  - 1652
PB  - American Society for Biochemistry and Molecular Biology, 9650 Rockville Pike Bethesda MD 20814-3996 USA, [mailto:asbmb@asbmb.faseb.org], [URL:http://www.asbmb.org/]
VL  - 4
IS  - 11
SN  - 1535-9476, 1535-9476
KW  - Microbiology Abstracts B: Bacteriology; Biotechnology and Bioengineering Abstracts
KW  - Caenorhabditis elegans
KW  - Escherichia coli
KW  - proteomics
KW  - protein purification
KW  - Open reading frames
KW  - Gel electrophoresis
KW  - Mass spectroscopy
KW  - J 02310:Genetics & Taxonomy
KW  - W 30960:Bioinformatics & Computer Applications
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Molecular+and+Cellular+Proteomics&rft.atitle=Pooled+ORF+Expression+Technology+%28POET%29%3A+Using+Proteomics+to+Screen+Pools+of+Open+Reading+Frames+for+Protein+Expression&rft.au=Gillette%2C+William+K%3BEsposito%2C+Dominic%3BFrank%2C+Peter+H%3BZhou%2C+Ming%3BYu%2C+Li-Rong%3BJozwik%2C+Catherine%3BZhang%2C+Xiuying%3BMcGowan%2C+Brighid%3BJacobowitz%2C+David+M%3BPollard%2C+Harvey+B%3BHao%2C+Tong%3BHill%2C+David+E%3BVidal%2C+Marc%3BConrads%2C+Thomas+P%3BVeenstra%2C+Timothy+D%3BHartley%2C+James+L&rft.aulast=Gillette&rft.aufirst=William&rft.date=2005-11-01&rft.volume=4&rft.issue=11&rft.spage=1647&rft.isbn=&rft.btitle=&rft.title=Molecular+and+Cellular+Proteomics&rft.issn=15359476&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - protein purification; proteomics; Mass spectroscopy; Gel electrophoresis; Open reading frames; Caenorhabditis elegans; Escherichia coli
ER  - 



TY  - JOUR
T1  - The observed effects of teenage passengers on the risky driving behavior of teenage drivers
AN  - 19719254; 7511129
AB  - The association between teenage passengers and crash risks among young drivers may be due to risky driving behavior. We investigated the effect on two measures of risky driving in the presence of young male and female passengers. Vehicles exiting from parking lots at 10 high schools were observed and the occupants were identified by gender and age (teen or adult). At a nearby site, the speed and headway of passing traffic were recorded using video and LIDAR technology. Teenage drivers drove faster than the general traffic and allowed shorter headways, particularly in the presence of a male teenage passenger. Both male and female teenage drivers allowed shorter headways (relative to no passenger or a female passenger) in the presence of a male teenage passenger, while the presence of a female teenage passenger resulted in longer headways for male teenage drivers. Overall, the observed rate of high risk driving (defined as speed >=15mph or more above the posted speed limit and/or headway of <=1.0s) for the teen male driver/male passenger condition was about double that of general traffic. In conclusion, the presence of male teenage passengers was associated with risky driving behavior among teenage drivers.
JF  - Accident Analysis & Prevention
AU  - Simons-Morton, Bruce
AU  - Lerner, Neil
AU  - Singer, Jeremiah
AD  - Prevention Research Branch, Division of Epidemiology, Statistics, and Prevention Research, National Institute of Child Health and Human Development, National Institutes of Health, 6100 Executive Blvd RM#7B13M, Bethesda, MD 20892-7510, USA, Mortonb@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 973
EP  - 982
PB  - Elsevier Science Ltd., Pergamon, P.O. Box 800 Kidlington Oxford OX5 1DX UK, [mailto:nlinfo-f@elsevier.nl], [URL:http://www.elsevier.nl]
VL  - 37
IS  - 6
SN  - 0001-4575, 0001-4575
KW  - Health & Safety Science Abstracts; Risk Abstracts
KW  - Motor vehicles
KW  - Adolescents
KW  - Risk taking
KW  - Social influences
KW  - Speeding
KW  - Passengers
KW  - Accidents
KW  - Behavior
KW  - driving ability
KW  - Gender
KW  - prevention
KW  - Traffic safety
KW  - decision making
KW  - H 2000:Transportation
KW  - R2 23110:Psychological aspects
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19719254?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ariskabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Accident+Analysis+%26+Prevention&rft.atitle=The+observed+effects+of+teenage+passengers+on+the+risky+driving+behavior+of+teenage+drivers&rft.au=Simons-Morton%2C+Bruce%3BLerner%2C+Neil%3BSinger%2C+Jeremiah&rft.aulast=Simons-Morton&rft.aufirst=Bruce&rft.date=2005-11-01&rft.volume=37&rft.issue=6&rft.spage=973&rft.isbn=&rft.btitle=&rft.title=Accident+Analysis+%26+Prevention&rft.issn=00014575&rft_id=info:doi/10.1016%2Fj.aap.2005.04.014
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-08-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Accidents; Behavior; driving ability; Gender; prevention; decision making; Traffic safety; Adolescents
DO  - http://dx.doi.org/10.1016/j.aap.2005.04.014
ER  - 



TY  - JOUR
T1  - Multicontrast delayed enhancement provides improved contrast between myocardial infarction and blood pool
AN  - 19687218; 7456794
AB  - To develop and test a delayed-enhancement imaging method for improving the contrast between myocardial infarction (MI) and blood pool. The T sub(2) of blood is significantly longer than that of acute or chronic MI. The proposed multicontrast delayed-enhancement (MCODE) imaging method produces a series of images with both T sub(1) and T sub(2) weightings, which provides both excellent contrast between normal and infarcted myocardium, and between blood and MI. The subendocardial border between MI and blood pool was easily discriminated in the T sub(2)-weighted image. The measured MI-to-blood contrast-to-noise ratio (CNR) was better in the T sub(2)-weighted image than in the T sub(1)-weighted image (22.5 +/- 8.7 vs. 2.9 +/- 3.1, mean +/- SD, N = 11, P < 0.001, for TrueFISP, and 19.4 +/- 10.8 vs. 3.9 +/- 2.3, N = 11, P < 0.001, for TurboFLASH). The MCODE method provides a significant improvement in the ability to easily discriminate subendocardial MI by providing a T sub(2)-weighted image with high contrast between blood and MI. MCODE should improve both the detection and accurate sizing of MI. J. Magn. Reson. Imaging 2005. Published by Wiley-Liss, Inc.
JF  - Journal of Magnetic Resonance Imaging
AU  - Kellman, Peter
AU  - Chung, Yiu-Cho
AU  - Simonetti, Orlando P
AU  - McVeigh, Elliot R
AU  - Arai, Andrew E
AD  - Laboratory of Cardiac Energetics, National Heart, Lung and Blood Institute, National Institutes of Health, DHHS, Bethesda, Maryland, USA, kellman@nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 605
EP  - 613
PB  - John Wiley & Sons, Inc., 111 River Street Hoboken NJ 07030 USA, [mailto:custserv@wiley.com], [URL:http://www.wiley.com/]
VL  - 22
IS  - 5
SN  - 1053-1807, 1053-1807
KW  - Biotechnology and Bioengineering Abstracts
KW  - Blood
KW  - Magnetic resonance imaging
KW  - Myocardial infarction
KW  - Myocardium
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19687218?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Magnetic+Resonance+Imaging&rft.atitle=Multicontrast+delayed+enhancement+provides+improved+contrast+between+myocardial+infarction+and+blood+pool&rft.au=Kellman%2C+Peter%3BChung%2C+Yiu-Cho%3BSimonetti%2C+Orlando+P%3BMcVeigh%2C+Elliot+R%3BArai%2C+Andrew+E&rft.aulast=Kellman&rft.aufirst=Peter&rft.date=2005-11-01&rft.volume=22&rft.issue=5&rft.spage=605&rft.isbn=&rft.btitle=&rft.title=Journal+of+Magnetic+Resonance+Imaging&rft.issn=10531807&rft_id=info:doi/10.1002%2Fjmri.20426
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Blood; Myocardial infarction; Magnetic resonance imaging; Myocardium
DO  - http://dx.doi.org/10.1002/jmri.20426
ER  - 



TY  - JOUR
T1  - The Progress and Promise of Molecular Imaging Probes in Oncologic Drug Development
AN  - 19464576; 7142108
AB  - As addressed by the recent Food and Drug Administration Critical Path Initiative, tools are urgently needed to increase the speed, efficiency, and cost-effectiveness of drug development for cancer and other diseases. Molecular imaging probes developed based on recent scientific advances have great potential as oncologic drug development tools. Basic science studies using molecular imaging probes can help to identify and characterize disease-specific targets for oncologic drug therapy. Imaging end points, based on these disease-specific biomarkers, hold great promise to better define, stratify, and enrich study groups and to provide direct biological measures of response. Imaging-based biomarkers also have promise for speeding drug evaluation by supplementing or replacing preclinical and clinical pharmacokinetic and pharmacodynamic evaluations, including target interaction and modulation. Such analyses may be particularly valuable in early comparative studies among candidates designed to interact with the same molecular target. Finally, as response biomarkers, imaging end points that characterize tumor vitality, growth, or apoptosis can also serve as early surrogates of therapy success. This article outlines the scientific basis of oncology imaging probes and presents examples of probes that could facilitate progress. The current regulatory opportunities for new and existing probe development and testing are also reviewed, with a focus on recent Food and Drug Administration guidance to facilitate early clinical development of promising probes.
JF  - Clinical Cancer Research
AU  - Kelloff, Gary J
AU  - Krohn, Kenneth A
AU  - Larson, Steven M
AU  - Weissleder, Ralph
AU  - Mankoff, David A
AU  - Hoffman, John M
AU  - Link, Jeanne M
AU  - Guyton, Kathryn Z
AU  - Eckelman, William C
AU  - Scher, Howard I
AU  - O'Shaughnessy, Joyce
AU  - Cheson, Bruce D
AU  - Sigman, Caroline C
AU  - Tatum, James L
AU  - Mills, George Q
AU  - Sullivan, Daniel C
AU  - Woodcock, Janet
AD  - Authors' Affiliations: Cancer Imaging Program, Division of Cancer Treatment and Diagnosis, National Cancer Institute, NIH
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 7967
EP  - 7985
PB  - American Association for Cancer Research, 615 Chestnut St., 17th Floor Philadelphia PA 19106-4404 USA, [URL:http://www.aacr.org/]
VL  - 11
IS  - 22
SN  - 1078-0432, 1078-0432
KW  - Biotechnology and Bioengineering Abstracts
KW  - Apoptosis
KW  - Reviews
KW  - Oncology
KW  - Drug development
KW  - Tumors
KW  - biomarkers
KW  - imaging
KW  - Pharmacodynamics
KW  - Pharmacokinetics
KW  - Cancer
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19464576?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+Cancer+Research&rft.atitle=The+Progress+and+Promise+of+Molecular+Imaging+Probes+in+Oncologic+Drug+Development&rft.au=Kelloff%2C+Gary+J%3BKrohn%2C+Kenneth+A%3BLarson%2C+Steven+M%3BWeissleder%2C+Ralph%3BMankoff%2C+David+A%3BHoffman%2C+John+M%3BLink%2C+Jeanne+M%3BGuyton%2C+Kathryn+Z%3BEckelman%2C+William+C%3BScher%2C+Howard+I%3BO%27Shaughnessy%2C+Joyce%3BCheson%2C+Bruce+D%3BSigman%2C+Caroline+C%3BTatum%2C+James+L%3BMills%2C+George+Q%3BSullivan%2C+Daniel+C%3BWoodcock%2C+Janet&rft.aulast=Kelloff&rft.aufirst=Gary&rft.date=2005-11-01&rft.volume=11&rft.issue=22&rft.spage=7967&rft.isbn=&rft.btitle=&rft.title=Clinical+Cancer+Research&rft.issn=10780432&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - imaging; Drug development; biomarkers; Reviews; Cancer; Tumors; Pharmacokinetics; Pharmacodynamics; Oncology; Apoptosis
ER  - 



TY  - JOUR
T1  - Impact of Hysterectomy on Endometrial Carcinoma Rates in the United States
AN  - 19461278; 7144218
AB  - In the United States, endometrial carcinoma incidence rates, uncorrected for hysterectomy prevalence, are higher among white women than black women. We estimated corrected endometrial carcinoma rates by racial/ethnic groups and age (30-74 years) for 1992-2000 using data from the Surveillance, Epidemiology, and End Results program and the Behavioral Risk Factor Surveillance Survey. Hysterectomy prevalence was higher among black women than among Hispanic and white non-Hispanic women. Correcting for hysterectomy prevalence increased age-adjusted endometrial carcinoma rates per 10 super(5) woman-years from 29.2 to 48.7 (66.8% increase) overall, from 14.6 to 28.5 (95.3% increase) in blacks, from 18.8 to 29.6 (57.6% increase) in Hispanics, and from 33.2 to 54.9 (65.1%) in white non-Hispanics. This correction reduced the rate ratio for white non-Hispanics compared with blacks from 2.27 to 1.93. Among blacks but not Hispanics or white non-Hispanics, the endometrial carcinoma risk factors of obesity and diabetes were more prevalent among hysterectomized than nonhysterectomized women. Failure to correct for hysterectomy prevalence may lead to underestimates of endometrial carcinoma risk, especially among blacks.The high prevalence of hysterectomy among blacks with strong endometrial cancer risk factors may partly account for lower cancer rates in this group.
JF  - Journal of the National Cancer Institute
AU  - Sherman, Mark E
AU  - Carreon, Joseph D
AU  - Lacey, James VJr
AU  - Devesa, Susan S
AD  - Hormonal and Reproductive Epidemiology (MES, JDC, JVL) and Biostatistics (SSD) Branches, Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Bethesda, MD
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1700
EP  - 1702
PB  - Oxford University Press, Oxford Journals, Great Clarendon Street Oxford OX2 6DP UK, [mailto:jnl.samples@oup.co.uk], [URL:http://www3.oup.co.uk/jnls/]
VL  - 97
IS  - 22
SN  - 0027-8874, 0027-8874
KW  - hysterectomy
KW  - Risk Abstracts
KW  - USA
KW  - obesity
KW  - Females
KW  - Cancer
KW  - Ethnic groups
KW  - R2 23060:Medical and environmental health
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19461278?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ariskabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+the+National+Cancer+Institute&rft.atitle=Impact+of+Hysterectomy+on+Endometrial+Carcinoma+Rates+in+the+United+States&rft.au=Sherman%2C+Mark+E%3BCarreon%2C+Joseph+D%3BLacey%2C+James+VJr%3BDevesa%2C+Susan+S&rft.aulast=Sherman&rft.aufirst=Mark&rft.date=2005-11-01&rft.volume=97&rft.issue=22&rft.spage=1700&rft.isbn=&rft.btitle=&rft.title=Journal+of+the+National+Cancer+Institute&rft.issn=00278874&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-01-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - obesity; Females; Ethnic groups; Cancer; USA
ER  - 



TY  - JOUR
T1  - Activity of anchored human matrix metalloproteinase-1 catalytic domain on Au (111) surfaces monitored by ESI-MS
AN  - 19422977; 6673152
AB  - Matrix metalloproteinases (MMPs) are a family of Zn-dependent endo- peptidases known for their ability to cleave several components of the extracellular matrix, but which can also cleave many non-matrix proteins. There are many evidences that MMPs are involved in physiological and pathological processes, and a huge effort has been put in the development of possible inhibitors that could reduce the activity of MMPs, as it is clear that the ability to monitor and control such activity plays a pivotal role in the search for potential drugs aimed at finding a cure for several diseases such as pulmonary emphysema, rheumatoid arthritis, fibrotic disorders and cancer.
JF  - Journal of Mass Spectrometry
AU  - Grasso, Giuseppe
AU  - D'Agata, Roberta
AU  - Rizzarelli, Enrico
AU  - Spoto, Giuseppe
AU  - D'Andrea, Luca
AU  - Pedone, Carlo
AU  - Picardi, Andrea
AU  - Romanelli, Alessandra
AU  - Fragai, Marco
AU  - Yeo, Kwon Joo
AD  - Consorzio Interuniversitario di Ricerca in Chimica dei Metalli nei Sistemi Biologici, Via C. Ulpiani 27, 70126, Bari, Italy, gspoto@dipchi.unict.it
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1565
EP  - 1571
PB  - John Wiley & Sons, Ltd., Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 40
IS  - 12
SN  - 1076-5174, 1076-5174
KW  - Biotechnology and Bioengineering Abstracts
KW  - Emphysema
KW  - Rheumatoid arthritis
KW  - Extracellular matrix
KW  - Lung diseases
KW  - Matrix metalloproteinase
KW  - Drug development
KW  - peptidase
KW  - Cancer
KW  - Mass spectroscopy
KW  - W 30905:Medical Applications
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19422977?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Mass+Spectrometry&rft.atitle=Activity+of+anchored+human+matrix+metalloproteinase-1+catalytic+domain+on+Au+%28111%29+surfaces+monitored+by+ESI-MS&rft.au=Grasso%2C+Giuseppe%3BD%27Agata%2C+Roberta%3BRizzarelli%2C+Enrico%3BSpoto%2C+Giuseppe%3BD%27Andrea%2C+Luca%3BPedone%2C+Carlo%3BPicardi%2C+Andrea%3BRomanelli%2C+Alessandra%3BFragai%2C+Marco%3BYeo%2C+Kwon+Joo&rft.aulast=Grasso&rft.aufirst=Giuseppe&rft.date=2005-11-01&rft.volume=40&rft.issue=12&rft.spage=1565&rft.isbn=&rft.btitle=&rft.title=Journal+of+Mass+Spectrometry&rft.issn=10765174&rft_id=info:doi/10.1002%2Fjms.929
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Drug development; peptidase; Mass spectroscopy; Emphysema; Cancer; Lung diseases; Extracellular matrix; Matrix metalloproteinase; Rheumatoid arthritis
DO  - http://dx.doi.org/10.1002/jms.929
ER  - 



TY  - JOUR
T1  - Analysis of mass spectral serum profiles for biomarker selection
AN  - 19419657; 6509140
AB  - MOTIVATION: Mass spectrometric profiles of peptides and proteins obtained by current technologies are characterized by complex spectra, high dimensionality and substantial noise. These characteristics generate challenges in the discovery of proteins and protein-profiles that distinguish disease states, e.g. cancer patients from healthy individuals. We present low-level methods for the processing of mass spectral data and a machine learning method that combines support vector machines, with particle swarm optimization for biomarker selection. RESULTS: The proposed method identified mass points that achieved high prediction accuracy in distinguishing liver cancer patients from healthy individuals in SELDI-QqTOF profiles of serum. AVAILABILITY: MATLAB scripts to implement the methods described in this paper are available from the HWR's lab website http://lombardi.georgetown.edu/labpage CONTACT: hwreorgetown.edu
JF  - Bioinformatics
AU  - Ressom, Habtom W
AU  - Varghese, Rency S
AU  - Abdel-Hamid, Mohamed
AU  - Eissa, Sohair Abdel-Latif
AU  - Saha, Daniel
AU  - Goldman, Lenka
AU  - Petricoin, Emanuel F
AU  - Conrads, Thomas P
AU  - Veenstra, Timothy D
AU  - Loffredo, Christopher A
AU  - Goldman, Radoslav
AD  - Lombardi Comprehensive Cancer Center, Georgetown University Washington, DC, USA. Viral Hepatitis Research Laboratory, NHTMRI Cairo, Egypt. Natinal Cancer Institute Cairo, Egypt. Clinical Proteomics Program, NCI/FDA, Center for Biologics Evaluation, FDA USA. SAIC-Frederick and Biomedical Proteomics Program, NCI Frederick, MD, USA
Y1  - 2005/11/01/
PY  - 2005
DA  - 2005 Nov 01
SP  - 4039
EP  - 4045
PB  - Oxford University Press, Oxford Journals, Great Clarendon Street Oxford OX2 6DP UK, [mailto:jnl.samples@oup.co.uk], [URL:http://www3.oup.co.uk/jnls/]
VL  - 21
IS  - 21
SN  - 1367-4803, 1367-4803
KW  - Biotechnology and Bioengineering Abstracts
KW  - Swarms
KW  - Bioinformatics
KW  - Learning algorithms
KW  - biomarkers
KW  - W 30960:Bioinformatics & Computer Applications
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19419657?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Bioinformatics&rft.atitle=Analysis+of+mass+spectral+serum+profiles+for+biomarker+selection&rft.au=Ressom%2C+Habtom+W%3BVarghese%2C+Rency+S%3BAbdel-Hamid%2C+Mohamed%3BEissa%2C+Sohair+Abdel-Latif%3BSaha%2C+Daniel%3BGoldman%2C+Lenka%3BPetricoin%2C+Emanuel+F%3BConrads%2C+Thomas+P%3BVeenstra%2C+Timothy+D%3BLoffredo%2C+Christopher+A%3BGoldman%2C+Radoslav&rft.aulast=Ressom&rft.aufirst=Habtom&rft.date=2005-11-01&rft.volume=21&rft.issue=21&rft.spage=4039&rft.isbn=&rft.btitle=&rft.title=Bioinformatics&rft.issn=13674803&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - biomarkers; Learning algorithms; Bioinformatics; Swarms
ER  - 



TY  - JOUR
T1  - A Family Portrait of the RIO Kinases
AN  - 19376981; 7143124
AB  - The RIO family of atypical serine protein kinases has been first characterized only recently. It consists of enzymes that contain a unique domain with a characteristic kinase sequence motif and usually some additional domains. At least two RIO proteins, Rio1 and Rio2, are present in organisms varying from Archaea to humans, with a third Rio3 subfamily present only in multicellular eukaryotes. Yeast Rio1 and Rio2 proteins have been implicated in the processing of 20 S pre-rRNA and are necessary for survival of the cells. Crystal structures of Archaeoglobus fulgidus Rio1 and Rio2 have shown that whereas the overall fold of these enzymes resembles typical protein kinases, some of the structural domains, particularly those involved in peptide substrate binding, are not present. The mode of binding of nucleotides also differs from that found in typical protein kinases. Although it has been shown that both Rio1 and Rio2 have the enzymatic activity of kinases and are capable of autophosphorylation, the biological substrates of RIO proteins and their full biological role still remain to be discovered.
JF  - Journal of Biological Chemistry
AU  - LaRonde-LeBlanc, Nicole
AU  - Wlodawer, Alexander
AD  - Protein Structure Section, Macromolecular Crystallography Laboratory, NCI-Frederick, National Institutes of Health, Frederick, Maryland 21702-1201
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 37297
EP  - 37300
PB  - American Society for Biochemistry and Molecular Biology, 9650 Rockville Pike Bethesda MD 20814-3996 USA, [mailto:asbmb@asbmb.faseb.org], [URL:http://www.jbc.org]
VL  - 280
IS  - 45
SN  - 0021-9258, 0021-9258
KW  - Microbiology Abstracts B: Bacteriology
KW  - Cell survival
KW  - Archaea
KW  - Archaeoglobus fulgidus
KW  - Crystal structure
KW  - Protein kinase
KW  - Enzymes
KW  - Enzymatic activity
KW  - Serine
KW  - Nucleotides
KW  - J 02330:Biochemistry
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19376981?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Biological+Chemistry&rft.atitle=A+Family+Portrait+of+the+RIO+Kinases&rft.au=LaRonde-LeBlanc%2C+Nicole%3BWlodawer%2C+Alexander&rft.aulast=LaRonde-LeBlanc&rft.aufirst=Nicole&rft.date=2005-11-01&rft.volume=280&rft.issue=45&rft.spage=37297&rft.isbn=&rft.btitle=&rft.title=Journal+of+Biological+Chemistry&rft.issn=00219258&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Cell survival; Crystal structure; Enzymes; Protein kinase; Enzymatic activity; Nucleotides; Serine; Archaea; Archaeoglobus fulgidus
ER  - 



TY  - JOUR
T1  - Toll-like Receptor 4 Signaling Regulates Cytosolic Phospholipase A sub(2) Activation and Lipid Generation in Lipopolysaccharide-stimulated Macrophages
AN  - 19375330; 7143319
AB  - Inflammatory lipid mediators such as prostaglandins and leukotrienes play crucial roles in the pathogenesis of bacterial lipopolysaccharide (LPS)-induced inflammation. Cytosolic phospholipase A sub(2) (cPLA sub(2)) is a key enzyme in the generation of pro-inflammatory lipid mediators. Here, we found that Toll-like receptor 4 (TLR4) is essential for LPS-induced cPLA sub(2) activation and lipid release. Inhibition of TLR4 protein expression by TLR4 small interfering RNA or neutralization of TLR4 by the specific antibody against TLR4/MD2 blocked cPLA sub(2) phosphorylation and cPLA sub(2)-hydrolyzed arachidonic acid release. Furthermore, activation of the TLR4 signaling pathway by LPS regulated cPLA sub(2) activation and lipid release. cPLA sub(2) phosphorylation and cPLA sub(2)-hydrolyzed lipid release were significantly impaired when TLR4 adaptor protein, either MyD88 or TRIF, was knocked down in LPS-stimulated macrophages. Similarly, LPS-induced arachidonate release was inhibited in cells transfected with a dominant-negative MyD88 or TRIF construct. Subsequently, cPLA sub(2) activation could be suppressed by inhibition of the TLR4 adaptor protein-directed p38 and ERK MAPK pathways. These findings suggest that, in LPS-induced inflammation, the TLR4-mediated MyD88- and TRIF-dependent MAPK pathways result in cPLA sub(2) activation and production of pro-inflammatory lipid mediators.
JF  - Journal of Biological Chemistry
AU  - Qi, Hai-Yan
AU  - Shelhamer, James H
AD  - Critical Care Medicine Department, Clinical Center, National Institutes of Health, Bethesda, Maryland 20892
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 38969
EP  - 38975
PB  - American Society for Biochemistry and Molecular Biology, 9650 Rockville Pike Bethesda MD 20814-3996 USA, [mailto:asbmb@asbmb.faseb.org], [URL:http://www.jbc.org]
VL  - 280
IS  - 47
SN  - 0021-9258, 0021-9258
KW  - Microbiology Abstracts B: Bacteriology; Immunology Abstracts
KW  - Macrophages
KW  - Leukotrienes
KW  - MAP kinase
KW  - MyD88 protein
KW  - Phospholipase A2
KW  - Lipids
KW  - Prostaglandins
KW  - Enzymes
KW  - Arachidonic acid
KW  - Inflammation
KW  - Cell activation
KW  - Extracellular signal-regulated kinase
KW  - adaptor proteins
KW  - Antibodies
KW  - Phosphorylation
KW  - siRNA
KW  - Lipopolysaccharides
KW  - TLR4 protein
KW  - Toll-like receptors
KW  - Signal transduction
KW  - J 02350:Immunology
KW  - F 06965:Immune Cells
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19375330?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Biological+Chemistry&rft.atitle=Toll-like+Receptor+4+Signaling+Regulates+Cytosolic+Phospholipase+A+sub%282%29+Activation+and+Lipid+Generation+in+Lipopolysaccharide-stimulated+Macrophages&rft.au=Qi%2C+Hai-Yan%3BShelhamer%2C+James+H&rft.aulast=Qi&rft.aufirst=Hai-Yan&rft.date=2005-11-01&rft.volume=280&rft.issue=47&rft.spage=38969&rft.isbn=&rft.btitle=&rft.title=Journal+of+Biological+Chemistry&rft.issn=00219258&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Leukotrienes; Macrophages; MAP kinase; Phospholipase A2; MyD88 protein; Lipids; Prostaglandins; Arachidonic acid; Enzymes; Cell activation; Inflammation; Extracellular signal-regulated kinase; Antibodies; adaptor proteins; siRNA; Phosphorylation; Lipopolysaccharides; TLR4 protein; Toll-like receptors; Signal transduction
ER  - 



TY  - JOUR
T1  - Epidemiology of Pediatric Tuberculosis Using Traditional and Molecular Techniques: Houston, Texas
AN  - 19288808; 6505413
AB  - OBJECTIVE: To investigate the transmission dynamics of pediatric tuberculosis (TB) by analyzing the clinical characteristics with the molecular profiles of Mycobacterium tuberculosis isolates during a 5-year period. METHODS: A retrospective review of a prospective population-based active surveillance and molecular epidemiology project was conducted in private and public pediatric clinics within Houston and Harris County, Texas. The study population consisted of patients who had pediatric TB diagnosed from October 1, 1995, through September 30, 2000. Cases and potential source cases (PSC) were interviewed using a standardized questionnaire. Available Mycobacterium tuberculosis isolates from cases and PSCs were characterized and compared by IS6110 restriction fragment length polymorphism, spoligotyping, and genetic group assignment. Clinical characteristics were described, and molecular characterizations were compared. Data were analyzed by using EpiInfo 6.02b and SAS 8.2. RESULTS: A total of 220 (92%) of 238 pediatric TB cases were included. Epidemiologic and clinical findings were consistent with previous studies. Molecular profiles from 3 cases did not match the profile of PSC. Four previously unknown PSCs were identified using molecular techniques. Fifty-one (71.8%) of 71 isolates matched at least 1 other Houston Tuberculosis Initiative TB database isolate and were grouped into 33 molecular clusters. Cases were more likely to be clustered when the patients were younger than 5 years, identified a source case, or were US born. CONCLUSIONS: Traditional contact tracing may not always be accurate, and molecular characterization can lead to identification of previously unrecognized source cases. Recent transmission plays a significant role in the transmission of TB to children as evident by the high degree of clustering found in our study population.
JF  - Pediatrics
AU  - Wootton, Susan H
AU  - Gonzalez, Blanca E
AU  - Pawlak, Rebecca
AU  - Teeter, Larry D
AU  - Smith, Kim Connelly
AU  - Musser, James M
AU  - Starke, Jeffrey R
AU  - Graviss, Edward A
AD  - Department of Pediatrics, Infectious Disease Section, Baylor College of Medicine and Texas Children's Hospital, Houston, Texas. Pathology. Medicine, Baylor College of Medicine, Houston, Texas. Department of Pediatrics, University of Texas-Houston Medical School, Houston, Texas. Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Hamilton, Montana
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 1141
EP  - 1147
PB  - American Academy of Pediatrics, 141 Northwest Point Blvd. Elk Grove Village IL 60007-1098 USA, [mailto:journals@aap.org], [URL:http://www.aap.org]
VL  - 116
IS  - 5
SN  - 0031-4005, 0031-4005
KW  - Microbiology Abstracts B: Bacteriology
KW  - Inventories
KW  - Data processing
KW  - Pediatrics
KW  - Restriction fragment length polymorphism
KW  - Population studies
KW  - Contact tracing
KW  - Children
KW  - spoligotyping
KW  - Disease transmission
KW  - Databases
KW  - Epidemiology
KW  - Tuberculosis
KW  - Mycobacterium tuberculosis
KW  - J 02310:Genetics & Taxonomy
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Pediatrics&rft.atitle=Epidemiology+of+Pediatric+Tuberculosis+Using+Traditional+and+Molecular+Techniques%3A+Houston%2C+Texas&rft.au=Wootton%2C+Susan+H%3BGonzalez%2C+Blanca+E%3BPawlak%2C+Rebecca%3BTeeter%2C+Larry+D%3BSmith%2C+Kim+Connelly%3BMusser%2C+James+M%3BStarke%2C+Jeffrey+R%3BGraviss%2C+Edward+A&rft.aulast=Wootton&rft.aufirst=Susan&rft.date=2005-11-01&rft.volume=116&rft.issue=5&rft.spage=1141&rft.isbn=&rft.btitle=&rft.title=Pediatrics&rft.issn=00314005&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-12-01
N1  - Last updated - 2015-03-27
N1  - SubjectsTermNotLitGenreText - Databases; Inventories; Data processing; Epidemiology; Pediatrics; Restriction fragment length polymorphism; Population studies; Tuberculosis; Children; Contact tracing; Disease transmission; spoligotyping; Mycobacterium tuberculosis
ER  - 



TY  - JOUR
T1  - Disposition of Cocaine and Its Metabolites in Human Sweat after Controlled Cocaine Administration
AN  - 17663267; 6502872
AB  - BACKGROUND: Sweat testing is a noninvasive technique for monitoring drug exposure in treatment, criminal justice, and employment settings. METHODS: We evaluated cocaine excretion in 9 participants' sweat after they received 3 low doses (75 mg/70 kg) of cocaine HCl subcutaneously within 1 week and, 3 weeks later, 3 high doses (150 mg/70 kg). Six additional participants completed portions of the study. PharmChek registered sweat patches (n = 1390) were collected throughout a 3-week washout period, reflecting previously self-administered drugs, and during and after controlled dosing. RESULTS: Cocaine was the primary analyte detected with 24% of patches positive at the gas chromatography-mass spectrometry limit of quantification of 2.5 ng/patch and 7% of patches at the proposed Substance Abuse and Mental Health Services Administration cutoff of 25 ng/patch. Ecgonine methyl ester (EME) was detected more often and at generally higher concentrations than benzoylecgonine. In patches containing both metabolites, there was no statistically significant difference in the benzoylecgonine/EME ratio based on length of patch wear. During washout, 2 participants' weekly patches tested positive ( greater than or equal to 25 ng/patch) during the first week; one remained positive during week 2; and none were positive during week 3. Cocaine and EME were detectable within 2 h; benzoylecgonine was not detected until 4-8 h after low doses and slightly sooner after high doses. The majority of drug was excreted within 24 h. Over 70% of weekly patches worn during low doses were positive for cocaine ( greater than or equal to 25 ng/patch), increasing to 100% during high doses. CONCLUSION: Sweat testing is an effective and reliable method of monitoring cocaine exposure.
JF  - Clinical Chemistry
AU  - Kacinko, Sherri L
AU  - Barnes, Allan J
AU  - Schwilke, Eugene W
AU  - Cone, Edward J
AU  - Moolchan, Eric T
AU  - Huestis, Marilyn A
AD  - Chemistry and Drug Metabolism, Intramural Research Program, National Institute on Drug Abuse, National Institutes of Health, Baltimore, MD. Johns Hopkins School of Medicine, Department of Psychiatry and Behavioral Sciences, Baltimore, MD
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 2085
EP  - 2094
PB  - American Association for Clinical Chemistry, Inc.
VL  - 51
IS  - 11
SN  - 0009-9147, 0009-9147
KW  - Toxicology Abstracts
KW  - X 24180:Social poisons & drug abuse
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxicologyabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+Chemistry&rft.atitle=Disposition+of+Cocaine+and+Its+Metabolites+in+Human+Sweat+after+Controlled+Cocaine+Administration&rft.au=Kacinko%2C+Sherri+L%3BBarnes%2C+Allan+J%3BSchwilke%2C+Eugene+W%3BCone%2C+Edward+J%3BMoolchan%2C+Eric+T%3BHuestis%2C+Marilyn+A&rft.aulast=Kacinko&rft.aufirst=Sherri&rft.date=2005-11-01&rft.volume=51&rft.issue=11&rft.spage=2085&rft.isbn=&rft.btitle=&rft.title=Clinical+Chemistry&rft.issn=00099147&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2005-11-01
N1  - Last updated - 2011-12-13
ER  - 



TY  - JOUR
T1  - Multipartite Regulation of rctB, the Replication Initiator Gene of Vibrio cholerae Chromosome II
AN  - 17662192; 6503238
AB  - Replication initiator proteins in bacteria not only allow DNA replication but also often regulate the rate of replication initiation as well. The regulation is mediated by limiting the synthesis or availability of initiator proteins. The applicability of this principle is demonstrated here for RctB, the replication initiator for the smaller of the two chromosomes of Vibrio cholerae. A strong promoter for the rctB gene named rctBp was identified and found to be autoregulated in Escherichia coli. Promoter activity was lower in V. cholerae than in E. coli, and a part of this reduction is likely to be due to autorepression. Sequences upstream of rctBp, implicated earlier in replication control, enhanced the repression. The action of the upstream sequences required that they be present in cis, implying long-range interactions in the control of the promoter activity. A second gene specific for chromosome II replication, rctA, reduced rctB translation, most likely by antisense RNA control. Finally, optimal rctBp activity was found to be dependent on Dam. Increasing RctB in trans increased the copy number of a miniplasmid carrying oriCII sub(VC), implying that RctB can be rate limiting for chromosome II replication. The multiple modes of control on RctB are expected to reduce fluctuations in the initiator concentration and thereby help maintain chromosome copy number homeostasis.
JF  - Journal of Bacteriology
AU  - Pal, Debasish
AU  - Venkova-Canova, Tatiana
AU  - Srivastava, Preeti
AU  - Chattoraj, Dhruba K
AD  - Laboratory of Biochemistry, Center for Cancer Research, NCI, NIH, Bethesda, Maryland 20892
Y1  - 2005/11/01/
PY  - 2005
DA  - 2005 Nov 01
SP  - 7167
EP  - 7175
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 187
IS  - 21
SN  - 0021-9193, 0021-9193
KW  - rctB gene
KW  - Microbiology Abstracts B: Bacteriology
KW  - J 02725:DNA
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17662192?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Bacteriology&rft.atitle=Multipartite+Regulation+of+rctB%2C+the+Replication+Initiator+Gene+of+Vibrio+cholerae+Chromosome+II&rft.au=Pal%2C+Debasish%3BVenkova-Canova%2C+Tatiana%3BSrivastava%2C+Preeti%3BChattoraj%2C+Dhruba+K&rft.aulast=Pal&rft.aufirst=Debasish&rft.date=2005-11-01&rft.volume=187&rft.issue=21&rft.spage=7167&rft.isbn=&rft.btitle=&rft.title=Journal+of+Bacteriology&rft.issn=00219193&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2005-12-01
N1  - Last updated - 2011-12-13
ER  - 



TY  - JOUR
T1  - Optimization of IPG strip equilibration for the basic membrane protein mABC1
AN  - 17541180; 6399636
AB  - Many proteins with extreme physical properties, including basic and acidic proteins, membrane proteins, and very large proteins, present specific challenges to 2-DE separation. Using a pressure-blotting approach, we demonstrate that a basic integral membrane protein, mitochondrial ATP-binding cassette protein 1 (mABC1), focuses in the IPG strip, but fails to enter into the 2-D SDS-PAGE gel. Through modifying the equilibration conditions between the IPG strip and 2nd dimension, we demonstrate that only by increasing both the volume (from 3 to 6 mL for a 7-cm strip) and SDS concentration (from 2 to 10%) of the equilibration buffer is migration of mABC1 into the 2nd dimension achieved. While 2-DE remains one of the core separation technologies of proteomic analysis, proteins that are extremely basic, hydrophobic, or of large mass present significant challenges to 2-DE separation due to aggregation, oxidation, precipitation, and the physical limitations of the 1-D IPG strip (for recent reviews, see [1-7]). Since the advent of commercially available IPG strips, numerous groups have experimented with IEF conditions using various detergents alone or in combination [8], alternative denaturants [9], and thiol oxidation agents [10] to improve protein focusing. Effective 2-DE separation of membrane proteins has been affected dramatically by these advances in protein solubilization, as well as improvements in isolation of membranes, delipidation, and active in-gel rehydration [11, for recent reviews see 4, 5, 7]. Since the development of commercially available basic IPG strips, the most significant advance in the separation of basic proteins has been the introduction of hydroxyethyldisulfides, either alone or in combination with DTT [10]. While hydrophobic proteins were once virtually absent from the 2-D gel, and basic proteins were only visible as dense streaks, now many groups are undertaking large-scale analyses of membranes and basic proteins. Using this base of experimental tools, we embarked on a proteomic analysis of cardiac mitochondrial membranes, hoping to combine the knowledge gained from ongoing targeted protein chemistry and molecular biology studies with a broader-based proteomic analysis. Of particular interest is the inner mitochondrial membrane protein mABC1 (mitochondrial ATP-binding cassette protein 1), which may play a significant role in cardioprotection as part of the mitochondrial ATP-sensitive potassium channels [12-14]. Therefore, in designing our 2-DE approach, it was crucial to ensure that mABC1 is focused, observable, and quantifiable, despite being an integral membrane protein of pI 9.37.
JF  - Proteomics
AU  - McDonough, Jason
AU  - Marban, Eduardo
AD  - Division of Cardiology, NHLBI Proteomics Center, Johns Hopkins University, Baltimore, MD, USA, marban@jhmi.edu
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 2892
EP  - 2895
PB  - Wiley-VCH, Postfach 101161 Weinheim 69451 Germany, [mailto:info@wiley-vch.de], [URL:http://www.wiley-vch.de/publish/en/]
VL  - 5
IS  - 11
SN  - 1615-9853, 1615-9853
KW  - ABC1 protein
KW  - Biotechnology and Bioengineering Abstracts; Medical and Pharmaceutical Biotechnology Abstracts
KW  - Heart
KW  - Rehydration
KW  - Mitochondria
KW  - Hydrophobicity
KW  - Precipitation
KW  - Membrane proteins
KW  - Migration
KW  - Reviews
KW  - Thiols
KW  - Oxidation
KW  - proteomics
KW  - Potassium channels
KW  - W3 33340:Other proteins, peptides, amino acids
KW  - W 30965:Miscellaneous, Reviews
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17541180?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Proteomics&rft.atitle=Optimization+of+IPG+strip+equilibration+for+the+basic+membrane+protein+mABC1&rft.au=McDonough%2C+Jason%3BMarban%2C+Eduardo&rft.aulast=McDonough&rft.aufirst=Jason&rft.date=2005-11-01&rft.volume=5&rft.issue=11&rft.spage=2892&rft.isbn=&rft.btitle=&rft.title=Proteomics&rft.issn=16159853&rft_id=info:doi/10.1002%2Fpmic.200401155
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-11-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Membrane proteins; Mitochondria; proteomics; Hydrophobicity; Reviews; Oxidation; Migration; Precipitation; Potassium channels; Rehydration; Heart; Thiols
DO  - http://dx.doi.org/10.1002/pmic.200401155
ER  - 



TY  - JOUR
T1  - DDT serum concentration and menstruation among young Chinese women
AN  - 17464035; 6633889
AB  - High DDE and DDT concentrations were found to be associated with shortened menstrual cycle length in Laotian immigrants to the United States. We examined this issue in a sample of young Chinese women. A total of 60 women aged 20-24 years were enrolled in three maternal and child health clinics (20 from urban, 20 from suburban, 20 from rural) in Shanghai, China, and vicinity, in 1998. Of these women, 47 who did not use hormonal contraceptives and had valid menstrual cycle characteristics were included in the analysis for associations among serum DDE and DDT concentration and menstrual cycle length, duration of menses, and heaviness of menstrual flow. In univariate analysis, higher p,p'-DDE concentration was associated with longer menstrual cycle length (0.66 day per 10 mu g /L, 95% confidence interval [CI]: 0.21, 1.11 day). With adjustment for age, body mass index, education, occupation, and resident location, the estimate was 0.42 day (95% CI: -0.35, 1.19 day). p,p'-DDE was not associated with duration of menses or heaviness of menstrual flow. Neither p,p'-DDT nor o,p'-DDT were associated with menstrual cycle length, duration of menses or heaviness of menstrual flow. The study largely suggests no association between DDE and DDT concentrations and menstrual cycle characteristics in young Chinese women, though the weak-to-no correlation of DDE with menstrual cycle length merits further study.
JF  - Environmental Research
AU  - Chen, A
AU  - Zhang, J
AU  - Zhou, L
AU  - Gao, Es
AU  - Chen, L
AU  - Rogan, W J
AU  - Wolff
AD  - National Institute of Child Health and Human Development, National Institutes of Health, Department of Health and Human Services, Bethesda, MD 20892, USA, zhangj@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 397
EP  - 402
VL  - 99
IS  - 3
SN  - 0013-9351, 0013-9351
KW  - Toxicology Abstracts
KW  - Menstrual cycle
KW  - DDE
KW  - DDT
KW  - Immigrants
KW  - Menstruation
KW  - China, People's Rep.
KW  - Body mass index
KW  - Contraceptives
KW  - X 24136:Environmental impact
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17464035?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxicologyabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Environmental+Research&rft.atitle=DDT+serum+concentration+and+menstruation+among+young+Chinese+women&rft.au=Chen%2C+A%3BZhang%2C+J%3BZhou%2C+L%3BGao%2C+Es%3BChen%2C+L%3BRogan%2C+W+J%3BWolff&rft.aulast=Chen&rft.aufirst=A&rft.date=2005-11-01&rft.volume=99&rft.issue=3&rft.spage=397&rft.isbn=&rft.btitle=&rft.title=Environmental+Research&rft.issn=00139351&rft_id=info:doi/10.1016%2Fj.envres.2004.12.015
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Menstrual cycle; DDT; DDE; Immigrants; Menstruation; Body mass index; Contraceptives; China, People's Rep.
DO  - http://dx.doi.org/10.1016/j.envres.2004.12.015
ER  - 



TY  - JOUR
T1  - Current Review in Basic Science: Update on the Neurobiology of Alcohol Withdrawal Seizures
AN  - 17449216; 6546177
AB  - Abrupt cessation of alcohol intake after prolonged heavy drinking may trigger alcohol withdrawal seizures. Generalized tonic-clonic seizures are the most characteristic and severe type of seizure that occur in this setting. Generalized seizures also occur in rodent models of alcohol withdrawal. In these models, the withdrawal seizures are triggered by neuronal networks in the brainstem, including the inferior colliculus; similar brainstem mechanisms may contribute to alcohol withdrawal seizures in humans. Alcohol causes intoxication through effects on diverse ion channels and neurotransmitter receptors, including GABA sub(A) receptors-particularly those containing delta subunits that are localized extrasynaptically and mediate tonic inhibition-and N-methyl-D-aspartate (NMDA) receptors. Alcohol dependence results from compensatory changes during prolonged alcohol exposure, including internalization of GABA sub(A) receptors, which allows adaptation to these effects. Withdrawal seizures are believed to reflect unmasking of these changes and may also involve specific withdrawal-induced cellular events, such as rapid increases in alpha 4 subunit-containing GABA sub(A) receptors that confer reduced inhibitory function. Optimizing approaches to the prevention of alcohol withdrawal seizures requires an understanding of the distinct neurobiologic mechanisms that underlie these seizures.
JF  - Epilepsy Currents
AU  - Rogawski, Michael A
AD  - Michael A. Rogawski, MD, PhD, Epilepsy Research Section, Porter Neuroscience Research Center, NINDS, NIH, Building 35, Room 1C-1002, 35 Convent Drive MSC 3702, Bethesda, MD 20892-3702, michael.rogawski@nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 225
EP  - 230
PB  - Blackwell Publishing Ltd., 9600 Garsington Road Oxford OX4 2DQ UK, [URL:http://www.blackwellpublishing.com]
VL  - 5
IS  - 6
SN  - 1535-7597, 1535-7597
KW  - CSA Neurosciences Abstracts; Toxicology Abstracts
KW  - Intoxication
KW  - Drinking
KW  - Inferior colliculus
KW  - N-Methyl-D-aspartic acid receptors
KW  - Adaptations
KW  - Neural networks
KW  - Brain stem
KW  - Seizures
KW  - Glutamic acid receptors
KW  - Drug dependence
KW  - Epilepsy
KW  - Reviews
KW  - Neurotransmitter receptors
KW  - gamma -Aminobutyric acid A receptors
KW  - Ion channels
KW  - Ethanol
KW  - N3 11106:Neurobiology of drug abuse
KW  - X 24180:Social poisons & drug abuse
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17449216?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxicologyabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Epilepsy+Currents&rft.atitle=Current+Review+in+Basic+Science%3A+Update+on+the+Neurobiology+of+Alcohol+Withdrawal+Seizures&rft.au=Rogawski%2C+Michael+A&rft.aulast=Rogawski&rft.aufirst=Michael&rft.date=2005-11-01&rft.volume=5&rft.issue=6&rft.spage=225&rft.isbn=&rft.btitle=&rft.title=Epilepsy+Currents&rft.issn=15357597&rft_id=info:doi/10.1111%2Fj.1535-7511.2005.00071.x
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-06-01
N1  - SuppNotes - Tables, 1; references, 96.
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Drinking; Intoxication; Inferior colliculus; N-Methyl-D-aspartic acid receptors; Adaptations; Neural networks; Seizures; Brain stem; Glutamic acid receptors; Drug dependence; Epilepsy; Neurotransmitter receptors; Reviews; Ion channels; gamma -Aminobutyric acid A receptors; Ethanol
DO  - http://dx.doi.org/10.1111/j.1535-7511.2005.00071.x
ER  - 



TY  - JOUR
T1  - Accelerometer Data Reduction: A Comparison of Four Reduction Algorithms on Select Outcome Variables
AN  - 17421418; 6537843
AB  - Accelerometers are recognized as a valid and objective tool to assess free-living physical activity. Despite the widespread use of accelerometers, there is no standardized way to process and summarize data from them, which limits our ability to compare results across studies. This paper a) reviews decision rules researchers have used in the past, b) compares the impact of using different decision rules on a common data set, and c) identifies issues to consider for accelerometer data reduction. The methods sections of studies published in 2003 and 2004 were reviewed to determine what decision rules previous researchers have used to identify wearing period, minimal wear requirement for a valid day, spurious data, number of days used to calculate the outcome variables, and extract bouts of moderate to vigorous physical activity (MVPA). For this study, four data reduction algorithms that employ different decision rules were used to analyze the same data set. The review showed that among studies that reported their decision rules, much variability was observed. Overall, the analyses suggested that using different algorithms impacted several important outcome variables. The most stringent algorithm yielded significantly lower wearing time, the lowest activity counts per minute and counts per day, and fewer minutes of MVPA per day. An exploratory sensitivity analysis revealed that the most stringent inclusion criterion had an impact on sample size and wearing time, which in turn affected many outcome variables. These findings suggest that the decision rules employed to process accelerometer data have a significant impact on important outcome variables. Until guidelines are developed, it will remain difficult to compare findings across studies.
JF  - Medicine & Science in Sports & Exercise
AU  - Masse, L C
AU  - Fuemmeler, B F
AU  - Anderson, C B
AU  - Matthews, CE
AU  - Trost, S G
AU  - Catellier, D J
AU  - Treuth, M
AD  - Health Promotion Research Branch, Behavioral Research Program, Division of Cancer Control and Population Sciences, National Cancer Institute, Executive Plaza North, Room 4080, 6130 Executive Boulevard, MSC 7335, Bethesda, MD 20892-7335, USA, massel@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - S544
EP  - S554
VL  - 37
IS  - 11
SN  - 0195-9131, 0195-9131
KW  - Physical Education Index
KW  - Issues
KW  - Analysis
KW  - Mainstreaming
KW  - Exercise
KW  - Rules
KW  - PE 070:Measurement & Evaluation
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17421418?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aphysicaleducation&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Medicine+%26+Science+in+Sports+%26+Exercise&rft.atitle=Accelerometer+Data+Reduction%3A+A+Comparison+of+Four+Reduction+Algorithms+on+Select+Outcome+Variables&rft.au=Masse%2C+L+C%3BFuemmeler%2C+B+F%3BAnderson%2C+C+B%3BMatthews%2C+CE%3BTrost%2C+S+G%3BCatellier%2C+D+J%3BTreuth%2C+M&rft.aulast=Masse&rft.aufirst=L&rft.date=2005-11-01&rft.volume=37&rft.issue=11&rft.spage=S544&rft.isbn=&rft.btitle=&rft.title=Medicine+%26+Science+in+Sports+%26+Exercise&rft.issn=01959131&rft_id=info:doi/10.1249%2F01.mss.0000185674.09066.8a
LA  - English
DB  - Physical Education Index
N1  - Date revised - 2006-08-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Issues; Analysis; Mainstreaming; Exercise; Rules
DO  - http://dx.doi.org/10.1249/01.mss.0000185674.09066.8a
ER  - 



TY  - JOUR
T1  - A Timely Meeting: Objective Measurement of Physical Activity
AN  - 17414468; 6537837
AB  - Accurate and reliable assessment of physical activity remains an important challenge for epidemiologists, exercise scientists, clinicians, and behavioral researchers. The desire to explain and stem the dramatic increase in overweight and obesity prevalence observed among youths and adults has focused attention on the need for better measures of physical activity. These measures fall into three general categories: direct observation, subjective reports, and portable monitors, such as accelerometers. These monitors measure body movement in terms of acceleration, which can then be used to estimate physical activity intensity. As recently as 1999, accelerometry was still considered to be in the developmental stage. In October of that year, the Cooper Institute hosted a meeting titled "Measurement of Physical Activity." One of the conclusions from the meeting was that objective motion sensors were not practical for large-scale studies because of high cost, uncertain reliability, and difficulties in the interpretation of data.
JF  - Medicine & Science in Sports & Exercise
AU  - Troiano, R P
AD  - US Public Health Service, Risk Factor Monitoring and Methods Branch, Applied Research Program, Division of Cancer Control and Population Sciences, National Cancer Institute, EPN 4005, 6130 Executive Blvd., MSC 7344, Bethesda, MD 20892-7344, USA, troianor@mail.nih.gov
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - S487
EP  - S489
VL  - 37
IS  - 11
SN  - 0195-9131, 0195-9131
KW  - Physical Education Index
KW  - Measurement
KW  - Obesity
KW  - Reliability
KW  - Sport science
KW  - Observation
KW  - Exercise
KW  - Adults
KW  - Movement
KW  - Acceleration
KW  - Evaluation
KW  - Objectives
KW  - Youth
KW  - PE 030:Exercise, Health & Physical Fitness
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LA  - English
DB  - Physical Education Index
N1  - Date revised - 2006-08-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Evaluation; Obesity; Measurement; Reliability; Objectives; Sport science; Observation; Adults; Exercise; Acceleration; Movement; Youth
DO  - http://dx.doi.org/10.1249/01.mss.0000185473.32846.c3
ER  - 



TY  - JOUR
T1  - Agricultural pesticide use and risk of glioma in Nebraska, United States
AN  - 17399374; 6508845
AB  - BACKGROUND: To evaluate the risk of the adult glioma associated with farming and agricultural pesticide use, the authors conducted a population based case control study in eastern Nebraska. METHODS: Telephone interviews were conducted with men and women diagnosed with gliomas (n = 251) between 1988 and 1993 and controls (n = 498) randomly selected from the same geographical area. Unconditional logistic regression was used to calculate adjusted odds ratios (ORs) for farming and for use of individual and chemical classes of insecticides and herbicides, including pesticides classified as nitrosatable (able to form N-nitroso compounds upon reaction with nitrite). Non-farmers were used as the reference category for all analyses. RESULTS: Among men, ever living or working on a farm and duration of farming were associated with significantly increased risks of glioma ( greater than or equal to 55 years on a farm OR = 3.9, 95% CI 1.8 to 8.6); however, positive findings were limited to proxy respondents. Among women, there were no positive associations with farming activities among self or proxy respondents. Specific pesticide families and individual pesticides were associated with significantly increased risks among male farmers; however, most of the positive associations were limited to proxy respondents. For two herbicides and three insecticides, use was positively associated with risk among both self and proxy respondents. Based on a small number of exposed cases, ORs were significantly increased for the herbicides metribuzin (OR = 3.4, 95% CI 1.2 to 9.7) and paraquat (OR = 11.1, 95% CI 1.2 to 101), and for the insecticides bufencarb (OR = 18.9, 95% CI 1.9 to 187), chlorpyrifos (OR = 22.6, 95% CI 2.7 to 191), and coumaphos (OR = 5.9, 95% CI 1.1 to 32). CONCLUSION: The authors found significant associations between some specific agricultural pesticide exposures and the risk of glioma among male farmers but not among female farmers in Nebraska; however, most of the positive associations were limited to proxy respondents. These findings warrant further evaluation in prospective cohort studies where issues of recall bias are not a concern.
JF  - Occupational and Environmental Medicine
AU  - Lee, W J
AU  - Colt, J S
AU  - Heineman, E F
AU  - McComb, R
AU  - Weisenburger, D D
AU  - Lijinsky, W
AU  - Ward, M H
AD  - Occupational and Environmental Epidemiology Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, Bethesda, MD, USA
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 786
EP  - 792
PB  - B M J Publishing Group, B.M.A. House Tavistock Sq. London WC1H 9JR UK
VL  - 62
IS  - 11
SN  - 1351-0711, 1351-0711
KW  - glioma
KW  - Risk Abstracts; Health & Safety Science Abstracts; Toxicology Abstracts
KW  - Farms
KW  - Herbicides
KW  - Agrochemicals
KW  - Brain tumors
KW  - Chlorpyrifos
KW  - N-Nitroso compounds
KW  - Insecticides
KW  - Nitrites
KW  - metribuzin
KW  - Pesticides
KW  - USA, Nebraska
KW  - Coumaphos
KW  - Glioma
KW  - Nitrite
KW  - Occupational exposure
KW  - Paraquat
KW  - R2 23080:Industrial and labor
KW  - H 5000:Pesticides
KW  - X 24136:Environmental impact
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Chlorpyrifos; Brain tumors; N-Nitroso compounds; Farms; Insecticides; metribuzin; Pesticides; Coumaphos; Herbicides; Glioma; Nitrite; Paraquat; Nitrites; Agrochemicals; Occupational exposure; USA, Nebraska
ER  - 



TY  - JOUR
T1  - Recombinant Newcastle Disease Virus Expressing a Foreign Viral Antigen Is Attenuated and Highly Immunogenic in Primates
AN  - 17394573; 6504680
AB  - Paramyxoviruses such as human parainfluenza viruses that bear inserts encoding protective antigens of heterologous viruses can induce an effective immunity against the heterologous viruses in experimental animals. However, vectors based on common human pathogens would be expected to be restricted in replication in the adult human population due to high seroprevalence, an effect that would reduce vector immunogenicity. To address this issue, we evaluated Newcastle disease virus (NDV), an avian paramyxovirus that is serotypically distinct from common human pathogens, as a vaccine vector. Two strains were evaluated: the attenuated vaccine strain LaSota (NDV-LS) that replicates mostly in the chicken respiratory tract and the Beaudette C (NDV-BC) strain of intermediate virulence that produces mild systemic infection in chickens. A recombinant version of each virus was modified by the insertion, between the P and M genes, of a gene cassette encoding the human parainfluenza virus type 3 (HPIV3) hemagglutinin-neuraminidase (HN) protein, a test antigen with considerable historic data. The recombinant viruses were administered to African green monkeys (NDV-BC and NDV-LS) and rhesus monkeys (NDV-BC only) by combined intranasal and intratracheal routes at a dose of 10 super(6.5) PFU per site, with a second equivalent dose administered 28 days later. Little or no virus shedding was detected in nose-throat swabs or tracheal lavages following immunization with either strain. In a separate experiment, direct examination of lung tissue confirmed a highly attenuated, restricted pattern of replication by parental NDV-BC. The serum antibody response to the foreign HN protein induced by the first immunization with either NDV vector was somewhat less than that observed following a wild-type HPIV3 infection; however, the titer following the second dose exceeded that observed with HPIV3 infection, even though HPIV3 replicates much more efficiently than NDV in these animals. NDV appears to be a promising vector for the development of vaccines for humans; one application would be in controlling localized outbreaks of emerging pathogens.
JF  - Journal of Virology
AU  - Bukreyev, Alexander
AU  - Huang, Zhuhui
AU  - Yang, Lijuan
AU  - Elankumaran, Subbiah
AU  - St Claire, Marisa
AU  - Murphy, Brian R
AU  - Samal, Siba K
AU  - Collins, Peter L
AD  - Laboratory of Infectious Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland 20892. Virginia-Maryland Regional College of Veterinary Medicine, University of Maryland, College Park, Maryland 20742. Bioqual, Rockville, Maryland 20850
Y1  - 2005/11/01/
PY  - 2005
DA  - 2005 Nov 01
SP  - 13275
EP  - 13284
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 79
IS  - 21
SN  - 0022-538X, 0022-538X
KW  - Rhesus macaque
KW  - Rhesus monkey
KW  - Biotechnology and Bioengineering Abstracts; Genetics Abstracts; Medical and Pharmaceutical Biotechnology Abstracts; Immunology Abstracts; Virology & AIDS Abstracts
KW  - Data processing
KW  - Replication
KW  - Disseminated infection
KW  - protective antigen
KW  - Paramyxovirus
KW  - Newcastle disease
KW  - Pathogens
KW  - Immunity
KW  - Antibody response
KW  - Primates
KW  - Immunization
KW  - Parainfluenza virus
KW  - Parainfluenza
KW  - Virulence
KW  - Newcastle disease virus
KW  - Immunogenicity
KW  - Lung
KW  - Insertion
KW  - Macaca mulatta
KW  - Vaccines
KW  - Trachea
KW  - Respiratory tract
KW  - double prime HN protein
KW  - W3 33365:Vaccines (other)
KW  - G 07313:Viruses
KW  - F 06100:Vaccines - active immunity
KW  - W 30965:Miscellaneous, Reviews
KW  - V 22092:Viral antigenic properties
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Data processing; Replication; protective antigen; Disseminated infection; Antibody response; Immunity; Pathogens; Newcastle disease; Immunization; Parainfluenza; Virulence; Insertion; Lung; Immunogenicity; Vaccines; Trachea; double prime HN protein; Respiratory tract; Newcastle disease virus; Paramyxovirus; Macaca mulatta; Primates; Parainfluenza virus
ER  - 



TY  - JOUR
T1  - Combinations of Polyclonal or Monoclonal Antibodies to Proteins of the Outer Membranes of the Two Infectious Forms of Vaccinia Virus Protect Mice against a Lethal Respiratory Challenge
AN  - 17394199; 6504696
AB  - Previous studies demonstrated that antibodies to live vaccinia virus infection are needed for optimal protection against orthopoxvirus infection. The present report is the first to compare the protective abilities of individual and combinations of specific polyclonal and monoclonal antibodies that target proteins of the intracellular (IMV) and extracellular (EV) forms of vaccinia virus. The antibodies were directed to one IMV membrane protein, L1, and to two outer EV membrane proteins, A33 and B5. In vitro studies showed that the antibodies to L1 neutralized IMV and that the antibodies to A33 and B5 prevented the spread of EV in liquid medium. Prophylactic administration of individual antibodies to BALB/c mice partially protected them against disease following intranasal challenge with lethal doses of vaccinia virus. Combinations of antibodies, particularly anti-L1 and -A33 or -L1 and -B5, provided enhanced protection when administered 1 day before or 2 days after challenge. Furthermore, the protection was superior to that achieved with pooled immune gamma globulin from human volunteers inoculated with live vaccinia virus. In addition, single injections of anti-L1 plus anti-A33 antibodies greatly delayed the deaths of severe combined immunodeficiency mice challenged with vaccinia virus. These studies suggest that antibodies to two or three viral membrane proteins optimally derived from the outer membranes of IMV and EV, may be beneficial for prophylaxis or therapy of orthopoxvirus infections.
JF  - Journal of Virology
AU  - Lustig, Shlomo
AU  - Fogg, Christiana
AU  - Whitbeck, JCharles
AU  - Eisenberg, Roselyn J
AU  - Cohen, Gary H
AU  - Moss, Bernard
AD  - Laboratory of Viral Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland. Schools of Dental and Veterinary Medicine, University of Pennsylvania, Philadelphia, Pennsylvania
Y1  - 2005/11/01/
PY  - 2005
DA  - 2005 Nov 01
SP  - 13454
EP  - 13462
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 79
IS  - 21
SN  - 0022-538X, 0022-538X
KW  - mice
KW  - Biotechnology and Bioengineering Abstracts; Medical and Pharmaceutical Biotechnology Abstracts; Virology & AIDS Abstracts
KW  - Orthopoxvirus
KW  - Monoclonal antibodies
KW  - Outer membranes
KW  - Globulins
KW  - Membrane proteins
KW  - Vaccinia virus
KW  - Prophylaxis
KW  - Severe combined immunodeficiency
KW  - Lethal dose
KW  - W3 33160:Antibody based
KW  - V 22091:Immunological techniques & reagents
KW  - W 30965:Miscellaneous, Reviews
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Virology&rft.atitle=Combinations+of+Polyclonal+or+Monoclonal+Antibodies+to+Proteins+of+the+Outer+Membranes+of+the+Two+Infectious+Forms+of+Vaccinia+Virus+Protect+Mice+against+a+Lethal+Respiratory+Challenge&rft.au=Lustig%2C+Shlomo%3BFogg%2C+Christiana%3BWhitbeck%2C+JCharles%3BEisenberg%2C+Roselyn+J%3BCohen%2C+Gary+H%3BMoss%2C+Bernard&rft.aulast=Lustig&rft.aufirst=Shlomo&rft.date=2005-11-01&rft.volume=79&rft.issue=21&rft.spage=13454&rft.isbn=&rft.btitle=&rft.title=Journal+of+Virology&rft.issn=0022538X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Vaccinia virus; Orthopoxvirus; Membrane proteins; Monoclonal antibodies; Outer membranes; Prophylaxis; Globulins; Lethal dose; Severe combined immunodeficiency
ER  - 



TY  - JOUR
T1  - Intranasal Immunization Strategy To Impede Pilin-Mediated Binding of Pseudomonas aeruginosa to Airway Epithelial Cells
AN  - 17394145; 6503163
AB  - Prevention of pulmonary Pseudomonas aeruginosa infections represents a critical unmet medical need for cystic fibrosis (CF) patients. We have examined the tenet that a mucosal immunization approach can reduce interactions of a piliated form of this opportunistic pathogen with respiratory epithelial cells. Vaccinations were performed using ntPEpilinPAK, a protein chimera composed of a nontoxic form of P. aeruginosa exotoxin A (ntPE), where the C-terminal loop amino acid sequence of the PAK strain pilin protein was inserted in place of the ntPE Ib domain. Intranasal (i.n.) immunization of BALB/c mice with ntPEpilinPAK generated both serum and saliva immune responses. A series of in vitro studies showed that diluted samples of saliva obtained from immunized mice reduced pilin-dependent P. aeruginosa binding to polarized human tracheal epithelial cells, protected human pulmonary epithelial cells from cytotoxic actions associated with bacterial challenge, and reduced exotoxin A toxicity. Overall, i.n. administration of ntPEpilinPAK induced mucosal and systemic immune responses that may be beneficial for blocking early stage adhesion and/or infection events of epithelial cell-P. aeruginosa interactions at oropharyngeal surfaces.
JF  - Infection and Immunity
AU  - Hsieh, Jennifer C
AU  - Tham, Doris M
AU  - Feng, Weijun
AU  - Huang, Fan
AU  - Embaie, Selamawit
AU  - Liu, Keyi
AU  - Dean, Deborah
AU  - Hertle, Ralf
AU  - FitzGerald, David J
AU  - Mrsny, Randall J
AD  - Trinity BioSystems, Inc., 1455 Adams Dr., Suite 1317, Menlo Park, California 94025-1438. Department of Medicine, University of California at San Francisco School of Medicine, San Francisco, California 94143, and Children's Hospital Oakland Research Institute, 5700 Martin Luther King Jr. Way, Oakland, California 94609. Biotherapy Section, Laboratory of Molecular Biology, CCR, National Cancer Institute, Bethesda, Maryland 20892-4255. University of Tuebingen, Institute of Microbiology/Membrane Physiology, Auf der Morgenstelle 28, D-72076 Tuebingen, Germany
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 7705
EP  - 7717
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 73
IS  - 11
SN  - 0019-9567, 0019-9567
KW  - Immunology Abstracts; Microbiology Abstracts B: Bacteriology
KW  - Epithelial cells
KW  - Mucosal immunity
KW  - pilin
KW  - Pathogens
KW  - Toxicity
KW  - Infection
KW  - Vaccination
KW  - exotoxin A
KW  - Immunization
KW  - Chimeras
KW  - Cytotoxicity
KW  - Lung
KW  - Saliva
KW  - Pseudomonas aeruginosa
KW  - Cystic fibrosis
KW  - Respiratory tract
KW  - Amino acid sequence
KW  - J 02834:Vaccination and immunization
KW  - F 06100:Vaccines - active immunity
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Infection+and+Immunity&rft.atitle=Intranasal+Immunization+Strategy+To+Impede+Pilin-Mediated+Binding+of+Pseudomonas+aeruginosa+to+Airway+Epithelial+Cells&rft.au=Hsieh%2C+Jennifer+C%3BTham%2C+Doris+M%3BFeng%2C+Weijun%3BHuang%2C+Fan%3BEmbaie%2C+Selamawit%3BLiu%2C+Keyi%3BDean%2C+Deborah%3BHertle%2C+Ralf%3BFitzGerald%2C+David+J%3BMrsny%2C+Randall+J&rft.aulast=Hsieh&rft.aufirst=Jennifer&rft.date=2005-11-01&rft.volume=73&rft.issue=11&rft.spage=7705&rft.isbn=&rft.btitle=&rft.title=Infection+and+Immunity&rft.issn=00199567&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Epithelial cells; Mucosal immunity; pilin; Toxicity; Pathogens; Infection; exotoxin A; Vaccination; Immunization; Chimeras; Cytotoxicity; Lung; Saliva; Cystic fibrosis; Amino acid sequence; Respiratory tract; Pseudomonas aeruginosa
ER  - 



TY  - JOUR
T1  - Laser-Capture Microdissection: Refining Estimates of the Quantity and Distribution of Latent Herpes Simplex Virus 1 and Varicella-Zoster Virus DNA in Human Trigeminal Ganglia at the Single-Cell Level
AN  - 17394012; 6504760
AB  - There remains uncertainty and some controversy about the percentages and types of cells in human sensory nerve ganglia that harbor latent herpes simplex virus 1 (HSV-1) and varicella-zoster virus (VZV) DNA. We developed and validated laser-capture microdissection and real-time PCR (LCM/PCR) assays for the presence and copy numbers of HSV-1 gG and VZV gene 62 sequences in single cells recovered from sections of human trigeminal ganglia (TG) obtained at autopsy. Among 970 individual sensory neurons from five subjects, 2.0 to 10.5% were positive for HSV-1 DNA, with a median of 11.3 copies/positive cell, compared with 0.2 to 1.5% of neurons found to be positive by in situ hybridization (ISH) for HSV-1 latency-associated transcripts (LAT), the classical surrogate marker for HSV latency. This indicates a more pervasive latent HSV-1 infection of human TG neurons than originally thought. Combined ISH/LCM/PCR assays revealed that the majority of the latently infected neurons do not accumulate LAT to detectable levels. We detected VZV DNA in 1.0 to 6.9% of individual neurons from 10 subjects. Of the total 1,722 neurons tested, 4.1% were VZV DNA positive, with a median of 6.9 viral genomes/positive cell. After removal by LCM of all visible neurons on a slide, all surrounding nonneuronal cells were harvested and assayed: 21 copies of HSV-1 DNA were detected in similar to 5,200 nonneuronal cells, while nine VZV genomes were detected in similar to 14,200 nonneuronal cells. These data indicate that both HSV-1 and VZV DNAs persist in human TG primarily, if not exclusively, in a moderate percentage of neuronal cells.
JF  - Journal of Virology
AU  - Wang, Kening
AU  - Lau, Tsz Y
AU  - Morales, Melissa
AU  - Mont, Erik K
AU  - Straus, Stephen E
AD  - Medical Virology Section, Laboratory of Clinical Infectious Diseases, National Institute of Allergy and Infectious Diseases, Bethesda, Maryland
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 14079
EP  - 14087
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 79
IS  - 22
SN  - 0022-538X, 0022-538X
KW  - Biotechnology and Bioengineering Abstracts; Medical and Pharmaceutical Biotechnology Abstracts; Virology & AIDS Abstracts; Biochemistry Abstracts 2: Nucleic Acids
KW  - Genomes
KW  - Autopsy
KW  - Infection
KW  - Polymerase chain reaction
KW  - Latent infection
KW  - Sensory neurons
KW  - Herpes simplex virus 1
KW  - Trigeminal ganglion
KW  - copy number
KW  - Varicella-zoster virus
KW  - Ganglia
KW  - N 14025:RNA/DNA role in infection & immune response
KW  - V 22022:Virus assay
KW  - W 30965:Miscellaneous, Reviews
KW  - W3 33250:Methods: Others
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Virology&rft.atitle=Laser-Capture+Microdissection%3A+Refining+Estimates+of+the+Quantity+and+Distribution+of+Latent+Herpes+Simplex+Virus+1+and+Varicella-Zoster+Virus+DNA+in+Human+Trigeminal+Ganglia+at+the+Single-Cell+Level&rft.au=Wang%2C+Kening%3BLau%2C+Tsz+Y%3BMorales%2C+Melissa%3BMont%2C+Erik+K%3BStraus%2C+Stephen+E&rft.aulast=Wang&rft.aufirst=Kening&rft.date=2005-11-01&rft.volume=79&rft.issue=22&rft.spage=14079&rft.isbn=&rft.btitle=&rft.title=Journal+of+Virology&rft.issn=0022538X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-04-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Herpes simplex virus 1; Varicella-zoster virus; Polymerase chain reaction; Sensory neurons; Genomes; Trigeminal ganglion; copy number; Ganglia; Latent infection; Autopsy; Infection
ER  - 



TY  - JOUR
T1  - Liver-Directed Gamma Interferon Gene Delivery in Chronic Hepatitis C
AN  - 17392307; 6504692
AB  - Gamma interferon (IFN- gamma ) has been shown to inhibit replication of subgenomic and genomic hepatitis C virus (HCV) RNAs in vitro and to noncytolytically suppress hepatitis B virus (HBV) replication in vivo. IFN- gamma is also known for its immunomodulatory effects and as a marker of a successful cellular immune response to HCV. Therapeutic expression of IFN- gamma in the liver may therefore facilitate resolution of chronic hepatitis C, an infection that is rarely resolved spontaneously. To analyze immunomodulatory and antiviral effects of liver-specific IFN- gamma expression in vivo, we intravenously injected two persistently HCV-infected chimpanzees twice with a recombinant, replication-deficient HBV vector and subsequently with a recombinant adenoviral vector. These vectors expressed human IFN- gamma under control of HBV- and liver-specific promoters, respectively. Gene transfer resulted in a transient increase of intrahepatic IFN- gamma mRNA, without increase in serum alanine aminotransferase levels. Ex vivo analysis of peripheral blood lymphocytes demonstrated enhanced CD16 expression on T cells and upregulation of the liver-homing marker CXCR3. Moreover, an increased frequency of HCV-specific T cells was detected ex vivo in the peripheral blood and in vitro in liver biopsy-derived, antigen-nonspecifically expanded T-cell lines. None of these immunologic effects were observed in the third chimpanzee injected with an HBV control vector. Despite these immunologic effects of the experimental vector, however, IFN- gamma gene transfer did not result in a significant and long-lasting decrease of HCV titers. In conclusion, liver-directed IFN- gamma gene delivery resulted in HCV-specific and nonspecific activation of cellular immune responses but did not result in effective control of HCV replication.
JF  - Journal of Virology
AU  - Shin, Eui-Cheol
AU  - Protzer, Ulrike
AU  - Untergasser, Andreas
AU  - Feinstone, Stephen M
AU  - Rice, Charles M
AU  - Hasselschwert, Dana
AU  - Rehermann, Barbara
AD  - Liver Diseases Branch, NIDDK, National Institutes of Health, DHHS, Bethesda, Maryland
Y1  - 2005/11/01/
PY  - 2005
DA  - 2005 Nov 01
SP  - 13412
EP  - 13420
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 79
IS  - 21
SN  - 0022-538X, 0022-538X
KW  - Genetics Abstracts; Biotechnology and Bioengineering Abstracts; Immunology Abstracts; Medical and Pharmaceutical Biotechnology Abstracts; Bioengineering Abstracts; Virology & AIDS Abstracts
KW  - gamma -Interferon
KW  - Hepatitis B virus
KW  - CD16 antigen
KW  - CXCR3 protein
KW  - Replication
KW  - Peripheral blood
KW  - Alanine transaminase
KW  - Immunomodulation
KW  - Pan troglodytes
KW  - mRNA
KW  - Expression vectors
KW  - Promoters
KW  - Hepatitis C virus
KW  - Gene transfer
KW  - Chronic infection
KW  - Liver
KW  - Lymphocytes T
KW  - genomics
KW  - Hepatitis C
KW  - Immune response
KW  - G 07720:Immunogenetics
KW  - W3 33181:Gene therapy vectors
KW  - W 30965:Miscellaneous, Reviews
KW  - V 22095:Interferon
KW  - F 06104:Virus
KW  - W4 120:Genetic Engineering in Medicine
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17392307?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Virology&rft.atitle=Liver-Directed+Gamma+Interferon+Gene+Delivery+in+Chronic+Hepatitis+C&rft.au=Shin%2C+Eui-Cheol%3BProtzer%2C+Ulrike%3BUntergasser%2C+Andreas%3BFeinstone%2C+Stephen+M%3BRice%2C+Charles+M%3BHasselschwert%2C+Dana%3BRehermann%2C+Barbara&rft.aulast=Shin&rft.aufirst=Eui-Cheol&rft.date=2005-11-01&rft.volume=79&rft.issue=21&rft.spage=13412&rft.isbn=&rft.btitle=&rft.title=Journal+of+Virology&rft.issn=0022538X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - gamma -Interferon; CD16 antigen; Replication; CXCR3 protein; Peripheral blood; Alanine transaminase; Immunomodulation; mRNA; Expression vectors; Promoters; Gene transfer; Chronic infection; Lymphocytes T; Liver; Immune response; Hepatitis C; genomics; Hepatitis C virus; Hepatitis B virus; Pan troglodytes
ER  - 



TY  - JOUR
T1  - Crystal structure of the N-terminal domain of E. coli Lon protease
AN  - 17384087; 6508287
AB  - We report here the first crystal structure of the N-terminal domain of an A-type Lon protease. Lon proteases are ubiquitous, multidomain, ATP-dependent enzymes with both highly specific and non-specific protein binding, unfolding, and degrading activities. We expressed and purified a stable, monomeric 119-amino acid N-terminal subdomain of the Escherichia coli A-type Lon protease and determined its crystal structure at 2.03 Aa (Protein Data Bank [PDB] code 2ANE). The structure was solved in two crystal forms, yielding 14 independent views. The domain exhibits a unique fold consisting primarily of three twisted beta -sheets and a single long alpha -helix. Analysis of recent PDB depositions identified a similar fold in BPP1347 (PDB code 1ZBO), a 203-amino acid protein of unknown function from Bordetella parapertussis, crystallized as part of a structural genomics effort. BPP1347 shares sequence homology with Lon N-domains and with a family of other independently expressed proteins of unknown functions. We postulate that, as is the case in Lon proteases, this structural domain represents a general protein and polypeptide interaction domain.
JF  - Protein Science
AU  - Li, Mi
AU  - Rasulova, Fatima
AU  - Melnikov, Edward E
AU  - Rotanova, Tatyana V
AU  - Gustchina, Alla
AU  - Maurizi, Michael R
AU  - Wlodawer, Alexander
AD  - Macromolecular Crystallography Laboratory, National Cancer Institute at Frederick, Frederick, Maryland 21702-1201, USA. Basic Research Program, SAIC-Frederick, Frederick, Maryland 21702, USA. Laboratory of Cell Biology, National Cancer Institute, Bethesda, Maryland 20892, USA. Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, Moscow 117997, Russia
Y1  - 2005/11//
PY  - 2005
DA  - Nov 2005
SP  - 2895
EP  - 2900
PB  - Cold Spring Harbor Laboratory Press, [mailto:cshpress@cshl.org], [URL:http://www.cshl.org/]
VL  - 14
IS  - 11
SN  - 0961-8368, 0961-8368
KW  - Microbiology Abstracts B: Bacteriology
KW  - Data banks
KW  - Protein folding
KW  - Bordetella parapertussis
KW  - Escherichia coli
KW  - Crystal structure
KW  - Proteinase
KW  - genomics
KW  - J 02728:Enzymes
KW  - J 02727:Amino acids, peptides and proteins
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17384087?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Protein+Science&rft.atitle=Crystal+structure+of+the+N-terminal+domain+of+E.+coli+Lon+protease&rft.au=Li%2C+Mi%3BRasulova%2C+Fatima%3BMelnikov%2C+Edward+E%3BRotanova%2C+Tatyana+V%3BGustchina%2C+Alla%3BMaurizi%2C+Michael+R%3BWlodawer%2C+Alexander&rft.aulast=Li&rft.aufirst=Mi&rft.date=2005-11-01&rft.volume=14&rft.issue=11&rft.spage=2895&rft.isbn=&rft.btitle=&rft.title=Protein+Science&rft.issn=09618368&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-04-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Data banks; Protein folding; Crystal structure; Proteinase; genomics; Escherichia coli; Bordetella parapertussis
ER  - 



TY  - JOUR
T1  - Efficient secretion of a folded protein domain by a monomeric bacterial autotransporter
AN  - 1439223009; 18436322
AB  - Bacterial autotransporters are proteins that contain a small C-terminal ' beta domain' that facilitates translocation of a large N-terminal 'passenger domain' across the outer membrane (OM) by an unknown mechanism. Here we used EspP, an autotransporter produced by Escherichia coli 0157:H7, as a model protein to gain insight into the transport reaction. Initially we found that the passenger domain of a truncated version of EspP (EspP Delta 1-851) was translocated efficiently across the OM. Blue Native polyacrylamide gel electrophoresis, analytical ultracentrifugation and other biochemical methods showed that EspP Delta 1-851 behaves as a compact monomer and strongly suggest that the channel formed by the beta domain is too narrow to accommodate folded polypeptides. Surprisingly, we found that a folded protein domain fused to the N-terminus of EspP Delta 1-851 was efficiently translocated across the OM. Further analysis revealed that the passenger domain of wild-type EspP also folds at least partially in the periplasm. To reconcile these data, we propose that the EspP beta domain functions primarily to target and anchor the protein and that an external factor transports the passenger domain across the OM.
JF  - Molecular Microbiology
AU  - Skillman, Kristen M
AU  - Barnard, Travis J
AU  - Peterson, Janine H
AU  - Ghirlando, Rodolfo
AU  - Bernstein, Harris D
AD  - Genetics and Biochemistry Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892, USA.
Y1  - 2005/11//
PY  - 2005
DA  - November 2005
SP  - 945
EP  - 958
PB  - Wiley-Blackwell, 111 River Street Hoboken NJ 07030-5774 United States
VL  - 58
IS  - 4
SN  - 0950-382X, 0950-382X
KW  - Microbiology Abstracts B: Bacteriology
KW  - Monomers
KW  - Data processing
KW  - Secretion
KW  - Outer membranes
KW  - Escherichia coli
KW  - Ultracentrifugation
KW  - Translocation
KW  - periplasm
KW  - Gel electrophoresis
KW  - Models
KW  - N-Terminus
KW  - J 02330:Biochemistry
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/1439223009?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Molecular+Microbiology&rft.atitle=Efficient+secretion+of+a+folded+protein+domain+by+a+monomeric+bacterial+autotransporter&rft.au=Skillman%2C+Kristen+M%3BBarnard%2C+Travis+J%3BPeterson%2C+Janine+H%3BGhirlando%2C+Rodolfo%3BBernstein%2C+Harris+D&rft.aulast=Skillman&rft.aufirst=Kristen&rft.date=2005-11-01&rft.volume=58&rft.issue=4&rft.spage=945&rft.isbn=&rft.btitle=&rft.title=Molecular+Microbiology&rft.issn=0950382X&rft_id=info:doi/10.1111%2Fj.1365-2958.2005.04885.x
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2013-10-01
N1  - Document feature - figure 6
N1  - Last updated - 2016-04-29
N1  - SubjectsTermNotLitGenreText - Monomers; Data processing; Secretion; Outer membranes; periplasm; Translocation; Ultracentrifugation; Gel electrophoresis; N-Terminus; Models; Escherichia coli
DO  - http://dx.doi.org/10.1111/j.1365-2958.2005.04885.x
ER  - 



TY  - CPAPER
T1  - The Epidemiology of Second Cancers
T2  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AN  - 40130915; 4016251
JF  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AU  - Travis, Lois B
Y1  - 2005/10/30/
PY  - 2005
DA  - 2005 Oct 30
KW  - Cancer
KW  - Epidemiology
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40130915?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.atitle=The+Epidemiology+of+Second+Cancers&rft.au=Travis%2C+Lois+B&rft.aulast=Travis&rft.aufirst=Lois&rft.date=2005-10-30&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.aacr.org/page4372.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Chemoprevention of Lung Cancer: Whats Next?
T2  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AN  - 40111758; 4016240
JF  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AU  - Szabo, Eva
Y1  - 2005/10/30/
PY  - 2005
DA  - 2005 Oct 30
KW  - Lung cancer
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40111758?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.atitle=Chemoprevention+of+Lung+Cancer%3A+Whats+Next%3F&rft.au=Szabo%2C+Eva&rft.aulast=Szabo&rft.aufirst=Eva&rft.date=2005-10-30&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.aacr.org/page4372.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Targeting the PI3K/Akt/mTOR Pathway for Cancer Prevention
T2  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AN  - 40101047; 4016249
JF  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AU  - Dennis, Phillip A
Y1  - 2005/10/30/
PY  - 2005
DA  - 2005 Oct 30
KW  - prevention
KW  - 1-Phosphatidylinositol 3-kinase
KW  - Cancer
KW  - AKT protein
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40101047?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.atitle=Targeting+the+PI3K%2FAkt%2FmTOR+Pathway+for+Cancer+Prevention&rft.au=Dennis%2C+Phillip+A&rft.aulast=Dennis&rft.aufirst=Phillip&rft.date=2005-10-30&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.aacr.org/page4372.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Genomic and Proteomic Approaches for Cancer "Signatures" and Antiangiogenic Therapy
T2  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AN  - 40100829; 4016192
JF  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AU  - Kohn, Elise C
Y1  - 2005/10/30/
PY  - 2005
DA  - 2005 Oct 30
KW  - Therapy
KW  - proteomics
KW  - Cancer
KW  - genomics
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40100829?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.atitle=Genomic+and+Proteomic+Approaches+for+Cancer+%22Signatures%22+and+Antiangiogenic+Therapy&rft.au=Kohn%2C+Elise+C&rft.aulast=Kohn&rft.aufirst=Elise&rft.date=2005-10-30&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.aacr.org/page4372.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Trends and Determinants of Cancer Screening Uptake
T2  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AN  - 40067720; 4016216
JF  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AU  - Meissner, Helen I
Y1  - 2005/10/30/
PY  - 2005
DA  - 2005 Oct 30
KW  - Screening
KW  - Cancer
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40067720?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.atitle=Trends+and+Determinants+of+Cancer+Screening+Uptake&rft.au=Meissner%2C+Helen+I&rft.aulast=Meissner&rft.aufirst=Helen&rft.date=2005-10-30&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.aacr.org/page4372.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - U.S. Demographic Imperative: Implication for the Science and Practice of Cancer Prevention in Older Persons
T2  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AN  - 40056016; 4016273
JF  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AU  - Yancik, Rosemary
Y1  - 2005/10/30/
PY  - 2005
DA  - 2005 Oct 30
KW  - USA
KW  - prevention
KW  - Demography
KW  - Cancer
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40056016?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.atitle=U.S.+Demographic+Imperative%3A+Implication+for+the+Science+and+Practice+of+Cancer+Prevention+in+Older+Persons&rft.au=Yancik%2C+Rosemary&rft.aulast=Yancik&rft.aufirst=Rosemary&rft.date=2005-10-30&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.aacr.org/page4372.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - SNP Selection for Genome Wide Association Studies
T2  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AN  - 40049367; 4016199
JF  - Fourth Annual AACR International Conference on Frontiers in Cancer Prevention Research
AU  - Thomas, Gilles
Y1  - 2005/10/30/
PY  - 2005
DA  - 2005 Oct 30
KW  - Genomes
KW  - Single-nucleotide polymorphism
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40049367?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.atitle=SNP+Selection+for+Genome+Wide+Association+Studies&rft.au=Thomas%2C+Gilles&rft.aulast=Thomas&rft.aufirst=Gilles&rft.date=2005-10-30&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=Fourth+Annual+AACR+International+Conference+on+Frontiers+in+Cancer+Prevention+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.aacr.org/page4372.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Macrophage Differentiation and Foam Cell Formation
T2  - 6th International Congress on Coronary Artery Disease: from Prevention to Intervention
AN  - 39741662; 4018768
JF  - 6th International Congress on Coronary Artery Disease: from Prevention to Intervention
AU  - Kruth, H S
AU  - Zhao, B
AU  - Li, Y F
AU  - Waldo, S W
AU  - Buono, C
AU  - Jones, N L
Y1  - 2005/10/29/
PY  - 2005
DA  - 2005 Oct 29
KW  - Differentiation
KW  - Macrophages
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39741662?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=6th+International+Congress+on+Coronary+Artery+Disease%3A+from+Prevention+to+Intervention&rft.atitle=Macrophage+Differentiation+and+Foam+Cell+Formation&rft.au=Kruth%2C+H+S%3BZhao%2C+B%3BLi%2C+Y+F%3BWaldo%2C+S+W%3BBuono%2C+C%3BJones%2C+N+L&rft.aulast=Kruth&rft.aufirst=H&rft.date=2005-10-29&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=6th+International+Congress+on+Coronary+Artery+Disease%3A+from+Prevention+to+Intervention&rft.issn=&rft_id=info:doi/
L2  - http://www.kenes.com/cad6/program/SessionIndex.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - A single pair of acidic residues in the kinase major groove mediates strong substrate preference for P-2 or P-5 arginine in the AGC, CAMK, and STE kinase families.
AN  - 68719290; 16131491
AB  - Most basophilic serine/threonine kinases preferentially phosphorylate substrates with Arg at P-3 but vary greatly in additional strong preference for Arg at P-2 or P-5. The structural basis for P-2 or P-5 preference is known for two AGC kinases (family of protein kinases A, G, and C) in which it is mediated by a single pair of acidic residues (PEN+1 and YEM+1). We sought a general understanding of P-2 and P-5 Arg preference. The strength of Arg preference at each position was assessed in 15 kinases using a new degenerate peptide library approach. Strong P-2 or P-5 Arg preference occurred not only in AGC kinases (7 of 8 studied) but also in calmodulin-dependent protein kinase (CAMK, 1 of 3) and Ste20 (STE) kinases (2 of 4). Analysis of sequence conservation demonstrated almost perfect correlation between (a) strong P-2 or P-5 Arg preference and (b) acidic residues at both PEN+1 and YEM+1. Mutation of two kinases (PKC-theta and p21-activated kinase 1 (PAK1)) confirmed critical roles of both PEN+1 and YEM+1 residues in determining strong R-2 Arg preference. PAK kinases were unique in having exceptionally strong Arg preference at P-2 but lacking strong Arg preference at P-3. Preference for Arg at P-2 was so critical to PAK recognition that PAK1 activity was virtually eliminated by mutating the PEN+1 or YEM+1 residues. The fact that this specific pair of acidic residues has been repeatedly and exclusively used by evolution for conferring strong Arg preference at two different substrate positions in three different kinase families implies it is uniquely well suited to mediate sufficiently good substrate binding without unduly restricting product release.
JF  - The Journal of biological chemistry
AU  - Zhu, Guozhi
AU  - Fujii, Koichi
AU  - Liu, Yin
AU  - Codrea, Vlad
AU  - Herrero, Juan
AU  - Shaw, Stephen
AD  - Experimental Immunology Branch, NCI, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/10/28/
PY  - 2005
DA  - 2005 Oct 28
SP  - 36372
EP  - 36379
VL  - 280
IS  - 43
SN  - 0021-9258, 0021-9258
KW  - Isoenzymes
KW  - 0
KW  - Peptides
KW  - PRKCQ protein, human
KW  - 148374-93-0
KW  - Arginine
KW  - 94ZLA3W45F
KW  - Protein Kinases
KW  - EC 2.7.-
KW  - protein kinase C zeta
KW  - EC 2.7.11.1
KW  - Protein Kinase C
KW  - EC 2.7.11.13
KW  - Calcium-Calmodulin-Dependent Protein Kinases
KW  - EC 2.7.11.17
KW  - Index Medicus
KW  - Animals
KW  - Chromatography
KW  - Models, Molecular
KW  - Humans
KW  - Amino Acid Sequence
KW  - Mice
KW  - Protein Binding
KW  - Biotinylation
KW  - Isoenzymes -- metabolism
KW  - Mutagenesis
KW  - Protein Kinase C -- metabolism
KW  - Mutagenesis, Site-Directed
KW  - Protein Kinases -- metabolism
KW  - Blotting, Western
KW  - Phosphorylation
KW  - Kinetics
KW  - Molecular Sequence Data
KW  - Peptides -- chemistry
KW  - Calcium-Calmodulin-Dependent Protein Kinases -- chemistry
KW  - Sequence Homology, Amino Acid
KW  - Protein Structure, Tertiary
KW  - Mutation
KW  - Protein Conformation
KW  - Arginine -- chemistry
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-04
N1  - Date created - 2005-10-24
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Lysophosphatidic acid and endothelin-induced proliferation of ovarian cancer cell lines is mitigated by neutralization of granulin-epithelin precursor (GEP), a prosurvival factor for ovarian cancer.
AN  - 68736427; 16044162
AB  - Granulin-epithelin precursor (GEP/progranulin) is an autocrine growth factor for ovarian cancer. We examined the production and function of GEP and report that: (1) GEP production is regulated by endothelin (ET-1), lysophosphatidic acid (LPA), and cAMP; (2) cAMP signals GEP production through exchange protein activated by cAMP (EPAC); (3) ET-1 and cAMP/EPAC induce GEP through ERK1/2; and (4) neutralization of GEP results in apoptosis. Exposure of HEY-A8 and OVCAR3 ovarian cancer cells to LPA and ET-1 yielded GEP production and secretion in a dose- and time-dependent fashion; neither stimulated significant concentrations of cAMP directly. Stimulation of cAMP production with pertussis and cholera toxin, or forskolin induced GEP in a PKA-independent fashion. EPAC, an intracellular cAMP receptor, is activated specifically by the cAMP analog, 8-CPT-2'-O-Me-cAMP (8-CPT); 8-CPT treatment stimulated GEP production and secretion. The MEK inhibitor, U0126, abrogated GEP production in response to ET-1 and 8-CPT, confirming involvement of MAPK. A partial inhibition of basal and stimulated GEP production was observed when cells were treated with a internal calcium chelator, BAPTA. Neutralizing anti-GEP antibody reversed basal as well as LPA, ET-1 and 8-CPT-induced ovarian cancer cell growth and induced apoptosis as demonstrated by caspase-3 and PARP cleavage, DNA fragmentation, and nuclear condensation. These results indicate that GEP is a growth and survival factor for ovarian cancer, induced by LPA and ET-1 and cAMP/EPAC through ERK1/2.
JF  - Oncogene
AU  - Kamrava, Mitchell
AU  - Simpkins, Fiona
AU  - Alejandro, Emilyn
AU  - Michener, Chad
AU  - Meltzer, Elizabeth
AU  - Kohn, Elise C
AD  - Howard Hughes Medical Institute/National Institutes of Health Research Scholars Program, National Institutes of Health, Bethesda, MD, USA.
Y1  - 2005/10/27/
PY  - 2005
DA  - 2005 Oct 27
SP  - 7084
EP  - 7093
VL  - 24
IS  - 47
SN  - 0950-9232, 0950-9232
KW  - Adjuvants, Immunologic
KW  - 0
KW  - Chelating Agents
KW  - Endothelins
KW  - Guanine Nucleotide Exchange Factors
KW  - Intercellular Signaling Peptides and Proteins
KW  - Lysophospholipids
KW  - RAPGEF3 protein, human
KW  - granulin precursor protein
KW  - 134710-81-9
KW  - Colforsin
KW  - 1F7A44V6OU
KW  - Egtazic Acid
KW  - 526U7A2651
KW  - Cholera Toxin
KW  - 9012-63-9
KW  - Cyclic AMP
KW  - E0399OZS9N
KW  - Poly(ADP-ribose) Polymerases
KW  - EC 2.4.2.30
KW  - Pertussis Toxin
KW  - EC 2.4.2.31
KW  - Cyclic AMP-Dependent Protein Kinases
KW  - EC 2.7.11.11
KW  - Mitogen-Activated Protein Kinase 1
KW  - EC 2.7.11.24
KW  - Mitogen-Activated Protein Kinase 3
KW  - MAP Kinase Kinase 1
KW  - EC 2.7.12.2
KW  - CASP3 protein, human
KW  - EC 3.4.22.-
KW  - Caspase 3
KW  - Caspases
KW  - 1,2-bis(2-aminophenoxy)ethane-N,N,N',N'-tetraacetic acid
KW  - K22DDW77C0
KW  - lysophosphatidic acid
KW  - PG6M3969SG
KW  - Index Medicus
KW  - Cyclic AMP-Dependent Protein Kinases -- metabolism
KW  - Egtazic Acid -- analogs & derivatives
KW  - Blotting, Northern
KW  - Cell Nucleus -- metabolism
KW  - Humans
KW  - Guanine Nucleotide Exchange Factors -- metabolism
KW  - Cholera Toxin -- pharmacology
KW  - Pertussis Toxin -- pharmacology
KW  - Cell Nucleus -- drug effects
KW  - Poly(ADP-ribose) Polymerases -- metabolism
KW  - Caspases -- metabolism
KW  - Mitogen-Activated Protein Kinase 3 -- metabolism
KW  - Chelating Agents -- pharmacology
KW  - Blotting, Western
KW  - Colforsin -- pharmacology
KW  - Tumor Cells, Cultured
KW  - Mitogen-Activated Protein Kinase 1 -- metabolism
KW  - Cyclic AMP -- metabolism
KW  - Adjuvants, Immunologic -- pharmacology
KW  - MAP Kinase Kinase 1 -- metabolism
KW  - Egtazic Acid -- pharmacology
KW  - Female
KW  - Cell Proliferation -- drug effects
KW  - Ovarian Neoplasms -- metabolism
KW  - Endothelins -- pharmacology
KW  - Intercellular Signaling Peptides and Proteins -- immunology
KW  - Ovarian Neoplasms -- pathology
KW  - Apoptosis -- drug effects
KW  - Lysophospholipids -- pharmacology
KW  - Intercellular Signaling Peptides and Proteins -- chemistry
KW  - Intercellular Signaling Peptides and Proteins -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-15
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - p53, Senescence and Cancer
T2  - 2005 Symposium on Stem Cells, Senescence and Cancer (D5)
AN  - 40006472; 3987884
JF  - 2005 Symposium on Stem Cells, Senescence and Cancer (D5)
AU  - Harris, Curtis C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - p53 protein
KW  - Cancer
KW  - Senescence
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40006472?accountid=14244
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L2  - http://www.keystonesymposia.org/Meetings/ViewMeetings.cfm?MeetingID=764
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Histopathological Improvement of Severe Acute Graft Versus Host Disease of the Gut with Unrelated Mesenchymal Stem Cells
T2  - 2005 Symposium on Stem Cells, Senescence and Cancer (D5)
AN  - 40003874; 3987860
JF  - 2005 Symposium on Stem Cells, Senescence and Cancer (D5)
AU  - Balakumaran, Arun
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Hosts
KW  - Stem cells
KW  - Digestive tract
KW  - Mesenchyme
KW  - Histopathology
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40003874?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Symposium+on+Stem+Cells%2C+Senescence+and+Cancer+%28D5%29&rft.atitle=Histopathological+Improvement+of+Severe+Acute+Graft+Versus+Host+Disease+of+the+Gut+with+Unrelated+Mesenchymal+Stem+Cells&rft.au=Balakumaran%2C+Arun&rft.aulast=Balakumaran&rft.aufirst=Arun&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Symposium+on+Stem+Cells%2C+Senescence+and+Cancer+%28D5%29&rft.issn=&rft_id=info:doi/
L2  - http://www.keystonesymposia.org/Meetings/ViewMeetings.cfm?MeetingID=764
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Genetic and Evolutionary Analysis of the ABCC6 Gene and Pseudoxanthoma Elasticum (PXE)
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39866328; 4038645
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Lou, H
AU  - Bergeron, J
AU  - Thomas, L
AU  - Terry, S F
AU  - Terry, P F
AU  - Dean, M
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - ABCC6 gene
KW  - Evolution
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Evidence for Constraint in Telomere Stability Genes
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39836102; 4037655
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Savage, S A
AU  - Yeager, M
AU  - Liao, J
AU  - Chanock, S J
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Telomeres
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39836102?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Physicians' Beliefs about the Role of Genetics in Health Differences and the Importance of Race/Ethnicity and Gender in Clinical Decision Making
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39835624; 4037545
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Warshauer-Baker, E
AU  - Bonham, V L
AU  - Jenkins, J
AU  - Stevens, N
AU  - Page, Z
AU  - Odunlami, A
AU  - McBride, C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Ethnic groups
KW  - Subpopulations
KW  - Races
KW  - Sex
KW  - Genetics
KW  - Decision making
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - DOCK9, a Candidate Bipolar Disorder Susceptibility Gene on Chromosome 13@Q32.3
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39817338; 4038275
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Detera-Wadleigh, S
AU  - Liu, C
AU  - Badner, J
AU  - Corona, W
AU  - Akula, N
AU  - Cardona, I
AU  - Kundu, M
AU  - Steele, C.J.M.
AU  - Maheshwari, M
AU  - Bonner, T
AU  - Gibbs, R
AU  - Gershon, E
AU  - Mcmahon, F
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Chromosome 13
KW  - Chromosomes
KW  - Bipolar disorder
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - PRKAR1A Mutations Leading to Carney Complex, PPNAD and Related Disorders: Analysis of the Largest Database to Date, Identification of Large Gene Rearrangments and Other Novel Disease-Causing Alterations, and Functional Characterization of Expressed Mutants
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39807555; 4036397
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Horvath, A
AU  - Boikos, S
AU  - Weinberg, F
AU  - Meoli, E
AU  - Stergiopoulos, S
AU  - Bei, T
AU  - Matyakhina, L
AU  - Bossis, I
AU  - Stratakis, C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Mutants
KW  - Mutation
KW  - Carney complex
KW  - Databases
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39807555?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=PRKAR1A+Mutations+Leading+to+Carney+Complex%2C+PPNAD+and+Related+Disorders%3A+Analysis+of+the+Largest+Database+to+Date%2C+Identification+of+Large+Gene+Rearrangments+and+Other+Novel+Disease-Causing+Alterations%2C+and+Functional+Characterization+of+Expressed+Mutants&rft.au=Horvath%2C+A%3BBoikos%2C+S%3BWeinberg%2C+F%3BMeoli%2C+E%3BStergiopoulos%2C+S%3BBei%2C+T%3BMatyakhina%2C+L%3BBossis%2C+I%3BStratakis%2C+C&rft.aulast=Horvath&rft.aufirst=A&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Design of a National Resource for Gene Discovery in Parkinsons Disease
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39804969; 4038096
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Horsford, D J
AU  - Keen, J
AU  - Beck, J
AU  - Murphy, D
AU  - Scudder, Q
AU  - Royds, C
AU  - Gwinn-Hardy, K
AU  - Rich, S
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Neurodegenerative diseases
KW  - Parkinson's disease
KW  - Movement disorders
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39804969?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Familial Autoimmune Myasthenia Gravis - Results of a Genome-Wide Scan
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39772922; 4038687
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Knight, M A
AU  - Landoure, G
AU  - Taye, A A
AU  - Fischbeck, K H
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Myasthenia gravis
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Consortium for Osteogenesis Imperfecta Mutations: Lethal Regions in the Helical Portion of Type I Collagen Chains Align with Collagen Binding Sites for Integrin and Proteoglycans
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39772019; 4038544
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Marini, J
AU  - Forlino, A
AU  - Cabral, W
AU  - Barnes, A
AU  - San Antonio, J
AU  - Milgrom, S
AU  - Hyland, J
AU  - Korkko, J
AU  - Prockop, D
AU  - DePaepe, A
AU  - Coucke, P
AU  - Glorieux, F
AU  - Roughley, P
AU  - Lund, A
AU  - Kuurila, K
AU  - Cohn, D
AU  - Krakow, D
AU  - Mottes, M
AU  - Dalgleish, R
AU  - Byers, P
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Collagen (type I)
KW  - Mutation
KW  - Osteogenesis imperfecta
KW  - Integrins
KW  - Proteoglycans
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39772019?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Animal Study of Direct Central Nervous System Administration of Copper Histidine: Prelude to Clinical Trial in Menkes Disease
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39771241; 4038134
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Lem, K
AU  - Brinster, L R
AU  - Tjurmina, O
AU  - Kaler, S G
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Menkes disease
KW  - Clinical trials
KW  - Histidine
KW  - Copper
KW  - Central nervous system
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39771241?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Autosomal Dominant Inheritance of Stuttering in a West African Population
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39770833; 4038036
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Levis, B
AU  - Lukong, J
AU  - Mundorff, J
AU  - Drayna, D
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Africa
KW  - Heredity
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Autosomal+Dominant+Inheritance+of+Stuttering+in+a+West+African+Population&rft.au=Levis%2C+B%3BLukong%2C+J%3BMundorff%2C+J%3BDrayna%2C+D&rft.aulast=Levis&rft.aufirst=B&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - NIEHS Environmental Genome Project: Functional Significance of Environmentally-Responsive Genotypes for Human Disease.
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39762539; 4037417
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - McAllister, K
AU  - Tyson, F
AU  - Maull, L
AU  - Gray, K
AU  - Srinivasan, S
AU  - Reinlib, L
AU  - Collman, G
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Genomes
KW  - Genotypes
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39762539?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=NIEHS+Environmental+Genome+Project%3A+Functional+Significance+of+Environmentally-Responsive+Genotypes+for+Human+Disease.&rft.au=McAllister%2C+K%3BTyson%2C+F%3BMaull%2C+L%3BGray%2C+K%3BSrinivasan%2C+S%3BReinlib%2C+L%3BCollman%2C+G&rft.aulast=McAllister&rft.aufirst=K&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - NCBI Entrez Phenotype Resources.
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39762509; 4037415
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Mailman, M D
AU  - Sherry, S T
AU  - Maglott, D R
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Phenotypes
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39762509?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=NCBI+Entrez+Phenotype+Resources.&rft.au=Mailman%2C+M+D%3BSherry%2C+S+T%3BMaglott%2C+D+R&rft.aulast=Mailman&rft.aufirst=M&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Using Hispanic Genetic Diversity to Infer the Haplotype Structure of Native Americans
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39761654; 4037632
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Tarazona-Santos, E
AU  - Yeager, M
AU  - Staats, B
AU  - Welch, R
AU  - Burdette, L
AU  - Packer, B
AU  - Chanock, S
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Ethnic groups
KW  - Haplotypes
KW  - Genetic diversity
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39761654?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Use of Nude and Identifiable Photographs in Medical Genetics Textbooks: Ethical Considerations
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39761016; 4037549
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Burchett, M E
AU  - Gustafson, A L
AU  - Francomano, C A
AU  - McDonnell, N B
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Photographs
KW  - Ethics
KW  - Genetics
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39761016?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=The+Use+of+Nude+and+Identifiable+Photographs+in+Medical+Genetics+Textbooks%3A+Ethical+Considerations&rft.au=Burchett%2C+M+E%3BGustafson%2C+A+L%3BFrancomano%2C+C+A%3BMcDonnell%2C+N+B&rft.aulast=Burchett&rft.aufirst=M&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Comprehensive Analysis of Sequence Variation in the Peptidyl Arginine Deiminase Type IV Gene (PADI4) Suggests a Novel Intronic Variant is Associated with Rheumatoid Arthritis in the North American Caucasian Population
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39756277; 4038336
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Remmers, E
AU  - Plenge, R
AU  - Le, J.
AU  - Lee, A
AU  - Aksentijevich, I
AU  - Kastner, D
AU  - Gregersen, P
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - North America
KW  - Rheumatoid arthritis
KW  - Arginine deiminase
KW  - Arginine
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39756277?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Comprehensive+Analysis+of+Sequence+Variation+in+the+Peptidyl+Arginine+Deiminase+Type+IV+Gene+%28PADI4%29+Suggests+a+Novel+Intronic+Variant+is+Associated+with+Rheumatoid+Arthritis+in+the+North+American+Caucasian+Population&rft.au=Remmers%2C+E%3BPlenge%2C+R%3BLe%2C+J.%3BLee%2C+A%3BAksentijevich%2C+I%3BKastner%2C+D%3BGregersen%2C+P&rft.aulast=Remmers&rft.aufirst=E&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Association of SNP Haplotypes of Interleukin-1 Beta with Persistent Sciatica Following Lumbar Diskectomy
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39756055; 4038468
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Wu, T.
AU  - Kingman, A
AU  - Bollettino, A
AU  - Hipp, H
AU  - Scully, M
AU  - Belfer, I
AU  - Atlas, S
AU  - Buzas, B
AU  - McKnight, C
AU  - Keller, R
AU  - Goldman, D
AU  - Max, M
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Haplotypes
KW  - Interleukin 1
KW  - Single-nucleotide polymorphism
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39756055?accountid=14244
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Arg16Gly Polymorphism in Beta2-Adrenoreceptor is Associated with Severe Obesity in Pima Indian Women
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39755494; 4037929
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Guo, T
AU  - Muller, Y
AU  - Ma, L.
AU  - Valenzuela, R
AU  - Hanson, R
AU  - Kobes, S
AU  - Bogardus, C
AU  - Baier, L
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Obesity
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Genetic Susceptibility to Neonatal-Onset Multisystem Inflammatory Disease (NOMID/CINCA): Novel CIAS1 Mutations and Genomic Strategies to Resolve Locus Heterogeneity
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39754108; 4038740
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Aksentijevich, I
AU  - Balow Jr, J
AU  - Jones, J
AU  - Dailey, N
AU  - Canna, S
AU  - Remmers, E F
AU  - Goldbach-Mansky, R
AU  - Kastner, D L
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Inflammatory diseases
KW  - Mutation
KW  - Genomics
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Caspase-1-Mediated Cleavage of Pyrin, the Familial Mediterranean Fever Protein, Activates NF-?
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39754053; 4038739
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Chae, B J
AU  - Richard, K
AU  - Wood, G
AU  - Jaffe, H
AU  - Gumucio, D
AU  - Shoham, N
AU  - Kastner, D
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Mediterranean
KW  - Pyrin
KW  - Fever
KW  - Mediterranean region
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A VCAM1 Promoter Mutation that Affects Transcription Factor Binding is Observed with Increased Prevalence in Adults with Sickle Cell Anemia
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39752613; 4038667
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Taylor, J G
AU  - Chen, R A
AU  - Haudenschild, C
AU  - Ragavachari, N
AU  - Bernig, T
AU  - Garcia-Rossi, D
AU  - Hutchinson, A
AU  - Hoppe, C
AU  - Gladwin, M T
AU  - Chanock, S J
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Mutation
KW  - Sickle cell disease
KW  - Promoters
KW  - Transcription factors
KW  - Anemia
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39752613?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Possible Founder Mutation for Juvenile Hyaline Fibromatosis in Brazil
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39746326; 4037579
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Ramaswami, M D
AU  - Hart, P S
AU  - Acevedo, A C
AU  - Pallos, D
AU  - Hart, T C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Brazil
KW  - Mutation
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Analysis of Mouse Inner Ear MPSS Libraries to Select for Rare and Novel Expressed Genes.
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39746072; 4037308
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Peters, L M
AU  - Belyantseva, I A
AU  - Battey, J F
AU  - Friedman, T B
AU  - Morell, R J
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Inner ear
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39746072?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Evolution and Distribution of Haplotypes in the Complement Factor H (HF1/CFH) Gene that Predispose to Age-Related Macular Degeneration
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39744596; 4037693
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Dean, M
AU  - Gold, B
AU  - Bergeron, J
AU  - Anderson, D H
AU  - Johnson, L V
AU  - Allikmets, R
AU  - Hageman, G
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Evolutionary genetics
KW  - Haplotypes
KW  - Macular degeneration
KW  - Complement factor H
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39744596?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Evolution+and+Distribution+of+Haplotypes+in+the+Complement+Factor+H+%28HF1%2FCFH%29+Gene+that+Predispose+to+Age-Related+Macular+Degeneration&rft.au=Dean%2C+M%3BGold%2C+B%3BBergeron%2C+J%3BAnderson%2C+D+H%3BJohnson%2C+L+V%3BAllikmets%2C+R%3BHageman%2C+G&rft.aulast=Dean&rft.aufirst=M&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Recruitment to a Familial Cancer Study: Balancing Privacy Protection and Research Quality
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39744019; 4037543
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Slutsman, J
AU  - Graubard, B
AU  - Garceau, A
AU  - Willis, G
AU  - Wideroff, L
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Recruitment
KW  - Cancer
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39744019?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Recruitment+to+a+Familial+Cancer+Study%3A+Balancing+Privacy+Protection+and+Research+Quality&rft.au=Slutsman%2C+J%3BGraubard%2C+B%3BGarceau%2C+A%3BWillis%2C+G%3BWideroff%2C+L&rft.aulast=Slutsman&rft.aufirst=J&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Adipokine Gene Variants Associated with Type 2 Diabetes in the Aboriginal Sakha (Yakut) Population of Eastern Siberia
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39743751; 4038322
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Sambuughin, N
AU  - Platonov, F
AU  - Ignatiev, P
AU  - Osakovskiy, V
AU  - Sivtseva, T
AU  - De Bantel, A
AU  - Shatunov, A
AU  - Krivoshapkin, V
AU  - Goldfarb, L
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Russia, Siberia
KW  - Russia, Sakha
KW  - Diabetes mellitus
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39743751?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Genetic Polymorphisms in Catechol O-Methyltransferase Gene (COMT) Affect Acute Post-Surgical Pain in Humans
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39743228; 4038187
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Kim, H
AU  - Mittal, D
AU  - Brahim, J
AU  - Rowan, J
AU  - Dionne, R
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Pain
KW  - Gene polymorphism
KW  - Catechol O-methyltransferase
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39743228?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Genetic+Polymorphisms+in+Catechol+O-Methyltransferase+Gene+%28COMT%29+Affect+Acute+Post-Surgical+Pain+in+Humans&rft.au=Kim%2C+H%3BMittal%2C+D%3BBrahim%2C+J%3BRowan%2C+J%3BDionne%2C+R&rft.aulast=Kim&rft.aufirst=H&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Evidence for Linkage of Serum Alkaline Phosphatase Levels: A Genome-Wide Scan in the Framingham Offspring Study
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39740560; 4037876
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Lin, J-P
AU  - Cupples, A
AU  - O'Donnell, C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Progeny
KW  - Phosphatase
KW  - Alkaline phosphatase
KW  - Offspring
KW  - Serum
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39740560?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Haplotype Diversity and Population Histories in the CEPH Human Genome Diversity Panel Based Upon Variation in Four Cytochrome P450 Genes and COMT
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39740422; 4037679
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Modi, W
AU  - Sicotte, H
AU  - Garcia-Ross, D
AU  - Yeager-Jeffery, M
AU  - Welch, R
AU  - Burdette, L
AU  - Cann, H
AU  - Thomas, G
AU  - Chanock, S
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Haplotypes
KW  - Genomes
KW  - Genetic diversity
KW  - Historical account
KW  - Cytochrome P450
KW  - Population genetics
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39740422?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Haplotype+Diversity+and+Population+Histories+in+the+CEPH+Human+Genome+Diversity+Panel+Based+Upon+Variation+in+Four+Cytochrome+P450+Genes+and+COMT&rft.au=Modi%2C+W%3BSicotte%2C+H%3BGarcia-Ross%2C+D%3BYeager-Jeffery%2C+M%3BWelch%2C+R%3BBurdette%2C+L%3BCann%2C+H%3BThomas%2C+G%3BChanock%2C+S&rft.aulast=Modi&rft.aufirst=W&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Detection of Glycine Substitutions in the Amino End of Type I Collagen by Biochemical Screening of Fibroblast Collagen Requires Supplementation by Direct Sequencing for Osteogenesis Imperfecta Probands.
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39739498; 4037197
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Cabral, W A
AU  - Milgrom, S
AU  - Moriarty, E
AU  - Marini, J C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Collagen (type I)
KW  - Supplementation
KW  - Glycine
KW  - Osteogenesis imperfecta
KW  - Fibroblasts
KW  - Screening
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39739498?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Morphologic Characteristics in Hemizygous Fabry Disease Patients
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39738357; 4036934
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Ries, M
AU  - Moore, D F
AU  - Robinson, C
AU  - Tifft, C
AU  - Rosenbaum, K
AU  - Brady, R O
AU  - Schiffmann, R
AU  - Krasnewich, D
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Fabry's disease
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39738357?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Late Evening Settling and Early Morning Sleep Maintenance Differentiate the Sleep Patterns of Adolescents and Younger Children with Smith-Magenis Syndrome (SMS)
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39737988; 4036820
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Duncan, W C
AU  - Morse, R S
AU  - Krasnewich, D
AU  - Smith, A.C.M.
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Symptoms
KW  - Children
KW  - Adolescents
KW  - Sleep
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39737988?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - FH Mutation Analysis, Enzyme Activity, Protein Modeling and Early Functional Study in Hereditary Leiomyomatosis and Renal Cell Cancer
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39736457; 4036536
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Pithukpakorn, M
AU  - Wei, M H
AU  - Toure, O
AU  - Glenn, G M
AU  - Middelton, L
AU  - Merino, M
AU  - Zbar, B
AU  - Neckers, L
AU  - Linehan, W M
AU  - Toro, J R
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Enzymatic activity
KW  - Kidneys
KW  - Mutation
KW  - Cancer
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39736457?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=FH+Mutation+Analysis%2C+Enzyme+Activity%2C+Protein+Modeling+and+Early+Functional+Study+in+Hereditary+Leiomyomatosis+and+Renal+Cell+Cancer&rft.au=Pithukpakorn%2C+M%3BWei%2C+M+H%3BToure%2C+O%3BGlenn%2C+G+M%3BMiddelton%2C+L%3BMerino%2C+M%3BZbar%2C+B%3BNeckers%2C+L%3BLinehan%2C+W+M%3BToro%2C+J+R&rft.aulast=Pithukpakorn&rft.aufirst=M&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Twin Study Heritability Estimates of Central Auditory Processing Functions
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39736000; 4038385
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Drayna, D
AU  - Brewer, C
AU  - Snieder, H
AU  - Zalewski, C
AU  - Friedman, T
AU  - Morell, R
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Information processing
KW  - Twins
KW  - Heritability
KW  - Auditory system
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39736000?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Twin+Study+Heritability+Estimates+of+Central+Auditory+Processing+Functions&rft.au=Drayna%2C+D%3BBrewer%2C+C%3BSnieder%2C+H%3BZalewski%2C+C%3BFriedman%2C+T%3BMorell%2C+R&rft.aulast=Drayna&rft.aufirst=D&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - SNPdetector: A Software Tool for Sensitive and Accurate Detection of Single Nucleotide Polymorphisms and Mutations in Fluorescence-Based Resequencing
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39733364; 4037578
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Zhang, J
AU  - Wheeler, D
AU  - Yakub, I
AU  - Wei, S
AU  - Sood, R
AU  - Rowe, W
AU  - Liu, P
AU  - Gibbs, R
AU  - Buetow, K
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Nucleotides
KW  - Mutation
KW  - Single-nucleotide polymorphism
KW  - Computer programs
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39733364?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=SNPdetector%3A+A+Software+Tool+for+Sensitive+and+Accurate+Detection+of+Single+Nucleotide+Polymorphisms+and+Mutations+in+Fluorescence-Based+Resequencing&rft.au=Zhang%2C+J%3BWheeler%2C+D%3BYakub%2C+I%3BWei%2C+S%3BSood%2C+R%3BRowe%2C+W%3BLiu%2C+P%3BGibbs%2C+R%3BBuetow%2C+K&rft.aulast=Zhang&rft.aufirst=J&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A Mutation Spectrum of MYO7A Associated with Usher Syndrome Type 1 and Evidence for the Existence of DFNB2
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39729433; 4038502
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Riazuddin, S
AU  - Nazli, S
AU  - Sheikh, R S
AU  - Khan, S N
AU  - Sabir, F
AU  - Javid, F T
AU  - Wilcox, E R
AU  - Ahmed, Z A
AU  - Friedman, T B
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Symptoms
KW  - Mutation
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39729433?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=A+Mutation+Spectrum+of+MYO7A+Associated+with+Usher+Syndrome+Type+1+and+Evidence+for+the+Existence+of+DFNB2&rft.au=Riazuddin%2C+S%3BNazli%2C+S%3BSheikh%2C+R+S%3BKhan%2C+S+N%3BSabir%2C+F%3BJavid%2C+F+T%3BWilcox%2C+E+R%3BAhmed%2C+Z+A%3BFriedman%2C+T+B&rft.aulast=Riazuddin&rft.aufirst=S&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Glucocerebrosidase Alterations E326K and T369M in Subjects with and without Parkinsonism
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39728553; 4038325 DE:
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Eblan, M J
AU  - Hruska, K
AU  - Nguyen, J
AU  - Walker, J
AU  - Sidransky, E
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39728553?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Glucocerebrosidase+Alterations+E326K+and+T369M+in+Subjects+with+and+without+Parkinsonism&rft.au=Eblan%2C+M+J%3BHruska%2C+K%3BNguyen%2C+J%3BWalker%2C+J%3BSidransky%2C+E&rft.aulast=Eblan&rft.aufirst=M&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Genome-Wide Scan for Familial Cutaneous Malignant Melanoma (CMM) Susceptibility Loci in A Northeastern Italian Population
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39727456; 4037819
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Kerstann, K F
AU  - Steighner, R
AU  - Ter-Minassian, M
AU  - Calista, D
AU  - Minghetti, P
AU  - Landi, G
AU  - Goldstein, A M
AU  - Landi, M T
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Melanoma
KW  - Population genetics
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39727456?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Genome-Wide+Scan+for+Familial+Cutaneous+Malignant+Melanoma+%28CMM%29+Susceptibility+Loci+in+A+Northeastern+Italian+Population&rft.au=Kerstann%2C+K+F%3BSteighner%2C+R%3BTer-Minassian%2C+M%3BCalista%2C+D%3BMinghetti%2C+P%3BLandi%2C+G%3BGoldstein%2C+A+M%3BLandi%2C+M+T&rft.aulast=Kerstann&rft.aufirst=K&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Development of Long-Term Treatment for Hypertension Using Human Skin Gene Therapy to Deliver Systemic Atrial Natriuretic Peptide (ANP)
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39723701; 4038292
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Therrien, J-P
AU  - Tock, C L
AU  - Ohyama, M
AU  - Voge, J C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Gene therapy
KW  - Atrial natriuretic peptide
KW  - Peptides
KW  - Hypertension
KW  - Skin
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39723701?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Development+of+Long-Term+Treatment+for+Hypertension+Using+Human+Skin+Gene+Therapy+to+Deliver+Systemic+Atrial+Natriuretic+Peptide+%28ANP%29&rft.au=Therrien%2C+J-P%3BTock%2C+C+L%3BOhyama%2C+M%3BVoge%2C+J+C&rft.aulast=Therrien&rft.aufirst=J-P&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Fine Mapping of a Putative Type II Diabetes Susceptibility Gene on 1Q in Native American Pimas
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39723268; 4038148
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Singer, J M
AU  - Ossowski, V
AU  - Mccarthy, M I
AU  - Deloukas, P
AU  - Zeggini, E
AU  - Rayner, W
AU  - Bogardus, C
AU  - Prochazka, M
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Ethnic groups
KW  - Chromosome 1
KW  - Diabetes mellitus
KW  - Gene mapping
KW  - U 2000:Biological Sciences
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Dysfunction of Endocytic and Autophagic Pathways in a Lysosomal Storage Disease
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39722371; 4037070
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Fukuda, T
AU  - Zaal, K
AU  - Ralston, E
AU  - Plotz, P
AU  - Raben, N
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Lysosomal storage diseases
KW  - Storage
KW  - U 2000:Biological Sciences
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Case-Control Statistical Comparison of LD Patterns for Genetic Association Studies
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39721948; 4038536
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Zaykin, D V
AU  - Meng, Z
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Statistics
KW  - U 2000:Biological Sciences
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N1  - Date revised - 2008-05-21
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TY  - CPAPER
T1  - Myotilin Mutations are Associated with a Significant Number of Myofibrillar Myopathy Cases
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39721936; 4036968
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Shatunov, A
AU  - Olive, M
AU  - Hilton-Jones, D
AU  - Ferrer, I
AU  - Dalakas, M C
AU  - Goldfarb, L G
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Mutation
KW  - Myopathy
KW  - U 2000:Biological Sciences
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Linkage Scans for HDL-C, Triglycerides and Apolipoprotein AI in Three Populations and Comparison with the NHLBI Genelink Meta-Analyses
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39720190; 4037966
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Klos, K.L.E.
AU  - Kardia, S.L.R.
AU  - Turner, S T
AU  - Hanis, C
AU  - Cupples, L A
AU  - Hunt, S C
AU  - Mahaney, M C
AU  - Pate, S R
AU  - Province, M A
AU  - Rice, T
AU  - Berenson, G S
AU  - Boerwinkle, E
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Triglycerides
KW  - Apolipoproteins
KW  - Reviews
KW  - U 2000:Biological Sciences
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LA  - English
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - How to Use the Online NCI/NCBI Entrez Cancer Chromosomes Search Database
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39719879; 4036346
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Knutsen, T
AU  - Gobu, V
AU  - Ried, T
AU  - Sirotkin, K
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Chromosomes
KW  - Databases
KW  - Cancer
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Factors Associated with an Increased Frequency of CDKN2A Mutations in Melanoma-Prone Families
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39719705; 4036507
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Goldstein, A M
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Mutation
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Analysis of IL-4, MxA, and IRF-1 Genes in Filipino Patients with Subacute Sclerosing Panencephalitis
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39717876; 4038621
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Silao, C.L.T.
AU  - Pipo-Deveza, J R
AU  - Kusuhara, K
AU  - Salonga, A M
AU  - Lukban, M B
AU  - Sanchez, B C
AU  - Kira, R
AU  - Torisu, H
AU  - Hara, T
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Interferon regulatory factor 1
KW  - Interleukin 4
KW  - Subacute sclerosing panencephalitis
KW  - U 2000:Biological Sciences
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Gene Expression Profiling of Murine Spermatogenesis Leads to the Identification of mArd2, a Novel Mouse Ard1 Homolog that is Preferentially Expressed Starting from Meiosis.
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39716077; 4037110
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Pang, A.L.Y.
AU  - Johnson, W
AU  - Bear, D H
AU  - Rennert, O M
AU  - Chan, W Y
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Profiling
KW  - Spermatogenesis
KW  - Gene expression
KW  - Meiosis
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Discoveries with Computational Analysis of SAGE Data of Mouse Germ-Cell Transcriptome at different Stages of Spermatogenesis
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39713486; 4037482
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Lee, T L
AU  - Alba, D
AU  - Baxendale, V
AU  - Rennert, O M
AU  - Chan, W Y
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Spermatogenesis
KW  - Computer applications
KW  - Data processing
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - High Density Mapping Studies On Chromosomal Regions 1, 3, 6, 12, 13 and 17 in 28 Families with Chronic Lymphocytic Leukemia.
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39712911; 4037732
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Ng, D.
AU  - Marti, G E
AU  - Fontaine, L
AU  - Toro, J R
AU  - Caporaso, N
AU  - Goldin, L R
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Chromosomes
KW  - Chronic lymphatic leukemia
KW  - Gene mapping
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=High+Density+Mapping+Studies+On+Chromosomal+Regions+1%2C+3%2C+6%2C+12%2C+13+and+17+in+28+Families+with+Chronic+Lymphocytic+Leukemia.&rft.au=Ng%2C+D.%3BMarti%2C+G+E%3BFontaine%2C+L%3BToro%2C+J+R%3BCaporaso%2C+N%3BGoldin%2C+L+R&rft.aulast=Ng&rft.aufirst=D.&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A Genetic Variant in the Neuropeptide Y Gene (NPY) is Associated with Energy Balance and Obesity in Pima Indians
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39712414; 4038113
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Muller, Y L
AU  - Bogardus, C
AU  - Baier, L
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Energy balance
KW  - Obesity
KW  - Neuropeptide Y
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Association of Variants in the CD244 Gene with Type 2 Diabetes in Pima Indians
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39711061; 4036927
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Guo, Y
AU  - Ossowski, V
AU  - Wolford, J
AU  - Hanson, R L
AU  - Kobes, S
AU  - Bogardus, C
AU  - Prochazka, M
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Diabetes mellitus
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Cognitive and Language Deficits Among Children with Chronic Neuronopathic Gaucher Disease
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39710543; 4036797
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Schiffmann, R
AU  - Goker-Alpan, O
AU  - Wiggs, E
AU  - Eblan, M
AU  - Sidransky, E
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Children
KW  - Language
KW  - Cognitive ability
KW  - U 2000:Biological Sciences
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LA  - English
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N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Occipital Horn Syndrome in Brothers with a Missense Mutation in the ATP-binding domain of ATP7A
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39708414; 4036454
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Tang, J
AU  - Robertson, S
AU  - Kaler, S G
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Symptoms
KW  - Horns
KW  - Missense mutation
KW  - U 2000:Biological Sciences
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LA  - English
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N1  - Date revised - 2008-05-21
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ER  - 



TY  - CPAPER
T1  - Perfect Sensitivity and Specificity of Plasma Catechol Measurements for Neonatal Diagnosis of Menkes Disease
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39708182; 4038363
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Holmes, C S
AU  - Kaler, S G
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Specificity
KW  - Menkes disease
KW  - Neonates
KW  - Catechol
KW  - U 2000:Biological Sciences
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Evidence for Multiple Distinct Obesity/Type 2 Diabetes Mellitus Loci Under A Single Peak of Linkage On Chromosome 11Q23: Replication in Ethnically Diverse Populations.
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39706177; 4037774
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Baier, L
AU  - Muller, Y
AU  - Ma, L.
AU  - Traurig, M
AU  - Kovacs, P
AU  - Bottner, A
AU  - Stone, S
AU  - Timms, K
AU  - Groves, C J
AU  - McCarthy, M
AU  - Erdos, M
AU  - Conneely, K
AU  - Boehnke, M
AU  - Miyake, K
AU  - Atwood, L
AU  - Johansson, L
AU  - Ridderstale, M
AU  - Knowler, W
AU  - Hanson, R
AU  - Bogardus, C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Obesity
KW  - Chromosomes
KW  - Chromosome 11
KW  - Replication
KW  - Population genetics
KW  - Diabetes mellitus
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39706177?accountid=14244
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DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - New dbSNP Resources to Support Genotype and Haplotype Submissions
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39704253; 4037586
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Sherry, S T
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Haplotypes
KW  - Genotypes
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39704253?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=New+dbSNP+Resources+to+Support+Genotype+and+Haplotype+Submissions&rft.au=Sherry%2C+S+T&rft.aulast=Sherry&rft.aufirst=S&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Cost-Benefit Analysis of the Newborn Screening Program of the Philippines
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39701247; 4037546
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Padilla, C D
AU  - Dans, L F
AU  - Estrada, S C
AU  - Tamondong, M R
AU  - Bernal, R.M.S.
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Philippines
KW  - Neonates
KW  - Screening
KW  - Cost-benefit analysis
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39701247?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Comparison of Methods for Stratified Analysis of Association Studies in Fine-Mapping Type 2 Diabetes in Multiple Populations for Chromosome 1q
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39699908; 4038422
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Hanson, R
AU  - Zeggini, E
AU  - Rayner, W
AU  - Mitchell, B
AU  - O'Connell, J
AU  - Shuldiner, A
AU  - Elbein, S
AU  - Ng, M.C.Y.
AU  - Xiang, K
AU  - Froguel, P
AU  - Deloukas, P
AU  - McCarthy, M
AU  - Knowler, W
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Chromosome 1
KW  - Chromosomes
KW  - Diabetes mellitus
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39699908?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Comparison+of+Methods+for+Stratified+Analysis+of+Association+Studies+in+Fine-Mapping+Type+2+Diabetes+in+Multiple+Populations+for+Chromosome+1q&rft.au=Hanson%2C+R%3BZeggini%2C+E%3BRayner%2C+W%3BMitchell%2C+B%3BO%27Connell%2C+J%3BShuldiner%2C+A%3BElbein%2C+S%3BNg%2C+M.C.Y.%3BXiang%2C+K%3BFroguel%2C+P%3BDeloukas%2C+P%3BMcCarthy%2C+M%3BKnowler%2C+W&rft.aulast=Hanson&rft.aufirst=R&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Molecular Chaperones in Gaucher Disease
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39692944; 4038744
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Urban, D
AU  - Goker-Alpan, O
AU  - Stubblefield, B K
AU  - Sidransky, E
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Chaperones
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Analysis of Conserved Regulatory Elements in the Glucocerebrosidase Gene Locus.
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39686808; 4037130 DE:
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Hruska, K S
AU  - LaMarca, M E
AU  - Ziegler, S G
AU  - Portnoy, M E
AU  - Green, E D
AU  - Sidransky, E
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39686808?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Analysis+of+Conserved+Regulatory+Elements+in+the+Glucocerebrosidase+Gene+Locus.&rft.au=Hruska%2C+K+S%3BLaMarca%2C+M+E%3BZiegler%2C+S+G%3BPortnoy%2C+M+E%3BGreen%2C+E+D%3BSidransky%2C+E&rft.aulast=Hruska&rft.aufirst=K&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Auditory and Vision Phenotype of Waltzer Cdh23v-6J and Ames Waltzer Pcdh15av-Jfb Double Mutant Mice: No Evidence of Retinitis Pigmentosa or Digenic Inheritance of Progressive Hearing Loss.
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39686634; 4037083
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Ahmed, Z
AU  - Haywood-Watson II, R.J.L.
AU  - Riazuddin, S
AU  - Kjellstrom, S
AU  - Bush, R A
AU  - Hampton, L L
AU  - Battey, J F
AU  - Sieving, P A
AU  - Frolenkov, G
AU  - Friedman, T B
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Vision
KW  - Phenotypes
KW  - Mutants
KW  - Mice
KW  - Retinitis pigmentosa
KW  - Heredity
KW  - Hearing loss
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39686634?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=Auditory+and+Vision+Phenotype+of+Waltzer+Cdh23v-6J+and+Ames+Waltzer+Pcdh15av-Jfb+Double+Mutant+Mice%3A+No+Evidence+of+Retinitis+Pigmentosa+or+Digenic+Inheritance+of+Progressive+Hearing+Loss.&rft.au=Ahmed%2C+Z%3BHaywood-Watson+II%2C+R.J.L.%3BRiazuddin%2C+S%3BKjellstrom%2C+S%3BBush%2C+R+A%3BHampton%2C+L+L%3BBattey%2C+J+F%3BSieving%2C+P+A%3BFrolenkov%2C+G%3BFriedman%2C+T+B&rft.aulast=Ahmed&rft.aufirst=Z&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A Mouse Model Employing the tet-off System in an Antisense Construct to Prkar1A Confirms tTA-Independent Expression of the Transgene and Develops Tumors Consistent with Carney Complex (MIM160980)
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39684284; 4036398
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Griffin, K J
AU  - Weinberg, F
AU  - Stergiopoulos, S
AU  - Matyakhina, L
AU  - Kirschner, L
AU  - Stratakis, C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Animal models
KW  - Carney complex
KW  - Antisense
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39684284?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.atitle=A+Mouse+Model+Employing+the+tet-off+System+in+an+Antisense+Construct+to+Prkar1A+Confirms+tTA-Independent+Expression+of+the+Transgene+and+Develops+Tumors+Consistent+with+Carney+Complex+%28MIM160980%29&rft.au=Griffin%2C+K+J%3BWeinberg%2C+F%3BStergiopoulos%2C+S%3BMatyakhina%2C+L%3BKirschner%2C+L%3BStratakis%2C+C&rft.aulast=Griffin&rft.aufirst=K&rft.date=2005-10-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=55th+Annual+Meeting+of+the+American+Society+of+Human+Genetics&rft.issn=&rft_id=info:doi/
L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Association of Common Variation in AGTR1 with Left Ventricular Mass in the Framingham Heart Study
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39678882; 4036420
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Hirschhorn, J N
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Heart
KW  - Circulatory system
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39678882?accountid=14244
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - An Investigation of Cholesterol Biosynthesis by Cortisol-Producing, Benign Tumors of the Adrenal Gland
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39675482; 4036492
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Wassif, C
AU  - Horvath, A
AU  - Sterner, A
AU  - Porter, F
AU  - Stratakis, C
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Cholesterol
KW  - Adrenal glands
KW  - Benign
KW  - Biosynthesis
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Genetic Variations of Non-Synonymous Mutations in MBL2 in different Human Populations Provide Evidence for Recent Natural Selection
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39647818; 4037615
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Bernig, T
AU  - Tarazona-Santos, E
AU  - Modi, W S
AU  - Yeager, M
AU  - Welch, R A
AU  - Chanock, S
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Natural selection
KW  - Mutation
KW  - Population genetics
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - MtDNA Sequence Heterogeneity in Single Cells from Leukemia Patients
T2  - 55th Annual Meeting of the American Society of Human Genetics
AN  - 39631614; 4036615
JF  - 55th Annual Meeting of the American Society of Human Genetics
AU  - Yao, Y G
AU  - Ogasawara, Y
AU  - Kajigaya, S
AU  - Molldrem, J J
AU  - Falcao, R P
AU  - Pintao, M C
AU  - McCoy, J P
AU  - Keyvanafar, K
AU  - Rizzatti, E G
AU  - Young, N S
Y1  - 2005/10/25/
PY  - 2005
DA  - 2005 Oct 25
KW  - Leukemia
KW  - Mitochondrial DNA
KW  - U 2000:Biological Sciences
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L2  - http://www.ashg.org/genetics/ashg/menu-annmeet.shtml
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Association of the CYP1B1*3 Allele with Survival in Patients with Prostate Cancer Receiving Docetaxel
T2  - 2005 Annual Meeting of the American College of Clinical Pharmacy
AN  - 39796172; 4039538
JF  - 2005 Annual Meeting of the American College of Clinical Pharmacy
AU  - Sissung, Tristan M
AU  - Danesi, Romano
AU  - Price, Douglas K
AU  - Steinberg, Seth M
AU  - Wit, Ronald De
AU  - Cox, Michael C
AU  - Dahut, William
AU  - Figg, William Sr
AU  - Sparreboom, Alex
Y1  - 2005/10/23/
PY  - 2005
DA  - 2005 Oct 23
KW  - Survival
KW  - Allelles
KW  - Prostate cancer
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39796172?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+American+College+of+Clinical+Pharmacy&rft.atitle=Association+of+the+CYP1B1*3+Allele+with+Survival+in+Patients+with+Prostate+Cancer+Receiving+Docetaxel&rft.au=Sissung%2C+Tristan+M%3BDanesi%2C+Romano%3BPrice%2C+Douglas+K%3BSteinberg%2C+Seth+M%3BWit%2C+Ronald+De%3BCox%2C+Michael+C%3BDahut%2C+William%3BFigg%2C+William+Sr%3BSparreboom%2C+Alex&rft.aulast=Sissung&rft.aufirst=Tristan&rft.date=2005-10-23&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+American+College+of+Clinical+Pharmacy&rft.issn=&rft_id=info:doi/
L2  - http://www.accp.com/am05_abstracts.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Polymorphism in the Hypoxia-Inducible Factor 1A Gene May Confer Susceptibility to Androgen-Independent Prostate Cancer
T2  - 2005 Annual Meeting of the American College of Clinical Pharmacy
AN  - 39728226; 4039495
JF  - 2005 Annual Meeting of the American College of Clinical Pharmacy
AU  - Chau, Cindy H
AU  - Permenter, Matthew G
AU  - Steinberg, Seth M
AU  - Retter, Avi S
AU  - Dahut, William L
AU  - Price, Douglas K
AU  - Figg, William D
Y1  - 2005/10/23/
PY  - 2005
DA  - 2005 Oct 23
KW  - Prostate cancer
KW  - Gene polymorphism
KW  - Hypoxia-inducible factors
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39728226?accountid=14244
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L2  - http://www.accp.com/am05_abstracts.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - A Pharmacokinetic (PK) Study of Oral CC-5013, a Novel Thalidomide Analogue, in Patients with Refractory Metastatic Cancer.
T2  - 2005 Annual Meeting of the American College of Clinical Pharmacy
AN  - 39727996; 4039421
JF  - 2005 Annual Meeting of the American College of Clinical Pharmacy
AU  - Tohnya, Tanyifor
AU  - Sparreboom, Alex
AU  - Venitz, Jurgen
AU  - Parker, Catherine
AU  - Dahut, William L
AU  - Figg, William D
Y1  - 2005/10/23/
PY  - 2005
DA  - 2005 Oct 23
KW  - Pharmacokinetics
KW  - Metastases
KW  - Cancer
KW  - Thalidomide
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39727996?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+American+College+of+Clinical+Pharmacy&rft.atitle=A+Pharmacokinetic+%28PK%29+Study+of+Oral+CC-5013%2C+a+Novel+Thalidomide+Analogue%2C+in+Patients+with+Refractory+Metastatic+Cancer.&rft.au=Tohnya%2C+Tanyifor%3BSparreboom%2C+Alex%3BVenitz%2C+Jurgen%3BParker%2C+Catherine%3BDahut%2C+William+L%3BFigg%2C+William+D&rft.aulast=Tohnya&rft.aufirst=Tanyifor&rft.date=2005-10-23&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+American+College+of+Clinical+Pharmacy&rft.issn=&rft_id=info:doi/
L2  - http://www.accp.com/am05_abstracts.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Association of Genetic Variants in ABCB1 and CYP3A4/5 with the Pharmacokinetics of Erlotinib
T2  - 2005 Annual Meeting of the American College of Clinical Pharmacy
AN  - 39709693; 4039542
JF  - 2005 Annual Meeting of the American College of Clinical Pharmacy
AU  - Scripture, Charity D
AU  - Sissung, Tristan M
AU  - Permenter, Matthew G
AU  - Price, Douglas K
AU  - Swain, Sandra M
AU  - Sparreboom, Alex
AU  - Figg, William D
Y1  - 2005/10/23/
PY  - 2005
DA  - 2005 Oct 23
KW  - Pharmacokinetics
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39709693?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+American+College+of+Clinical+Pharmacy&rft.atitle=Association+of+Genetic+Variants+in+ABCB1+and+CYP3A4%2F5+with+the+Pharmacokinetics+of+Erlotinib&rft.au=Scripture%2C+Charity+D%3BSissung%2C+Tristan+M%3BPermenter%2C+Matthew+G%3BPrice%2C+Douglas+K%3BSwain%2C+Sandra+M%3BSparreboom%2C+Alex%3BFigg%2C+William+D&rft.aulast=Scripture&rft.aufirst=Charity&rft.date=2005-10-23&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+American+College+of+Clinical+Pharmacy&rft.issn=&rft_id=info:doi/
L2  - http://www.accp.com/am05_abstracts.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Human mitochondrial ClpP is a stable heptamer that assembles into a tetradecamer in the presence of ClpX.
AN  - 68693876; 16115876
AB  - The functional form of ClpP, the proteolytic component of ATP-dependent Clp proteases, is a hollow-cored particle composed of two heptameric rings joined face-to-face forming an aqueous chamber containing the proteolytic active sites. We have found that isolated human mitochondrial ClpP (hClpP) is stable as a heptamer and remains a monodisperse species (s(20,w) 7.0 S; M(app) 169, 200) at concentrations > or = 3 mg/ml. Heptameric hClpP has no proteolytic activity and very low peptidase activity. In the presence of ATP, hClpX interacts with hClpP forming a complex, which by equilibrium sedimentation measurements has a M(app) of 1 x 10(6). Electron microscopy confirmed that the complex consisted of a double ring of hClpP with an hClpX ring axially aligned on each end. The hClpXP complex has protease activity and greatly increased peptidase activity, indicating that interaction with hClpX affects the conformation of the hClpP catalytic active site. A mutant of hClpP, in which a cysteine residue was introduced into the handle region at the interface between the two rings formed stable tetradecamers under oxidizing conditions but spontaneously dissociated into two heptamers upon reduction. Thus, hClpP rings interact transiently but very weakly in solution, and hClpX must exert an allosteric effect on hClpP to promote a conformation that stabilizes the tetradecamer. These data suggest that hClpX can regulate the appearance of hClpP peptidase activity in mitochondria and might affect the nature of the degradation products released during ATP-dependent proteolytic cycles.
JF  - The Journal of biological chemistry
AU  - Kang, Sung Gyun
AU  - Dimitrova, Mariana N
AU  - Ortega, Joaquin
AU  - Ginsburg, Ann
AU  - Maurizi, Michael R
AD  - Laboratory of Cell Biology, NCI, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/10/21/
PY  - 2005
DA  - 2005 Oct 21
SP  - 35424
EP  - 35432
VL  - 280
IS  - 42
SN  - 0021-9258, 0021-9258
KW  - Cross-Linking Reagents
KW  - 0
KW  - Disulfides
KW  - Recombinant Proteins
KW  - Green Fluorescent Proteins
KW  - 147336-22-9
KW  - Histidine
KW  - 4QD397987E
KW  - Adenosine Triphosphate
KW  - 8L70Q75FXE
KW  - Peptide Hydrolases
KW  - EC 3.4.-
KW  - Trypsin
KW  - EC 3.4.21.4
KW  - Endopeptidase Clp
KW  - EC 3.4.21.92
KW  - Cysteine
KW  - K848JZ4886
KW  - Glutaral
KW  - T3C89M417N
KW  - Index Medicus
KW  - Animals
KW  - Humans
KW  - Hydrogen-Ion Concentration
KW  - Liver -- metabolism
KW  - Mutagenesis
KW  - Rats
KW  - Cysteine -- chemistry
KW  - Chromatography, Gel
KW  - Chromatin Immunoprecipitation
KW  - Microscopy, Electron
KW  - Recombinant Proteins -- chemistry
KW  - Time Factors
KW  - Protein Conformation
KW  - Peptide Hydrolases -- chemistry
KW  - Green Fluorescent Proteins -- chemistry
KW  - Glutaral -- pharmacology
KW  - Dimerization
KW  - Cross-Linking Reagents -- pharmacology
KW  - Ultracentrifugation
KW  - Hydrolysis
KW  - Protein Binding
KW  - Binding Sites
KW  - Adenosine Triphosphate -- chemistry
KW  - Histidine -- chemistry
KW  - Disulfides -- chemistry
KW  - Allosteric Site
KW  - Protein Structure, Tertiary
KW  - Trypsin -- pharmacology
KW  - Mutation
KW  - Mitochondria -- enzymology
KW  - Mitochondria -- metabolism
KW  - Endopeptidase Clp -- chemistry
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=The+Journal+of+biological+chemistry&rft.atitle=Human+mitochondrial+ClpP+is+a+stable+heptamer+that+assembles+into+a+tetradecamer+in+the+presence+of+ClpX.&rft.au=Kang%2C+Sung+Gyun%3BDimitrova%2C+Mariana+N%3BOrtega%2C+Joaquin%3BGinsburg%2C+Ann%3BMaurizi%2C+Michael+R&rft.aulast=Kang&rft.aufirst=Sung&rft.date=2005-10-21&rft.volume=280&rft.issue=42&rft.spage=35424&rft.isbn=&rft.btitle=&rft.title=The+Journal+of+biological+chemistry&rft.issn=00219258&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-13
N1  - Date created - 2005-10-17
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Mutational analysis of the catalytic domain of O-linked N-acetylglucosaminyl transferase.
AN  - 68692561; 16105839
AB  - O-Linked N-acetylglucosaminyltransferase (OGT) catalyzes the transfer of O-linked GlcNAc to serine/threonine residues of a variety of target proteins, many of which have been implicated in such diseases as diabetes and neurodegeneration. The addition of O-GlcNAc to proteins occurs in response to fluctuations in cellular concentrations of UDP-GlcNAc, which result from nutrients entering the hexosamine biosynthetic pathway. However, the molecular mechanisms involved in sugar nucleotide recognition and transfer to protein are poorly understood. We employed site-directed mutagenesis to target potentially important amino acid residues within the two conserved catalytic domains of OGT (CD I and CD II), followed by an in vitro glycosylation assay to evaluate N-acetylglucosaminyltransferase activity after bacterial expression. Although many of the amino acid substitutions caused inactivation of the enzyme, we identified three amino acid residues (two in CD I and one in CD II) that produced viable enzymes when mutated. Structure-based homology modeling revealed that these permissive mutants may be either in or near the sugar nucleotide-binding site. Our findings suggest a model in which the two conserved regions of the catalytic domain, CD I and CD II, contribute to the formation of a UDP-GlcNAc-binding pocket that catalyzes the transfer of O-GlcNAc to substrate proteins. Identification of viable OGT mutants may facilitate examination of its role in nutrient sensing and signal transduction cascades.
JF  - The Journal of biological chemistry
AU  - Lazarus, Brooke D
AU  - Roos, Mark D
AU  - Hanover, John A
AD  - Laboratory of Cell Biology and Biochemistry, NIDDK, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/10/21/
PY  - 2005
DA  - 2005 Oct 21
SP  - 35537
EP  - 35544
VL  - 280
IS  - 42
SN  - 0021-9258, 0021-9258
KW  - Hexosamines
KW  - 0
KW  - Nucleotides
KW  - N-Acetylglucosaminyltransferases
KW  - EC 2.4.1.-
KW  - O-GlcNAc transferase
KW  - Index Medicus
KW  - Hexosamines -- chemistry
KW  - Electrophoresis, Polyacrylamide Gel
KW  - Models, Molecular
KW  - Humans
KW  - Nuclear Pore -- chemistry
KW  - Catalytic Domain
KW  - Nucleotides -- chemistry
KW  - Amino Acid Sequence
KW  - Glycosylation
KW  - Protein Binding
KW  - Binding Sites
KW  - Mutagenesis, Site-Directed
KW  - Genetic Vectors
KW  - Kinetics
KW  - Point Mutation
KW  - Molecular Sequence Data
KW  - Insulin Resistance
KW  - Sequence Homology, Amino Acid
KW  - Protein Structure, Tertiary
KW  - Mutation
KW  - Signal Transduction
KW  - Protein Conformation
KW  - N-Acetylglucosaminyltransferases -- metabolism
KW  - DNA Mutational Analysis
KW  - N-Acetylglucosaminyltransferases -- chemistry
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68692561?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=The+Journal+of+biological+chemistry&rft.atitle=Mutational+analysis+of+the+catalytic+domain+of+O-linked+N-acetylglucosaminyl+transferase.&rft.au=Lazarus%2C+Brooke+D%3BRoos%2C+Mark+D%3BHanover%2C+John+A&rft.aulast=Lazarus&rft.aufirst=Brooke&rft.date=2005-10-21&rft.volume=280&rft.issue=42&rft.spage=35537&rft.isbn=&rft.btitle=&rft.title=The+Journal+of+biological+chemistry&rft.issn=00219258&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-13
N1  - Date created - 2005-10-17
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Changing Sequence Specificity of Human Pumilio-Homology Domain
T2  - VI Symposium on RNA Biology
AN  - 39758428; 4032357
JF  - VI Symposium on RNA Biology
AU  - Cheong, Cheom-gil
AU  - Hall, Traci M. Tanaka
Y1  - 2005/10/21/
PY  - 2005
DA  - 2005 Oct 21
KW  - Specificity
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39758428?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=VI+Symposium+on+RNA+Biology&rft.atitle=Changing+Sequence+Specificity+of+Human+Pumilio-Homology+Domain&rft.au=Cheong%2C+Cheom-gil%3BHall%2C+Traci+M.+Tanaka&rft.aulast=Cheong&rft.aufirst=Cheom-gil&rft.date=2005-10-21&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=VI+Symposium+on+RNA+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.med.unc.edu/pmbb/Schedule_Abstracts.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Small RNAs as Part of the Cellular Stress Response
T2  - VI Symposium on RNA Biology
AN  - 39758275; 4032335
JF  - VI Symposium on RNA Biology
AU  - Gottesman, Susan
AU  - Guillier, Maude
AU  - Vanderpool, Carin
AU  - Thompson, Karl
AU  - Majdalani, Nadim
Y1  - 2005/10/21/
PY  - 2005
DA  - 2005 Oct 21
KW  - Stress
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39758275?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=VI+Symposium+on+RNA+Biology&rft.atitle=Small+RNAs+as+Part+of+the+Cellular+Stress+Response&rft.au=Gottesman%2C+Susan%3BGuillier%2C+Maude%3BVanderpool%2C+Carin%3BThompson%2C+Karl%3BMajdalani%2C+Nadim&rft.aulast=Gottesman&rft.aufirst=Susan&rft.date=2005-10-21&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=VI+Symposium+on+RNA+Biology&rft.issn=&rft_id=info:doi/
L2  - http://www.med.unc.edu/pmbb/Schedule_Abstracts.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Exon Definition Regulates Alternative RNA Splicing in DNA Tumor Virus Gene Expression
T2  - VI Symposium on RNA Biology
AN  - 39754833; 4032402
JF  - VI Symposium on RNA Biology
AU  - Zheng, Zhi-Ming
Y1  - 2005/10/21/
PY  - 2005
DA  - 2005 Oct 21
KW  - Nucleic acids
KW  - Alternative splicing
KW  - Exons
KW  - Gene expression
KW  - RNA
KW  - DNA tumor viruses
KW  - U 7000:Multidisciplinary
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39754833?accountid=14244
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L2  - http://www.med.unc.edu/pmbb/Schedule_Abstracts.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Phase I study of O6-benzylguanine and temozolomide administered daily for 5 days to pediatric patients with solid tumors.
AN  - 68700934; 16234526
AB  - This pediatric phase I trial of O6-benzylguanine (O6BG) and temozolomide (TMZ) on a daily schedule for 5 days, every 28 days was performed to determine the maximum-tolerated dose of TMZ when given with a biologically active dose of O6BG and to define the toxicity profile of the combination in children with solid tumors.
          Patients < or = 21 years old with refractory solid tumors were eligible. O6BG was administered intravenously over 60 minutes daily for 5 days. TMZ was administered orally 30 minutes after completion of each O6BG infusion. Starting doses of O6BG and TMZ were 60 mg/m2/d and 28 mg/m2/d, respectively. O6BG was escalated to 90 and 120 mg/m2/d; TMZ was subsequently escalated to 40, 55, 75, and 100 mg/m2/d. Cycles were repeated every 28 days.
          Forty-one patients were enrolled; 32 patients were assessable for toxicity. The combination of O6BG and TMZ was tolerable at TMZ doses less than half of the conventional dose of 200 mg/m2/d. Myelosuppression occurred sporadically at all dose levels and was the dose-limiting toxicity (DLT) at 100 mg/m2/d of TMZ combined with 120 mg/m2/d O6BG. Nonhematologic toxicities were generally mild. Evidence of antitumor activity was observed at 120 mg/m2/d O6BG combined with TMZ doses of 55 mg/m2/d and above. The recommended doses of O6BG administered with TMZ on a 5-day schedule in children are 120 mg/m2/d of O6BG and 75 mg/m2/d of TMZ. Evidence of activity was observed at these doses. Myelosuppression was the DLT.
JF  - Journal of clinical oncology : official journal of the American Society of Clinical Oncology
AU  - Warren, Katherine E
AU  - Aikin, Alberta A
AU  - Libucha, Madeleine
AU  - Widemann, Brigitte C
AU  - Fox, Elizabeth
AU  - Packer, Roger J
AU  - Balis, Frank M
AD  - National Cancer Institute Neuro-Oncology Branch, Building 82, Room 219, 9030 Old Georgetown Rd, Bethesda, MD 20892-8200, USA. warrenk@mail.nih.gov
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
SP  - 7646
EP  - 7653
VL  - 23
IS  - 30
SN  - 0732-183X, 0732-183X
KW  - O(6)-benzylguanine
KW  - 01KC87F8FE
KW  - Guanine
KW  - 5Z93L87A1R
KW  - Dacarbazine
KW  - 7GR28W0FJI
KW  - temozolomide
KW  - YF1K15M17Y
KW  - Index Medicus
KW  - Drug Administration Schedule
KW  - Injections, Intravenous
KW  - Dose-Response Relationship, Drug
KW  - Humans
KW  - Prognosis
KW  - Child
KW  - Guanine -- administration & dosage
KW  - Child, Preschool
KW  - Dacarbazine -- analogs & derivatives
KW  - Adult
KW  - Dacarbazine -- administration & dosage
KW  - Guanine -- analogs & derivatives
KW  - Maximum Tolerated Dose
KW  - Adolescent
KW  - Male
KW  - Female
KW  - Neoplasms -- drug therapy
KW  - Antineoplastic Combined Chemotherapy Protocols -- adverse effects
KW  - Antineoplastic Combined Chemotherapy Protocols -- therapeutic use
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68700934?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+clinical+oncology+%3A+official+journal+of+the+American+Society+of+Clinical+Oncology&rft.atitle=Phase+I+study+of+O6-benzylguanine+and+temozolomide+administered+daily+for+5+days+to+pediatric+patients+with+solid+tumors.&rft.au=Warren%2C+Katherine+E%3BAikin%2C+Alberta+A%3BLibucha%2C+Madeleine%3BWidemann%2C+Brigitte+C%3BFox%2C+Elizabeth%3BPacker%2C+Roger+J%3BBalis%2C+Frank+M&rft.aulast=Warren&rft.aufirst=Katherine&rft.date=2005-10-20&rft.volume=23&rft.issue=30&rft.spage=7646&rft.isbn=&rft.btitle=&rft.title=Journal+of+clinical+oncology+%3A+official+journal+of+the+American+Society+of+Clinical+Oncology&rft.issn=0732183X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-21
N1  - Date created - 2005-10-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Pegylated arginine deiminase treatment of patients with metastatic melanoma: results from phase I and II studies.
AN  - 68699758; 16234528
AB  - Individuals with metastatic melanoma have a poor prognosis. Many human melanomas are auxotrophic for arginine, and arginine is not an essential amino acid in humans. We hypothesized that this auxotrophy may be therapeutically exploited. A novel amino acid-degrading enzyme (arginine deiminase) conjugated to polyethylene glycol (ADI-SS PEG 20,000 mw) was used to lower plasma arginine in individuals with metastatic melanoma.
          Two cohort dose-escalation studies were performed. A phase I study in the United States enrolled 15 patients, and a phase I to II study in Italy enrolled 24 patients. The Italian patients also received two subsequent cycles of treatment, each consisting of four once-weekly injections of 160 U/m2. The goals of these studies were to determine pharmacokinetics (PK), pharmacodynamics (PD), safety, and the antitumor activity of ADI-SS PEG 20,000 mw. PK and PD studies indicated that a dose of 160 U/m2 lowered plasma arginine from a resting level of approximately 130 micromol/L to less than 2 micromol/L for at least 7 days; nitric oxide levels also were lowered. There were no grade 3 or 4 toxicities directly attributable to the drug. Six of 24 phase I to II patients responded to treatment (five partial responses and one complete response; 25% response rate) and also had prolonged survival. CONCLUSION Elimination of all detectable plasma arginine in patients with metastatic melanoma was well tolerated and may be effective in the treatment of this cancer. Further testing of ADI-SS PEG 20,000 mw in a larger population of individuals with metastatic melanoma is warranted.
JF  - Journal of clinical oncology : official journal of the American Society of Clinical Oncology
AU  - Ascierto, Paolo A
AU  - Scala, Stefania
AU  - Castello, Giuseppe
AU  - Daponte, Antonio
AU  - Simeone, Ester
AU  - Ottaiano, Alessandro
AU  - Beneduce, Gerardo
AU  - De Rosa, Vincenzo
AU  - Izzo, Francesco
AU  - Melucci, Maria Teresa
AU  - Ensor, C Mark
AU  - Prestayko, Archie W
AU  - Holtsberg, Frederick W
AU  - Bomalaski, John S
AU  - Clark, Mike A
AU  - Savaraj, Niramol
AU  - Feun, Lynn G
AU  - Logan, Theodore F
AD  - Pascale National Cancer Institute, Naples, Italy.
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
SP  - 7660
EP  - 7668
VL  - 23
IS  - 30
SN  - 0732-183X, 0732-183X
KW  - Polyethylene Glycols
KW  - 30IQX730WE
KW  - Nitric Oxide
KW  - 31C4KY9ESH
KW  - Arginine
KW  - 94ZLA3W45F
KW  - Hydrolases
KW  - EC 3.-
KW  - arginine deiminase
KW  - EC 3.5.3.6
KW  - Index Medicus
KW  - United States
KW  - Survival Rate
KW  - Aged, 80 and over
KW  - Humans
KW  - Adult
KW  - Treatment Outcome
KW  - Nitric Oxide -- metabolism
KW  - Aged
KW  - Middle Aged
KW  - Arginine -- blood
KW  - Maximum Tolerated Dose
KW  - Male
KW  - Italy
KW  - Female
KW  - Skin Neoplasms -- drug therapy
KW  - Skin Neoplasms -- enzymology
KW  - Hydrolases -- pharmacology
KW  - Melanoma -- genetics
KW  - Melanoma -- enzymology
KW  - Polyethylene Glycols -- pharmacokinetics
KW  - Melanoma -- drug therapy
KW  - Hydrolases -- pharmacokinetics
KW  - Hydrolases -- administration & dosage
KW  - Polyethylene Glycols -- pharmacology
KW  - Polyethylene Glycols -- administration & dosage
KW  - Skin Neoplasms -- secondary
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+clinical+oncology+%3A+official+journal+of+the+American+Society+of+Clinical+Oncology&rft.atitle=Pegylated+arginine+deiminase+treatment+of+patients+with+metastatic+melanoma%3A+results+from+phase+I+and+II+studies.&rft.au=Ascierto%2C+Paolo+A%3BScala%2C+Stefania%3BCastello%2C+Giuseppe%3BDaponte%2C+Antonio%3BSimeone%2C+Ester%3BOttaiano%2C+Alessandro%3BBeneduce%2C+Gerardo%3BDe+Rosa%2C+Vincenzo%3BIzzo%2C+Francesco%3BMelucci%2C+Maria+Teresa%3BEnsor%2C+C+Mark%3BPrestayko%2C+Archie+W%3BHoltsberg%2C+Frederick+W%3BBomalaski%2C+John+S%3BClark%2C+Mike+A%3BSavaraj%2C+Niramol%3BFeun%2C+Lynn+G%3BLogan%2C+Theodore+F&rft.aulast=Ascierto&rft.aufirst=Paolo&rft.date=2005-10-20&rft.volume=23&rft.issue=30&rft.spage=7660&rft.isbn=&rft.btitle=&rft.title=Journal+of+clinical+oncology+%3A+official+journal+of+the+American+Society+of+Clinical+Oncology&rft.issn=0732183X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-21
N1  - Date created - 2005-10-19
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Erratum In:
J Clin Oncol. 2006 Aug 20;24(24):4047
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Interferon Regulation of IL-15 and IL-15 Receptor Alpha Expression: Implications for Immunotherapy
T2  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AN  - 39905190; 4076223
JF  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AU  - Waldmann, Thomas A
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
KW  - Immunotherapy
KW  - Interleukin 15 receptors
KW  - Interferon
KW  - Interleukin 15
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39905190?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.atitle=Interferon+Regulation+of+IL-15+and+IL-15+Receptor+Alpha+Expression%3A+Implications+for+Immunotherapy&rft.au=Waldmann%2C+Thomas+A&rft.aulast=Waldmann&rft.aufirst=Thomas&rft.date=2005-10-20&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.sibcb.ac.cn/Final%20Announcement.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - GATA3 and the Induction and Maintenance of Th2 Function
T2  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AN  - 39905076; 4076197
JF  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AU  - Paul, William E
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
KW  - Lymphocytes T
KW  - GATA-3 protein
KW  - Helper cells
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39905076?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.atitle=GATA3+and+the+Induction+and+Maintenance+of+Th2+Function&rft.au=Paul%2C+William+E&rft.aulast=Paul&rft.aufirst=William&rft.date=2005-10-20&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.sibcb.ac.cn/Final%20Announcement.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Glucocorticoid Receptor: One Gene, Many Proteins, Extensive Post Translational Modifications: Mechanisms Tissue Specific Anti-Inflammatory Actions
T2  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AN  - 39830828; 4076208
JF  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AU  - Cidlowski, John A
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
KW  - Translation
KW  - Glucocorticoid receptors
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39830828?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.atitle=The+Glucocorticoid+Receptor%3A+One+Gene%2C+Many+Proteins%2C+Extensive+Post+Translational+Modifications%3A+Mechanisms+Tissue+Specific+Anti-Inflammatory+Actions&rft.au=Cidlowski%2C+John+A&rft.aulast=Cidlowski&rft.aufirst=John&rft.date=2005-10-20&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.sibcb.ac.cn/Final%20Announcement.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Cytokines as Critical Co-Stimulatory Molecules in Modulating the Immune Response of Natural Killer Cells
T2  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AN  - 39813826; 4076198
JF  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AU  - Young, Howard A
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
KW  - Immune response
KW  - Cytokines
KW  - Natural killer cells
KW  - Immunity
KW  - Defense mechanisms
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39813826?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.atitle=Cytokines+as+Critical+Co-Stimulatory+Molecules+in+Modulating+the+Immune+Response+of+Natural+Killer+Cells&rft.au=Young%2C+Howard+A&rft.aulast=Young&rft.aufirst=Howard&rft.date=2005-10-20&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.sibcb.ac.cn/Final%20Announcement.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Human Interferon alphas: Structure and Function
T2  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AN  - 39805881; 4076213
JF  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AU  - Zoon, Kathryn C
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
KW  - Interferon
KW  - Structure-function relationships
KW  - U 2000:Biological Sciences
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L2  - http://www.sibcb.ac.cn/Final%20Announcement.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Decreased Expression of Interferon-g in CD4@@u+@T Cells Due to Hypermethylation of Following HAART Treatment in Normal and HIV Infected Donors
T2  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AN  - 39799584; 4076244
JF  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AU  - Ruscetti, Frank
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
KW  - ^g-Interferon
KW  - Highly active antiretroviral therapy
KW  - Disease control
KW  - Human immunodeficiency virus
KW  - U 2000:Biological Sciences
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L2  - http://www.sibcb.ac.cn/Final%20Announcement.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Dendritic Cells and Type I Interferon: Virus Infection and More
T2  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AN  - 39785931; 4076199
JF  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AU  - Trinchieri, Giorgio
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
KW  - Infection
KW  - Interferon
KW  - Dendritic cells
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.atitle=Dendritic+Cells+and+Type+I+Interferon%3A+Virus+Infection+and+More&rft.au=Trinchieri%2C+Giorgio&rft.aulast=Trinchieri&rft.aufirst=Giorgio&rft.date=2005-10-20&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.sibcb.ac.cn/Final%20Announcement.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Role of IRF-8 in the Development of Dendritic Cell Subtypes and Type I IFN Transcription
T2  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AN  - 39777390; 4076188
JF  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AU  - Ozato, Keiko
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
KW  - Transcription
KW  - Dendritic cells
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.atitle=The+Role+of+IRF-8+in+the+Development+of+Dendritic+Cell+Subtypes+and+Type+I+IFN+Transcription&rft.au=Ozato%2C+Keiko&rft.aulast=Ozato&rft.aufirst=Keiko&rft.date=2005-10-20&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.sibcb.ac.cn/Final%20Announcement.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Alternative p38 Activation Pathway in T Cells: Regulation by the Autoimmune Suppressor Gadd45 a
T2  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AN  - 39758720; 4076201
JF  - 2005 Annual Meeting of the International Society for Interferon and Cytokine Research
AU  - Ashwell, Jonathan D
Y1  - 2005/10/20/
PY  - 2005
DA  - 2005 Oct 20
KW  - GADD45 protein
KW  - Lymphocytes T
KW  - Cell activation
KW  - Suppressors
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.atitle=Alternative+p38+Activation+Pathway+in+T+Cells%3A+Regulation+by+the+Autoimmune+Suppressor+Gadd45+a&rft.au=Ashwell%2C+Jonathan+D&rft.aulast=Ashwell&rft.aufirst=Jonathan&rft.date=2005-10-20&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=2005+Annual+Meeting+of+the+International+Society+for+Interferon+and+Cytokine+Research&rft.issn=&rft_id=info:doi/
L2  - http://www.sibcb.ac.cn/Final%20Announcement.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - The eIF1A C-terminal domain promotes initiation complex assembly, scanning and AUG selection in vivo.
AN  - 68704218; 16193068
AB  - Translation initiation factor 1A stimulates 40S-binding of the eukaryotic initiation factor 2 (eIF2)/GTP/Met-tRNA(iMet) ternary complex (TC) and promotes scanning in vitro. eIF1A contains an OB-fold present in bacterial IF1 plus N- and C-terminal extensions. Truncating the C-terminus (deltaC) or mutating OB-fold residues (66-70) of eIF1A reduced general translation in vivo but increased GCN4 translation (Gcd- phenotype) in a manner suppressed by overexpressing TC. Consistent with this, both mutations diminished 40S-bound TC, eIF5 and eIF3 in vivo, and deltaC impaired TC recruitment in vitro. The assembly defects of the OB-fold mutation can be attributed to reduced 40S-binding of eIF1A, whereas deltaC impairs eIF1A function on the ribosome. A substitution in the C-terminal helix (98-101) also reduced 43S assembly in vivo. Rather than producing a Gcd- phenotype, however, 98-101 impairs GCN4 derepression in a manner consistent with defective scanning by reinitiating ribosomes. Indeed, 98-101 allows formation of aberrant 48S complexes in vitro and increases utilization of non-AUG codons in vivo. Thus, the OB-fold is crucial for ribosome-binding and the C-terminal domain of eIF1A has eukaryotic-specific functions in TC recruitment and scanning.
JF  - The EMBO journal
AU  - Fekete, Christie A
AU  - Applefield, Drew J
AU  - Blakely, Stephen A
AU  - Shirokikh, Nikolay
AU  - Pestova, Tatyana
AU  - Lorsch, Jon R
AU  - Hinnebusch, Alan G
AD  - Laboratory of Gene Regulation and Development, National Institute of Child Health and Human Development, NIH, Bethesda, MD 20892, USA.
Y1  - 2005/10/19/
PY  - 2005
DA  - 2005 Oct 19
SP  - 3588
EP  - 3601
VL  - 24
IS  - 20
SN  - 0261-4189, 0261-4189
KW  - Codon, Initiator
KW  - 0
KW  - Eukaryotic Initiation Factor-1
KW  - Saccharomyces cerevisiae Proteins
KW  - eukaryotic peptide initiation factor-1A
KW  - Index Medicus
KW  - Protein Structure, Tertiary -- genetics
KW  - Mutation
KW  - Sequence Deletion
KW  - Mutagenesis
KW  - Codon, Initiator -- metabolism
KW  - Saccharomyces cerevisiae Proteins -- metabolism
KW  - Saccharomyces cerevisiae Proteins -- genetics
KW  - Peptide Chain Initiation, Translational
KW  - Eukaryotic Initiation Factor-1 -- metabolism
KW  - Eukaryotic Initiation Factor-1 -- chemistry
KW  - Saccharomyces cerevisiae Proteins -- chemistry
KW  - Eukaryotic Initiation Factor-1 -- genetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-20
N1  - Date created - 2005-10-19
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
J Mol Biol. 1995 Apr 28;248(2):207-10 [7739034]
Mol Cell Biol. 1991 May;11(5):2723-35 [2017175]
EMBO J. 1997 Mar 17;16(6):1436-43 [9135158]
Yeast. 1997 Jun 15;13(7):647-53 [9200814]
Genes Dev. 1997 Sep 15;11(18):2396-413 [9308967]
Electrophoresis. 1997 Dec;18(15):2714-23 [9504803]
Mol Cell Biol. 1998 Aug;18(8):4935-46 [9671501]
Nature. 1998 Aug 27;394(6696):854-9 [9732867]
EMBO J. 1999 Mar 15;18(6):1673-88 [10075937]
J Biol Chem. 2004 Nov 26;279(48):49644-55 [15377664]
Mol Cell. 2005 Jan 21;17(2):265-75 [15664195]
RNA. 2005 Apr;11(4):470-86 [15703437]
Mol Cell Biol. 2005 Jul;25(13):5480-91 [15964804]
Mol Cell. 2000 Jan;5(1):109-19 [10678173]
Mol Cell Biol. 2000 Oct;20(19):7183-91 [10982835]
Genes Dev. 2000 Oct 1;14(19):2534-46 [11018020]
Cell. 1992 Feb 7;68(3):585-96 [1739968]
Mol Cell Biol. 1994 Apr;14(4):2616-28 [8139562]
Nucleic Acids Res. 1994 Nov 11;22(22):4673-80 [7984417]
Science. 2001 Jan 19;291(5503):498-501 [11228145]
EMBO J. 2001 May 1;20(9):2326-37 [11331597]
RNA. 2002 Mar;8(3):382-97 [12008673]
EMBO J. 2002 Nov 1;21(21):5886-98 [12411506]
Genes Dev. 2002 Nov 15;16(22):2906-22 [12435632]
EMBO J. 2003 Jan 15;22(2):193-204 [12514125]
J Biol Chem. 2003 Feb 21;278(8):6580-7 [12493757]
Genes Dev. 2003 Mar 15;17(6):786-99 [12651896]
J Mol Biol. 2003 Jul 25;330(5):917-24 [12860115]
Mol Cell Biol. 2003 Aug;23(15):5431-45 [12861028]
EMBO J. 2004 Mar 10;23(5):1166-77 [14976554]
Mol Cell Biol. 2004 Nov;24(21):9437-55 [15485912]
Mol Cell Biol. 1985 Sep;5(9):2349-60 [3915540]
Mol Cell Biol. 1988 Jul;8(7):2955-63 [3043200]
Yeast. 1985 Dec;1(2):83-138 [3916863]
Gene. 1988 Dec 30;74(2):527-34 [3073106]
Proc Natl Acad Sci U S A. 1990 Nov;87(21):8301-5 [2236042]
Mol Cell Biol. 1991 Jan;11(1):486-96 [1986242]
Mol Cell Biol. 1995 Nov;15(11):6351-63 [7565788]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Diazeniumdiolate ions as leaving groups in anomeric displacement reactions: a protection-deprotection strategy for ionic diazeniumdiolates.
AN  - 68684924; 16218605
AB  - Diazeniumdiolate ions [R2N-N(O)=N-O-] are of growing interest pharmacologically for their ability to generate up to two molar equivalents of bioactive nitric oxide (NO) spontaneously on protonating the amino nitrogen. Accordingly, their stability increases as the pH is raised. Here we show that the corresponding beta-glucosides [R2N-N(O)=N-O-Glc] decreased in stability with pH; when R2N was diethylamino, the rate equation was kobs = ko + kOH- [OH-], where ko = 7.8 x 10-7 s-1 and kOH- = 5.3 x 10-3 M-1 s-1. The primary products were 1,6-anhydroglucose and the regenerated R2N-N(O)=N-O- ion. The results were qualitatively similar to those of beta-glucosyl fluoride and p-nitrophenoxide, whose hydrolyses have been rationalized as proceeding via a glycal oxide intermediate. This chemistry offers a convenient strategy for protecting heat- and acid-sensitive diazeniumdiolate ions during manipulations that would otherwise destroy them. As an example, a poly(urethane) film that generated NO in physiological buffer at a surface flux comparable to that of the mammalian vascular endothelium was prepared by glucosylating the ionic diazeniumdiolate group attached to the diol monomer before reacting it with the bis-isocyanate, then removing the saccharide with base when the protecting group was no longer needed.
JF  - Journal of the American Chemical Society
AU  - Showalter, Brett M
AU  - Reynolds, Melissa M
AU  - Valdez, Carlos A
AU  - Saavedra, Joseph E
AU  - Davies, Keith M
AU  - Klose, John R
AU  - Chmurny, Gwendolyn N
AU  - Citro, Michael L
AU  - Barchi, Joseph J
AU  - Merz, Scott I
AU  - Meyerhoff, Mark E
AU  - Keefer, Larry K
AD  - Chemistry Section, Laboratory of Comparative Carcinogenesis, National Cancer Institute at Frederick, Frederick, MD 21702, USA.
Y1  - 2005/10/19/
PY  - 2005
DA  - 2005 Oct 19
SP  - 14188
EP  - 14189
VL  - 127
IS  - 41
SN  - 0002-7863, 0002-7863
KW  - Azo Compounds
KW  - 0
KW  - diazeniumdiolate
KW  - Index Medicus
KW  - Molecular Structure
KW  - Hydrogen-Ion Concentration
KW  - Time Factors
KW  - Hydrolysis
KW  - Azo Compounds -- chemical synthesis
KW  - Azo Compounds -- chemistry
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-24
N1  - Date created - 2005-10-12
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Introduction to Nci'S Integrative Cancer Biology Program
T2  - Sixth International Conference on Systems Biology (ICSB 2005)
AN  - 40053581; 4017306
JF  - Sixth International Conference on Systems Biology (ICSB 2005)
AU  - Gallahan, Dan
Y1  - 2005/10/19/
PY  - 2005
DA  - 2005 Oct 19
KW  - Cancer
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=Sixth+International+Conference+on+Systems+Biology+%28ICSB+2005%29&rft.atitle=Introduction+to+Nci%27S+Integrative+Cancer+Biology+Program&rft.au=Gallahan%2C+Dan&rft.aulast=Gallahan&rft.aufirst=Dan&rft.date=2005-10-19&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=Sixth+International+Conference+on+Systems+Biology+%28ICSB+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://csbi.mit.edu/icsb-2005/program/program.htm
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Assessing the Health Effects of Dietary Supplements and Food Ingredients
T2  - 6th International Conference and Exhibition on Nutraceuticals and Functional Foods (WORLDNUTRA 2005)
AN  - 40105917; 4001175
JF  - 6th International Conference and Exhibition on Nutraceuticals and Functional Foods (WORLDNUTRA 2005)
AU  - Coates, Paul M
Y1  - 2005/10/16/
PY  - 2005
DA  - 2005 Oct 16
KW  - Food
KW  - Dietary supplements
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40105917?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=6th+International+Conference+and+Exhibition+on+Nutraceuticals+and+Functional+Foods+%28WORLDNUTRA+2005%29&rft.atitle=Assessing+the+Health+Effects+of+Dietary+Supplements+and+Food+Ingredients&rft.au=Coates%2C+Paul+M&rft.aulast=Coates&rft.aufirst=Paul&rft.date=2005-10-16&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=6th+International+Conference+and+Exhibition+on+Nutraceuticals+and+Functional+Foods+%28WORLDNUTRA+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.worldnutra.com/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Challenges in Identyfying and Characterizing Bioactive Components in Foods and Supplements
T2  - 6th International Conference and Exhibition on Nutraceuticals and Functional Foods (WORLDNUTRA 2005)
AN  - 40056709; 4001231
JF  - 6th International Conference and Exhibition on Nutraceuticals and Functional Foods (WORLDNUTRA 2005)
AU  - Betz, Joseph M
Y1  - 2005/10/16/
PY  - 2005
DA  - 2005 Oct 16
KW  - Food
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40056709?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=6th+International+Conference+and+Exhibition+on+Nutraceuticals+and+Functional+Foods+%28WORLDNUTRA+2005%29&rft.atitle=Challenges+in+Identyfying+and+Characterizing+Bioactive+Components+in+Foods+and+Supplements&rft.au=Betz%2C+Joseph+M&rft.aulast=Betz&rft.aufirst=Joseph&rft.date=2005-10-16&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=6th+International+Conference+and+Exhibition+on+Nutraceuticals+and+Functional+Foods+%28WORLDNUTRA+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.worldnutra.com/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - The Latest on Dietary Supplement Research and Development
T2  - 6th International Conference and Exhibition on Nutraceuticals and Functional Foods (WORLDNUTRA 2005)
AN  - 40002627; 4001146
JF  - 6th International Conference and Exhibition on Nutraceuticals and Functional Foods (WORLDNUTRA 2005)
AU  - Coates, Paul M
Y1  - 2005/10/16/
PY  - 2005
DA  - 2005 Oct 16
KW  - Research
KW  - Dietary supplements
KW  - Development
KW  - U 2000:Biological Sciences
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L2  - http://www.worldnutra.com/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Kinetics of tempol for prevention of xerostomia following head and neck irradiation in a mouse model.
AN  - 68709412; 16243832
AB  - Radiotherapy is commonly used to treat the majority of patients with head and neck cancers. Salivary glands in the radiation field are dramatically affected by this procedure. The purpose of this study was to examine pharmacokinetic characteristics of the stable nitroxide 4-hydroxy-2,2,6,6-tetramethylpiperidine-N-oxyl (tempol) with respect to radioprotection of the salivary glands.
          To evaluate the effect of different doses and times of administration, the heads of C3H mice were exposed to a single irradiation dose of 15 Gy, with i.p. tempol injection. To analyze other routes of administration, we injected 275 mg/kg tempol by an i.m., i.v., or s.c. route, 10 minutes before irradiation. We also tested whether oral administration of tempol in a topical form (either in a mouthwash or gel) provided any salivary gland protection. Tempol treatment (137.5 or 275 mg/kg, i.p., 10 minutes before irradiation) significantly reduced irradiation-induced salivary hypofunction (approximately 50-60%). I.v. or s.c. administration of tempol also showed significant radioprotection, whereas i.m. administration proved to be ineffective. Topical use of tempol, either as a mouthwash or gel, also was radioprotective.
          Our results strongly suggest that tempol is a promising candidate for clinical application to protect salivary glands in patients undergoing radiotherapy for head and neck cancers.
JF  - Clinical cancer research : an official journal of the American Association for Cancer Research
AU  - Cotrim, Ana P
AU  - Sowers, Anastasia L
AU  - Lodde, Beatrijs M
AU  - Vitolo, Joseph M
AU  - Kingman, Albert
AU  - Russo, Angelo
AU  - Mitchell, James B
AU  - Baum, Bruce J
AD  - Gene Therapy and Therapeutics Branch and Biostatistics Core, Division of Clinical Research and Health Promotion, National Institute of Dental and Craniofacial Research, NIH, Bethesda, Maryland 20892, USA. acotrim@nidcr.nih.gov
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 7564
EP  - 7568
VL  - 11
IS  - 20
SN  - 1078-0432, 1078-0432
KW  - Cyclic N-Oxides
KW  - 0
KW  - Radiation-Protective Agents
KW  - Spin Labels
KW  - tempol
KW  - U78ZX2F65X
KW  - Index Medicus
KW  - Models, Animal
KW  - Injections, Intraperitoneal
KW  - Salivary Glands -- radiation effects
KW  - Animals
KW  - Salivary Glands -- drug effects
KW  - Salivation -- radiation effects
KW  - Salivation -- drug effects
KW  - Salivary Glands -- pathology
KW  - Mice, Inbred C3H
KW  - Injections, Subcutaneous
KW  - Mice
KW  - Female
KW  - Drug Administration Routes
KW  - Xerostomia -- etiology
KW  - Xerostomia -- prevention & control
KW  - Radiation-Protective Agents -- administration & dosage
KW  - Radiation-Protective Agents -- pharmacokinetics
KW  - Cranial Irradiation -- adverse effects
KW  - Cyclic N-Oxides -- administration & dosage
KW  - Xerostomia -- metabolism
KW  - Cyclic N-Oxides -- pharmacokinetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-13
N1  - Date created - 2005-10-24
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Polymorphisms in cytokine and cellular adhesion molecule genes and susceptibility to hematotoxicity among workers exposed to benzene.
AN  - 68699300; 16230423
AB  - Benzene is a recognized hematotoxin and leukemogen but its mechanism of action and the role of genetic susceptibility are still unclear. Cytokines, chemokines, and cellular adhesion molecules are soluble proteins that play an important regulatory role in hematopoiesis. We therefore hypothesized that variation in these genes could influence benzene-induced hematotoxicity. We analyzed common, well-studied single-nucleotide polymorphisms (SNPs) in 20 candidate genes drawn from these pathways in a study of 250 workers exposed to benzene and 140 unexposed controls in China. After accounting for multiple comparisons, SNPs in five genes were associated with a statistically significant decrease in total WBC counts among exposed workers [IL-1A (-889C>T), IL-4 (-1098T>G), IL-10 (-819T>C), IL-12A (8685G>A), and VCAM1 (-1591T>C)], and one SNP [CSF3 (Ex4-165C>T)] was associated with an increase in WBC counts. The adhesion molecule VCAM1 variant was particularly noteworthy as it was associated with a decrease in B cells, natural killer cells, CD4+ T cells, and monocytes. Further, VCAM1 (-1591T>C) and CSF3 (Ex4-165C>T) were associated, respectively, with decreased (P = 0.041) and increased (P = 0.076) CFU-GEMM progenitor cell colony formation in 29 benzene-exposed workers. This is the first report to provide evidence that SNPs in genes that regulate hematopoiesis influence benzene-induced hematotoxicity.
JF  - Cancer research
AU  - Lan, Qing
AU  - Zhang, Luoping
AU  - Shen, Min
AU  - Smith, Martyn T
AU  - Li, Guilan
AU  - Vermeulen, Roel
AU  - Rappaport, Stephen M
AU  - Forrest, Matthew S
AU  - Hayes, Richard B
AU  - Linet, Martha
AU  - Dosemeci, Mustafa
AU  - Alter, Blanche P
AU  - Weinberg, Rona S
AU  - Yin, Songnian
AU  - Yeager, Meredith
AU  - Welch, Robert
AU  - Waidyanatha, Suramya
AU  - Kim, Sungkyoon
AU  - Chanock, Stephen
AU  - Rothman, Nathaniel
AD  - Division of Cancer Epidemiology, National Cancer Institute, NIH, Department of Health and Human Services, Bethesda, MD 20892-7240, USA. qingl@mail.nih.gov
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 9574
EP  - 9581
VL  - 65
IS  - 20
SN  - 0008-5472, 0008-5472
KW  - Cell Adhesion Molecules
KW  - 0
KW  - Cytokines
KW  - Benzene
KW  - J64922108F
KW  - Index Medicus
KW  - Polymorphism, Single Nucleotide
KW  - Hematopoiesis -- drug effects
KW  - Humans
KW  - Adult
KW  - Male
KW  - Hematopoiesis -- genetics
KW  - Female
KW  - Occupational Exposure
KW  - Hematologic Diseases -- genetics
KW  - Hematologic Diseases -- chemically induced
KW  - Occupational Diseases -- genetics
KW  - Cytokines -- genetics
KW  - Cell Adhesion Molecules -- genetics
KW  - Occupational Diseases -- chemically induced
KW  - Benzene -- poisoning
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-19
N1  - Date created - 2005-10-18
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Less efficient g2-m checkpoint is associated with an increased risk of lung cancer in African Americans.
AN  - 68699250; 16230422
AB  - Cell cycle checkpoints play critical roles in the maintenance of genomic integrity. The inactivation of checkpoint genes by genetic and epigenetic mechanisms is frequent in all cancer types, as a less-efficient cell cycle control can lead to genetic instability and tumorigenesis. In an on-going case-control study consisting of 216 patients with non-small cell lung cancer, 226 population-based controls, and 114 hospital-based controls, we investigated the relationship of gamma-radiation-induced G2-M arrest and lung cancer risk. Peripheral blood lymphocytes were cultured for 90 hours, exposed to 1.0 Gy gamma-radiation, and harvested at 3 hours after gamma-radiation treatment. gamma-Radiation-induced G2-M arrest was measured as the percentage of mitotic cells in untreated cultures minus the percentage of mitotic cells in gamma-radiation-treated cultures from the same subject. The mean percentage of gamma-radiation-induced G2-M arrest was significantly lower in cases than in population controls (1.18 versus 1.44, P < 0.01) and hospital controls (1.18 versus 1.40, P = 0.01). When dichotomized at the 50th percentile value in combined controls (population and hospital controls), a lower level of gamma-radiation-induced G2-M arrest was associated with an increased risk of lung cancer among African Americans after adjusting for baseline mitotic index, age, gender, and pack-years of smoking [adjusted odd ratio (OR), 2.25; 95% confidence interval (95% CI), 0.97-5.20]. A significant trend of an increased risk of lung cancer with a decreased level of G2-M arrest was observed (P(trend) = 0.02) among African Americans, with a lowest-versus-highest quartile adjusted OR of 3.74 (95% CI, 0.98-14.3). This trend was most apparent among African American females (P(trend) < 0.01), with a lowest-versus-highest quartile adjusted OR of 11.75 (95% CI, 1.47-94.04). The results suggest that a less-efficient DNA damage-induced G2-M checkpoint is associated with an increased risk of lung cancer among African Americans. Interestingly, we observed a stronger association of DNA damage-induced G2-M arrest and lung cancer among African Americans when compared with Caucasians. If replicated, these results may provide clues to the exceedingly high lung cancer incidence experienced by African Americans.
JF  - Cancer research
AU  - Zheng, Yun-Ling
AU  - Loffredo, Christopher A
AU  - Alberg, Anthony J
AU  - Yu, Zhipeng
AU  - Jones, Raymond T
AU  - Perlmutter, Donna
AU  - Enewold, Lindsey
AU  - Krasna, Mark J
AU  - Yung, Rex
AU  - Shields, Peter G
AU  - Harris, Curtis C
AD  - Laboratory of Human Carcinogenesis, National Cancer Institute, Bethesda, MD 20892-4255, USA.
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 9566
EP  - 9573
VL  - 65
IS  - 20
SN  - 0008-5472, 0008-5472
KW  - Index Medicus
KW  - Gamma Rays
KW  - Risk Factors
KW  - Humans
KW  - Lymphocytes -- radiation effects
KW  - Case-Control Studies
KW  - Aged
KW  - African Americans
KW  - Middle Aged
KW  - Lymphocytes -- cytology
KW  - Dose-Response Relationship, Radiation
KW  - Male
KW  - Female
KW  - G2 Phase -- radiation effects
KW  - Carcinoma, Non-Small-Cell Lung -- blood
KW  - G2 Phase -- genetics
KW  - Lung Neoplasms -- blood
KW  - Carcinoma, Non-Small-Cell Lung -- genetics
KW  - Lung Neoplasms -- genetics
KW  - African Continental Ancestry Group
KW  - Cell Division -- genetics
KW  - Lung Neoplasms -- pathology
KW  - Cell Division -- radiation effects
KW  - Carcinoma, Non-Small-Cell Lung -- pathology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-19
N1  - Date created - 2005-10-18
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Pathol Biol (Paris). 2000 Apr;48(3):174-81 [10858951]
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Cell Prolif. 2000 Oct;33(5):261-74 [11063129]
Pharmacogenetics. 2000 Dec;10(9):761-6 [11221602]
Lung Cancer. 2001 Feb-Mar;31(2-3):157-62 [11165394]
Nat Genet. 2001 Apr;27(4):383-91 [11279519]
Cancer Epidemiol Biomarkers Prev. 2001 Mar;10(3):217-22 [11303590]
Science. 1999 Dec 24;286(5449):2528-31 [10617473]
Mol Diagn. 1999 Dec;4(4):299-307 [10671640]
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J Clin Oncol. 2000 Jun;18(11):2309-15 [10829052]
Genes Chromosomes Cancer. 2002 Jan;33(1):17-21 [11746983]
Neoplasma. 2001;48(5):407-11 [11845987]
J Natl Cancer Inst. 2002 May 1;94(9):681-90 [11983757]
Semin Oncol. 2002 Jun;29(3):246-57 [12063677]
Oncogene. 2002 Jun 20;21(27):4191-9 [12082606]
Cancer Res. 2002 Aug 15;62(16):4588-91 [12183412]
Carcinogenesis. 2003 Feb;24(2):269-74 [12584177]
Hum Hered. 2003;55(4):171-8 [14566095]
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Mol Cancer. 2004 May 4;3:14 [15125777]
Mutat Res. 1985 Jan-Feb;148(1-2):71-82 [3969079]
Proc Natl Acad Sci U S A. 1985 Aug;82(16):5400-3 [3860870]
Int J Cancer. 1989 Mar 15;43(3):403-9 [2466800]
Science. 1989 Nov 3;246(4930):629-34 [2683079]
Int J Radiat Biol. 1989 Nov;56(5):677-84 [2573663]
J Natl Cancer Inst. 1990 Jun 20;82(12):1050-4 [2348470]
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J Natl Cancer Inst. 1991 Aug 21;83(16):1142-8 [1886147]
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Lancet. 1992 May 23;339(8804):1268-78 [1349675]
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Cell. 1992 Sep 18;70(6):923-35 [1356076]
Cancer Epidemiol Biomarkers Prev. 1993 Jan-Feb;2(1):53-7 [8093594]
Proc Natl Acad Sci U S A. 1993 May 1;90(9):3988-92 [8387205]
Int J Cancer. 1993 Jun 19;54(4):589-93 [8514450]
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J Natl Cancer Inst. 2000 Nov 1;92(21):1764-72 [11058619]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Role of aspartate 298 in mouse 5-HT3A receptor gating and modulation by extracellular Ca2+.
AN  - 68689155; 16096341
AB  - The TM2-TM3 extracellular loop is critical for activation of the Cys-loop family of ligand-gated ion channels. The contribution of aspartate 298 (D298), an amino acid that links the transmembrane domain 2 (TM2) to the TM2-TM3 loop, in mouse 5-hydroxytryptamine(3A) (5-HT(3A)) receptor function was probed with site-directed mutagenesis in the present study. This negatively charged residue was replaced with an alanine to neutralize the charge, with a glutamate to conserve the charge, or with an arginine to reverse the charge. Human embryonic kidney 293 (HEK 293) cells transfected with the wild-type and mutant receptors were studied by combining whole-cell patch-clamp recording with fast agonist application. The D-->A or D-->R mutations resulted in a receptor with reduced 5-HT potency, and accelerated kinetics of desensitization and deactivation. In addition, the efficacy of partial agonists was reduced by the D-->A mutation. The D-->E mutation produced a receptor with properties similar to those of the wild-type receptor. In addition, the potential role of this residue in modulation of the receptor by extracellular calcium ([Ca(2)(+)](o)) was investigated. Increasing [Ca(2)(+)](o) inhibited 5-HT-activated currents and altered receptor kinetics in a similar manner in the wild-type and D298E receptors, and this alteration was eliminated by the D-->A and D-->R mutations. Our data suggest that the charge at D298 participates in transitions between functional states of the 5-HT(3A) receptor, and provide evidence that the charge of the side-chain at residue D298 contributes to channel gating kinetics and is crucial for Ca(2)(+) modulation.
JF  - The Journal of physiology
AU  - Hu, Xiang-Qun
AU  - Lovinger, David M
AD  - Laboratory for Integrative Neuroscience, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Bethesda, MD 20852, USA.
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 381
EP  - 396
VL  - 568
SN  - 0022-3751, 0022-3751
KW  - Receptors, Serotonin, 5-HT3
KW  - 0
KW  - Serotonin 5-HT3 Receptor Agonists
KW  - Serotonin Receptor Agonists
KW  - Aspartic Acid
KW  - 30KYC7MIAI
KW  - Serotonin
KW  - 333DO1RDJY
KW  - 2-methyl-5-HT
KW  - 78263-90-8
KW  - Calcium
KW  - SY7Q814VUP
KW  - Dopamine
KW  - VTD58H1Z2X
KW  - Index Medicus
KW  - Serotonin Receptor Agonists -- pharmacology
KW  - Serotonin -- pharmacology
KW  - Animals
KW  - Dopamine -- pharmacology
KW  - Dose-Response Relationship, Drug
KW  - Humans
KW  - Serotonin -- analogs & derivatives
KW  - Amino Acid Sequence
KW  - Mice
KW  - Transfection
KW  - Molecular Sequence Data
KW  - Point Mutation
KW  - Membrane Potentials -- drug effects
KW  - Protein Structure, Tertiary
KW  - Cell Line
KW  - Aspartic Acid -- metabolism
KW  - Kidney -- metabolism
KW  - Receptors, Serotonin, 5-HT3 -- metabolism
KW  - Kidney -- drug effects
KW  - Calcium -- pharmacology
KW  - Receptors, Serotonin, 5-HT3 -- genetics
KW  - Receptors, Serotonin, 5-HT3 -- chemistry
KW  - Aspartic Acid -- chemistry
KW  - Ion Channel Gating -- drug effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-27
N1  - Date created - 2005-10-17
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
J Physiol. 1998 Jan 1;506 ( Pt 1):53-72 [9481672]
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Mol Pharmacol. 1998 Mar;53(3):511-23 [9495819]
J Physiol. 1998 Mar 15;507 ( Pt 3):653-65 [9508827]
Pflugers Arch. 1999 Dec;439(1-2):86-92 [10651004]
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Mol Pharmacol. 2001 Apr;59(4):844-51 [11259629]
J Neurosci. 2001 Apr 15;21(8):2589-99 [11306612]
J Neurosci. 2001 Jun 15;21(12):4143-53 [11404399]
Eur J Pharmacol. 2001 Oct 5;428(2):153-61 [11675031]
J Biol Chem. 2001 Nov 9;276(45):42035-42 [11557761]
J Neurosci. 2001 Dec 1;21(23):9083-91 [11717341]
Nat Rev Neurosci. 2002 Feb;3(2):102-14 [11836518]
Mol Membr Biol. 2002 Jan-Mar;19(1):11-26 [11989819]
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N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Selective cellular effects of overexpressed pleckstrin-homology domains that recognize PtdIns(3,4,5)P3 suggest their interaction with protein binding partners.
AN  - 68679933; 16219693
AB  - Several pleckstrin-homology (PH) domains with the ability to bind phosphatidylinositol (3,4,5)-trisphosphate [PtdIns(3,4,5)P3, PIP3] were expressed as green fluorescent protein (GFP) fusion proteins to determine their effects on various cellular responses known to be activated by PIP3. These proteins comprised the PH domains of Akt, ARNO, Btk or GRP1, and were found to show growth-factor-stimulated and wortmannin-sensitive translocation from the cytosol to the plasma membrane in several cell types, indicating their ability to recognize PIP3. Remarkably, although overexpressed Akt-PH-GFP and Btk-PH-GFP were quite potent in antagonizing the PIP3-mediated activation of the Akt protein kinase, such inhibition was not observed with the other PH domains. By contrast, expression of the PH domains of GRP1 and ARNO, but not of Akt or Btk, inhibited the attachment and spreading of freshly seeded cells to culture dishes. Activation of PLCgamma by epidermal growth factor (EGF) was attenuated by the PH domains of GRP1, ARNO and Akt, but was significantly enhanced by the Btk PH domain. By following the kinetics of expression of the various GFP-fused PH domains for several days, only the PH domain of Akt showed a lipid-binding-dependent self-elimination, consistent with its interference with the anti-apoptotic Akt signaling pathway. Mutations of selective residues that do not directly participate in PIP3 binding in the GRP1-PH and Akt-PH domain were able to reduce the dominant-negative effects of these constructs yet retain their lipid binding. These data suggest that interaction with and sequestration of PIP3 may not be the sole mechanism by which PH domains interfere with cellular responses and that their interaction with other membrane components, most probably with proteins, allows a more specific participation in the regulation of specific signaling pathways.
JF  - Journal of cell science
AU  - Várnai, Péter
AU  - Bondeva, Tzvetanka
AU  - Tamás, Péter
AU  - Tóth, Balázs
AU  - Buday, László
AU  - Hunyady, László
AU  - Balla, Tamas
AD  - Endocrinology and Reproduction Research Branch, National Institutes of Child Health and Human Development, National Institutes of Health, Bethesda, MD 20892, USA.
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 4879
EP  - 4888
VL  - 118
SN  - 0021-9533, 0021-9533
KW  - Androstadienes
KW  - 0
KW  - Blood Proteins
KW  - Phosphatidylinositol Phosphates
KW  - Phosphoproteins
KW  - Receptors, Cytoplasmic and Nuclear
KW  - phosphatidylinositol 3,4,5-triphosphate
KW  - phosphatidylinositol receptors
KW  - platelet protein P47
KW  - Epidermal Growth Factor
KW  - 62229-50-9
KW  - Proto-Oncogene Proteins c-akt
KW  - EC 2.7.11.1
KW  - Phospholipase C gamma
KW  - EC 3.1.4.3
KW  - wortmannin
KW  - XVA4O219QW
KW  - Index Medicus
KW  - Cell Movement
KW  - Animals
KW  - Fibroblasts -- drug effects
KW  - COS Cells
KW  - Humans
KW  - Androstadienes -- pharmacology
KW  - Gene Expression
KW  - Fibroblasts -- cytology
KW  - Mice
KW  - Proto-Oncogene Proteins c-akt -- chemistry
KW  - Protein Binding
KW  - NIH 3T3 Cells
KW  - Mutagenesis
KW  - Phospholipase C gamma -- metabolism
KW  - Transfection
KW  - Receptors, Cytoplasmic and Nuclear -- metabolism
KW  - Cercopithecus aethiops
KW  - Protein Structure, Tertiary
KW  - Proto-Oncogene Proteins c-akt -- antagonists & inhibitors
KW  - Epidermal Growth Factor -- metabolism
KW  - Cell Adhesion
KW  - Phosphatidylinositol Phosphates -- biosynthesis
KW  - Phosphoproteins -- chemistry
KW  - Phosphatidylinositol Phosphates -- metabolism
KW  - Blood Proteins -- chemistry
KW  - Blood Proteins -- metabolism
KW  - Phosphoproteins -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-24
N1  - Date created - 2005-10-12
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Mutations in dopachrome tautomerase (Dct) affect eumelanin/pheomelanin synthesis, but do not affect intracellular trafficking of the mutant protein.
AN  - 68669845; 15960609
AB  - Dopachrome tautomerase (Dct) is a type I membrane protein and an important regulatory enzyme that plays a pivotal role in the biosynthesis of melanin and in the rapid metabolism of its toxic intermediates. Dct-mutant melanocytes carrying the slaty or slaty light mutations were derived from the skin of newborn congenic C57BL/6J non-agouti black mice and were used to study the effect(s) of these mutations on the intracellular trafficking of Dct and on the pigmentation of the cells. Dct activity is 3-fold lower in slaty cells compared with non-agouti black melanocytes, whereas slaty light melanocytes have a surprisingly 28-fold lower Dct activity. Homology modelling of the active site of Dct suggests that the slaty mutation [R194Q (Arg194-->Gln)] is located in the active site and may alter the ability of the enzyme to transform the substrate. Transmembrane prediction methods indicate that the slaty light mutation [G486R (Gly486-->Arg)] may result in the sliding of the transmembrane domain towards the N-terminus, thus interfering with Dct function. Chemical analysis showed that both Dct mutations increase pheomelanin and reduce eumelanin produced by melanocytes in culture. Thus the enzymatic activity of Dct may play a role in determining whether the eumelanin or pheomelanin pathway is preferred for pigment biosynthesis.
JF  - The Biochemical journal
AU  - Costin, Gertrude-E
AU  - Valencia, Julio C
AU  - Wakamatsu, Kazumasa
AU  - Ito, Shosuke
AU  - Solano, Francisco
AU  - Milac, Adina L
AU  - Vieira, Wilfred D
AU  - Yamaguchi, Yuji
AU  - Rouzaud, François
AU  - Petrescu, Andrei-J
AU  - Lamoreux, M Lynn
AU  - Hearing, Vincent J
AD  - Pigment Cell Biology Section, Laboratory of Cell Biology, National Cancer Institute, National Institutes of Health (NIH), Bethesda, MD 20892, USA.
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 249
EP  - 259
VL  - 391
KW  - Melanins
KW  - 0
KW  - pheomelanin
KW  - eumelanin
KW  - 12627-86-0
KW  - Intramolecular Oxidoreductases
KW  - EC 5.3.-
KW  - dopachrome isomerase
KW  - EC 5.3.3.12
KW  - Index Medicus
KW  - Animals
KW  - Gene Expression Regulation, Enzymologic
KW  - Cells, Cultured
KW  - Molecular Sequence Data
KW  - Mice
KW  - Amino Acid Sequence
KW  - Sequence Homology, Amino Acid
KW  - Protein Transport
KW  - Protein Conformation
KW  - Binding Sites
KW  - Melanins -- biosynthesis
KW  - Intramolecular Oxidoreductases -- genetics
KW  - Melanocytes -- metabolism
KW  - Intramolecular Oxidoreductases -- metabolism
KW  - Melanocytes -- cytology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=The+Biochemical+journal&rft.atitle=Mutations+in+dopachrome+tautomerase+%28Dct%29+affect+eumelanin%2Fpheomelanin+synthesis%2C+but+do+not+affect+intracellular+trafficking+of+the+mutant+protein.&rft.au=Costin%2C+Gertrude-E%3BValencia%2C+Julio+C%3BWakamatsu%2C+Kazumasa%3BIto%2C+Shosuke%3BSolano%2C+Francisco%3BMilac%2C+Adina+L%3BVieira%2C+Wilfred+D%3BYamaguchi%2C+Yuji%3BRouzaud%2C+Fran%C3%A7ois%3BPetrescu%2C+Andrei-J%3BLamoreux%2C+M+Lynn%3BHearing%2C+Vincent+J&rft.aulast=Costin&rft.aufirst=Gertrude-E&rft.date=2005-10-15&rft.volume=391&rft.issue=&rft.spage=249&rft.isbn=&rft.btitle=&rft.title=The+Biochemical+journal&rft.issn=1470-8728&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-26
N1  - Date created - 2005-10-10
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
J Hered. 1963 Mar-Apr;54:47-50 [13943454]
Nucleic Acids Res. 1988 Nov 25;16(22):10881-90 [2849754]
J Biol Chem. 2000 Mar 17;275(11):8169-75 [10713140]
J Mol Biol. 2000 Jun 2;299(2):499-520 [10860755]
Bioinformatics. 2000 Apr;16(4):404-5 [10869041]
Pigment Cell Res. 2000 Oct;13(5):364-74 [11041214]
Pigment Cell Res. 2000;13 Suppl 8:103-9 [11041366]
J Mol Biol. 2001 Jan 19;305(3):567-80 [11152613]
Pigment Cell Res. 2001 Feb;14(1):23-31 [11277491]
Biochem J. 2001 Apr 15;355(Pt 2):259-69 [11284711]
Proc Natl Acad Sci U S A. 2001 Sep 11;98(19):10698-703 [11526213]
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Proteins. 2002 May 1;47(2):228-35 [11933069]
Pigment Cell Res. 2002 Jun;15(3):174-83 [12028581]
J Cell Sci. 2003 Aug 1;116(Pt 15):3203-12 [12829739]
Pigment Cell Res. 2003 Aug;16(4):333-44 [12859616]
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Science. 1969 May 16;164(3881):838-9 [4976615]
Biochem J. 1976 Sep 1;157(3):549-57 [825109]
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Biochim Biophys Acta. 1987 Aug 13;925(2):203-9 [3113493]
J Biol Chem. 1989 Feb 25;264(6):3397-403 [2492536]
Cell. 1990 Jun 29;61(7):1349-57 [2194670]
J Cutan Pathol. 1991 Dec;18(6):432-5 [1774353]
EMBO J. 1992 Feb;11(2):519-26 [1537333]
EMBO J. 1992 Feb;11(2):527-35 [1537334]
Biochim Biophys Acta. 1994 Apr 28;1221(3):272-8 [8167148]
J Invest Dermatol. 1994 Aug;103(2):196-201 [8040609]
Biochem Biophys Res Commun. 1994 Jul 29;202(2):1060-8 [8048919]
Proteins. 1994 May;19(1):55-72 [8066087]
Pigment Cell Res. 1994 Jun;7(3):141-4 [7971746]
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Biochem J. 1996 Jan 15;313 ( Pt 2):447-53 [8573077]
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Proc Natl Acad Sci U S A. 1998 Jun 23;95(13):7374-8 [9636156]
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Anal Biochem. 2004 Dec 1;335(1):171-4 [15519586]
J Chromatogr. 1987 Sep 25;420(2):404-10 [3693511]
Biochem Biophys Res Commun. 2005 Mar 25;328(4):914-21 [15707965]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Invited Commentary: Why DDT matters now.
AN  - 68639666; 16120697
JF  - American journal of epidemiology
AU  - Longnecker, Matthew P
AD  - Epidemiology Branch, National Institute of Environmental Health Sciences, National Institutes of Health, Department of Health and Human Services, Research Triangle Park, NC 27709, USA. longnec1@niehs.nih.gov
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 726
EP  - 728
VL  - 162
IS  - 8
SN  - 0002-9262, 0002-9262
KW  - Biomarkers
KW  - 0
KW  - DDT
KW  - CIW5S16655
KW  - Index Medicus
KW  - Maternal Exposure -- adverse effects
KW  - Global Health
KW  - Humans
KW  - Infant, Newborn
KW  - Incidence
KW  - Biomarkers -- blood
KW  - Female
KW  - Pregnancy
KW  - DDT -- blood
KW  - Pregnancy Complications -- chemically induced
KW  - DDT -- adverse effects
KW  - Birth Weight -- drug effects
KW  - Pregnancy Complications -- blood
KW  - Environmental Exposure -- adverse effects
KW  - Pregnancy Complications -- epidemiology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-01
N1  - Date created - 2005-10-03
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment On:
Am J Epidemiol. 2005 Oct 15;162(8):709-16 [16120699]
Am J Epidemiol. 2005 Oct 15;162(8):717-25 [16120698]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Prooxidant activity of resveratrol in the presence of copper ions: mutagenicity in plasmid DNA.
AN  - 68596064; 15913925
AB  - Resveratrol, a polyphenolic compound of plant origin, has been of much interest to researchers because of its anticancer and cardiovascular properties. Although antioxidant action of this compound is believed responsible for its reported properties, it has also been shown to exhibit prooxidant properties, especially in the presence of copper ions. Here we report the mutagenicity of resveratrol in plasmid DNA. Plasmid bluescript SK(+) DNA was treated with increasing concentrations of resveratrol in the presence and absence of copper ions, transformed into competent DH5alpha cells and sequenced. We looked for mutations caused by resveratrol treatment by comparing the sequences of treated plasmids versus control (untreated plasmid). The results show a decrease in the transformation efficiency of the plasmid after resveratrol treatment, and although all types of mutations were recorded, point mutations (deletions/substitutions) were found to be the predominant ones. Resveratrol alone resulted in deletion of mainly guanine bases. Since copper ions are known to be found in the nucleus, bound to guanine bases in chromatin, our results suggest mobilization of such endogenous copper by resveratrol resulting in prooxidant DNA cleavage at the site. Concentration of copper is reported to be elevated in various malignancies and the present studies might explain the reported anticancer activity of resveratrol in various cancer cell lines.
JF  - Toxicology letters
AU  - Ahmad, Aamir
AU  - Syed, Farhan Asad
AU  - Singh, Saurabh
AU  - Hadi, S M
AD  - Department of Biochemistry, Faculty of Life Sciences, AMU, Aligarh, UP 202002, India. ahmada@mail.nih.gov
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 1
EP  - 12
VL  - 159
IS  - 1
SN  - 0378-4274, 0378-4274
KW  - Antineoplastic Agents, Phytogenic
KW  - 0
KW  - Mutagens
KW  - Oxidants
KW  - Stilbenes
KW  - Guanine
KW  - 5Z93L87A1R
KW  - Copper
KW  - 789U1901C5
KW  - DNA
KW  - 9007-49-2
KW  - resveratrol
KW  - Q369O8926L
KW  - Index Medicus
KW  - Lac Operon -- genetics
KW  - Spectrometry, Fluorescence
KW  - Guanine -- chemistry
KW  - DNA Mutational Analysis
KW  - Apoptosis -- drug effects
KW  - Escherichia coli -- drug effects
KW  - Escherichia coli -- genetics
KW  - Gene Deletion
KW  - DNA Damage -- drug effects
KW  - DNA -- isolation & purification
KW  - Antineoplastic Agents, Phytogenic -- toxicity
KW  - Plasmids -- genetics
KW  - DNA -- genetics
KW  - Stilbenes -- toxicity
KW  - Plasmids -- drug effects
KW  - Copper -- chemistry
KW  - DNA -- drug effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-09
N1  - Date created - 2005-09-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Synthesis and evaluation of antioxidative properties of a series of organoselenium compounds.
AN  - 68554328; 16019215
AB  - A series of organoselenocyanate compounds 4a-d were synthesized utilizing 1,8-naphthalic anhydride as the building unit. These compounds were evaluated for their antioxidative activities against DMBA-PMA-induced oxidative stress in a two-stage mouse skin carcinogenic model. Compound 4d was found to have the maximum antioxidative property in comparison with the other compounds. Also, the pretreatment group showed better results than the concomitant treatment groups.
JF  - Bioorganic & medicinal chemistry
AU  - Hossain, Sk Ugir
AU  - Sengupta, Sumitra
AU  - Bhattacharya, Sudin
AD  - Department of Cancer Chemoprevention, Chittaranjan National Cancer Institute, 37, SP Mukherjee Road, Kolkata 700 026, India.
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 5750
EP  - 5758
VL  - 13
IS  - 20
SN  - 0968-0896, 0968-0896
KW  - Antioxidants
KW  - 0
KW  - Organoselenium Compounds
KW  - Index Medicus
KW  - Animals
KW  - Microsomes, Liver -- drug effects
KW  - Mice
KW  - Lipid Peroxidation
KW  - Spectrometry, Mass, Fast Atom Bombardment
KW  - Female
KW  - Magnetic Resonance Spectroscopy
KW  - Organoselenium Compounds -- pharmacology
KW  - Antioxidants -- chemical synthesis
KW  - Antioxidants -- pharmacology
KW  - Organoselenium Compounds -- chemical synthesis
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-22
N1  - Date created - 2005-09-06
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Absence of acrylamide-induced genotoxicity in CYP2E1-null mice: Evidence consistent with a glycidamide-mediated effect
AN  - 20830616; 6523789
AB  - Acrylamide, an animal carcinogen and germ cell mutagen present at low (ppm) levels in heated carbohydrate-containing foodstuffs, is oxidized by cytochrome P4502E1 (CYP2E1) to the epoxide glycidamide, which is believed to be responsible for the mutagenic and carcinogenic activity of acrylamide. We recently reported a comparison of the effects of acrylamide on the genetic integrity of germ cells of male wild-type and CYP2E1-null mice [B.I. Ghanayem, K.L. Witt, L. El-Hadri, U. Hoffler, G.E. Kissling, M.D. Shelby, J.B. Bishop, Comparison of germ-cell mutagenicity in male CYP2E1-null and wild-type mice treated with acrylamide: evidence supporting a glycidamide-mediated effect, Biol. Reprod. 72 (2005) 157-163]. In those experiments, dose-related increases in dominant lethal mutations were detected in uterine contents of female mice mated to acrylamide-treated wild-type males but not CYP2E1-null males, clearly implicating CYP2E1-mediated formation of glycidamide in the induction of genetic damage in male germ cells. We hypothesized that acrylamide-induced somatic cell damage is also caused by glycidamide. Therefore, to examine this hypothesis, female wild-type and CYP2E1-null mice were administered acrylamide (0, 25, 50mg/kg) by intraperitoneal injection once daily for 5 consecutive days. Twenty-four hours after the final treatment, blood and tissue samples were collected. Erythrocyte micronucleus frequencies were determined using flow cytometry and DNA damage was assessed in leukocytes, liver, and lung using the alkaline (pH>13) single cell gel electrophoresis (Comet) assay. Results were consistent with the earlier observations in male germ cells: significant dose-related increases in micronucleated erythrocytes and DNA damage in somatic cells were induced in acrylamide-treated wild-type but not in the CYP2E1-null mice. These results support the hypothesis that genetic damage in somatic and germ cells of mice-treated with acrylamide is dependent upon metabolism of the parent compound by CYP2E1. This dependency on metabolism has implications for the assessment of human risks resulting from occupational or dietary exposure to acrylamide. CYP2E1 polymorphisms and variability in CYP2E1 activity associated with, for example, diabetes, obesity, starvation, and alcohol consumption, may result in altered metabolic efficiencies leading to differential susceptibilities to acrylamide toxicities in humans.
JF  - Mutation Research-Fundamental and Molecular Mechanisms of Mutagenesis
AU  - Ghanayem, B I
AU  - Witt, K L
AU  - Kissling, GE
AU  - Tice, R R
AU  - Recio, L
AD  - National Institute of Environmental Health Sciences, National Institutes of Health, P.O. Box 12233, Research Triangle Park, NC 27709, USA, ghanayem@niehs.nih.gov
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 284
EP  - 297
VL  - 578
IS  - 1-2
SN  - 0027-5107, 0027-5107
KW  - Genetics Abstracts; Toxicology Abstracts
KW  - Risk assessment
KW  - Mutagens
KW  - Molecular modelling
KW  - Epoxides
KW  - Food
KW  - Erythrocytes
KW  - Carcinogens
KW  - Somatic cells
KW  - Mutagenesis
KW  - Flow cytometry
KW  - Occupational exposure
KW  - Ethanol
KW  - Starvation
KW  - Obesity
KW  - Uterus
KW  - Mutagenicity
KW  - Leukocytes
KW  - Genotoxicity
KW  - Germ cells
KW  - Toxicity
KW  - Gel electrophoresis
KW  - Diabetes mellitus
KW  - DNA damage
KW  - Blood
KW  - Acrylamide
KW  - Lung
KW  - Liver
KW  - Comet assay
KW  - Mutation
KW  - Metabolism
KW  - X 24120:Food, additives & contaminants
KW  - G 07730:Development & Cell Cycle
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Risk assessment; Molecular modelling; Mutagens; Epoxides; Food; Erythrocytes; Carcinogens; Somatic cells; Mutagenesis; Flow cytometry; Occupational exposure; Ethanol; Starvation; Obesity; Mutagenicity; Uterus; Genotoxicity; Leukocytes; Germ cells; Toxicity; Gel electrophoresis; Diabetes mellitus; Blood; DNA damage; Acrylamide; Lung; Liver; Comet assay; Mutation; Metabolism
DO  - http://dx.doi.org/10.1016/j.mrfmmm.2005.05.004
ER  - 



TY  - JOUR
T1  - Measuring Fifteen Endogenous Estrogens Simultaneously in Human Urine by High-Performance Liquid Chromatography-Mass Spectrometry
AN  - 19419636; 6538323
AB  - A sensitive, specific, accurate, and precise high-performance liquid chromatography-electrospray ionization-tandem mass spectrometry method for measuring the absolute quantities of 15 endogenous estrogens and their metabolites in human urine has been developed and validated. The method requires a single hydrolysis/extraction/derivatization step and only 0.5 mL of urine, yet is capable of simultaneously quantifying estrone and its 2-, 4-methoxy and 2-, 4-, and 16 alpha -hydroxy derivatives, and 2-hydroxyestrone-3-methyl ether; estradiol and its 2-, 4-methoxy and 2-, 16 alpha -hydroxy derivatives, 16-epiestriol, 17-epiestriol, and 16-ketoestradiol in pre- and postmenopausal women as well as men. Standard curves are linear over a 10 super(3)-fold concentration range with the standard error of the estimate (SEE) and the relative standard error of the estimate (RSEE) for the linear regression line ranging from 0.0131 to 0.1760 and 1.2 to 7.3%, respectively. The lower limit of quantitation for each estrogen is 0.02 ng/0.5 mL urine sample (2 pg on column), with the percent recovery of a known added amount of compound (accuracy) of 96-107% and an overall precision, including the hydrolysis, extraction, and derivatization steps, of 1-5% relative standard deviation (RSD) for samples prepared concurrently and 1-12% RSD for samples prepared in separate batches. Since individual patterns of estrogen metabolism may influence the risk of breast cancer, accurate, precise, and specific measurement of endogenous estrogen metabolites in biological matrixes will facilitate future research on breast cancer prevention, screening, and treatment.
JF  - Analytical Chemistry (Washington)
AU  - Xu, X
AU  - Veenstra, T D
AU  - Fox, S D
AU  - Roman, J M
AU  - Issaq, HJ
AU  - Falk, R
AU  - Saavedra, JE
AU  - Keefer, L K
AU  - Ziegler, R G
AD  - Laboratory of Proteomics and Analytical Technologies, SAIC-Frederick, Inc., National Cancer Institute at Frederick, Frederick, Maryland 21702, USA
Y1  - 2005/10/15/
PY  - 2005
DA  - 2005 Oct 15
SP  - 6646
EP  - 6654
VL  - 77
IS  - 20
SN  - 0003-2700, 0003-2700
KW  - Biotechnology and Bioengineering Abstracts
KW  - Estrogens
KW  - Metabolites
KW  - Hydrolysis
KW  - Mass spectroscopy
KW  - Estradiol
KW  - Spectrometry
KW  - Standard deviation
KW  - Post-menopause
KW  - Urine
KW  - Breast cancer
KW  - Ethers
KW  - Quantitation
KW  - Metabolism
KW  - Estrone
KW  - W 30900:Methods
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Analytical+Chemistry+%28Washington%29&rft.atitle=Measuring+Fifteen+Endogenous+Estrogens+Simultaneously+in+Human+Urine+by+High-Performance+Liquid+Chromatography-Mass+Spectrometry&rft.au=Xu%2C+X%3BVeenstra%2C+T+D%3BFox%2C+S+D%3BRoman%2C+J+M%3BIssaq%2C+HJ%3BFalk%2C+R%3BSaavedra%2C+JE%3BKeefer%2C+L+K%3BZiegler%2C+R+G&rft.aulast=Xu&rft.aufirst=X&rft.date=2005-10-15&rft.volume=77&rft.issue=20&rft.spage=6646&rft.isbn=&rft.btitle=&rft.title=Analytical+Chemistry+%28Washington%29&rft.issn=00032700&rft_id=info:doi/10.1021%2Fac050697c
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Estrogens; Urine; Hydrolysis; Breast cancer; Metabolites; Estradiol; Spectrometry; Ethers; Standard deviation; Mass spectroscopy; Post-menopause; Metabolism; Estrone; Quantitation
DO  - http://dx.doi.org/10.1021/ac050697c
ER  - 



TY  - JOUR
T1  - Identification of an agonist-induced conformational change occurring adjacent to the ligand-binding pocket of the M(3) muscarinic acetylcholine receptor.
AN  - 68673487; 16093246
AB  - To study the conformational changes that convert G protein-coupled receptors (GPCRs) from their resting to their active state, we used the M(3) muscarinic acetylcholine receptor, a prototypical class A GPCR, as a model system. Specifically, we employed a recently developed in situ disulfide cross-linking strategy that allows the formation of disulfide bonds in Cys-substituted mutant M(3) muscarinic receptors present in their native membrane environment. At present, little is known about the conformational changes that GPCR ligands induce in the immediate vicinity of the ligand-binding pocket. To address this issue, we generated 11 Cys-substituted mutant M(3) muscarinic receptors and characterized these receptors in transfected COS-7 cells. All analyzed mutant receptors contained an endogenous Cys residue (Cys-532(7.42)) located within the exofacial segment of transmembrane domain (TM) VII, close to the agonist-binding site. In addition, all mutant receptors harbored a second Cys residue that was introduced into the exofacial segment of TM III, within the sequence Leu-142(3.27)-Asn-152(3.37). Disulfide cross-linking studies showed that muscarinic agonists, but not antagonists, promoted the formation of a disulfide bond between S151(3.36)C and Cys-532. A three-dimensional model of the inactive state of the M(3) muscarinic receptor indicated that Cys-532 and Ser-151 face each other in the center of the TM receptor core. Our cross-linking data therefore support the concept that agonist activation pulls the exofacial segments of TMs VII and III closer to each other. This structural change may represent one of the early conformational events triggering the more pronounced structural reorganization of the intracellular receptor surface. To the best of our knowledge, this is the first direct demonstration of a conformational change occurring in the immediate vicinity of the binding site of a GPCR activated by a diffusible ligand.
JF  - The Journal of biological chemistry
AU  - Han, Sung-Jun
AU  - Hamdan, Fadi F
AU  - Kim, Soo-Kyung
AU  - Jacobson, Kenneth A
AU  - Bloodworth, Lanh M
AU  - Li, Bo
AU  - Wess, Jürgen
AD  - Molecular Signaling and Molecular Recognition Sections, Laboratory of Bioorganic Chemistry, NIDDK, National Institutes of Health, Bethesda, Maryland 20892-0810, USA.
Y1  - 2005/10/14/
PY  - 2005
DA  - 2005 Oct 14
SP  - 34849
EP  - 34858
VL  - 280
IS  - 41
SN  - 0021-9258, 0021-9258
KW  - Cross-Linking Reagents
KW  - 0
KW  - Disulfides
KW  - Ligands
KW  - Phosphatidylinositols
KW  - Receptors, Muscarinic
KW  - Serine
KW  - 452VLY9402
KW  - Asparagine
KW  - 7006-34-0
KW  - Carbachol
KW  - 8Y164V895Y
KW  - Luciferases
KW  - EC 1.13.12.-
KW  - Leucine
KW  - GMW67QNF9C
KW  - Cysteine
KW  - K848JZ4886
KW  - Oxygen
KW  - S88TT14065
KW  - Index Medicus
KW  - Phosphatidylinositols -- chemistry
KW  - Animals
KW  - COS Cells
KW  - Leucine -- chemistry
KW  - Carbachol -- chemistry
KW  - Rats
KW  - Mutagenesis, Site-Directed
KW  - Cysteine -- chemistry
KW  - Molecular Sequence Data
KW  - Protein Conformation
KW  - Dose-Response Relationship, Drug
KW  - Models, Molecular
KW  - Cross-Linking Reagents -- pharmacology
KW  - Luciferases -- metabolism
KW  - Amino Acid Sequence
KW  - Protein Binding
KW  - Serine -- chemistry
KW  - Binding Sites
KW  - Blotting, Western
KW  - Disulfides -- chemistry
KW  - Transfection
KW  - Kinetics
KW  - Cercopithecus aethiops
KW  - Oxygen -- chemistry
KW  - Models, Chemical
KW  - Cell Membrane -- metabolism
KW  - Protein Structure, Tertiary
KW  - Carbachol -- pharmacology
KW  - Mutation
KW  - Asparagine -- chemistry
KW  - Receptors, Muscarinic -- chemistry
KW  - Receptors, Muscarinic -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-13
N1  - Date created - 2005-10-10
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Whole-Body Hypothermia for Neonates with Hypoxic-Ischemic Encephalopathy
AN  - 223942405; 16221780
AB  - Background  
Hypothermia is protective against brain injury after asphyxiation in animal models. However, the safety and effectiveness of hypothermia in term infants with encephalopathy is uncertain.  
Methods  
We conducted a randomized trial of hypothermia in infants with a gestational age of at least 36 weeks who were admitted to the hospital at or before six hours of age with either severe acidosis or perinatal complications and resuscitation at birth and who had moderate or severe encephalopathy. Infants were randomly assigned to usual care (control group) or whole-body cooling to an esophageal temperature of 33.5°C for 72 hours, followed by slow rewarming (hypothermia group). Neurodevelopmental outcome was assessed at 18 to 22 months of age. The primary outcome was a combined end point of death or moderate or severe disability.  
Results  
Of 239 eligible infants, 102 were assigned to the hypothermia group and 106 to the control group. Adverse events were similar in the two groups during the 72 hours of cooling. Primary outcome data were available for 205 infants. Death or moderate or severe disability occurred in 45 of 102 infants (44 percent) in the hypothermia group and 64 of 103 infants (62 percent) in the control group (risk ratio, 0.72; 95 percent confidence interval, 0.54 to 0.95; P=0.01). Twenty-four infants (24 percent) in the hypothermia group and 38 (37 percent) in the control group died (risk ratio, 0.68; 95 percent confidence interval, 0.44 to 1.05; P=0.08). There was no increase in major disability among survivors; the rate of cerebral palsy was 15 of 77 (19 percent) in the hypothermia group as compared with 19 of 64 (30 percent) in the control group (risk ratio, 0.68; 95 percent confidence interval, 0.38 to 1.22; P=0.20).  
Conclusions  
Whole-body hypothermia reduces the risk of death or disability in infants with moderate or severe hypoxic-ischemic encephalopathy.
JF  - The New England Journal of Medicine
AU  - Shankaran, Seetha, MD
AU  - Laptook, Abbot R, MD
AU  - Ehrenkranz, Richard A, MD
AU  - Tyson, Jon E, MD, MPH
AU  - McDonald, Scott A, BS
AU  - Donovan, Edward F, MD
AU  - Fanaroff, Avroy A, MD
AU  - Poole, W Kenneth, PhD
AU  - Wright, Linda L, MD
AU  - Higgins, Rosemary D, MD
AU  - Finer, Neil N, MD
AU  - Carlo, Waldemar A, MD
AU  - Duara, Shahnaz, MD
AU  - Oh, William, MD
AU  - Cotten, C Michael, MD
AU  - Stevenson, David K, MD
AU  - Stoll, Barbara J, MD
AU  - Lemons, James A, MD
AU  - Guillet, Ronnie, MD, PhD
AU  - Jobe, Alan H, MD, PhD
Y1  - 2005/10/13/
PY  - 2005
DA  - 2005 Oct 13
SP  - 1574
EP  - 84
CY  - Boston
PB  - Massachusetts Medical Society
VL  - 353
IS  - 15
SN  - 00284793
KW  - Medical Sciences
KW  - Babies
KW  - Brain damage
KW  - Age
KW  - Cooling
KW  - Nitric oxide
KW  - Ischemia
KW  - Brain research
KW  - Consciousness
KW  - Consent
KW  - Intensive care
KW  - Pregnancy Complications
KW  - Asphyxia Neonatorum -- complications
KW  - Hypoxia-Ischemia, Brain -- mortality
KW  - Blindness -- prevention & control
KW  - Humans
KW  - Infant, Newborn
KW  - Obstetric Labor Complications
KW  - Pregnancy
KW  - Hearing Loss -- prevention & control
KW  - Acidosis -- etiology
KW  - Follow-Up Studies
KW  - Hypoxia-Ischemia, Brain -- complications
KW  - Female
KW  - Male
KW  - Cerebral Palsy -- prevention & control
KW  - Developmental Disabilities -- prevention & control
KW  - Hypoxia-Ischemia, Brain -- therapy
KW  - Hypothermia, Induced -- adverse effects
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ahealthcompleteshell&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=The+New+England+Journal+of+Medicine&rft.atitle=Whole-Body+Hypothermia+for+Neonates+with+Hypoxic-Ischemic+Encephalopathy&rft.au=Shankaran%2C+Seetha%2C+MD%3BLaptook%2C+Abbot+R%2C+MD%3BEhrenkranz%2C+Richard+A%2C+MD%3BTyson%2C+Jon+E%2C+MD%2C+MPH%3BMcDonald%2C+Scott+A%2C+BS%3BDonovan%2C+Edward+F%2C+MD%3BFanaroff%2C+Avroy+A%2C+MD%3BPoole%2C+W+Kenneth%2C+PhD%3BWright%2C+Linda+L%2C+MD%3BHiggins%2C+Rosemary+D%2C+MD%3BFiner%2C+Neil+N%2C+MD%3BCarlo%2C+Waldemar+A%2C+MD%3BDuara%2C+Shahnaz%2C+MD%3BOh%2C+William%2C+MD%3BCotten%2C+C+Michael%2C+MD%3BStevenson%2C+David+K%2C+MD%3BStoll%2C+Barbara+J%2C+MD%3BLemons%2C+James+A%2C+MD%3BGuillet%2C+Ronnie%2C+MD%2C+PhD%3BJobe%2C+Alan+H%2C+MD%2C+PhD&rft.aulast=Shankaran&rft.aufirst=Seetha&rft.date=2005-10-13&rft.volume=353&rft.issue=15&rft.spage=1574&rft.isbn=&rft.btitle=&rft.title=The+New+England+Journal+of+Medicine&rft.issn=00284793&rft_id=info:doi/
LA  - English
DB  - ProQuest Central
N1  - Copyright - Copyright © 2005 Massachusetts Medical Society. All rights reserved.
N1  - Document feature - Tables; Graphs; References
N1  - Last updated - 2014-04-29
N1  - CODEN - NEJMAG
ER  - 



TY  - JOUR
T1  - Influence of nonameric AU-rich tristetraprolin-binding sites on mRNA deadenylation and turnover.
AN  - 68646264; 16061475
AB  - Tristetraprolin (TTP), a member of the tandem CCCH zinc finger protein family, promotes deadenylation of tumor necrosis factor-alpha and granulocyte-macrophage colony-stimulating factor mRNAs after binding to the AU-rich elements (ARE) in their 3'-untranslated regions. The high affinity TTP-ARE binding occurs between the tandem zinc finger domain and the preferred nonamer UUAUUUAUU. By mutating a well defined core sequence of 24 bases from the tumor necrosis factor-alpha ARE, we compared the influence of four possible nonameric TTP-binding sites in the wild-type ARE with that of a single binding site in the mutated probe on the binding of TTP to the RNA and the subsequent deadenylation of the poly(A) tail. By inserting this 24-base ARE into an otherwise stable transcript, we also attempted to determine the extent of the instability conferred by the presence of one or two TTP-binding sites. These sites were created or modified by mutating the As in the UUAUUUAUU nonamer or by changing the central U in the nonamer, in both cases to C residues. The results suggest that even a single nonamer TTP-binding site can confer at least partial sensitivity to the TTP-mediated mRNA turnover on an otherwise stable mRNA, but that two binding sites make the transcript much more unstable. Even though the central U of the nonamer binding site was predicted by structural studies possibly to permit base substitution, mutation of this U to C greatly inhibited the binding of TTP to the ARE, thus reducing the ability of the TTP to promote deadenylation and instability of the mRNA.
JF  - The Journal of biological chemistry
AU  - Lai, Wi S
AU  - Carrick, Danielle M
AU  - Blackshear, Perry J
AD  - Laboratory of Neurobiology, NIEHS, National Institutes of Health, Research Triangle Park, North Carolina 27709, USA.
Y1  - 2005/10/07/
PY  - 2005
DA  - 2005 Oct 07
SP  - 34365
EP  - 34377
VL  - 280
IS  - 40
SN  - 0021-9258, 0021-9258
KW  - RNA, Messenger
KW  - 0
KW  - Tristetraprolin
KW  - Uracil
KW  - 56HH86ZVCT
KW  - Adenine
KW  - JAC85A2161
KW  - Index Medicus
KW  - Mutagenesis, Site-Directed
KW  - Base Sequence
KW  - Genomic Instability
KW  - Molecular Sequence Data
KW  - Binding Sites -- physiology
KW  - RNA, Messenger -- metabolism
KW  - Tristetraprolin -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-02
N1  - Date created - 2005-10-03
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Anthrax Biosensor, Protective Antigen Ion Channel Asymmetric Blockade
AN  - 17393875; 6503357
AB  - The significant threat posed by biological agents (e.g. anthrax, tetanus, botulinum, and diphtheria toxins) requires innovative technologies and approaches to understand the mechanisms of toxin action and to develop better therapies. Anthrax toxins are formed from three proteins secreted by fully virulent Bacillus anthracis, protective antigen (PA, 83 kDa), lethal factor (LF, 90 kDa), and edema factor (EF, 89 kDa). Here we present electrophysiological measurements demonstrating that full-length LF and EF convert the current-voltage relationship of the heptameric PA sub(63) ion channel from slightly nonlinear to highly rectifying and diode-like at pH 6.6. This effect provides a novel method for characterizing functional toxin interactions. The method confirms that a previously well characterized PA sub(63) monoclonal antibody, which neutralizes anthrax lethal toxin in animals in vivo and in vitro, prevents the binding of LF to the PA sub(63) pore. The technique can also detect the presence of anthrax lethal toxin complex from plasma of infected animals. The latter two results suggest the potential application of PA sub(63) nanopore-based biosensors in anthrax therapeutics and diagnostics.
JF  - Journal of Biological Chemistry
AU  - Halverson, Kelly M
AU  - Panchal, Rekha G
AU  - Nguyen, Tam L
AU  - Gussio, Rick
AU  - Little, Stephen F
AU  - Misakian, Martin
AU  - Bavari, Sina
AU  - Kasianowicz, John J
AD  - United States Army Medical Research Institute of Infectious Diseases, Fort Detrick, Frederick, Maryland 21702-5011, Developmental Therapeutics Program, Target Structure-based Drug Discovery Group, National Cancer Institute-Science Applications International Corporation, Frederick, Maryland 21702, National Institute of Standards and Technology, Electronics and Electrical Engineering Laboratory, Gaithersburg, Maryland 20899-8172, and National Institute of Standards and Technology, Advanced Chemical Sciences Laboratory and the Electronics and Electrical Engineering Laboratory, Semiconductor Engineering Division, Gaithersburg, Maryland 20899-8120
Y1  - 2005/10/07/
PY  - 2005
DA  - 2005 Oct 07
SP  - 34056
EP  - 34062
PB  - American Society for Biochemistry and Molecular Biology, 9650 Rockville Pike Bethesda MD 20814-3996 USA, [mailto:asbmb@asbmb.faseb.org], [URL:http://www.jbc.org]
VL  - 280
IS  - 40
SN  - 0021-9258, 0021-9258
KW  - Biotechnology and Bioengineering Abstracts; Microbiology Abstracts B: Bacteriology; Bioengineering Abstracts
KW  - Anthrax lethal toxin
KW  - Channel pores
KW  - Monoclonal antibodies
KW  - Lethal factor
KW  - protective antigen
KW  - Edema
KW  - Bacillus anthracis
KW  - Tetanus
KW  - Diphtheria toxin
KW  - Biosensors
KW  - Ion channels
KW  - Anthrax
KW  - pH effects
KW  - J 02822:Biosynthesis and physicochemical properties
KW  - W4 140:Bioinformatics & Computers in Health & Medicine
KW  - W 30965:Miscellaneous, Reviews
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Biological+Chemistry&rft.atitle=Anthrax+Biosensor%2C+Protective+Antigen+Ion+Channel+Asymmetric+Blockade&rft.au=Halverson%2C+Kelly+M%3BPanchal%2C+Rekha+G%3BNguyen%2C+Tam+L%3BGussio%2C+Rick%3BLittle%2C+Stephen+F%3BMisakian%2C+Martin%3BBavari%2C+Sina%3BKasianowicz%2C+John+J&rft.aulast=Halverson&rft.aufirst=Kelly&rft.date=2005-10-07&rft.volume=280&rft.issue=40&rft.spage=34056&rft.isbn=&rft.btitle=&rft.title=Journal+of+Biological+Chemistry&rft.issn=00219258&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-04-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Biosensors; Anthrax lethal toxin; Monoclonal antibodies; Channel pores; Lethal factor; protective antigen; Ion channels; Edema; Anthrax; Tetanus; pH effects; Diphtheria toxin; Bacillus anthracis
ER  - 



TY  - JOUR
T1  - Cumulative Absolute Breast Cancer Risk for Young Women Treated for Hodgkin Lymphoma
AN  - 20716196; 6505273
AB  - BACKGROUND: Many women develop breast cancer after treatment for Hodgkin lymphoma (HL) at a young age. We estimated this future risk, taking into account age and calendar year of HL diagnosis, HL treatment information, population breast cancer incidence rates, and competing causes of death. METHODS: Relative risks of breast cancer for categories defined by radiation dose to the chest (0, 20-<40 Gy, or greater than or equal to 40 Gy) and use of alkylating agents (yes or no) were estimated from a case-control study conducted within an international population-based cohort of 3817 female 1-year survivors of HL diagnosed at age 30 years or younger from January 1, 1965, through December 31, 1994. To compute cumulative absolute risks of breast cancer, we used modified standardized incidence ratios to relate cohort breast cancer risks to those in the general population, enabling application of population-based breast cancer rates, and we allowed for competing risks by using population-based mortality rates in female HL survivors. RESULTS: Cumulative absolute risks of breast cancer increased with age at end of follow-up, time since HL diagnosis, and radiation dose. For an HL survivor who was treated at age 25 years with a chest radiation dose of at least 40 Gy without alkylating agents, estimated cumulative absolute risks of breast cancer by age 35, 45, and 55 years were 1.4% (95% confidence interval [CI] = 0.9% to 2.1%), 11.1% (95% CI = 7.4% to 16.3%), and 29.0% (95% CI = 20.2% to 40.1%), respectively. Cumulative absolute risks were lower in women treated with alkylating agents. CONCLUSIONS: Breast cancer projections varied considerably by type of HL therapy, time since HL diagnosis, and age at end of follow-up. These estimates are applicable to HL survivors treated with regimens of the past and can be used to counsel such patients and plan management and preventive strategies. Projections should be used with caution, however, in patients treated with more recent approaches, including limited-field radiotherapy and/or ovary-sparing chemotherapy.
JF  - Journal of the National Cancer Institute
AU  - Travis, Lois B
AU  - Hill, Deirdre
AU  - Dores, Graca M
AU  - Gospodarowicz, Mary
AU  - van Leeuwen, Flora E
AU  - Holowaty, Eric
AU  - Glimelius, Bengt
AU  - Andersson, Michael
AU  - Pukkala, Eero
AU  - Lynch, Charles F
AU  - Pee, David
AU  - Smith, Susan A
AU  - Van't Veer, Mars B
AU  - Joensuu, Timo
AU  - Storm, Hans
AU  - Stovall, Marilyn
AU  - Boice, John DJr
AU  - Gilbert, Ethel
AU  - Gail, Mitchell H
AD  - Division of Cancer Epidemiology and Genetics (LBT, DH, EG, MHG) and Division of Cancer Prevention (GMD), National Cancer Institute, National Institutes of Health, Department of Health and Human Services, Bethesda, MD
Y1  - 2005/10/05/
PY  - 2005
DA  - 2005 Oct 05
SP  - 1428
EP  - 1437
PB  - Oxford University Press, Oxford Journals, Great Clarendon Street Oxford OX2 6DP UK, [mailto:jnl.samples@oup.co.uk], [URL:http://www3.oup.co.uk/jnls/]
VL  - 97
IS  - 19
SN  - 0027-8874, 0027-8874
KW  - Risk Abstracts; Immunology Abstracts
KW  - Alkylating agents
KW  - Risk assessment
KW  - Mortality
KW  - Age
KW  - Hodgkin's disease
KW  - Chemotherapy
KW  - Radiotherapy
KW  - Chest
KW  - radiotherapy
KW  - Cancer
KW  - chemotherapy
KW  - Radiation
KW  - Risk factors
KW  - risk taking
KW  - Breast cancer
KW  - Standards
KW  - Females
KW  - lymphoma
KW  - F 06915:Cancer Immunology
KW  - R2 23060:Medical and environmental health
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-04-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Risk assessment; Alkylating agents; Mortality; Age; Hodgkin's disease; Radiation; Chemotherapy; Risk factors; Radiotherapy; Breast cancer; Chest; risk taking; Standards; Females; radiotherapy; lymphoma; chemotherapy; Cancer
ER  - 



TY  - JOUR
T1  - Cytolytic granule polarization and degranulation controlled by different receptors in resting NK cells.
AN  - 68655455; 16203869
AB  - The relative contribution to cytotoxicity of each of the multiple NK cell activation receptors has been difficult to assess. Using Drosophila insect cells, which express ligands of human NK cell receptors, we show that target cell lysis by resting NK cells is controlled by different receptor signals for cytolytic granule polarization and degranulation. Intercellular adhesion molecule (ICAM)-1 on insect cells was sufficient to induce polarization of granules, but not degranulation, in resting NK cells. Conversely, engagement of the Fc receptor CD16 by rabbit IgG on insect cells induced degranulation without specific polarization. Lysis by resting NK cells occurred when polarization and degranulation were induced by the combined presence of ICAM-1 and IgG on insect cells. Engagement of receptor 2B4 by CD48 on insect cells induced weak polarization and no degranulation. However, coengagement of 2B4 and CD16 by their respective ligands resulted in granule polarization and cytotoxicity in the absence of leukocyte functional antigen-1-mediated adhesion to target cells. These data show that cytotoxicity by resting NK cells is controlled tightly by separate or cooperative signals from different receptors for granule polarization and degranulation.
JF  - The Journal of experimental medicine
AU  - Bryceson, Yenan T
AU  - March, Michael E
AU  - Barber, Domingo F
AU  - Ljunggren, Hans-Gustaf
AU  - Long, Eric O
AD  - Laboratory of Immunogenetics, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rockville, MD 20852, USA.
Y1  - 2005/10/03/
PY  - 2005
DA  - 2005 Oct 03
SP  - 1001
EP  - 1012
VL  - 202
IS  - 7
SN  - 0022-1007, 0022-1007
KW  - Antigens, CD
KW  - 0
KW  - CD244 protein, human
KW  - DNA Primers
KW  - Membrane Glycoproteins
KW  - Receptors, IgG
KW  - Receptors, Immunologic
KW  - Signaling Lymphocytic Activation Molecule Family
KW  - Intercellular Adhesion Molecule-1
KW  - 126547-89-5
KW  - Index Medicus
KW  - Animals
KW  - Humans
KW  - Receptors, IgG -- metabolism
KW  - Cloning, Molecular
KW  - Cells, Cultured
KW  - Receptors, Immunologic -- metabolism
KW  - Antigens, CD -- metabolism
KW  - Cytotoxicity Tests, Immunologic
KW  - Enzyme-Linked Immunosorbent Assay
KW  - Cell Adhesion -- immunology
KW  - Drosophila
KW  - Membrane Glycoproteins -- metabolism
KW  - Signal Transduction -- immunology
KW  - Intercellular Adhesion Molecule-1 -- genetics
KW  - Cytotoxicity, Immunologic -- immunology
KW  - Killer Cells, Natural -- metabolism
KW  - Cytoplasmic Granules -- metabolism
KW  - Intercellular Adhesion Molecule-1 -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-05-02
N1  - Date created - 2005-10-05
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
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J Immunol. 2004 Sep 15;173(6):3653-9 [15356110]
Clin Cancer Res. 2004 Sep 15;10(18 Pt 1):6248-55 [15448014]
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Immunity. 1995 Dec;3(6):801-9 [8777725]
Immunity. 1997 Jun;6(6):655-61 [9208838]
Curr Opin Cell Biol. 1997 Oct;9(5):643-50 [9330867]
Curr Top Microbiol Immunol. 1998;230:63-88 [9586351]
Curr Top Microbiol Immunol. 1998;230:89-99 [9586352]
J Immunol. 1998 Jun 15;160(12):5781-9 [9637488]
J Exp Med. 1998 Aug 3;188(3):549-59 [9687532]
Immunol Rev. 1998 Jun;163:197-215 [9700512]
J Immunol. 1998 Dec 1;161(11):5809-12 [9834056]
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Eur J Immunol. 1999 May;29(5):1676-83 [10359122]
Mol Immunol. 2005 Feb;42(4):477-84 [15607802]
Annu Rev Immunol. 2005;23:225-74 [15771571]
Nat Immunol. 2005 May;6(5):515-23 [15821739]
Leukemia. 2005 May;19(5):835-40 [15744340]
Proc Natl Acad Sci U S A. 2005 May 3;102(18):6437-42 [15851656]
Blood. 2005 Jun 1;105(11):4416-23 [15728129]
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Eur J Immunol. 2000 Mar;30(3):787-93 [10741393]
Curr Opin Cell Biol. 2000 Oct;12(5):542-7 [10978887]
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J Biol Chem. 2001 May 11;276(19):16469-77 [11297532]
Eur J Immunol. 2001 Oct;31(10):3121-7 [11592089]
Trends Immunol. 2001 Nov;22(11):633-40 [11698225]
Curr Opin Hematol. 2002 Jan;9(1):30-5 [11753075]
Annu Rev Immunol. 2002;20:323-70 [11861606]
Nat Rev Immunol. 2001 Oct;1(1):41-9 [11905813]
Nat Rev Immunol. 2002 Oct;2(10):735-47 [12360212]
J Immunol. 2003 Jan 1;170(1):294-9 [12496412]
Nat Immunol. 2003 May;4(5):399-403 [12719728]
J Exp Med. 2003 Aug 4;198(3):469-74 [12885870]
Mol Cell Biol. 2003 Sep;23(17):6291-9 [12917349]
J Immunol Methods. 2003 Oct 1;281(1-2):65-78 [14580882]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - DNA damage among thyroid cancer and multiple cancer cases, controls, and long-lived individuals
AN  - 21044660; 6500578
AB  - Variation in the detection, signaling, and repair of DNA damage contributes to human cancer risk. To assess capacity to modulate endogenous DNA damage among radiologic technologists who had been diagnosed with breast cancer and another malignancy (breast-other, n=42), early-onset breast cancer (early-onset, age approximately equal to 35; n=38), thyroid cancer (n=68), long-lived cancer-free individuals (hyper-normals, n=20) and cancer-free controls (n=49) we quantified DNA damage (single strand breaks and abasic sites) in untreated lymphoblastoid cell lines using the alkaline comet assay. Komet(TM) software provided comet tail length, % DNA in tail (tail DNA), comet distributed moment (CDM), and Olive tail moment (OTM) summarized as the geometric mean of 100 cells. Category cut-points (median and 75th percentile) were determined from the distribution among controls. Tail length (for >=75% versus below the median, age-adjusted) was most consistently associated with the highest odds ratios in the breast-other, early-onset, and thyroid cancer groups (with risk increased 10-, 5- or 19-fold, respectively, with wide confidence intervals) and decreased risk among the hyper-normal group. For the other three comet measures, risk of breast-other was elevated approximately three-fold. Risk of early-onset breast cancer was mixed and risk of thyroid cancer ranged from null to a two-fold increase. The hyper-normal group showed decreased odds ratios for tail DNA and OTM, but not CDM. DNA damage, as estimated by all comet measures, was relatively unaffected by survival time, reproductive factors, and prior radiation treatment. We detected a continuum of endogenous DNA damage that was highest among cancer cases, less in controls, and suggestively lowest in hyper-normal individuals. Measuring this DNA damage phenotype may contribute to the identification of susceptible sub-groups. Our observations require replication in a prospective study with a large number of pre-diagnostic samples.
JF  - Mutation Research-Genetic Toxicology and Environmental Mutagenesis
AU  - Sigurdson, A J
AU  - Hauptmann, M
AU  - Alexander, B H
AU  - Doody, M M
AU  - Thomas, C B
AU  - Struewing, J P
AU  - Jones, I M
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, NIH, DHHS, 6120 Executive Boulevard, EPS 7092, MSC 7238, Bethesda, MD 20892-7238, USA, sigurdsa@mail.nih.gov
Y1  - 2005/10/03/
PY  - 2005
DA  - 2005 Oct 03
SP  - 173
EP  - 188
PB  - Elsevier B.V.
VL  - 586
IS  - 2
SN  - 1383-5718, 1383-5718
KW  - Toxicology Abstracts; Biochemistry Abstracts 2: Nucleic Acids
KW  - Olea
KW  - Age
KW  - Replication
KW  - Tails
KW  - Survival
KW  - Mutagenesis
KW  - Computer programs
KW  - DNA damage
KW  - software
KW  - Malignancy
KW  - Lymphoblastoid cell lines
KW  - Radiation
KW  - thyroid cancer
KW  - Breast cancer
KW  - Comet assay
KW  - Signal transduction
KW  - N 14100:Reviews
KW  - X 24300:Methods
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxicologyabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Mutation+Research-Genetic+Toxicology+and+Environmental+Mutagenesis&rft.atitle=DNA+damage+among+thyroid+cancer+and+multiple+cancer+cases%2C+controls%2C+and+long-lived+individuals&rft.au=Sigurdson%2C+A+J%3BHauptmann%2C+M%3BAlexander%2C+B+H%3BDoody%2C+M+M%3BThomas%2C+C+B%3BStruewing%2C+J+P%3BJones%2C+I+M&rft.aulast=Sigurdson&rft.aufirst=A&rft.date=2005-10-03&rft.volume=586&rft.issue=2&rft.spage=173&rft.isbn=&rft.btitle=&rft.title=Mutation+Research-Genetic+Toxicology+and+Environmental+Mutagenesis&rft.issn=13835718&rft_id=info:doi/10.1016%2Fj.mrgentox.2005.07.001
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Age; Tails; Replication; Survival; Mutagenesis; DNA damage; Computer programs; Malignancy; software; Radiation; Lymphoblastoid cell lines; thyroid cancer; Breast cancer; Comet assay; Signal transduction; Olea
DO  - http://dx.doi.org/10.1016/j.mrgentox.2005.07.001
ER  - 



TY  - CPAPER
T1  - Does Treatment-Induced Recovery from Hepatitis C Result in the Same Immunological Memory as Spontaneous Recovery?
T2  - 12th International Symposium on Hepatitis C Virus and Related Viruses
AN  - 40121190; 4001109
JF  - 12th International Symposium on Hepatitis C Virus and Related Viruses
AU  - Weiler-Normann, Christina
Y1  - 2005/10/02/
PY  - 2005
DA  - 2005 Oct 02
KW  - Immunological memory
KW  - Spontaneous recovery
KW  - Hepatitis C
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40121190?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=12th+International+Symposium+on+Hepatitis+C+Virus+and+Related+Viruses&rft.atitle=Does+Treatment-Induced+Recovery+from+Hepatitis+C+Result+in+the+Same+Immunological+Memory+as+Spontaneous+Recovery%3F&rft.au=Weiler-Normann%2C+Christina&rft.aulast=Weiler-Normann&rft.aufirst=Christina&rft.date=2005-10-02&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=12th+International+Symposium+on+Hepatitis+C+Virus+and+Related+Viruses&rft.issn=&rft_id=info:doi/
L2  - http://www.hcv2005.com/ProgramThemes.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Production of Infectious Hepatitis C Virus in Cell Culture
T2  - 12th International Symposium on Hepatitis C Virus and Related Viruses
AN  - 40093951; 4001066
JF  - 12th International Symposium on Hepatitis C Virus and Related Viruses
AU  - Kato, Takanobu
Y1  - 2005/10/02/
PY  - 2005
DA  - 2005 Oct 02
KW  - Viral diseases
KW  - Cell culture
KW  - Hepatitis
KW  - Hepatitis C virus
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=12th+International+Symposium+on+Hepatitis+C+Virus+and+Related+Viruses&rft.atitle=Production+of+Infectious+Hepatitis+C+Virus+in+Cell+Culture&rft.au=Kato%2C+Takanobu&rft.aulast=Kato&rft.aufirst=Takanobu&rft.date=2005-10-02&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=12th+International+Symposium+on+Hepatitis+C+Virus+and+Related+Viruses&rft.issn=&rft_id=info:doi/
L2  - http://www.hcv2005.com/ProgramThemes.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Immunization of Chimpanzees with Hepatitis C Virus-Like Particles Induces Partial Protection Against Hepatitis C Virus Infection
T2  - 12th International Symposium on Hepatitis C Virus and Related Viruses
AN  - 40044806; 4001112
JF  - 12th International Symposium on Hepatitis C Virus and Related Viruses
AU  - Elmowalid, Gamal
Y1  - 2005/10/02/
PY  - 2005
DA  - 2005 Oct 02
KW  - Virus-like particles
KW  - Particulates
KW  - Infectious diseases
KW  - Immunization
KW  - Hepatitis C
KW  - Hepatitis C virus
KW  - U 2000:Biological Sciences
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L2  - http://www.hcv2005.com/ProgramThemes.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Only the C- Terminal Subunit of the Gbv-B P13 Protein is Required for Infectivity in Tamarins: Generation of a Recombinant Gbv-B Virus with a P7 Protein
T2  - 12th International Symposium on Hepatitis C Virus and Related Viruses
AN  - 40044572; 4001069
JF  - 12th International Symposium on Hepatitis C Virus and Related Viruses
AU  - Takikawa, Shingo
Y1  - 2005/10/02/
PY  - 2005
DA  - 2005 Oct 02
KW  - Recombinants
KW  - Infectivity
KW  - p7 protein
KW  - U 2000:Biological Sciences
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L2  - http://www.hcv2005.com/ProgramThemes.aspx
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Sustained cadherin 23 expression in young and adult cochlea of normal and hearing-impaired mice.
AN  - 85395695; pmid-16005171
AB  - Cadherin 23 encodes a single-pass transmembrane protein with 27 extracellular cadherin-domains and localizes to stereocilia where it functions as an inter-stereocilia link. Cadherin 23-deficient mice show congenital deafness in combination with circling behavior as a result of organizational defects in the stereocilia hair bundle; common inbred mouse strains carrying the hypomorphic Cdh23(753A) allele are highly susceptible to sensorineural hearing loss. Here, we show that an antibody (N1086) directed against the intracellular carboxyterminus reacts specifically with cadherin 23 and detects with high sensitivity the isoform devoid of the peptide encoded by exon 68 (CDH23Delta68). Cochlea, vestibule, eye, brain and testis produce the CDH23Delta68 isoform in abundance and form moieties with different molecular weight due to variations in glycosylation content. In the cochlea, CDH23Delta68 expression is highest at postnatal day 1 (P1) and P7; expression is down regulated through P14 and P21 and persists at a low steady-state level throughout adulthood (P160). Furthermore, CDH23Delta68 expression levels in young and adult cochlea are similar among normal and hearing deficient strains (C3HeB/FeJ, C57BL/6J and BUB/BnJ). Finally, by immunofluorescence using an antibody (Pb240) specific for ectodomain 14, we show that cadherin 23 localizes to stereocilia during hair bundle development in late gestation and early postnatal days. Cadherin 23-specific labeling becomes weaker as the hair bundle matures but faint labeling concentrated near the top of stereocilia is still detectable at P35. No labeling of cochlea stereocilia was observed with N1086. In conclusion, our data describe a cadherin 23-specific antibody with high affinity to the CDH23Delta68 isoform, reveal a dynamic cochlea expression and localization profile and show sustained cadherin 23 levels in adult cochlea of normal and hearing-impaired mice.
JF  - Hearing research
AU  - Rzadzinska, Agnieszka K
AU  - Derr, Adam
AU  - Kachar, Bechara
AU  - Noben-Trauth, Konrad
AD  - Section on Structural Cell Biology, Laboratory of Cellular Biology, National Institute on Deafness and Other Communication Disorders, National Institutes of Health, Bethesda, MD 20892, USA.
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 114
EP  - 121
VL  - 208
IS  - 1-2
SN  - 0378-5955, 0378-5955
KW  - Index Medicus
KW  - National Library of Medicine
KW  - Amino Acid Sequence
KW  - Animals
KW  - Animals, Newborn
KW  - Antibody Specificity
KW  - Base Sequence
KW  - Cadherins: chemistry
KW  - *Cadherins: genetics
KW  - Cadherins: immunology
KW  - Cadherins: metabolism
KW  - Cochlea: embryology
KW  - Cochlea: growth & development
KW  - Cochlea: metabolism
KW  - Cochlea: pathology
KW  - DNA, Complementary: genetics
KW  - Female
KW  - Gene Expression Regulation, Developmental
KW  - Glycosylation
KW  - *Hearing Loss, Sensorineural: genetics
KW  - Hearing Loss, Sensorineural: metabolism
KW  - Hearing Loss, Sensorineural: pathology
KW  - Male
KW  - Mice
KW  - Mice, Inbred C3H
KW  - Mice, Inbred CBA
KW  - Mice, Knockout
KW  - Mice, Mutant Strains
KW  - Rats
KW  - Rats, Sprague-Dawley
KW  - Tissue Distribution
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LA  - English (eng)
DB  - ComDisDome
N1  - Date revised - 2011-12-15
N1  - Last updated - 2012-07-13
ER  - 



TY  - JOUR
T1  - Role of the liver-specific transporters OATP1B1 and OATP1B3 in governing drug elimination.
AN  - 70182647; 16863454
AB  - Members of the organic anion transporting polypeptide (OATP) family are responsible for the cellular uptake of a broad range of endogenous compounds and xenobiotics in multiple tissues. This review focuses on OATP1B1 and -1B3, which are specifically expressed in the liver and considered to be of particular importance for hepatic drug elimination and drug pharmacokinetics. Recent literature has indicated that inhibition of these transporters may result in drug-drug interactions. Furthermore, genetic polymorphisms in the genes encoding OATP1B1 and -1B3 have been described that increase or decrease transport in vitro and in vivo. Alteration of transporter function by either of these mechanisms may contribute to interindividual variability in drug disposition and response. In this review an update of this rapidly emerging field is provided.
JF  - Expert opinion on drug metabolism & toxicology
AU  - Smith, Nicola F
AU  - Figg, William D
AU  - Sparreboom, Alex
AD  - National Cancer Institute, Molecular Pharmacology Section, Medical Oncology Branch, Center for Cancer Research, 9000 Rockville Pike, Bethesda, MD 20892, USA. smithni@mail.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 429
EP  - 445
VL  - 1
IS  - 3
SN  - 1742-5255, 1742-5255
KW  - Organic Anion Transporters
KW  - 0
KW  - Organic Anion Transporters, Sodium-Independent
KW  - Pharmaceutical Preparations
KW  - SLCO1B1 protein, human
KW  - SLCO1B3 protein, human
KW  - Solute Carrier Organic Anion Transporter Family Member 1b1
KW  - Index Medicus
KW  - Animals
KW  - Drug Interactions
KW  - Humans
KW  - Pharmacogenetics
KW  - Organic Anion Transporters, Sodium-Independent -- metabolism
KW  - Organic Anion Transporters, Sodium-Independent -- genetics
KW  - Pharmaceutical Preparations -- metabolism
KW  - Organic Anion Transporters -- genetics
KW  - Organic Anion Transporters -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-08-29
N1  - Date created - 2006-07-25
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CONF
T1  - Predictive ADME-Tox London, UK, 27 -- 28 April 2005.
AN  - 70182495; 16863462
AB  - The Predictive ADME-Tox conference brought together scientists responsible for innovative in vitro and in silico screens to predict particular chemical liabilities. Oral bioavailability without adverse effects requires good absorption, distribution, metabolism and excretion (ADME) and minimal toxicity. Traditionally, these properties are measured late in development, when sufficient material is available for classical assays. Although these assays remain the gold standard, the conference focused on novel methods to predict liabilities early in the development pipeline, when a course change has less impact in the development timeline. Emerging themes from the meeting were i) integration - of data from a number of predictive assays into a 'profile' of a new class, and of safety scientists into discovery teams, in order to guide interpretation of the profile and identify tests to include in the hit-to-lead process; and ii) collaboration. As in silico predictive models are increasingly accepted, from reactivity and genetic toxicity to models for hERG inhibition, kinase crossreactivity and cytochrome P450 reactivity, increasing amounts of high-quality data will be needed to 'feed' the models. Such data will soon be beyond the capabilities of individual organisations to generate, and methods for pooling data are needed to advance the generation of predictive models for new toxicities. In addition, collaboration to apply novel methods such as metabonomics profiling to withdrawn drugs may permit the identification of new safety biomarkers to prevent such costly failures.
JF  - Expert opinion on drug metabolism & toxicology
AU  - Fostel, Jennifer
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 565
EP  - 570
VL  - 1
IS  - 3
KW  - Pharmaceutical Preparations
KW  - 0
KW  - Index Medicus
KW  - Computer Simulation
KW  - Pharmacology
KW  - Toxicogenetics
KW  - Drug Design
KW  - Pharmaceutical Preparations -- metabolism
KW  - Biotransformation
KW  - Tissue Distribution
KW  - Pharmacokinetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-08-29
N1  - Date created - 2006-07-25
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Usefulness of salivary trans-3'-hydroxycotinine concentration and trans-3'-hydroxycotinine/cotinine ratio as biomarkers of cigarette smoke in pregnant women.
AN  - 69071253; 16419402
AB  - Nicotine is rapidly and extensively metabolized in humans and negatively impacts the developing fetus. The concentrations of nicotine, cotinine, trans-3'-hydroxycotinine (hydroxycotinine), and norcotinine in pregnant smokers' oral fluid were evaluated to determine usefulness as biomarkers of cigarette smoking. Sixteen participants were divided into two groups: eight light smokers (LS) who smoked  or =20 cigarettes/day. Oral fluid specimens (n=415) were collected throughout pregnancy and analyzed with solid-phase extraction followed by gas chromatography-mass spectrometry-electron impact selected ion monitoring. Median concentrations of nicotine, cotinine, and hydroxycotinine in oral fluid of LS ranged from 241.1 to 622.0, 80.6 to 387.5, and 14.4 to 117.7 ng/mL and for HS 146.5-1372.2, 66.0-245.8, and 38.3-184.4 ng/mL, respectively. Salivary cotinine and hydroxycotinine concentrations were significantly correlated in LS (r = 0.55, p < 0.01) and HS (r = 0.74, p < 0.01). Ratios of hydroxycotinine/cotinine in oral fluid from pregnant women averaged 0.30 +/- 0.18 (range, 0.07-1.05) for LS and 0.68 +/- 0.25 (range, 0.29-1.83) for HS. Based on these preliminary data, the best ratio to differentiate light from heavy pregnant smokers was 0.41. Salivary hydroxycotinine and cotinine concentrations are both good biomarkers of cigarette smoking. Determining the hydroxycotinine/cotinine ratio may differentiate light from heavy tobacco use and help predict increased fetal tobacco exposure.
JF  - Journal of analytical toxicology
AU  - Kim, Insook
AU  - Wtsadik, Abraham
AU  - Choo, Robin E
AU  - Jones, Hendrée E
AU  - Huestis, Marilyn A
AD  - Chemistry and Drug Metabolism, Intramural Research Program, National Institute on Drug Abuse, National Institutes of Health, 5500 Nathan Shock Drive, Baltimore, Maryland 21224, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 689
EP  - 695
VL  - 29
IS  - 7
SN  - 0146-4760, 0146-4760
KW  - Biomarkers
KW  - 0
KW  - hydroxycotinine
KW  - 27323-64-4
KW  - Cotinine
KW  - K5161X06LL
KW  - Index Medicus
KW  - Tobacco Use Disorder -- metabolism
KW  - Dose-Response Relationship, Drug
KW  - Humans
KW  - Adult
KW  - Tobacco Use Disorder -- prevention & control
KW  - Female
KW  - Pregnancy
KW  - Cotinine -- analysis
KW  - Smoking
KW  - Saliva -- chemistry
KW  - Biomarkers -- analysis
KW  - Cotinine -- analogs & derivatives
KW  - Saliva -- metabolism
KW  - Cotinine -- metabolism
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+analytical+toxicology&rft.atitle=Usefulness+of+salivary+trans-3%27-hydroxycotinine+concentration+and+trans-3%27-hydroxycotinine%2Fcotinine+ratio+as+biomarkers+of+cigarette+smoke+in+pregnant+women.&rft.au=Kim%2C+Insook%3BWtsadik%2C+Abraham%3BChoo%2C+Robin+E%3BJones%2C+Hendr%C3%A9e+E%3BHuestis%2C+Marilyn+A&rft.aulast=Kim&rft.aufirst=Insook&rft.date=2005-10-01&rft.volume=29&rft.issue=7&rft.spage=689&rft.isbn=&rft.btitle=&rft.title=Journal+of+analytical+toxicology&rft.issn=01464760&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-03
N1  - Date created - 2006-01-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Mode of action: impaired fetal leydig cell function--effects on male reproductive development produced by certain phthalate esters.
AN  - 69070513; 16417038
AB  - Certain phthalate esters (di-2-ethylhexyl; di-n-butyl and butyl benzyl) have profound effects on the developing male reproductive system when administered orally to pregnant experimental animals during a critical window of development. These esters produce a syndrome of adverse effects that are characteristic of a disturbance in androgen-mediated development and include a variety of reproductive tract malformations and effects on developmental phenotypic markers. A testicular dysgenesis syndrome has been proposed to explain the secular increases in a number of human male reproductive deficits, including decreased semen parameters, increased incidence of cryptorchidism and hypospadias (two of the most common human birth defects), and increased incidence of testicular (germ cell derived) cancer. The rodent phthalate data lend support to the hypothesis. This example illustrates a number of points in the use of the Human Relevance Framework. First, chemical agents may have more than one mode of action (MOA): for example, phthalate-induced peroxisome proliferation leading to hepatocarcinogensis, compared with the induction of developmental effects via effects on androgen signaling. Second, the case demonstrates the life-stage sensitivity of the response to these compounds. Third, because humans may be exposed to multiple phthalate esters producing adverse effects on reproductive development, these compounds may be useful in testing the utility of the Human Relevance Framework (HRF) approach for evaluating cumulative and aggregate risk.
JF  - Critical reviews in toxicology
AU  - Foster, Paul M D
AD  - National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina 27709, USA. foster2@niehs.nih.gov
PY  - 2005
SP  - 713
EP  - 719
VL  - 35
IS  - 8-9
SN  - 1040-8444, 1040-8444
KW  - Phthalic Acids
KW  - 0
KW  - Teratogens
KW  - Index Medicus
KW  - Animals
KW  - Humans
KW  - Species Specificity
KW  - Male
KW  - Female
KW  - Pregnancy
KW  - Abnormalities, Drug-Induced -- pathology
KW  - Leydig Cells -- physiology
KW  - Genitalia, Male -- embryology
KW  - Genitalia, Male -- drug effects
KW  - Fetus -- physiology
KW  - Leydig Cells -- drug effects
KW  - Phthalic Acids -- toxicity
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-08
N1  - Date created - 2006-01-18
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Symptomatological structure of volatile solvent-induced psychosis: is "solvent psychosis" a discernible syndrome?
AN  - 68853533; 16316074
AB  - Solvent-induced psychosis has been clinically identified among patients suffering from dependence on volatile solvents and those in psychotic state due to chronic solvent use. To clarify the symptomatological difference between solvent-induced psychosis and schizophrenia, the principal component analysis with VARIMAX rotation was applied to the point and duration estimates of symptoms observed among the solvent group and among the schizophrenic group. There were no significant group differences in age and family history of any psychosis. The study findings are as follows: (1) It is difficult to distinguish two groups based on the prevalence rates of symptoms alone. (2) However, the principal component VARIMAX rotation analysis of the prevalence and duration observing among the solvent group revealed seven factors consisting of "amotivation", "intoxication", "emotional instability", "delusion", "hallucination", "disinhibition" and "memory". The seven factors explained 75.4% of the variance of the symptoms in this group. (3) The same analysis applied to the data from the schizophrenic group showed six factors consisting of "thought progression", "emotional instability", "amotivation (or negative symptoms)", "delusion", "hallucination" and "anxiety". These factors explained 62.9% of the variance in the data of the schizophrenic group. These results support clinical observations the "amotivational syndrome" may be a characteristic feature of patients suffering from solvent-induced psychosis. The results also suggest "solvent psychosis" is a discernible syndrome, and is distinctive from psychotic symptoms of typical schizophrenia.
JF  - Nihon Arukoru Yakubutsu Igakkai zasshi = Japanese journal of alcohol studies & drug dependence
AU  - Wada, Kiyoshi
AU  - Nakayama, Kazuhiro
AU  - Koishikawa, Hiraki
AU  - Katayama, Masafumi
AU  - Hirai, Shinji
AU  - Yabana, Tatsuo
AU  - Aoki, Tsutomu
AU  - Iwashita, Satoru
AD  - National Institute of Mental Health, NCNP, 4-1-1 Ogawahigashi-cho, Kodairashi, Tokyo 187-8553, Japan.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 471
EP  - 484
VL  - 40
IS  - 5
SN  - 1341-8963, 1341-8963
KW  - Solvents
KW  - 0
KW  - Index Medicus
KW  - Schizophrenia -- classification
KW  - Humans
KW  - Adult
KW  - Male
KW  - Female
KW  - Solvents -- adverse effects
KW  - Psychoses, Substance-Induced -- etiology
KW  - Psychoses, Substance-Induced -- classification
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-19
N1  - Date created - 2005-11-30
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - A phase II study of perifosine in androgen independent prostate cancer.
AN  - 68825438; 16138006
AB  - Perifosine is an alkylphospholipid that has exhibited broad antineoplastic activity in preclinical studies. The primary objective of this study was to determine the clinical efficacy of this agent in the treatment of androgen-independent prostate cancer (AIPC) using PSA and clinical criteria.
          Nineteen patients with progressive, metastatic AIPC were treated with oral perifosine. Cycles were 28 days in length. A loading dose of 900 mg was given on day 1 of cycle 1 followed by a maintenance dose of 150 mg daily for the next 20 days. A loading dose of 600 mg was administered on the first day of subsequent cycles by the maintenance dose of 150 mg daily for the next 20 days. Pharmacokinetic measurements were made throughout the course of the study. Circulating epithelial cells were collected via leukapheresis on day 0, 3, and 28. Median patient age was 67 years and median PSA was 180 ng/mL (range: 19-904 ng/ml). Grade 1-2 fatigue and gastrointestinal toxicities were common. Pharmacokinetic studies showed an average minimum concentration at steady-state of approximately 4059 ng/ml which correlated well with previous studies. Median time to progression was four weeks. There were no radiographic responses or PSA declines of 50% or greater related to perifosine.
          Treatment with perifosine was complicated by fatigue and gastrointestinal toxicity. No significant clinical activity against prostate cancer was observed. This agent does not merit further study in the setting of monotherapy in this population.
JF  - Cancer biology & therapy
AU  - Posadas, Edwin M
AU  - Gulley, James
AU  - Arlen, Philip M
AU  - Trout, Alisa
AU  - Parnes, Howard L
AU  - Wright, John
AU  - Lee, Min-Jung
AU  - Chung, Eun Joo
AU  - Trepel, Jane B
AU  - Sparreboom, Alex
AU  - Chen, Clara
AU  - Jones, Elizabeth
AU  - Steinberg, Seth M
AU  - Daniels, Andrew
AU  - Figg, William D
AU  - Dahut, William L
AD  - Medical Oncology Clinical Research Unit, Center for Cancer Research, National Cancer Institute, Bethesda, Maryland, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1133
EP  - 1137
VL  - 4
IS  - 10
SN  - 1538-4047, 1538-4047
KW  - Androgens
KW  - 0
KW  - Antineoplastic Agents
KW  - Phosphorylcholine
KW  - 107-73-3
KW  - perifosine
KW  - 2GWV496552
KW  - Prostate-Specific Antigen
KW  - EC 3.4.21.77
KW  - Index Medicus
KW  - Leukapheresis
KW  - Drug Administration Schedule
KW  - Aged, 80 and over
KW  - Humans
KW  - Prostate-Specific Antigen -- blood
KW  - Treatment Outcome
KW  - Neoplasm Metastasis
KW  - Disease Progression
KW  - Aged
KW  - Middle Aged
KW  - Time Factors
KW  - Male
KW  - Prostatic Neoplasms -- pathology
KW  - Phosphorylcholine -- administration & dosage
KW  - Antineoplastic Agents -- administration & dosage
KW  - Antineoplastic Agents -- pharmacokinetics
KW  - Prostatic Neoplasms -- blood
KW  - Androgens -- physiology
KW  - Phosphorylcholine -- pharmacokinetics
KW  - Phosphorylcholine -- pharmacology
KW  - Prostatic Neoplasms -- drug therapy
KW  - Antineoplastic Agents -- pharmacology
KW  - Phosphorylcholine -- analogs & derivatives
KW  - Phosphorylcholine -- adverse effects
KW  - Antineoplastic Agents -- adverse effects
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cancer+biology+%26+therapy&rft.atitle=A+phase+II+study+of+perifosine+in+androgen+independent+prostate+cancer.&rft.au=Posadas%2C+Edwin+M%3BGulley%2C+James%3BArlen%2C+Philip+M%3BTrout%2C+Alisa%3BParnes%2C+Howard+L%3BWright%2C+John%3BLee%2C+Min-Jung%3BChung%2C+Eun+Joo%3BTrepel%2C+Jane+B%3BSparreboom%2C+Alex%3BChen%2C+Clara%3BJones%2C+Elizabeth%3BSteinberg%2C+Seth+M%3BDaniels%2C+Andrew%3BFigg%2C+William+D%3BDahut%2C+William+L&rft.aulast=Posadas&rft.aufirst=Edwin&rft.date=2005-10-01&rft.volume=4&rft.issue=10&rft.spage=1133&rft.isbn=&rft.btitle=&rft.title=Cancer+biology+%26+therapy&rft.issn=15384047&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-22
N1  - Date created - 2005-11-24
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Hodgkin lymphoma in temporal association with growth hormone replacement.
AN  - 68796226; 16284435
AB  - The association between growth hormone (GH) replacement and malignancy has long been debated. We report a case of Hodgkin lymphoma that developed in temporal association with the initiation of GH replacement in a 57-year-old woman with panhypopituitarism secondary to a non-secretory pituitary macroadenoma. Treatment of her pituitary tumor included transphenoidal surgery, external beam radiation, Bromocriptine and Cabergaline therapy. In addition to replacement steroid, thyroid and sex hormones, she insisted on GH replacement. Approximately 2 years after GH initiation, the diagnosis of Hodgkin lymphoma was made. Although the exact contribution of GH to the development of Hodgkin disease in our patient is unclear and a causal effect cannot be concluded, the temporal association is suggestive, and warrants reporting as part of ongoing surveillance for potential complications of GH replacement.
JF  - Endocrine journal
AU  - Freedman, Renee J
AU  - Malkovska, Vera
AU  - LeRoith, Derek
AU  - Collins, Michael T
AD  - Developmental Endocrinology Branch, National Institute of Child Health and Human Development, Bethesda, MD 20892, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 571
EP  - 575
VL  - 52
IS  - 5
SN  - 0918-8959, 0918-8959
KW  - Human Growth Hormone
KW  - 12629-01-5
KW  - Index Medicus
KW  - Humans
KW  - Adult
KW  - Middle Aged
KW  - Female
KW  - Adenoma -- therapy
KW  - Pituitary Neoplasms -- therapy
KW  - Human Growth Hormone -- therapeutic use
KW  - Hodgkin Disease -- chemically induced
KW  - Human Growth Hormone -- adverse effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-26
N1  - Date created - 2005-11-14
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Identification and treatment of patients with nicotine problems in routine clinical psychiatry practice.
AN  - 68747058; 16257881
AB  - The aim of this study is to assess the rates of nicotine problems diagnosed by psychiatrists, the characteristics of psychiatric patients who smoke, and the services provided to them in routine psychiatric practice. Data were obtained by asking psychiatrists participating in the American Psychiatric Institute for Psychiatric Research and Education's Practice Research Network to complete a self-administered questionnaire to provide detailed sociodemographic, clinical, and health plan information on three of their patients seen during routine clinical practice. A total of 615 psychiatrists provided information on 1,843 patients, of which 280 (16.6%) were reported to have a current nicotine problem. Of these, 9.1% were reported to receive treatment for nicotine dependence. Patients with nicotine problems were significantly more likely to be males, divorced or separated, disabled, and uninsured, and have fewer years of education. They also had significantly more co-morbid psychiatric disorders, particularly schizophrenia or alcohol/substance use disorders; a lower Global Assessment Functioning score; and poorer treatment compliance than their counterparts. The results suggest a very low rate of identification and treatment of nicotine problems among patients treated by psychiatrists, even though psychiatric patients who smoke seem to have more clinical and psychosocial stressors and more severe psychiatric problems than those who do not smoke. Programs should be developed to raise the awareness and ability of psychiatrists to diagnose and treat patients with nicotine problems, with a particular emphasis on the increased medical and psychosocial needs of psychiatric patients who smoke.
JF  - The American journal on addictions
AU  - Montoya, Ivan D
AU  - Herbeck, Diane M
AU  - Svikis, Dace S
AU  - Pincus, Harold Alan
AD  - National Institute on Drug Abuse, Division of Pharmacotherapies and Medical Consequences of Drug Abuse, 6001 Executive Blvd., Bethesda, MD 20892-9551, USA. imontoya@mail.nih.gov
PY  - 2005
SP  - 441
EP  - 454
VL  - 14
IS  - 5
SN  - 1055-0496, 1055-0496
KW  - Index Medicus
KW  - United States
KW  - Humans
KW  - Adult
KW  - Diagnosis, Dual (Psychiatry)
KW  - Aged
KW  - Middle Aged
KW  - Adolescent
KW  - Male
KW  - Female
KW  - Mental Disorders -- diagnosis
KW  - Mental Disorders -- therapy
KW  - Tobacco Use Disorder -- therapy
KW  - Mental Disorders -- psychology
KW  - Tobacco Use Disorder -- diagnosis
KW  - Psychiatry
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-30
N1  - Date created - 2005-10-31
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Am J Psychiatry. 1996 Oct;153(10):1247-8 [8831429]
Am J Psychiatry. 1996 Oct;153(10 Suppl):1-31 [8831466]
Psychiatr Serv. 1995 May;46(5):435-6 [7627666]
Prev Med. 1992 Mar;21(2):262-9 [1579560]
Psychiatr Serv. 1997 Jan;48(1):100-2 [9117487]
Schizophr Bull. 1997;23(2):247-54 [9165635]
J Addict Dis. 1998;17(1):47-54 [9549602]
Am J Psychiatry. 1998 Jul;155(7):974-6 [9659869]
Subst Use Misuse. 1998 Aug;33(10):2021-47 [9744841]
Am J Psychiatry. 1999 Mar;156(3):451-7 [10080563]
Arch Gen Psychiatry. 1999 May;56(5):441-9 [10232299]
J Subst Abuse Treat. 1999 Jun;16(4):315-20 [10349604]
Med Care. 1999 Jan;37(1):104-11 [10413398]
Ann Clin Psychiatry. 1999 Sep;11(3):129-36 [10482122]
Aust N Z J Psychiatry. 1999 Dec;33(6):869-73 [10619214]
J Clin Psychiatry. 2000 Sep;61(9):698-705; quiz 706 [11030495]
JAMA. 2000 Nov 22-29;284(20):2606-10 [11086367]
Am J Public Health. 2000 Dec;90(12):1898-904 [11111263]
Nicotine Tob Res. 2001 Aug;3(3):225-34 [11506766]
Arch Gen Psychiatry. 2001 Sep;58(9):810-6 [11545662]
Prog Neuropsychopharmacol Biol Psychiatry. 2002 Apr;26(3):529-37 [11999904]
Addiction. 2002 Jul;97(7):861-9 [12133125]
Psychiatr Serv. 2002 Sep;53(9):1166-70 [12221317]
J Clin Oncol. 2003 Jan 15;21(2):355-65 [12525530]
Arch Gen Psychiatry. 1986 Mar;43(3):289-94 [3954551]
Am J Psychiatry. 1986 Aug;143(8):993-7 [3487983]
Psychiatr J Univ Ott. 1988 Mar;13(1):25-7 [3283798]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Prevalence, correlates, and comorbidity of bipolar I disorder and axis I and II disorders: results from the National Epidemiologic Survey on Alcohol and Related Conditions.
AN  - 68746613; 16259532
AB  - To present nationally representative data on 12-month and lifetime prevalence, correlates, and comorbidity of bipolar I disorder.
          The data were derived from the 2001-2002 National Epidemiologic Survey on Alcohol and Related Conditions (N = 43,093). Prevalences and associations of bipolar I disorder with sociodemographic correlates and Axis I and II disorders were determined. Prevalences of 12-month and lifetime DSM-IV bipolar I disorder were 2.0% (95% CI = 1.82 to 2.18) and 3.3% (95% CI = 2.76 to 3.84), respectively, and no sex differences were observed. The odds of bipolar I disorder were significantly greater among Native Americans, younger adults, and respondents who were widowed/separated/divorced and of lower socioeconomic status and significantly lower among Asians and Hispanics (p < .05). Men were significantly (p < .05) more likely to have unipolar mania and earlier onset and longer duration of manic episodes, while women were more likely to have mixed and major depressive episodes and to be treated for manic, mixed, and major depressive episodes. Bipolar I disorder was found to be highly and significantly related (p < .05) to substance use, anxiety, and personality disorders, but not to alcohol abuse.
          Bipolar I disorder is more prevalent in the U.S. population than previously estimated, highlighting the underestimation of the economic costs associated with this illness. Associations between bipolar I disorder and Axis I and II disorders were all significant, underscoring the need for systematic assessment of comorbidity among bipolar I patients.
JF  - The Journal of clinical psychiatry
AU  - Grant, Bridget F
AU  - Stinson, Frederick S
AU  - Hasin, Deborah S
AU  - Dawson, Deborah A
AU  - Chou, S Patricia
AU  - Ruan, W June
AU  - Huang, Boji
AD  - Division of Intramural Clinical and Biological Research, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Department of Health and Human Services, Bethesda, MD 20892-9304, USA. bgrant@willco.niaaa.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1205
EP  - 1215
VL  - 66
IS  - 10
SN  - 0160-6689, 0160-6689
KW  - Index Medicus
KW  - Age of Onset
KW  - Humans
KW  - Aged
KW  - Child
KW  - Comorbidity
KW  - Age Distribution
KW  - Health Care Costs
KW  - Adult
KW  - Middle Aged
KW  - Psychiatric Status Rating Scales -- statistics & numerical data
KW  - Adolescent
KW  - United States -- epidemiology
KW  - Sex Distribution
KW  - Male
KW  - Diagnostic and Statistical Manual of Mental Disorders
KW  - Female
KW  - Prevalence
KW  - Alcohol-Related Disorders -- epidemiology
KW  - Mental Disorders -- diagnosis
KW  - Bipolar Disorder -- epidemiology
KW  - Mental Disorders -- epidemiology
KW  - Health Surveys
KW  - Bipolar Disorder -- classification
KW  - Mental Disorders -- economics
KW  - Bipolar Disorder -- economics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-09
N1  - Date created - 2005-11-01
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Alkaloids from amphibian skin: a tabulation of over eight-hundred compounds.
AN  - 68740940; 16252926
AB  - A diverse array of biologically active, lipid-soluble alkaloids have been discovered in amphibian skin. Such alkaloids include the following: the steroidal samandarines from salamanders, the batrachotoxins, histrionicotoxins, gephyrotoxins, and epibatidine from neotropical poison frogs (Dendrobatidae), the pumiliotoxins, allopumiliotoxins, homopumiliotoxins, and decahydroquinolines from certain genera of anurans from four families (Dendrobatidae, Mantellidae, Bufonidae, and Myobatrachidae), a variety of izidines (pyrrolizidines, indolizidines, quinolizidines, lehmizidines), pyrrolidines, piperidines, various tricyclics (related in structures to the coccinellines), and spiropyrrolizidines from the first three of these four families, the pseudophrynamines from one genus of Australian frogs, and a variety of unclassified alkaloids as yet of undetermined structure. With the exception of the samandarines and the pseudophrynamines, all alkaloids appear to be derived from dietary sources. Although only a few of the over 800 amphibian skin alkaloids have been detected in arthropods, putative arthropod sources for the batrachotoxins and coccinelline-like tricyclics (beetles), the pumiliotoxins (ants, mites), the decahydroquinolines, izidines, pyrrolidines, and piperidines (ants), and the spiropyrrolizidines (millipedes) have been discovered. Ants are likely sources for histrionicotoxins, lehmizidines, and tricyclic gephyrotoxins. Epibatidines represent an important alkaloid class without a putative dietary source. The structures for many of these alkaloids have been rigorously established, while the structures of others represent tentative proposals, based only on mass spectral and FTIR spectral data, along with analogies to structures of well-defined alkaloids.
JF  - Journal of natural products
AU  - Daly, John W
AU  - Spande, Thomas F
AU  - Garraffo, H Martin
AD  - Laboratory of Bioorganic Chemistry, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Department of Health and Human Services, Bethesda, Maryland 20892-0820, USA. jdaly@nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1556
EP  - 1575
VL  - 68
IS  - 10
SN  - 0163-3864, 0163-3864
KW  - Alkaloids
KW  - 0
KW  - Amphibian Venoms
KW  - Index Medicus
KW  - Molecular Structure
KW  - Animals
KW  - Amphibians -- physiology
KW  - Skin -- chemistry
KW  - Amphibian Venoms -- isolation & purification
KW  - Amphibian Venoms -- chemistry
KW  - Alkaloids -- chemistry
KW  - Alkaloids -- pharmacology
KW  - Alkaloids -- isolation & purification
KW  - Amphibian Venoms -- pharmacology
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-30
N1  - Date created - 2005-10-28
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Integration of pharmacotherapy for opioid addiction into HIV primary care for HIV/hepatitis C virus-co-infected patients.
AN  - 68734149; 16251822
AB  - Pharmacotherapy for substance abuse is a rapidly evolving field comprising both old and new effective treatments for substance use. Opiate agonist therapy has been shown to diminish and often eliminate opiate use. This behavior change has resulted in the reduced transmission of many infections, including HIV, hepatitis C virus (HCV), and an enhanced quality of life. For the past 35 years, the provision of opioid agonist therapy has been limited to opioid treatment programmes. Opioid treatment programmes treat approximately 200,000 of the estimated million opiate-addicted individuals in the United States. With the need to increase the number of treatment opportunities available for opioid-dependent patients, Congress passed the Drug Addiction Treatment Act of 2000, which allows for the treatment of opioid dependence using buprenorphine by a properly licensed physician, including HIV primary care physicians. The integration of buprenorphine treatment for opioid addiction into HIV primary care thus provides a new treatment paradigm to address substance abuse in patients with HIV and HCV infections.
JF  - AIDS (London, England)
AU  - Kresina, Thomas F
AU  - Eldred, Lois
AU  - Bruce, R Douglas
AU  - Francis, Henry
AD  - Center on AIDS and other Medical Consequences of Drug Abuse, National Institute on Drug Abuse, National Institutes of Health, Bethesda, MD, USA. tk13v@nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - S221
EP  - S226
VL  - 19 Suppl 3
SN  - 0269-9370, 0269-9370
KW  - Narcotic Antagonists
KW  - 0
KW  - Buprenorphine
KW  - 40D3SCR4GZ
KW  - Index Medicus
KW  - AIDS/HIV
KW  - United States
KW  - Buprenorphine -- therapeutic use
KW  - Narcotic Antagonists -- therapeutic use
KW  - Humans
KW  - Substance Abuse Treatment Centers -- organization & administration
KW  - HIV Infections -- complications
KW  - Opioid-Related Disorders -- complications
KW  - Hepatitis C -- complications
KW  - Opioid-Related Disorders -- rehabilitation
KW  - Primary Health Care -- organization & administration
KW  - Delivery of Health Care, Integrated
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-29
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - HIV/hepatitis C virus co-infection: its human face.
AN  - 68733814; 16251804
JF  - AIDS (London, England)
AU  - Cargill, Victoria A
AD  - Office of AIDS Research, National Institutes of Health, DHHS, Bethesda, MD, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - S1
EP  - S2
VL  - 19 Suppl 3
SN  - 0269-9370, 0269-9370
KW  - Antiviral Agents
KW  - 0
KW  - Index Medicus
KW  - AIDS/HIV
KW  - Antiviral Agents -- therapeutic use
KW  - Humans
KW  - Antiviral Agents -- adverse effects
KW  - Hepatitis C -- drug therapy
KW  - HIV Infections -- complications
KW  - Hepatitis C -- complications
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=AIDS+%28London%2C+England%29&rft.atitle=HIV%2Fhepatitis+C+virus+co-infection%3A+its+human+face.&rft.au=Cargill%2C+Victoria+A&rft.aulast=Cargill&rft.aufirst=Victoria&rft.date=2005-10-01&rft.volume=19+Suppl+3&rft.issue=&rft.spage=S1&rft.isbn=&rft.btitle=&rft.title=AIDS+%28London%2C+England%29&rft.issn=02699370&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-29
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Integrating care for patients with infectious, psychiatric, and substance use disorders: concepts and approaches.
AN  - 68732727; 16251823
AB  - Patients with chronic viral infections such as HIV/AIDS or hepatitis C often have multiple co-existing problems such as psychiatric and addictive disorders, as well as social problems such as lack of housing, transportation and income that present challenging obstacles to successful management. Because services for these different problems are usually provided by different disciplines in varying locations, fragmentation of care can lead to treatment dropouts, lack of adherence, and poor outcomes. Integration strategies, ranging from simple efforts to improve communication and coordinate care to fully integrated multidisciplinary teams have been used to improve disease management. Although evidence for effectiveness is comprised primarily of observational studies of demonstration programmes, integration may be desirable on a pragmatic basis alone. Quality improvement strategies are attractive vehicles for implementing care integration and measuring its impact. Careful assessment of the problem to be solved and the development of targeted strategies will maximize chances of a successful outcome.
JF  - AIDS (London, England)
AU  - Willenbring, Mark L
AD  - National Institute on Alcohol Abuse and Alcoholism, Bethesda, MD 20892-9304, USA. mlw@niaaa.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - S227
EP  - S237
VL  - 19 Suppl 3
SN  - 0269-9370, 0269-9370
KW  - Index Medicus
KW  - AIDS/HIV
KW  - Substance-Related Disorders -- therapy
KW  - Humans
KW  - Disease Management
KW  - Diagnosis, Dual (Psychiatry)
KW  - Substance-Related Disorders -- complications
KW  - Comorbidity
KW  - Hepatitis C -- therapy
KW  - Mental Disorders -- therapy
KW  - Patient Care Team
KW  - HIV Infections -- complications
KW  - Hepatitis C -- complications
KW  - HIV Infections -- therapy
KW  - Mental Disorders -- complications
KW  - Delivery of Health Care, Integrated
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-29
N1  - Date created - 2005-10-27
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Framework for environmental exposure research: the disease-first approach.
AN  - 68729464; 16249520
JF  - Molecular interventions
AU  - Wilson, Samuel H
AU  - Suk, William A
AD  - National Institute of Environmental Health Sciences, National Institutes of Health, Department of Health and Human Services, Research Triangle Park, NC 27709, USA. wilson5@niehs.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 262
EP  - 267
VL  - 5
IS  - 5
SN  - 1534-0384, 1534-0384
KW  - Index Medicus
KW  - Information Systems
KW  - Environmental Health
KW  - Humans
KW  - Research Design
KW  - Risk Assessment
KW  - Population Surveillance
KW  - Health Status
KW  - Disease Susceptibility -- etiology
KW  - Environmental Exposure -- adverse effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-24
N1  - Date created - 2005-10-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Alpha-particle radioimmunotherapy of disseminated peritoneal disease using a (212)Pb-labeled radioimmunoconjugate targeting HER2.
AN  - 68729142; 16248771
AB  - These studies demonstrate the feasibility of targeted therapy for the treatment of disseminated peritoneal disease using (212)Pb-labeled Herceptin as an in vivo generator of (212)Bi. In vitro studies compare the potential of the bismuth radioisotopes, (213)Bi and (212)Bi, to that of (212)Pb. Overall, (212)Pb results in a higher therapeutic index than either bismuth radioisotope, requiring lower radioactivity (microCi) for effective cytotoxic response. A pilot radioimmunotherapy (RIT) experiment treating mice bearing 5 d LS-174T intraperitoneally (i.p.) xenografts determined a maximum tolerated dose (MTD) of 20-40 microCi with i.p. administration. A specific dose response was observed and 10 microCi was selected as the effective operating dose for future experiments. Median survival of tumor-bearing mice receiving 10 microCi increased from 19 to 56 days (p = 0.008). The efficacy of (212)Pb-Herceptin was also assessed in a human pancreatic carcinoma xenograft (Shaw; i.p.) animal model previously reported as unresponsive to 213Bi-Herceptin (p = 0.002). Multiple dosing of (212)Pb-Herceptin was evaluated in both animal models. The median survival of mice bearing 3 d LS-174T i.p. xenografts increased to 110 days, with up to 3 doses of (212)Pb-Herceptin given at approximately monthly intervals; however, there was no evidence of a correlation with the second and third doses (p = 0.98). No improvement in median survival was noted with a similar regimen in the Shaw xenograft model.
JF  - Cancer biotherapy & radiopharmaceuticals
AU  - Milenic, Diane E
AU  - Garmestani, Kayhan
AU  - Brady, Erik D
AU  - Albert, Paul S
AU  - Ma, Dangshe
AU  - Abdulla, Alia
AU  - Brechbiel, Martin W
AD  - Radioimmune and Inorganic Chemistry Section, Radiation Oncology Branch, National Cancer Institute, National Institutes of Health, 10 Center Drive, MSC-1088, Building 10, Bethesda, MD 20892, USA. dm71q@nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 557
EP  - 568
VL  - 20
IS  - 5
SN  - 1084-9785, 1084-9785
KW  - Antibodies, Monoclonal
KW  - 0
KW  - Antibodies, Monoclonal, Humanized
KW  - Immunoconjugates
KW  - Lead Radioisotopes
KW  - Receptor, ErbB-2
KW  - EC 2.7.10.1
KW  - Trastuzumab
KW  - P188ANX8CK
KW  - Index Medicus
KW  - Animals
KW  - Genes, erbB-2
KW  - Humans
KW  - Cell Line, Tumor
KW  - Mice
KW  - Antibodies, Monoclonal -- chemistry
KW  - Radioimmunoassay
KW  - Neoplasm Transplantation
KW  - Immunoconjugates -- chemistry
KW  - Alpha Particles
KW  - Flow Cytometry
KW  - Maximum Tolerated Dose
KW  - Time Factors
KW  - Receptor, ErbB-2 -- metabolism
KW  - Receptor, ErbB-2 -- immunology
KW  - Peritoneal Diseases -- therapy
KW  - Radioimmunotherapy -- methods
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-27
N1  - Date created - 2005-10-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Drosophila ATM and Mre11 are essential for the G2/M checkpoint induced by low-dose irradiation.
AN  - 68728942; 16020777
AB  - Others have suggested recently that the conserved ATM checkpoint kinase is minimally involved in controlling the G(2)/M checkpoint in Drosophila that serves to prevent mitotic entry in the presence of DNA damage. Our data indicate that both ATM and its regulator Mre11 are important for the checkpoint and that their roles become essential when animals are challenged with a low dose of X rays or when they have compromised checkpoint function of the ATM-related ATR kinase.
JF  - Genetics
AU  - Bi, Xiaolin
AU  - Gong, Min
AU  - Srikanta, Deepa
AU  - Rong, Yikang S
AD  - Laboratory of Molecular Cell Biology, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 845
EP  - 847
VL  - 171
IS  - 2
SN  - 0016-6731, 0016-6731
KW  - Cell Cycle Proteins
KW  - 0
KW  - Drosophila Proteins
KW  - Protein-Serine-Threonine Kinases
KW  - EC 2.7.11.1
KW  - meiotic 41 protein, Drosophila
KW  - Endodeoxyribonucleases
KW  - EC 3.1.-
KW  - Mre11 protein, Drosophila
KW  - Index Medicus
KW  - Animals
KW  - Cell Cycle Proteins -- genetics
KW  - Models, Genetic
KW  - Protein-Serine-Threonine Kinases -- genetics
KW  - Dose-Response Relationship, Radiation
KW  - Mutagenesis
KW  - Mitosis -- genetics
KW  - Genes, cdc
KW  - Mitosis -- radiation effects
KW  - Endodeoxyribonucleases -- genetics
KW  - Drosophila Proteins -- genetics
KW  - Drosophila -- genetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-27
N1  - Date created - 2005-10-26
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Int J Radiat Biol. 1996 May;69(5):527-37 [8648240]
Curr Biol. 2004 Aug 10;14(15):1354-9 [15296752]
Genes Dev. 2000 Mar 15;14(6):666-78 [10733527]
Mol Cell Biol. 2001 Aug;21(15):5214-22 [11438675]
Genes Dev. 2001 Sep 1;15(17):2177-96 [11544175]
Mol Cell Biol. 2002 Feb;22(4):1049-59 [11809797]
Nat Cell Biol. 2002 Dec;4(12):993-7 [12447390]
Mol Cell. 2003 Jan;11(1):203-13 [12535533]
Proc Natl Acad Sci U S A. 2003 Apr 15;100(8):4696-701 [12672954]
Science. 2003 Jun 6;300(5625):1542-8 [12791985]
Genetics. 2003 Jun;164(2):589-601 [12807779]
Mol Cell Biol. 2004 Nov;24(22):10016-25 [15509802]
Cell. 1995 Sep 8;82(5):815-21 [7671309]
Mol Cell. 2003 Dec;12(6):1511-23 [14690604]
Genes Dev. 2004 Aug 1;18(15):1850-61 [15256487]
Curr Biol. 2004 Aug 10;14(15):1341-7 [15296750]
Curr Biol. 2004 Aug 10;14(15):1348-53 [15296751]
Cell. 1998 Jun 26;93(7):1183-93 [9657151]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Anticholinesterase and pharmacokinetic profile of phenserine in healthy elderly human subjects.
AN  - 68725880; 16248851
AB  - To evaluate the safety, maximum tolerated dose (MTD), pharmacokinetics (PK), and pharmacodynamics (PD) of the acetyl-selective anticholinesterase, phenserine tartrate, in healthy elderly subjects.
          32 healthy elderly volunteers received single oral doses of phenserine tartrate (5-20 mg). Physical and vital signs were monitored over the ensuing 24 hours. Analyses were performed on plasma samples to determine PK, and PD were assessed using an erythrocyte acetylcholinesterase (AChE) inhibition assay. No serious adverse events (AEs) occurred; the most common were headache and vomiting. The MTD of phenserine tartrate was 10 mg. The Cmax and AUC(0-24) of phenserine increased with dose, but neither were dose-proportional. Subjects receiving 10 mg of phenserine tartrate had a Cmax of 1.95 ng/mL at 1.5 hours, and the mean peak inhibition (Imax) of AChE was 26% (range: 18-34%) at 1.75 hours (tImax) following dosing. The half-life of AChE inhibition (tI1/2) was 11 hours. Evaluation of PK/PD relationships suggested a linear correlation between plasma phenserine concentration and AChE inhibition in the blood.
          Phenserine tartrate was safe and well tolerated when administered as a single oral dose of either 5 mg or 10 mg. An increase in the severity and frequency of AEs occurred at the 20 mg dose level.
JF  - Current Alzheimer research
AU  - Greig, Nigel H
AU  - Ruckle, Jon
AU  - Comer, Patrick
AU  - Brownell, Lidia
AU  - Holloway, Harold W
AU  - Flanagan, Douglas R
AU  - Canfield, Craig J
AU  - Burford, Robert G
AD  - Drug Design & Development Section, Laboratory of Neurosciences, National Institute on Aging, National Institutes of Health, Baltimore, MD 21224 USA. Greign@grc.nia.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 483
EP  - 492
VL  - 2
IS  - 4
SN  - 1567-2050, 1567-2050
KW  - Cholinesterase Inhibitors
KW  - 0
KW  - phenserine
KW  - Physostigmine
KW  - 9U1VM840SP
KW  - Acetylcholinesterase
KW  - EC 3.1.1.7
KW  - Index Medicus
KW  - Erythrocytes -- drug effects
KW  - Erythrocytes -- enzymology
KW  - Area Under Curve
KW  - Humans
KW  - Aged
KW  - Middle Aged
KW  - Maximum Tolerated Dose
KW  - Male
KW  - Female
KW  - Acetylcholinesterase -- drug effects
KW  - Cholinesterase Inhibitors -- adverse effects
KW  - Physostigmine -- analogs & derivatives
KW  - Cholinesterase Inhibitors -- pharmacokinetics
KW  - Physostigmine -- adverse effects
KW  - Physostigmine -- pharmacokinetics
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-30
N1  - Date created - 2005-10-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The impact of reward, punishment, and frustration on attention in pediatric bipolar disorder.
AN  - 68709106; 15953589
AB  - Theories in affective neuroscience suggest that mood disorders involve perturbations in attention-emotion interactions. We tested the hypothesis that frustration adversely impacts attention and behavior in children with bipolar disorder (BPD).
          Thirty-five children with BPD and 26 normal control subjects completed: 1) a Posner attention task with feedback but no contingencies; 2) an affective Posner with contingencies; and 3) an affective Posner that used rigged feedback to induce frustration. Reaction time (RT) and event-related potential (ERP) data were collected. At baseline (task 1), there were no between-group differences in behavior or ERPs. Children with BPD exhibited reduced parietal P3 amplitude on task 3 only. On trials occurring after negative feedback, control subjects showed decreased RT when contingencies were introduced (task 2), whereas BPD subjects did not.
          The introduction of contingencies was associated with impaired performance of children with BPD, suggesting deficits in their ability to adapt to changing contingencies. In addition, frustration was associated with disrupted attention allocation in children with BPD. We hypothesize that children with BPD inappropriately deployed attention to their internal frustration rather than to the task, causing impaired performance.
JF  - Biological psychiatry
AU  - Rich, Brendan A
AU  - Schmajuk, Mariana
AU  - Perez-Edgar, Koraly E
AU  - Pine, Daniel S
AU  - Fox, Nathan A
AU  - Leibenluft, Ellen
AD  - Pediatrics and Developmental Neuropsychiatry Branch, Mood and Anxiety Program, National Institute of Mental Health, National Institutes of Health, Bethesda, MD 20892-1255, USA. brendanrich@mail.nih.gov
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 532
EP  - 539
VL  - 58
IS  - 7
SN  - 0006-3223, 0006-3223
KW  - Antimanic Agents
KW  - 0
KW  - Index Medicus
KW  - Reproducibility of Results
KW  - Affect -- physiology
KW  - Humans
KW  - Antimanic Agents -- adverse effects
KW  - Electroencephalography
KW  - Evoked Potentials -- physiology
KW  - Child
KW  - Reaction Time -- physiology
KW  - Psychomotor Performance -- physiology
KW  - Psychiatric Status Rating Scales
KW  - Emotions -- physiology
KW  - Antimanic Agents -- therapeutic use
KW  - Adolescent
KW  - Female
KW  - Male
KW  - Reward
KW  - Punishment
KW  - Frustration
KW  - Bipolar Disorder -- drug therapy
KW  - Bipolar Disorder -- psychology
KW  - Attention -- physiology
KW  - Bipolar Disorder -- complications
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-30
N1  - Date created - 2005-10-21
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Complementary and alternative medicine patients are talking about: black cohosh.
AN  - 68707766; 16235591
JF  - Clinical journal of oncology nursing
AU  - Lee, Colleen O
AD  - Office of Cancer Complementary and Alternative Medicine at the National Cancer Institute in Bethesda, MD, USA. leeco@mail.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 628
EP  - 629
VL  - 9
IS  - 5
SN  - 1092-1095, 1092-1095
KW  - Nursing
KW  - United States
KW  - Patient Education as Topic
KW  - Evidence-Based Medicine
KW  - Drug Interactions
KW  - United States Food and Drug Administration
KW  - Menstruation Disturbances -- drug therapy
KW  - Drug and Narcotic Control
KW  - Menopause -- drug effects
KW  - Humans
KW  - Clinical Trials as Topic
KW  - Patient Selection
KW  - Female
KW  - Phytotherapy -- methods
KW  - Cimicifuga
KW  - Phytotherapy -- adverse effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-15
N1  - Date created - 2005-10-20
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - WMC-79, a potent agent against colon cancers, induces apoptosis through a p53-dependent pathway.
AN  - 68696927; 16227412
AB  - WMC-79 is a synthetic agent with potent activity against colon and hematopoietic tumors. In vitro, the agent is most potent against colon cancer cells that carry the wild-type p53 tumor suppressor gene (HCT-116 and RKO cells: GI50<1 nmol/L, LC50 approximately 40 nmol/L). Growth arrest of HCT-116 and RKO cells occurs at the G1 and G2-M check points at sublethal concentrations (10 nmol/L) but the entire cell population was killed at 100 nmol/L. WMC-79 is localized to the nucleus where it binds to DNA. We hypothesized that WMC-79 binding to DNA is recognized as an unrepairable damage in the tumor cells, which results in p53 activation. This triggers transcriptional up-regulation of p53-dependent genes involved in replication, cell cycle progression, growth arrest, and apoptosis as evidenced by DNA microarrays. The change in the transcriptional profile of HCT-116 cells is followed by a change in the levels of cell cycle regulatory proteins and apoptosis. The recruitment of the p53-dependent apoptosis pathway was suggested by the up-regulation of p53, p21, Bax, DR-4, DR-5, and p53 phosphorylated on Ser15; down-regulation of Bcl-2; and activation of caspase-8, -9, -7, and -3 in cells treated with 100 nmol/L WMC-79. Apoptosis was also evident from the flow cytometric studies of drug-treated HCT-116 cells as well as from the appearance of nuclear fragmentation. However, whereas this pathway is important in wild-type p53 colon tumors, other pathways are also in operation because colon cancer cell lines in which the p53 gene is mutated are also affected by higher concentrations of WMC-79.
JF  - Molecular cancer therapeutics
AU  - Kosakowska-Cholody, Teresa
AU  - Cholody, W Marek
AU  - Monks, Anne
AU  - Woynarowska, Barbara A
AU  - Michejda, Christopher J
AD  - Molecular Aspects of Drug Design, Structural Biophysics Laboratory, Center for Cancer Research, National Cancer Institute at Frederick, Frederick, MD 21702, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1617
EP  - 1627
VL  - 4
IS  - 10
SN  - 1535-7163, 1535-7163
KW  - Heterocyclic Compounds, 4 or More Rings
KW  - 0
KW  - RNA, Messenger
KW  - Tumor Suppressor Protein p53
KW  - WMC-79
KW  - Index Medicus
KW  - Microscopy, Confocal
KW  - Blotting, Western
KW  - Humans
KW  - Cell Line, Tumor
KW  - HCT116 Cells
KW  - RNA, Messenger -- genetics
KW  - Gene Expression Regulation, Neoplastic -- drug effects
KW  - RNA, Messenger -- biosynthesis
KW  - Cell Cycle -- drug effects
KW  - Tumor Suppressor Protein p53 -- physiology
KW  - Colonic Neoplasms -- genetics
KW  - Colonic Neoplasms -- drug therapy
KW  - Apoptosis -- drug effects
KW  - Heterocyclic Compounds, 4 or More Rings -- pharmacology
KW  - Colonic Neoplasms -- metabolism
KW  - Heterocyclic Compounds, 4 or More Rings -- pharmacokinetics
KW  - Colonic Neoplasms -- pathology
KW  - Tumor Suppressor Protein p53 -- deficiency
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Molecular+cancer+therapeutics&rft.atitle=WMC-79%2C+a+potent+agent+against+colon+cancers%2C+induces+apoptosis+through+a+p53-dependent+pathway.&rft.au=Kosakowska-Cholody%2C+Teresa%3BCholody%2C+W+Marek%3BMonks%2C+Anne%3BWoynarowska%2C+Barbara+A%3BMichejda%2C+Christopher+J&rft.aulast=Kosakowska-Cholody&rft.aufirst=Teresa&rft.date=2005-10-01&rft.volume=4&rft.issue=10&rft.spage=1617&rft.isbn=&rft.btitle=&rft.title=Molecular+cancer+therapeutics&rft.issn=15357163&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-18
N1  - Date created - 2005-10-17
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Suppression of tumor cell invasion by cyclooxygenase inhibitors is mediated by thrombospondin-1 via the early growth response gene Egr-1.
AN  - 68696277; 16227405
AB  - Cyclooxygenase (COX) inhibitors have antitumorigenic activity and increase the expression of the early growth response gene Egr-1, a tumor suppressor gene and transcription factor. In this study, we have investigated the gene regulatory and anti-invasive activity of two traditional nonsteroidal anti-inflammatory drugs (NSAID), sulindac sulfide and indomethacin. These compounds inhibited tumor cell invasion and induced Egr-1 expression in lung adenocarcinoma A549 cells. Overexpression of Egr-1 reduced cellular invasion in the Matrigel system, whereas suppression of Egr-1 by small interference RNA (siRNA) attenuated the inhibition of Matrigel invasion by these compounds, indicating that Egr-1 is responsible for the decrease in invasion reported following treatment with NSAIDs. Egr-1-overexpressing cells were analyzed for genes involved in invasion and metastasis. Thrombospondin-1 (TSP-1) an antiangiogenic and anti-invasion protein was up-regulated by Egr-1 overexpression, which was confirmed following treatment with sulindac sulfide. Furthermore, the induction of TSP-1 by sulindac sulfide was blocked by Egr-1 siRNA. When TSP-1 was sequestered by the addition of anti-TSP-1 antibody, the inhibition of invasion by sulindac sulfide was attenuated, indicating that TSP-1 is involved in the inhibition of invasion by NSAIDs. We used the Min mouse model to determine if sulindac sulfide would increase Egr-1 and TSP-1 in vivo, because this model is widely used to study the effects of NSAIDs on tumor formation. Treatment of Min mice with concentrations of sulindac sulfide that inhibit tumor formation increased the expression of Egr-1 and TSP-1 in colonic tissues and in the polyps of these mice. This is the first report suggesting that COX inhibitors suppress tumor cell invasion via TSP-1, which occurs downstream of Egr-1.
JF  - Molecular cancer therapeutics
AU  - Moon, Yuseok
AU  - Bottone, Frank G
AU  - McEntee, Michael F
AU  - Eling, Thomas E
AD  - Eicosanoid Biochemistry Section, Laboratory of Molecular Carcinogenesis, National Institute of Environmental Health Sciences, 111 T.W. Alexander Drive, Research Triangle Park, NC 27709, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1551
EP  - 1558
VL  - 4
IS  - 10
SN  - 1535-7163, 1535-7163
KW  - Anti-Inflammatory Agents, Non-Steroidal
KW  - 0
KW  - Cyclooxygenase Inhibitors
KW  - Early Growth Response Protein 1
KW  - RNA, Messenger
KW  - RNA, Small Interfering
KW  - Thrombospondin 1
KW  - Sulindac
KW  - 184SNS8VUH
KW  - sulindac sulfide
KW  - 6UVA8S2DEY
KW  - Indomethacin
KW  - XXE1CET956
KW  - Index Medicus
KW  - Neoplasm Invasiveness
KW  - Animals
KW  - Humans
KW  - Sulindac -- pharmacology
KW  - Sulindac -- analogs & derivatives
KW  - RNA, Small Interfering -- genetics
KW  - Mice
KW  - Cell Line, Tumor
KW  - RNA, Messenger -- genetics
KW  - RNA, Messenger -- biosynthesis
KW  - Indomethacin -- pharmacology
KW  - Anti-Inflammatory Agents, Non-Steroidal -- pharmacology
KW  - Adenocarcinoma -- metabolism
KW  - Colorectal Neoplasms -- metabolism
KW  - Lung Neoplasms -- drug therapy
KW  - Thrombospondin 1 -- metabolism
KW  - Early Growth Response Protein 1 -- genetics
KW  - Adenocarcinoma -- genetics
KW  - Colorectal Neoplasms -- genetics
KW  - Colorectal Neoplasms -- drug therapy
KW  - Thrombospondin 1 -- biosynthesis
KW  - Adenocarcinoma -- pathology
KW  - Cyclooxygenase Inhibitors -- pharmacology
KW  - Genes, Tumor Suppressor -- drug effects
KW  - Colorectal Neoplasms -- pathology
KW  - Early Growth Response Protein 1 -- biosynthesis
KW  - Lung Neoplasms -- genetics
KW  - Genes, Tumor Suppressor -- physiology
KW  - Adenocarcinoma -- drug therapy
KW  - Lung Neoplasms -- pathology
KW  - Lung Neoplasms -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-18
N1  - Date created - 2005-10-17
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Advances in antifungal therapy.
AN  - 68688461; 16220093
JF  - The Pediatric infectious disease journal
AU  - Pannaraj, Pia S
AU  - Walsh, Thomas J
AU  - Baker, Carol J
AD  - National Cancer Institute, National Institutes of Health, Bethesda, MD, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 921
EP  - 922
VL  - 24
IS  - 10
SN  - 0891-3668, 0891-3668
KW  - Antifungal Agents
KW  - 0
KW  - ER 30346
KW  - Echinocandins
KW  - Fungal Proteins
KW  - Lipopeptides
KW  - Lipoproteins
KW  - Peptides, Cyclic
KW  - Pyrimidines
KW  - Thiazoles
KW  - Triazoles
KW  - echinocandin B
KW  - 54651-05-7
KW  - posaconazole
KW  - 6TK1G07BHZ
KW  - anidulafungin
KW  - 9HLM53094I
KW  - caspofungin
KW  - F0XDI6ZL63
KW  - Voriconazole
KW  - JFU09I87TR
KW  - micafungin
KW  - R10H71BSWG
KW  - Index Medicus
KW  - Fungal Proteins -- therapeutic use
KW  - Pyrimidines -- adverse effects
KW  - Animals
KW  - Lipoproteins -- pharmacology
KW  - Pyrimidines -- therapeutic use
KW  - Lipoproteins -- therapeutic use
KW  - Humans
KW  - Lipoproteins -- adverse effects
KW  - Aged
KW  - Child
KW  - Infant
KW  - Peptides, Cyclic -- therapeutic use
KW  - Aged, 80 and over
KW  - Adult
KW  - Treatment Outcome
KW  - Fungal Proteins -- adverse effects
KW  - Triazoles -- therapeutic use
KW  - Peptides, Cyclic -- pharmacokinetics
KW  - Fungal Proteins -- pharmacology
KW  - Adolescent
KW  - Peptides, Cyclic -- pharmacology
KW  - Peptides, Cyclic -- adverse effects
KW  - Clinical Trials as Topic
KW  - Infant, Newborn
KW  - Pyrimidines -- pharmacology
KW  - Triazoles -- pharmacology
KW  - Triazoles -- adverse effects
KW  - Thiazoles -- adverse effects
KW  - Pyrimidines -- pharmacokinetics
KW  - Triazoles -- pharmacokinetics
KW  - Child, Preschool
KW  - Thiazoles -- pharmacology
KW  - Middle Aged
KW  - Thiazoles -- therapeutic use
KW  - Antifungal Agents -- pharmacokinetics
KW  - Antifungal Agents -- adverse effects
KW  - Mycoses -- microbiology
KW  - Mycoses -- drug therapy
KW  - Antifungal Agents -- therapeutic use
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=The+Pediatric+infectious+disease+journal&rft.atitle=Advances+in+antifungal+therapy.&rft.au=Pannaraj%2C+Pia+S%3BWalsh%2C+Thomas+J%3BBaker%2C+Carol+J&rft.aulast=Pannaraj&rft.aufirst=Pia&rft.date=2005-10-01&rft.volume=24&rft.issue=10&rft.spage=921&rft.isbn=&rft.btitle=&rft.title=The+Pediatric+infectious+disease+journal&rft.issn=08913668&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-05
N1  - Date created - 2005-10-12
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Proteomic signature of myeloproliferation and neutrophilia: analysis of serum and plasma from healthy subjects given granulocyte colony-stimulating factor.
AN  - 68681850; 16219533
AB  - Proteomic analysis could improve our understanding of the mechanisms and consequences of myeloproliferation. Healthy subjects treated with granulocyte colony-stimulating factor (G-CSF) were used as a model of myeloproliferation.
          Levels of 80 soluble factors were measured by enzyme-linked immunosorbent assay before and after 5 days of G-CSF. Both serum and plasma levels were measured to generate a comprehensive profile and determine whether serum or plasma best portrays biological and physiological changes. Comparison of samples collected prior to G-CSF demonstrated that 44 factors differed between serum and plasma. Concentrations of several growth factors and chemokines were greater in serum than in plasma, while the opposite was true for several interleukins. Following G-CSF serum levels of 14 factors and plasma levels of 15 factors changed. Eleven increased in both serum and plasma, including cell adhesion molecules (vascular cell adhesion molecule-1, E-selectin, and L-selectin), matrix metalloproteases (MMP-1, -8, and -13), cytokine receptors (tumor necrosis factor receptor 1 and 2, and interleukin-2 receptor), the acute phase reactant, serum amyloid A, and a growth factor, hepatocyte growth factor.
          Some protein levels differ markedly in serum and plasma. Myeloproliferation is associated with changes in the levels of several proteases, adhesion molecules, and cytokines.
JF  - Experimental hematology
AU  - Stroncek, David
AU  - Slezak, Stefanie
AU  - Khuu, Hanh
AU  - Basil, Christopher
AU  - Tisdale, John
AU  - Leitman, Susan F
AU  - Marincola, Francesco M
AU  - Panelli, Monica C
AD  - Department of Transfusion Medicine, Warren G. Magnuson Clinical Center, National Institutes of Health, Bethesda, MD 20892, USA. dstroncek@cc.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1109
EP  - 1117
VL  - 33
IS  - 10
SN  - 0301-472X, 0301-472X
KW  - Blood Proteins
KW  - 0
KW  - Recombinant Proteins
KW  - Granulocyte Colony-Stimulating Factor
KW  - 143011-72-7
KW  - Filgrastim
KW  - PVI5M0M1GW
KW  - Index Medicus
KW  - Enzyme-Linked Immunosorbent Assay -- methods
KW  - Humans
KW  - Male
KW  - Female
KW  - Granulocyte Colony-Stimulating Factor -- blood
KW  - Leukocytosis -- chemically induced
KW  - Leukocytosis -- blood
KW  - Granulocyte Colony-Stimulating Factor -- administration & dosage
KW  - Blood Proteins -- analysis
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Experimental+hematology&rft.atitle=Proteomic+signature+of+myeloproliferation+and+neutrophilia%3A+analysis+of+serum+and+plasma+from+healthy+subjects+given+granulocyte+colony-stimulating+factor.&rft.au=Stroncek%2C+David%3BSlezak%2C+Stefanie%3BKhuu%2C+Hanh%3BBasil%2C+Christopher%3BTisdale%2C+John%3BLeitman%2C+Susan+F%3BMarincola%2C+Francesco+M%3BPanelli%2C+Monica+C&rft.aulast=Stroncek&rft.aufirst=David&rft.date=2005-10-01&rft.volume=33&rft.issue=10&rft.spage=1109&rft.isbn=&rft.btitle=&rft.title=Experimental+hematology&rft.issn=0301472X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-02
N1  - Date created - 2005-10-12
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Targeting the epigenome for the treatment and prevention of lung cancer.
AN  - 68673352; 16210090
AB  - Alterations in chromatin structure resulting from aberrant DNA methylation and perturbations of the histone code profoundly influence gene expression during pulmonary carcinogenesis. Recent studies indicate that DNA demethylating agents and histone deacetylase (HDAC) inhibitors synergistically induce gene expression and apoptosis in cultured lung cancer cells, and prevent lung cancer development in animals following exposure to tobacco carcinogens. Preliminary clinical trials have established proof of principle regarding the use of DNA demethylating agents and HDAC inhibitors for enhancing immunogenicity and apoptosis of lung cancer cells, and have revealed the complexities concerning the mechanisms by which chromatin remodeling agents mediate antitumor effects in vivo. These data support additional investigations pertaining to the epigenetics of lung cancer, and the evaluation of chromatin remodeling agents for the treatment and prevention of this disease.
JF  - Seminars in oncology
AU  - Schrump, David S
AU  - Nguyen, Dao M
AD  - Thoracic Oncology Section, Surgery Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, 10 Center Drive, Bethesda, MD 20892-1201, USA. David_Schrump@nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 488
EP  - 502
VL  - 32
IS  - 5
SN  - 0093-7754, 0093-7754
KW  - Antineoplastic Agents
KW  - 0
KW  - Chromatin
KW  - Enzyme Inhibitors
KW  - Histone Deacetylase Inhibitors
KW  - Histones
KW  - Index Medicus
KW  - Animals
KW  - Apoptosis
KW  - Chromatin -- metabolism
KW  - Humans
KW  - Clinical Trials as Topic
KW  - Cell Line, Tumor
KW  - DNA Methylation
KW  - Histones -- metabolism
KW  - Enzyme Inhibitors -- pharmacology
KW  - Flow Cytometry
KW  - Time Factors
KW  - Antineoplastic Agents -- pharmacology
KW  - Gene Expression Regulation, Neoplastic
KW  - Lung Neoplasms -- prevention & control
KW  - Lung Neoplasms -- drug therapy
KW  - Lung Neoplasms -- genetics
KW  - Epigenesis, Genetic
KW  - Lung Neoplasms -- metabolism
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68673352?accountid=14244
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-08
N1  - Date created - 2005-10-07
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Amelioration of inflammatory arthritis by targeting the pre-ligand assembly domain of tumor necrosis factor receptors.
AN  - 68668607; 16170321
AB  - Tumor necrosis factor (TNF)-alpha has an important role in the pathogenesis of autoimmune and inflammatory diseases such as rheumatoid and septic arthritis. The biological effects of TNF-alpha are mediated by binding to TNF receptors TNFR1 (also known as P60) or TNFR2 (also known as P80). The pre-ligand assembly domain (PLAD) is a portion of the extracellular region of TNFRs that mediates receptor-chain association essential for signaling. We found that soluble versions of PLAD, especially those derived from P60, block the biochemical effects of TNF-alpha in vitro and potently inhibit arthritis in animal models. Thus, targeting the PLAD may have clinical value in the treatment of human arthritis and other disorders involving receptors of the TNFR superfamily.
JF  - Nature medicine
AU  - Deng, Guo-Min
AU  - Zheng, Lixin
AU  - Chan, Francis Ka-Ming
AU  - Lenardo, Michael
AD  - Laboratory of Immunology, Building 10, Room 11N311, 10 Center Drive, MSC 1892, National Institute of Allergy and Infectious Disease, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1066
EP  - 1072
VL  - 11
IS  - 10
SN  - 1078-8956, 1078-8956
KW  - Ligands
KW  - 0
KW  - Receptors, Tumor Necrosis Factor
KW  - Receptors, Tumor Necrosis Factor, Type I
KW  - Receptors, Tumor Necrosis Factor, Type II
KW  - Recombinant Fusion Proteins
KW  - Tumor Necrosis Factor-alpha
KW  - Collagen
KW  - 9007-34-5
KW  - DNA
KW  - 9007-49-2
KW  - Index Medicus
KW  - Receptors, Tumor Necrosis Factor, Type I -- antagonists & inhibitors
KW  - Animals
KW  - Receptors, Tumor Necrosis Factor, Type I -- therapeutic use
KW  - DNA -- pharmacology
KW  - Mice
KW  - Receptors, Tumor Necrosis Factor, Type I -- chemistry
KW  - Mice, Transgenic
KW  - Cell Death -- drug effects
KW  - Receptors, Tumor Necrosis Factor, Type II -- metabolism
KW  - Binding Sites
KW  - Mice, Knockout
KW  - Recombinant Fusion Proteins -- metabolism
KW  - Receptors, Tumor Necrosis Factor, Type II -- therapeutic use
KW  - Receptors, Tumor Necrosis Factor, Type I -- metabolism
KW  - Binding, Competitive
KW  - DNA -- genetics
KW  - Recombinant Fusion Proteins -- genetics
KW  - CpG Islands -- genetics
KW  - Receptors, Tumor Necrosis Factor, Type II -- antagonists & inhibitors
KW  - Protein Structure, Tertiary
KW  - Receptors, Tumor Necrosis Factor, Type II -- chemistry
KW  - Cell Line
KW  - Arthritis -- pathology
KW  - Receptors, Tumor Necrosis Factor -- therapeutic use
KW  - Receptors, Tumor Necrosis Factor -- metabolism
KW  - Arthritis -- chemically induced
KW  - Tumor Necrosis Factor-alpha -- metabolism
KW  - Arthritis -- drug therapy
KW  - Receptors, Tumor Necrosis Factor -- antagonists & inhibitors
KW  - Receptors, Tumor Necrosis Factor -- chemistry
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68668607?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Nature+medicine&rft.atitle=Amelioration+of+inflammatory+arthritis+by+targeting+the+pre-ligand+assembly+domain+of+tumor+necrosis+factor+receptors.&rft.au=Deng%2C+Guo-Min%3BZheng%2C+Lixin%3BChan%2C+Francis+Ka-Ming%3BLenardo%2C+Michael&rft.aulast=Deng&rft.aufirst=Guo-Min&rft.date=2005-10-01&rft.volume=11&rft.issue=10&rft.spage=1066&rft.isbn=&rft.btitle=&rft.title=Nature+medicine&rft.issn=10788956&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-07
N1  - Date created - 2005-10-07
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Therapeutics development for triplet repeat expansion diseases.
AN  - 68664747; 16205715
AB  - The underlying genetic mutations for many inherited neurodegenerative disorders have been identified in recent years. One frequent type of mutation is trinucleotide repeat expansion. Depending on the location of the repeat expansion, the mutation might result in a loss of function of the disease gene, a toxic gain of function or both. Disease gene identification has led to the development of model systems for investigating disease mechanisms and evaluating treatments. Examination of experimental findings reveals similarities in disease mechanisms as well as possibilities for treatment.
JF  - Nature reviews. Genetics
AU  - Di Prospero, Nicholas A
AU  - Fischbeck, Kenneth H
AD  - Neurogenetics Branch, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892-3705, USA. DiProsperN@ninds.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 756
EP  - 765
VL  - 6
IS  - 10
SN  - 1471-0056, 1471-0056
KW  - Peptides
KW  - 0
KW  - polyalanine
KW  - 25191-17-7
KW  - polyglutamine
KW  - 26700-71-0
KW  - Index Medicus
KW  - Fragile X Syndrome -- genetics
KW  - Humans
KW  - Gene Expression Regulation
KW  - Peptides -- genetics
KW  - Huntington Disease -- genetics
KW  - Trinucleotide Repeats
KW  - Heredodegenerative Disorders, Nervous System -- therapy
KW  - Heredodegenerative Disorders, Nervous System -- genetics
KW  - Mutation
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-10-19
N1  - Date created - 2005-10-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Fundamental flaws of hormesis for public health decisions.
AN  - 68663711; 16203233
AB  - Hormesis (defined operationally as low-dose stimulation, high-dose inhibition) is often used to promote the notion that while high-level exposures to toxic chemicals could be detrimental to human health, low-level exposures would be beneficial. Some proponents claim hormesis is an adaptive, generalizable phenomenon and argue that the default assumption for risk assessments should be that toxic chemicals induce stimulatory (i.e., "beneficial") effects at low exposures. In many cases, nonmonotonic dose-response curves are called hormetic responses even in the absence of any mechanistic characterization of that response. Use of the term "hormesis," with its associated descriptors, distracts from the broader and more important questions regarding the frequency and interpretation of nonmonotonic dose responses in biological systems. A better understanding of the biological basis and consequences of nonmonotonic dose-response curves is warranted for evaluating human health risks. The assumption that hormesis is generally adaptive is an oversimplification of complex biological processes. Even if certain low-dose effects were sometimes considered beneficial, this should not influence regulatory decisions to allow increased environmental exposures to toxic and carcinogenic agents, given factors such as interindividual differences in susceptibility and multiplicity in exposures. In this commentary we evaluate the hormesis hypothesis and potential adverse consequences of incorporating low-dose beneficial effects into public health decisions. Key words: biphasic dose response, hormesis, individual susceptibility, low-dose exposures, nonmonotonic dose response, nonlinear dose response, public health, regulation, risk assessment.
JF  - Environmental health perspectives
AU  - Thayer, Kristina A
AU  - Melnick, Ronald
AU  - Burns, Kathy
AU  - Davis, Devra
AU  - Huff, James
AD  - National Institute of Environmental Health Sciences, National Institutes of Health, Department of Health and Human Services, Research Triangle Park, North Carolina, USA. thayer@niehs.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1271
EP  - 1276
VL  - 113
IS  - 10
SN  - 0091-6765, 0091-6765
KW  - Index Medicus
KW  - Dose-Response Relationship, Drug
KW  - Humans
KW  - Health Status
KW  - Occupational Exposure
KW  - Public Health
KW  - Environmental Exposure
KW  - Decision Making, Organizational
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-23
N1  - Date created - 2005-10-05
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
J Fam Pract. 2004 Feb;53(2):146-50 [14764301]
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Alcohol Alcohol. 2002 Sep-Oct;37(5):409-15 [12217928]
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N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The need for exposure health sciences.
AN  - 68659506; 16203220
JF  - Environmental health perspectives
AU  - Schwartz, David A
AU  - Weis, Brenda
AU  - Wilson, Samuel H
AD  - NIEHS, Durham, North Carolina, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1
VL  - 113
IS  - 10
SN  - 0091-6765, 0091-6765
KW  - Index Medicus
KW  - Genome, Human
KW  - Humans
KW  - Research
KW  - Risk Assessment
KW  - Health Status
KW  - Environmental Exposure
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68659506?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Environmental+health+perspectives&rft.atitle=The+need+for+exposure+health+sciences.&rft.au=Schwartz%2C+David+A%3BWeis%2C+Brenda%3BWilson%2C+Samuel+H&rft.aulast=Schwartz&rft.aufirst=David&rft.date=2005-10-01&rft.volume=113&rft.issue=10&rft.spage=A650&rft.isbn=&rft.btitle=&rft.title=Environmental+health+perspectives&rft.issn=00916765&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-23
N1  - Date created - 2005-10-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Carboxylesterase isoform 2 mRNA expression in peripheral blood mononuclear cells is a predictive marker of the irinotecan to SN38 activation step in colorectal cancer patients.
AN  - 68655438; 16203781
AB  - Irinotecan (CPT11) is a prodrug activated in humans mainly by carboxylesterase 2 (CES2) generating the SN38 metabolite responsible for the drug efficacy and toxicity. The interpatients variability in CPT11 activation step could cause unpredictable toxicity. To identify a predictive molecular marker for CPT11 activation in cancer patients, we investigated the CES2 mRNA expression in peripheral blood mononuclear cells (PBMC) and correlated it to CPT11 activation rate, toxic effects, and response.
          Forty-five colorectal cancer patients were treated with a CPT11-including regimen (FOLFIRI). CES2 mRNA expression in PBMC was quantified by reverse transcription-PCR in real time. Plasma concentrations of CPT11, SN38, and SN38-glucuronide were determined by high-performance liquid chromatography and the pharmacokinetic variables calculated adopting the noncompartmental model. Toxicity was evaluated by the National Cancer Institute Common Toxicity Criteria scale and response by the WHO criteria. A high interindividual variability in CES2 mRNA relative expression was observed (median, 1.45; range, 0.01-28.21). CES2 mRNA expression level was significantly associated with CPT11 activation ratio [(AUC(SN38) + AUC(SN38G))/AUC(CPT11)]. Patients with CES2 mRNA expression above the median cutoff value presented an activation ratio higher (median, 0.25; range, 0.15-0.42) than those with CES2 mRNA below the median (median, 0.20; range, 0.10-0.40; P = 0.013). This was associated with a nonsignificant trend of 1.34-fold increase of SN38 AUC in the group of patients with high CES2 mRNA expression (mean, 1.03 +/- 0.62 versus 0.77 +/- 0.32 micromol/L hour). Eight of 23 high CES2 mRNA-expressing patients (34.8%) developed grade 3 to 4 neutropenia or diarrhea compared with 2 of 22 (9.1%) in the low CES2-expressing group (P = 0.071). Our data support a predictive power of CES2 mRNA expression in PBMC for the activation rate of CPT11.
JF  - Clinical cancer research : an official journal of the American Association for Cancer Research
AU  - Cecchin, Erika
AU  - Corona, Giuseppe
AU  - Masier, Sara
AU  - Biason, Paola
AU  - Cattarossi, Giulio
AU  - Frustaci, Sergio
AU  - Buonadonna, Angela
AU  - Colussi, Annamaria
AU  - Toffoli, Giuseppe
AD  - Experimental and Clinical Pharmacology, Centro di Riferimento Oncologico, National Cancer Institute, Aviano, Italy.
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 6901
EP  - 6907
VL  - 11
IS  - 19 Pt 1
SN  - 1078-0432, 1078-0432
KW  - Protein Isoforms
KW  - 0
KW  - RNA, Messenger
KW  - irinotecan
KW  - 0H43101T0J
KW  - Carboxylesterase
KW  - EC 3.1.1.1
KW  - DNA Topoisomerases, Type I
KW  - EC 5.99.1.2
KW  - Leucovorin
KW  - Q573I9DVLP
KW  - Fluorouracil
KW  - U3P01618RT
KW  - Camptothecin
KW  - XT3Z54Z28A
KW  - Index Medicus
KW  - Area Under Curve
KW  - Humans
KW  - Leucovorin -- administration & dosage
KW  - Aged
KW  - Antineoplastic Combined Chemotherapy Protocols -- administration & dosage
KW  - Reverse Transcriptase Polymerase Chain Reaction
KW  - Chromatography, High Pressure Liquid
KW  - Fluorouracil -- administration & dosage
KW  - Kinetics
KW  - Middle Aged
KW  - Antineoplastic Combined Chemotherapy Protocols -- therapeutic use
KW  - Time Factors
KW  - DNA Topoisomerases, Type I -- metabolism
KW  - Female
KW  - Male
KW  - RNA, Messenger -- metabolism
KW  - Camptothecin -- pharmacology
KW  - Colorectal Neoplasms -- metabolism
KW  - Leukocytes, Mononuclear -- metabolism
KW  - Camptothecin -- analogs & derivatives
KW  - Colorectal Neoplasms -- drug therapy
KW  - Leukocytes, Mononuclear -- cytology
KW  - Camptothecin -- administration & dosage
KW  - Carboxylesterase -- chemistry
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+cancer+research+%3A+an+official+journal+of+the+American+Association+for+Cancer+Research&rft.atitle=Carboxylesterase+isoform+2+mRNA+expression+in+peripheral+blood+mononuclear+cells+is+a+predictive+marker+of+the+irinotecan+to+SN38+activation+step+in+colorectal+cancer+patients.&rft.au=Cecchin%2C+Erika%3BCorona%2C+Giuseppe%3BMasier%2C+Sara%3BBiason%2C+Paola%3BCattarossi%2C+Giulio%3BFrustaci%2C+Sergio%3BBuonadonna%2C+Angela%3BColussi%2C+Annamaria%3BToffoli%2C+Giuseppe&rft.aulast=Cecchin&rft.aufirst=Erika&rft.date=2005-10-01&rft.volume=11&rft.issue=19+Pt+1&rft.spage=6901&rft.isbn=&rft.btitle=&rft.title=Clinical+cancer+research+%3A+an+official+journal+of+the+American+Association+for+Cancer+Research&rft.issn=10780432&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-08
N1  - Date created - 2005-10-05
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment In:
Clin Cancer Res. 2006 Mar 15;12(6):1942; author reply 1942-3 [16551882]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Regulating SWI/SNF subunit levels via protein-protein interactions and proteasomal degradation: BAF155 and BAF170 limit expression of BAF57.
AN  - 68654957; 16199878
AB  - The mammalian SWI/SNF chromatin remodeling complex, whose function is of critical importance in transcriptional regulation, contains approximately 10 protein components. The expression levels of the core SWI/SNF subunits, including BRG1/Brm, BAF155, BAF170, BAF60, hSNF/Ini1, and BAF57, are stoichiometric, with few to no unbound molecules in the cell. Here we report that exogenous expression of the wild type or certain deletion mutants of BAF57, a key subunit that mediates the interaction between the remodeling complex and transcription factors, results in diminished expression of endogenous BAF57. This down-regulation process is mediated by an increase in proteasome-dependent degradation of the BAF57 protein. Furthermore, the protein levels of BAF155/170 dictate the maximum cellular amount of BAF57. We mapped the domains responsible for the interaction between BAF57 and BAF155 and demonstrated that protein-protein interactions between them play an important role in this regulatory process. These findings provide insights into the physiological mechanisms responsible for maintaining the proper stoichiometric levels of the protein components comprising multimeric enzyme complexes.
JF  - Molecular and cellular biology
AU  - Chen, Jianguang
AU  - Archer, Trevor K
AD  - Chromatin and Gene Expression Section, Laboratory of Molecular Carcinogenesis, National Institute of Environmental Health Sciences, Research Triangle Park, NC 27709, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 9016
EP  - 9027
VL  - 25
IS  - 20
SN  - 0270-7306, 0270-7306
KW  - Chromosomal Proteins, Non-Histone
KW  - 0
KW  - DNA-Binding Proteins
KW  - Multiprotein Complexes
KW  - Protein Subunits
KW  - Recombinant Proteins
KW  - SMARCC1 protein, human
KW  - SMARCC2 protein, human
KW  - SMARCE1 protein, human
KW  - Transcription Factors
KW  - DNA
KW  - 9007-49-2
KW  - Proteasome Endopeptidase Complex
KW  - EC 3.4.25.1
KW  - Index Medicus
KW  - Humans
KW  - Recombinant Proteins -- genetics
KW  - Protein Binding
KW  - Base Sequence
KW  - Down-Regulation
KW  - Proteasome Endopeptidase Complex -- metabolism
KW  - Recombinant Proteins -- metabolism
KW  - DNA -- genetics
KW  - Recombinant Proteins -- chemistry
KW  - Protein Structure, Tertiary
KW  - Cell Line
KW  - Sequence Deletion
KW  - DNA-Binding Proteins -- chemistry
KW  - Transcription Factors -- metabolism
KW  - Transcription Factors -- chemistry
KW  - DNA-Binding Proteins -- genetics
KW  - Transcription Factors -- genetics
KW  - DNA-Binding Proteins -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-21
N1  - Date created - 2005-10-03
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Nature. 2002 Jul 11;418(6894):195-9 [12110891]
Curr Opin Genet Dev. 2002 Feb;12(1):73-9 [11790558]
Genome Biol. 2002 Jul 24;3(8):RESEARCH0039 [12186646]
Nat Struct Biol. 2003 Feb;10(2):141-5 [12524530]
Rev Med Virol. 2003 Mar-Apr;13(2):99-110 [12627393]
Curr Opin Genet Dev. 2003 Apr;13(2):136-42 [12672490]
J Biol Chem. 2003 May 16;278(20):17876-84 [12637547]
Mol Cell Biol. 2003 Nov;23(21):7475-87 [14559996]
Nature. 2003 Dec 18;426(6968):895-9 [14685250]
J Biol Chem. 2004 Feb 6;279(6):4180-5 [14630919]
Nat Rev Mol Cell Biol. 2004 Feb;5(2):158-63 [15040448]
Mol Cell Biol. 2004 Apr;24(8):3347-58 [15060156]
Genes Dev. 2004 Mar 15;18(6):602-16 [15075289]
Oncogene. 2004 Apr 22;23(19):3462-73 [14990991]
Mol Cell Biol. 2004 Jun;24(11):4651-63 [15143161]
Genes Dev. 2004 Aug 1;18(15):1862-74 [15289458]
Biochimie. 1994;76(9):867-79 [7880904]
Genes Dev. 1996 Sep 1;10(17):2117-30 [8804307]
Trends Biochem Sci. 1996 Mar;21(3):87-8 [8882580]
EMBO J. 1996 Oct 1;15(19):5370-82 [8895581]
Proc Natl Acad Sci U S A. 1998 Jan 20;95(2):492-8 [9435219]
Nature. 1998 May 7;393(6680):88-91 [9590696]
Cell. 1998 Jul 24;94(2):217-27 [9695950]
EMBO J. 1998 Dec 1;17(23):6979-91 [9843504]
RNA. 1999 Mar;5(3):409-19 [10094309]
Nat Genet. 2005 Mar;37(3):254-64 [15696166]
Mol Cell Biol. 2005 Mar;25(6):2200-15 [15743818]
Cell. 2005 Mar 25;120(6):803-15 [15797381]
J Mol Endocrinol. 2005 Apr;34(2):281-97 [15821097]
Mol Cell Biol. 2005 May;25(10):3997-4009 [15870273]
Mol Cell Biol. 2000 Mar;20(6):1899-910 [10688638]
J Biol Chem. 2000 Jun 9;275(23):17771-7 [10748103]
J Cell Physiol. 2001 Jan;186(1):136-45 [11147808]
Proc Natl Acad Sci U S A. 2001 May 8;98(10):5728-33 [11331758]
Oncogene. 2001 May 28;20(24):3067-75 [11420722]
Chem Biol. 2001 Aug;8(8):739-58 [11514224]
EMBO J. 2002 Aug 1;21(15):4094-103 [12145209]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - N-methyl-D-aspartate subunit expression during mouse development altered by in utero alcohol exposure.
AN  - 68651465; 16202752
AB  - Alcohol-related neurodevelopmental disorders are contributors to long-term learning disabilities. By using a model for fetal alcohol syndrome, we have shown that prenatal alcohol exposure results in adult learning deficits of unknown mechanisms. In the developing hippocampus, the N-methyl-D-aspartate (NMDA) receptor subunit NR2B triggers long-term potentiation, fundamental to learning and memory; this is supplemented by the less plastic NR2A subunit in the adult. To understand the mechanism of learning deficits in FAS, we evaluated NR2B and NR2A expression in embryonic and adult mice.
          Pregnant C57Bl6/J mice were treated on gestational day 8 with alcohol or control (saline solution). Embryos were harvested at 6 hours, 24 hours, and 10 days, and brains from adult offspring were collected at 3 months (after evaluation for learning deficit). Calibrator-normalized relative real-time polymerase chain reaction was performed for NR2B and NR2A with glyceraldehyde-3-phosphate dehydrogenase standardization. Statistical analysis included analysis of variance. At 6 hours, NR2B expression in the alcohol-exposed embryos was higher than in controls (P < .01). NR2A was not expressed in either group. By 24 hours there was no difference in NR2B (P = .3). However, at 10 days NR2B was lower in alcohol-exposed animals (P = .02). In the adult brains there was a relative decrease in NR2B (P = .03) and an increase in NR2A (P < .01).
          Prenatal alcohol exposure during development induces NR2B expression deregulation in the embryos that persists until adulthood, when a relative increase in the less modifiable subunit NR2A occurs. This alteration in NMDA receptor subunits may underlie the learning abnormalities in fetal alcohol syndrome.
JF  - American journal of obstetrics and gynecology
AU  - Toso, Laura
AU  - Poggi, Sarah H
AU  - Abebe, Daniel
AU  - Roberson, Robin
AU  - Dunlap, Veronica
AU  - Park, Jane
AU  - Spong, Catherine Y
AD  - NICHD, National Institutes of Health, Bethesda, MD 20892-0925, USA. laura_toso@hotmail.com
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1534
EP  - 1539
VL  - 193
IS  - 4
KW  - NR2A NMDA receptor
KW  - 0
KW  - NR2B NMDA receptor
KW  - Receptors, N-Methyl-D-Aspartate
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Animals
KW  - Mice, Inbred C57BL
KW  - Fetal Development -- drug effects
KW  - Mice
KW  - Female
KW  - Pregnancy
KW  - Receptors, N-Methyl-D-Aspartate -- biosynthesis
KW  - Fetal Alcohol Spectrum Disorders -- metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-19
N1  - Date created - 2005-10-05
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Medications development: successes and challenges.
AN  - 68617832; 16083966
AB  - The National Institute on Drug Abuse has funded a medications program that has concentrated on the development of medications for opiate and cocaine dependence. Levomethadyl acetate (LAAM) and buprenorphine and buprenorphine/naloxone sublingual tablets were developed in conjunction with pharmaceutical partners and approved by the Food and Drug Administration. The remaining challenges for medications development for opiate dependence involves Phase IV studies in special populations, for example, pregnant opiate-dependent patients, and to translate neuroscience-based findings into treatments. Several marketed medications have shown initial efficacy to reduce cocaine use in well-controlled clinical trials. Disulfiram has been shown to reduce cocaine use in several clinical trials, while baclofen, modafinil, naltrexone, ondansetron, tiagabine, and topiramate have shown preliminary efficacy in initial clinical studies. Confirmatory studies of many of these medications is underway. More recently, the NIDA medications program has evaluated medications for their ability to reduce methamphetamine use. To date, no medications tested have shown efficacy to reduce methamphetamine use. Both marketed medications and investigational agents will be tested. Finally, NIDA has begun to test medications for efficacy to reduce cannabis use. Initial studies are underway. Both agonist and antagonist approaches will be evaluated. Additionally, medications will be tested in cannabis-dependent patients for the management of insomnia, withdrawal, and concurrent depression.
JF  - Pharmacology & therapeutics
AU  - Vocci, Frank
AU  - Ling, Walter
AD  - Division of Pharmacotherapies and Medical Consequences of Drug Abuse, National Institute on Drug Abuse, National Institutes of Health, 6001 Executive Boulevard, Ste 4123, MSC 9551, Bethesda, MD 20892, USA. fv6k@nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 94
EP  - 108
VL  - 108
IS  - 1
SN  - 0163-7258, 0163-7258
KW  - Narcotic Antagonists
KW  - 0
KW  - Methadone
KW  - UC6VBE7V1Z
KW  - Index Medicus
KW  - Animals
KW  - Humans
KW  - Methadone -- administration & dosage
KW  - Narcotic Antagonists -- therapeutic use
KW  - Substance-Related Disorders -- drug therapy
KW  - Substance-Related Disorders -- rehabilitation
KW  - Drug Design
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-05
N1  - Date created - 2005-09-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Drugs and alcohol: treating and preventing abuse, addiction and their medical consequences.
AN  - 68616853; 16098597
AB  - Recent advances in the fields of genetics, molecular biology, behavioral neuropharmacology, and brain imaging have dramatically changed our understanding of the addictive process and why relapse occurs even in the face of catastrophic consequences. Addiction is now recognized as a chronic brain disease that involves complex interactions between repeated exposure to drugs, biological (i.e., genetic and developmental), and environmental (i.e., drug availability, social, and economic variables) factors. Its treatment, therefore, requires, in general, not only a long-term intervention but also a multipronged approach that addresses the psychiatric, medical, legal, and social consequences of addiction. Also, because addiction usually starts in adolescence or early adulthood and is frequently comorbid with mental illness, we need to expand our treatment interventions in this age group both for substance abuse and psychiatric disorders.
JF  - Pharmacology & therapeutics
AU  - Volkow, Nora D
AU  - Li, Ting-Kai
AD  - National Institute on Drug Abuse, National Institutes of Health, Bethesda, MD 20892, USA. nvolkow@nida.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 3
EP  - 17
VL  - 108
IS  - 1
SN  - 0163-7258, 0163-7258
KW  - Index Medicus
KW  - Humans
KW  - Alcoholism -- therapy
KW  - Alcoholism -- prevention & control
KW  - Alcoholism -- complications
KW  - Substance-Related Disorders -- therapy
KW  - Brain -- drug effects
KW  - Substance-Related Disorders -- complications
KW  - Substance-Related Disorders -- prevention & control
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-05
N1  - Date created - 2005-09-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Charting a course for health services research at the National Institute on Drug Abuse.
AN  - 68608469; 16183465
AB  - Through research, we continue to develop and refine an array of safe and efficacious interventions to prevent and treat drug abuse; however, these interventions have not led to widespread improvements in prevention and treatment services in nonresearch settings. In addition, investigator-initiated research rarely examine or refine interventions that practitioners have found relevant and that are widely practiced. To address these problems, the National Institute on Drug Abuse convened a blue ribbon task force to examine its health services research program. The report served as a catalyst for the institute to promote a vigorous program of research that seeks to examine prevention and treatment intervention delivery systems and policies that facilitate provision of effective care in a range of real world settings. Findings from this research should help address the translational bottleneck of bringing evidence-based interventions into the community.
JF  - Journal of substance abuse treatment
AU  - Compton, Wilson M
AU  - Stein, Jack B
AU  - Robertson, Elizabeth B
AU  - Pintello, Denise
AU  - Pringle, Beverly
AU  - Volkow, Nora D
AD  - National Institute on Drug Abuse, Bethesda, MD 20892-9589, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 167
EP  - 172
VL  - 29
IS  - 3
SN  - 0740-5472, 0740-5472
KW  - Index Medicus
KW  - United States
KW  - Humans
KW  - Research Design
KW  - United States Substance Abuse and Mental Health Services Administration
KW  - Health Services Research
KW  - Health Planning Guidelines
KW  - Substance-Related Disorders -- prevention & control
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-06-22
N1  - Date created - 2005-09-26
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Int J Clin Exp Hypn. 2002 Apr;50(2):114-48 [11939275]
Eval Rev. 2002 Dec;26(6):575-601 [12465571]
Qual Saf Health Care. 2003 Feb;12(1):47-52 [12571345]
Am J Public Health. 2003 Aug;93(8):1261-7 [12893608]
N Engl J Med. 2003 Aug 28;349(9):868-74 [12944573]
Health Policy. 2003 Dec;66(3):247-60 [14637010]
Prev Sci. 2004 Mar;5(1):31-9 [15058910]
Arch Phys Med Rehabil. 2004 Apr;85(4 Suppl 2):S3-12 [15083417]
Health Serv Res. 1974 Fall;9(3):208-20 [4436074]
J Health Soc Behav. 1995 Mar;36(1):1-10 [7738325]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Nephrotic syndrome: an under-recognised immune-mediated complication of non-myeloablative allogeneic haematopoietic cell transplantation.
AN  - 68607270; 16173966
AB  - Nephrotic syndrome (NS) is an extremely rare complication of myeloablative allogeneic haematopoietic cell transplantation (HCT) that usually occurs in association with chronic graft-versus-host disease (C-GVHD). We observed an unexpectedly high incidence of NS in a cohort of 163 consecutive patients undergoing non-myeloablative HCT from a related human leucocyte antigen-compatible donor. Seven patients developed NS at a median 318 d post-transplant (range 119-1203 d; cumulative incidence 6.1%). The median age at onset of NS was 46 years (range 33-59 years); three of the seven patients had no evidence of C-GVHD while four had accompanying limited C-GVHD. At diagnosis, median proteinuria was 16.5 g/24 h (range 3-24 g/24 h). Renal biopsy was performed in four cases and revealed membranous nephropathy. NS was not always associated with other symptoms of C-GVHD, and in contrast to previous reports, usually did not improve with the re-initiation of aggressive immunosuppression, resulting in progressive renal failure necessitating dialysis in three of seven cases. Membranous nephropathy resulting in NS is a previously unrecognised and clinically significant complication of non-myeloablative HCT.
JF  - British journal of haematology
AU  - Srinivasan, R
AU  - Balow, J E
AU  - Sabnis, S
AU  - Lundqvist, A
AU  - Igarashi, T
AU  - Takahashi, Y
AU  - Austin, H
AU  - Tisdale, J
AU  - Barrett, J
AU  - Geller, N
AU  - Childs, R
AD  - Hematology Branch, National Heart, Lung and Blood Institute, Bethesda, MD 20892-1652, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 74
EP  - 79
VL  - 131
IS  - 1
SN  - 0007-1048, 0007-1048
KW  - Immunosuppressive Agents
KW  - 0
KW  - Cyclophosphamide
KW  - 8N3DW7272P
KW  - Vidarabine
KW  - FA2DM6879K
KW  - fludarabine
KW  - P2K93U8740
KW  - Index Medicus
KW  - Vidarabine -- analogs & derivatives
KW  - Humans
KW  - Aged
KW  - Kidney Failure, Chronic -- therapy
KW  - Kidney Failure, Chronic -- etiology
KW  - Transplantation, Homologous
KW  - Proteinuria -- etiology
KW  - Cyclophosphamide -- therapeutic use
KW  - Adult
KW  - Graft vs Host Disease
KW  - Middle Aged
KW  - Chronic Disease
KW  - Vidarabine -- therapeutic use
KW  - Adolescent
KW  - Time Factors
KW  - Immunosuppressive Agents -- therapeutic use
KW  - Kidney Glomerulus -- pathology
KW  - T-Lymphocytes -- immunology
KW  - Male
KW  - Female
KW  - Hematologic Neoplasms -- therapy
KW  - Nephrotic Syndrome -- immunology
KW  - Transplantation Conditioning -- methods
KW  - Nephrotic Syndrome -- pathology
KW  - Hematologic Neoplasms -- immunology
KW  - Hematopoietic Stem Cell Transplantation -- adverse effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-15
N1  - Date created - 2005-09-21
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment In:
Br J Haematol. 2007 Mar;136(6):857-9; author reply 859-60 [17341274]
Br J Haematol. 2006 Mar;132(6):801-2; author reply 802-3 [16487189]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Adverse effects on female development and reproduction in CD-1 mice following neonatal exposure to the phytoestrogen genistein at environmentally relevant doses.
AN  - 68606288; 15930323
AB  - Outbred female CD-1 mice were treated with genistein (Gen), the primary phytoestrogen in soy, by s.c. injections on Neonatal Days 1-5 at doses of 0.5, 5, or 50 mg/kg per day (Gen-0.5, Gen-5, and Gen-50). The day of vaginal opening was observed in mice treated with Gen and compared with controls, and although there were some differences, they were not statistically significant. Gen-treated mice had prolonged estrous cycles with a dose- and age-related increase in severity of abnormal cycles. Females treated with Gen-0.5 or Gen-5 bred to control males at 2, 4, and 6 mo showed statistically significant decreases in the number of live pups over time with increasing dose; at 6 mo, 60% of the females in the Gen-0.5 group and 40% in the Gen-5 group delivered live pups compared with 100% of controls. Mice treated with Gen-50 did not deliver live pups. At 2 mo, >60% of the mice treated with Gen-50 were fertile as determined by uterine implantation sites, but pregnancy was not maintained; pregnancy loss was characterized by fewer, smaller implantation sites and increased reabsorptions. Mice treated with lower doses of Gen had increased numbers of corpora lutea compared with controls, while mice treated with the highest dose had decreased numbers; however, superovulation with eCG/hCG yielded similar numbers of oocytes as controls. Serum levels of progesterone, estradiol, and testosterone were similar between Gen-treated and control mice when measured before puberty and during pregnancy. In summary, neonatal treatment with Gen caused abnormal estrous cycles, altered ovarian function, early reproductive senescence, and subfertility/infertility at environmentally relevant doses.
JF  - Biology of reproduction
AU  - Jefferson, Wendy N
AU  - Padilla-Banks, Elizabeth
AU  - Newbold, Retha R
AD  - Developmental Endocrinology Section, Laboratory of Molecular Toxicology, National Institute of Environmental Health Sciences, Research Triangle Park, NC 27709, USA. jeffers1@niehs.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 798
EP  - 806
VL  - 73
IS  - 4
SN  - 0006-3363, 0006-3363
KW  - Phytoestrogens
KW  - 0
KW  - Genistein
KW  - DH2M523P0H
KW  - Index Medicus
KW  - Environment
KW  - Animals
KW  - Animals, Outbred Strains
KW  - Embryo Implantation
KW  - Dose-Response Relationship, Drug
KW  - Mice
KW  - Pregnancy
KW  - Animals, Newborn
KW  - Litter Size
KW  - Abortion, Spontaneous
KW  - Female
KW  - Male
KW  - Phytoestrogens -- adverse effects
KW  - Pregnancy Outcome
KW  - Ovary -- growth & development
KW  - Reproduction -- drug effects
KW  - Genistein -- adverse effects
KW  - Ovary -- drug effects
KW  - Ovary -- physiology
KW  - Estrous Cycle -- drug effects
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-23
N1  - Date created - 2005-09-21
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Testosterone suppression of CRH-stimulated cortisol in men.
AN  - 68603005; 15841103
AB  - Despite observations of age-dependent sexual dimorphisms in hypothalamic-pituitary-adrenal (HPA) axis activity, the role of androgens in the regulation of HPA axis activity in men has not been examined. We assessed this role by performing CRH stimulation tests in 10 men (ages 18-45 years) during gonadal suppression with leuprolide acetate and during testosterone addition to leuprolide. CRH-stimulated cortisol levels as well as peak cortisol and greatest cortisol excursion were significantly lower (p<0.05, 0.005, and 0.01, respectively) during testosterone replacement compared with the induced hypogonadal condition (leuprolide plus placebo); cortisol area under the curve was lower at a trend level (p<0.1). Paradoxically, CRH-stimulated corticotropin (ACTH) was increased significantly during testosterone replacement (p<0.05). The cortisol : ACTH ratio, a measure of adrenal sensitivity, was lower during testosterone replacement (p<0.1). A mixed effects regression model showed that testosterone but not estradiol or CBG significantly contributed to the variance of cortisol. These data demonstrate that testosterone regulates CRH-stimulated HPA axis activity in men, with the divergent effects on ACTH and cortisol suggesting a peripheral (adrenal) locus for the suppressive effects on cortisol. Our results further demonstrate that the enhanced stimulated HPA axis activity previously described in young men compared with young women cannot be ascribed to an activational upregulation of the axis by testosterone.
JF  - Neuropsychopharmacology : official publication of the American College of Neuropsychopharmacology
AU  - Rubinow, David R
AU  - Roca, Catherine A
AU  - Schmidt, Peter J
AU  - Danaceau, Merry A
AU  - Putnam, Karen
AU  - Cizza, Giovanni
AU  - Chrousos, George
AU  - Nieman, Lynnette
AD  - Behavioral Endocrinology Branch, National Institute of Mental Health, Building 10-CRC, 10 Center Drive MSC 1276, Bethesda, MD 20892-1276, USA. rubinowd@mail.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1906
EP  - 1912
VL  - 30
IS  - 10
SN  - 0893-133X, 0893-133X
KW  - Testosterone
KW  - 3XMK78S47O
KW  - Adrenocorticotropic Hormone
KW  - 9002-60-2
KW  - Corticotropin-Releasing Hormone
KW  - 9015-71-8
KW  - Leuprolide
KW  - EFY6W0M8TG
KW  - Hydrocortisone
KW  - WI4X0X7BPJ
KW  - Index Medicus
KW  - Drug Interactions
KW  - Drug Administration Schedule
KW  - Testosterone -- pharmacology
KW  - Double-Blind Method
KW  - Area Under Curve
KW  - Humans
KW  - Adult
KW  - Radioimmunoassay -- methods
KW  - Middle Aged
KW  - Adolescent
KW  - Time Factors
KW  - Male
KW  - Adrenocorticotropic Hormone -- blood
KW  - Corticotropin-Releasing Hormone -- antagonists & inhibitors
KW  - Corticotropin-Releasing Hormone -- administration & dosage
KW  - Leuprolide -- administration & dosage
KW  - Hydrocortisone -- blood
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Neuropsychopharmacology+%3A+official+publication+of+the+American+College+of+Neuropsychopharmacology&rft.atitle=Testosterone+suppression+of+CRH-stimulated+cortisol+in+men.&rft.au=Rubinow%2C+David+R%3BRoca%2C+Catherine+A%3BSchmidt%2C+Peter+J%3BDanaceau%2C+Merry+A%3BPutnam%2C+Karen%3BCizza%2C+Giovanni%3BChrousos%2C+George%3BNieman%2C+Lynnette&rft.aulast=Rubinow&rft.aufirst=David&rft.date=2005-10-01&rft.volume=30&rft.issue=10&rft.spage=1906&rft.isbn=&rft.btitle=&rft.title=Neuropsychopharmacology+%3A+official+publication+of+the+American+College+of+Neuropsychopharmacology&rft.issn=0893133X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-29
N1  - Date created - 2005-09-19
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Psychosom Med. 1995 Jan-Feb;57(1):23-31 [7732155]
J Endocrinol. 1995 Feb;144(2):311-21 [7706984]
J Neurosci. 1996 Mar 1;16(5):1866-76 [8774455]
J Neurosci. 1996 Nov 1;16(21):7077-84 [8824343]
J Clin Endocrinol Metab. 1996 Oct;81(10):3639-43 [8855815]
Am J Physiol. 1998 Oct;275(4 Pt 1):E671-8 [9755087]
Neuropsychopharmacology. 1999 May;20(5):434-46 [10192824]
Psychosom Med. 1999 Mar-Apr;61(2):154-62 [10204967]
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N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Cooperating cancer-gene identification through oncogenic-retrovirus-induced insertional mutagenesis.
AN  - 68596621; 15961513
AB  - Multiple cooperating mutations that deregulate different signaling pathways are required to induce cancer. Identifying these cooperating mutations is a prerequisite for developing better combinatorial therapies for treating cancer. Here we show that cooperating cancer mutations can be identified through oncogenic-retrovirus-induced insertional mutagenesis. Among 13 myeloid leukemias induced by transplanting into mice bone marrow cells infected in vitro with a replication-defective retrovirus carrying the Sox4 oncogene, 9 contained insertional mutations at known or suspected cancer genes. This likely occurred because rare bone marrow cells, in which the oncogenic retrovirus happened to integrate and in which it mutated a cooperating cancer gene, were selected because the host harbored a cooperating cancer mutation. Cooperativity between Sox4 and another gene, Mef2c, was subsequently confirmed in transplantation studies, in which deregulated Mef2c expression was shown to accelerate the myeloid leukemia induced by Sox4. Insertional mutagenesis of cooperating cancer genes by a defective oncogenic retrovirus provides a new method for identifying cooperating cancer genes and could aid in the development of better therapies for treating cancer.
JF  - Blood
AU  - Du, Yang
AU  - Spence, Sally E
AU  - Jenkins, Nancy A
AU  - Copeland, Neal G
AD  - Mouse Cancer Genetics Program, National Cancer Institute, Center for Cancer Research, Frederick, MD, USA.
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 2498
EP  - 2505
VL  - 106
IS  - 7
SN  - 0006-4971, 0006-4971
KW  - High Mobility Group Proteins
KW  - 0
KW  - SOXC Transcription Factors
KW  - Sox4 protein, mouse
KW  - Trans-Activators
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Trans-Activators -- metabolism
KW  - Animals
KW  - Blotting, Northern
KW  - Humans
KW  - Leukemia, Myeloid -- genetics
KW  - Mice
KW  - Reverse Transcriptase Polymerase Chain Reaction
KW  - Polymerase Chain Reaction
KW  - Bone Marrow Cells -- metabolism
KW  - Stem Cells -- cytology
KW  - High Mobility Group Proteins -- genetics
KW  - Trans-Activators -- genetics
KW  - Blotting, Southern
KW  - Models, Genetic
KW  - Genetic Vectors
KW  - Mice, Inbred C57BL
KW  - Genetic Therapy -- methods
KW  - Bone Marrow Cells -- cytology
KW  - Cell Transplantation
KW  - Time Factors
KW  - Mutation
KW  - High Mobility Group Proteins -- metabolism
KW  - Bone Marrow Transplantation
KW  - Genetic Techniques
KW  - Retroviridae -- genetics
KW  - Neoplasms -- genetics
KW  - Mutagenesis, Insertional
KW  - Oncogenic Viruses -- genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68596621?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Blood&rft.atitle=Cooperating+cancer-gene+identification+through+oncogenic-retrovirus-induced+insertional+mutagenesis.&rft.au=Du%2C+Yang%3BSpence%2C+Sally+E%3BJenkins%2C+Nancy+A%3BCopeland%2C+Neal+G&rft.aulast=Du&rft.aufirst=Yang&rft.date=2005-10-01&rft.volume=106&rft.issue=7&rft.spage=2498&rft.isbn=&rft.btitle=&rft.title=Blood&rft.issn=00064971&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-28
N1  - Date created - 2005-09-20
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Nat Genet. 1999 Nov;23(3):348-53 [10610183]
Blood. 2005 Jun 1;105(11):4235-46 [15713797]
Hum Mol Genet. 2000 Sep 22;9(15):2297-304 [11001933]
Cancer Res. 2000 Nov 15;60(22):6303-6 [11103788]
Genesis. 2001 Jun;30(2):82-8 [11416868]
Trends Biochem Sci. 2002 Jan;27(1):40-7 [11796223]
Nat Cell Biol. 2002 Jul;4(7):540-4 [12080349]
J Neurooncol. 2002 May;57(3):201-14 [12125983]
Blood. 2002 Aug 1;100(3):998-1007 [12130514]
Dev Cell. 2002 Aug;3(2):167-70 [12194848]
Nat Genet. 2002 Sep;32(1):166-74 [12185365]
Am J Pathol. 2002 Oct;161(4):1315-23 [12368205]
Nucleic Acids Res. 2003 Jan 1;31(1):51-4 [12519945]
J Virol. 2003 Feb;77(3):2056-62 [12525640]
N Engl J Med. 2003 Jan 16;348(3):255-6 [12529469]
Gene. 2003 Mar 13;306:1-12 [12657462]
Adv Cancer Res. 2003;88:53-99 [12665053]
Nat Immunol. 2003 Jun;4(6):525-32 [12717432]
Science. 2003 Oct 17;302(5644):415-9 [14564000]
Science. 2004 Jan 16;303(5656):333 [14726584]
Oncogene. 2004 Apr 22;23(19):3444-53 [15064731]
Nat Genet. 2004 Jun;36(6):624-30 [15146183]
Cancer Sci. 2004 Jun;95(6):503-7 [15182431]
Cytogenet Genome Res. 2004;105(2-4):442-7 [15237232]
Proc Natl Acad Sci U S A. 2004 Aug 3;101(31):11334-7 [15273287]
Oncogene. 1989 Jun;4(6):789-94 [2734021]
Nature. 1994 Feb 17;367(6464):645-8 [7509044]
Nat Genet. 1996 Feb;12(2):149-53 [8563752]
Nature. 1996 Apr 25;380(6576):711-4 [8614465]
Eur J Immunol. 1997 May;27(5):1292-5 [9174623]
Cancer Res. 1998 Jan 15;58(2):198-203 [9443391]
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Blood. 2004 Dec 1;104(12):3437-44 [15304397]
Cancer Res. 2005 Jan 1;65(1):166-76 [15665292]
Cell. 2000 Jan 7;100(1):57-70 [10647931]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Recurrent retroviral vector integration at the Mds1/Evi1 locus in nonhuman primate hematopoietic cells.
AN  - 68596253; 15933056
AB  - Recent reports linking insertional activation of LMO2 following gene therapy for X-linked severe combined immunodeficiency (X-SCID) have led to a re-evaluation of risks following gene therapy with retroviral vectors. In our analysis of 702 integration sites in rhesus macaques that underwent transplantation up to 7 years earlier with autologous CD34+ cells transduced with amphotropic murine leukemia virus (MLV)-derived retroviral vectors containing marker genes, we detected insertion into one locus, the Mds1/Evi1 region, a total of 14 times in 9 animals. Mds1/Evi1 integrations were observed stably long term, primarily in myeloid cells. We hypothesize that this over-representation likely results from an impact on the self-renewal and engraftment potential of CD34+ progenitor cells via insertional mutagenesis at this specific locus. There is no evidence of ongoing in vivo clonal expansion of the Mds1/Evi1 populations, and all animals are hematologically normal without evidence for leukemia. Characterization of integration sites in this relevant preclinical model provides critical information for gene therapy risk assessment as well as identification of genes controlling hematopoiesis.
JF  - Blood
AU  - Calmels, Boris
AU  - Ferguson, Cole
AU  - Laukkanen, Mikko O
AU  - Adler, Rima
AU  - Faulhaber, Marion
AU  - Kim, Hyeoung-Joon
AU  - Sellers, Stephanie
AU  - Hematti, Peiman
AU  - Schmidt, Manfred
AU  - von Kalle, Christof
AU  - Akagi, Keiko
AU  - Donahue, Robert E
AU  - Dunbar, Cynthia E
AD  - Hematology Branch, National Heart, Lung, and Blood Institute, Bethesda, MD, USA.
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 2530
EP  - 2533
VL  - 106
IS  - 7
SN  - 0006-4971, 0006-4971
KW  - Antigens, CD34
KW  - 0
KW  - DNA-Binding Proteins
KW  - MECOM protein, human
KW  - Transcription Factors
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - Animals
KW  - Leukemia Virus, Murine -- genetics
KW  - Humans
KW  - Antigens, CD34 -- biosynthesis
KW  - Disease Progression
KW  - Primates
KW  - Hematopoiesis
KW  - Leukemia -- genetics
KW  - Risk
KW  - Genetic Vectors
KW  - Genetic Therapy -- methods
KW  - Macaca mulatta
KW  - Stem Cells
KW  - Time Factors
KW  - Mutagenesis, Insertional
KW  - Leukocytes, Mononuclear -- cytology
KW  - Granulocytes -- cytology
KW  - Proto-Oncogenes -- genetics
KW  - DNA-Binding Proteins -- genetics
KW  - Retroviridae -- genetics
KW  - Hematopoietic Stem Cells -- metabolism
KW  - Transcription Factors -- genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68596253?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Blood&rft.atitle=Recurrent+retroviral+vector+integration+at+the+Mds1%2FEvi1+locus+in+nonhuman+primate+hematopoietic+cells.&rft.au=Calmels%2C+Boris%3BFerguson%2C+Cole%3BLaukkanen%2C+Mikko+O%3BAdler%2C+Rima%3BFaulhaber%2C+Marion%3BKim%2C+Hyeoung-Joon%3BSellers%2C+Stephanie%3BHematti%2C+Peiman%3BSchmidt%2C+Manfred%3Bvon+Kalle%2C+Christof%3BAkagi%2C+Keiko%3BDonahue%2C+Robert+E%3BDunbar%2C+Cynthia+E&rft.aulast=Calmels&rft.aufirst=Boris&rft.date=2005-10-01&rft.volume=106&rft.issue=7&rft.spage=2530&rft.isbn=&rft.btitle=&rft.title=Blood&rft.issn=00064971&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-28
N1  - Date created - 2005-09-20
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Histol Histopathol. 2000 Jan;15(1):109-17 [10668202]
Blood. 2005 Dec 1;106(12):3932-9 [16109773]
Mol Ther. 2000 Mar;1(3):285-93 [10933944]
Hum Gene Ther. 2001 Apr 10;12(6):607-17 [11426461]
J Clin Invest. 2001 Aug;108(3):447-55 [11489938]
Br J Haematol. 2001 Sep;114(3):566-73 [11552981]
Science. 2002 Apr 19;296(5567):497 [11964471]
Nat Genet. 2002 Sep;32(1):166-74 [12185365]
Blood. 2002 Oct 15;100(8):2737-43 [12351380]
Blood. 2003 Feb 1;101(3):837-45 [12393383]
Blood. 2003 Mar 15;101(6):2199-205 [12424191]
Blood. 2003 Mar 15;101(6):2099-114 [12511419]
Blood Cells Mol Dis. 2003 Sep-Oct;31(2):206-12 [12972028]
Science. 2003 Oct 17;302(5644):415-9 [14564000]
Nucleic Acids Res. 2004 Jan 1;32(Database issue):D523-7 [14681473]
Mol Ther. 2004 Jan;9(1):5-13 [14741772]
J Gene Med. 2004 Apr;6(4):367-73 [15079811]
Exp Hematol. 2004 Feb;32(2):163-70 [15102477]
J Clin Invest. 2004 Sep;114(5):713-9 [15343390]
Nat Med. 1996 Feb;2(2):190-7 [8574964]
PLoS Biol. 2004 Dec;2(12):e423 [15550989]
Blood. 2000 Jul 1;96(1):1-8 [10891424]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Carbohydrate engineering of the recognition motifs in streptococcal co-aggregation receptor polysaccharides.
AN  - 68589364; 16164562
AB  - The cell wall polysaccharides of certain oral streptococci function as receptors for the lectin-like surface adhesins on other members of the oral biofilm community. Recognition of these receptor polysaccharides (RPS) depends on the presence of a host-like motif, either GalNAcbeta1-3Gal (Gn) or Galbeta1-3GalNAc (G), within the oligosaccharide repeating units of different RPS structural types. Type 2Gn RPS of Streptococcus gordonii 38 and type 2G RPS of Streptococcus oralis J22 are composed of heptasaccharide repeats that are identical except for their host-like motifs. In the current investigation, the genes for the glycosyltransferases that synthesize these motifs were identified by high-resolution nuclear magnetic resonance (NMR) analysis of genetically altered polysaccharides. RPS production was switched from type 2Gn to 2G by replacing wefC and wefD in the type 2Gn gene cluster of S. gordonii 38 with wefF and wefG from the type 2G cluster of S. oralis J22. Disruption of either wefC or wefF abolished cell surface RPS production. In contrast, disruption of wefD in the type 2Gn cluster or wefG in the type 2G cluster eliminated beta-GalNAc from the Gn motif or beta-Gal from the G motif, resulting in mutant polysaccharides with hexa- rather than heptasaccharide subunits. The mutant polysaccharides reacted like wild-type RPS with rabbit antibodies against type 2Gn or 2G RPS but were inactive as co-aggregation receptors. Additional mutant polysaccharides with GalNAcbeta1-3GalNAc or Galbeta1-3Gal recognition motifs were engineered by replacing wefC in the type 2Gn cluster with wefF or wefF in the type 2G cluster with wefC respectively. The reactions of these genetically modified polysaccharides as antigens and receptors provide further insight into the structural basis of RPS function.
JF  - Molecular microbiology
AU  - Yoshida, Yasuo
AU  - Ganguly, Soumya
AU  - Bush, C Allen
AU  - Cisar, John O
AD  - Oral Infection and Immunity Branch, National Institute of Dental and Craniofacial Research, National Institutes of Health, Bethesda, MD 20892, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 244
EP  - 256
VL  - 58
IS  - 1
SN  - 0950-382X, 0950-382X
KW  - DNA, Bacterial
KW  - 0
KW  - Polysaccharides, Bacterial
KW  - Receptors, Cell Surface
KW  - Glycosyltransferases
KW  - EC 2.4.-
KW  - Index Medicus
KW  - Genes, Bacterial
KW  - Genetic Engineering
KW  - Cell Wall -- chemistry
KW  - Glycosyltransferases -- genetics
KW  - Sequence Analysis, DNA
KW  - Receptors, Cell Surface -- chemistry
KW  - Gene Deletion
KW  - Magnetic Resonance Spectroscopy
KW  - Bacterial Adhesion -- genetics
KW  - Amino Acid Motifs
KW  - Recombination, Genetic
KW  - Carbohydrate Sequence
KW  - Molecular Sequence Data
KW  - Receptors, Cell Surface -- genetics
KW  - Mutagenesis, Insertional
KW  - Streptococcus -- genetics
KW  - Polysaccharides, Bacterial -- chemistry
KW  - Polysaccharides, Bacterial -- metabolism
KW  - Streptococcus -- metabolism
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68589364?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Molecular+microbiology&rft.atitle=Carbohydrate+engineering+of+the+recognition+motifs+in+streptococcal+co-aggregation+receptor+polysaccharides.&rft.au=Yoshida%2C+Yasuo%3BGanguly%2C+Soumya%3BBush%2C+C+Allen%3BCisar%2C+John+O&rft.aulast=Yoshida&rft.aufirst=Yasuo&rft.date=2005-10-01&rft.volume=58&rft.issue=1&rft.spage=244&rft.isbn=&rft.btitle=&rft.title=Molecular+microbiology&rft.issn=0950382X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-04-13
N1  - Date created - 2005-09-16
N1  - Date revised - 2017-01-13
N1  - Genetic sequence - AB181235; GENBANK
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Adverse events among patients in a behavioral treatment trial for heroin and cocaine dependence: effects of age, race, and gender.
AN  - 68579258; 16157230
AB  - Safety monitoring is a critical element of clinical trials evaluating treatment for substance dependence, but is complicated by participants' high levels of medical and psychiatric comorbidity. This paper describes AEs reported in a large (N = 286), 29-week outpatient study of behavioral interventions for heroin and cocaine dependence in methadone-maintained outpatients. A total of 884 AEs were reported (3.1 per patient, 0.12 per patient-week), the most common being infections (26.8%), gastrointestinal (20.5%), musculoskeletal (12.3%), and general (10%) disorders. Serious AEs were uncommon (1.6% of total). Female participants reported significantly higher rates of AEs (incidence density ratio, IDR = 1.38, p < 0.0001); lower rates of AEs were reported by African Americans (IDR = 0.73, p<0.0001) and participants over age 40 reported lower rates of AEs (IDR = 0.84, p = 0.0095). AE incidence was not associated with the study intervention or with psychiatric comorbidity. Further work is needed to adapt AE coding systems for behavioral trials for substance dependence; the standard Medical Dictionary for Regulatory Activities, International Federation of Pharmaceutical Manufacturers Associations (MedDRA) coding system used in this report did not contain a separate category for one of the most common types of AE, dental problems. Nonetheless, the data reported here should help provide a context in which investigators and IRBs can interpret the patterns of AEs they encounter.
JF  - Drug and alcohol dependence
AU  - Schroeder, Jennifer R
AU  - Schmittner, John P
AU  - Epstein, David H
AU  - Preston, Kenzie L
AD  - Intramural Research Program, National Institute on Drug Abuse, 5500 Nathan Shock Drive, Baltimore, MD 21224, USA. jschroed@intra.nida.nih.gov
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 45
EP  - 51
VL  - 80
IS  - 1
SN  - 0376-8716, 0376-8716
KW  - Narcotics
KW  - 0
KW  - Methadone
KW  - UC6VBE7V1Z
KW  - Index Medicus
KW  - Administration, Oral
KW  - Motivation
KW  - Combined Modality Therapy
KW  - Humans
KW  - Narcotics -- administration & dosage
KW  - Methadone -- administration & dosage
KW  - Counseling
KW  - Comorbidity
KW  - Ambulatory Care
KW  - Psychotherapy, Group
KW  - Risk Factors
KW  - Adult
KW  - Incidence
KW  - Middle Aged
KW  - Female
KW  - Male
KW  - Heroin Dependence -- ethnology
KW  - Heroin Dependence -- epidemiology
KW  - Cognitive Therapy
KW  - Cocaine-Related Disorders -- ethnology
KW  - Health Status
KW  - European Continental Ancestry Group -- psychology
KW  - Heroin Dependence -- rehabilitation
KW  - European Continental Ancestry Group -- statistics & numerical data
KW  - Cocaine-Related Disorders -- epidemiology
KW  - African Continental Ancestry Group -- psychology
KW  - Cocaine-Related Disorders -- rehabilitation
KW  - African Continental Ancestry Group -- statistics & numerical data
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Drug+and+alcohol+dependence&rft.atitle=Adverse+events+among+patients+in+a+behavioral+treatment+trial+for+heroin+and+cocaine+dependence%3A+effects+of+age%2C+race%2C+and+gender.&rft.au=Schroeder%2C+Jennifer+R%3BSchmittner%2C+John+P%3BEpstein%2C+David+H%3BPreston%2C+Kenzie+L&rft.aulast=Schroeder&rft.aufirst=Jennifer&rft.date=2005-10-01&rft.volume=80&rft.issue=1&rft.spage=45&rft.isbn=&rft.btitle=&rft.title=Drug+and+alcohol+dependence&rft.issn=03768716&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-27
N1  - Date created - 2005-09-13
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Advances in pediatric asthma and atopic dermatitis.
AN  - 68572752; 16160544
AB  - Allergic diseases, including asthma, allergic rhinitis, atopic dermatitis, food allergy, and urticaria are common in general pediatric practice. This review highlights several significant advances in pediatric allergy over the past year, focusing on asthma and atopic dermatitis.
          With increasing options for the treatment of allergic diseases, much work is now focused on methods for individualizing treatments to a patient's phenotype and genotype. Progress over the past year includes the characterization of effects of regular albuterol use in patients with genetic variations in the beta-adrenergic receptor. Maintenance asthma regimens for children in the first years of life are also an ongoing focus. The relation between upper airway allergic inflammation and asthma has continued to accumulate support and now extends to the middle ear. Environmental influences on asthma and interventions have been described, including environmental controls for asthma and the role of air pollution on lung development in children. Finally, concerns have been raised regarding the use of topical immunomodulators in young children with atopic dermatitis. Progress continues in the care of children with atopic diseases. Attention to treatment with appropriate medications, patient-individualized environmental controls, and extensive education are the keys to successfully treating atopic children. This review highlights several recent advances but is not intended to be a comprehensive review.
JF  - Current opinion in pediatrics
AU  - Foroughi, Shabnam
AU  - Thyagarajan, Ananth
AU  - Stone, Kelly D
AD  - Laboratory of Allergic Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 658
EP  - 663
VL  - 17
IS  - 5
SN  - 1040-8703, 1040-8703
KW  - Bronchodilator Agents
KW  - 0
KW  - Calcineurin Inhibitors
KW  - Dermatologic Agents
KW  - Albuterol
KW  - QF8SVZ843E
KW  - Index Medicus
KW  - Albuterol -- administration & dosage
KW  - Nebulizers and Vaporizers
KW  - Humans
KW  - Bronchodilator Agents -- administration & dosage
KW  - Lymphoma -- chemically induced
KW  - Child
KW  - Dermatologic Agents -- adverse effects
KW  - Dermatitis, Atopic -- therapy
KW  - Asthma -- genetics
KW  - Asthma -- therapy
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Current+opinion+in+pediatrics&rft.atitle=Advances+in+pediatric+asthma+and+atopic+dermatitis.&rft.au=Foroughi%2C+Shabnam%3BThyagarajan%2C+Ananth%3BStone%2C+Kelly+D&rft.aulast=Foroughi&rft.aufirst=Shabnam&rft.date=2005-10-01&rft.volume=17&rft.issue=5&rft.spage=658&rft.isbn=&rft.btitle=&rft.title=Current+opinion+in+pediatrics&rft.issn=10408703&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-14
N1  - Date created - 2005-09-14
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Occupation, hobbies, and acute leukemia in adults.
AN  - 68504568; 16111530
AB  - Occupational and industrial exposures have been implicated in the etiology of leukemia, yet uncertainty remains regarding potential high risk occupations. We examined the associations between self-reported occupations and hobbies and acute leukemia risk using data from 811 cases and 637 controls participating in a case-control study in the U.S. and Canada. We found that several occupations may increase the risk of acute leukemia, particularly occupations related to petroleum products, rubber, nuclear energy, munitions, plastics, and electronics manufacturing. Differences were noted according to histological type. Other occupations and hobbies were not clearly associated with risk.
JF  - Leukemia research
AU  - Terry, Paul D
AU  - Shore, David L
AU  - Rauscher, Garth H
AU  - Sandler, Dale P
AD  - Epidemiology Branch, National Institute of Environmental Health Sciences, Research, Triangle Park, NC 27709, USA. pdterry@sph.emory.edu
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 1117
EP  - 1130
VL  - 29
IS  - 10
SN  - 0145-2126, 0145-2126
KW  - Index Medicus
KW  - Canada -- epidemiology
KW  - Acute Disease
KW  - Odds Ratio
KW  - Risk Factors
KW  - Humans
KW  - Adult
KW  - Case-Control Studies
KW  - Aged
KW  - Middle Aged
KW  - United States -- epidemiology
KW  - Male
KW  - Female
KW  - Precursor Cell Lymphoblastic Leukemia-Lymphoma -- epidemiology
KW  - Occupational Exposure
KW  - Leukemia, Myeloid -- epidemiology
KW  - Hobbies
KW  - Leukemia, Myeloid -- etiology
KW  - Occupations
KW  - Precursor Cell Lymphoblastic Leukemia-Lymphoma -- etiology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Leukemia+research&rft.atitle=Occupation%2C+hobbies%2C+and+acute+leukemia+in+adults.&rft.au=Terry%2C+Paul+D%3BShore%2C+David+L%3BRauscher%2C+Garth+H%3BSandler%2C+Dale+P&rft.aulast=Terry&rft.aufirst=Paul&rft.date=2005-10-01&rft.volume=29&rft.issue=10&rft.spage=1117&rft.isbn=&rft.btitle=&rft.title=Leukemia+research&rft.issn=01452126&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-10-18
N1  - Date created - 2005-08-22
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment In:
Leuk Res. 2005 Oct;29(10):1105-6 [15913775]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Interactive role of the toll-like receptor 4 and reactive oxygen species in LPS-induced microglia activation.
AN  - 68501361; 15920727
AB  - Microglia are activated by lipopolysaccharide (LPS) to produce neurotoxic pro-inflammatory factors and reactive oxygen species (ROS). While a multitude of LPS receptors and corresponding pathways have been identified, the detailed mechanisms mediating the microglial response to LPS are unclear. Using mice lacking a functional toll-like receptor 4 (TLR4), we demonstrate that TLR4 and ROS work in concert to mediate microglia activation, where the contribution from each pathway is dependent on the concentration of LPS. Immunocytochemical staining of microglia in neuron-glia cultures with antibodies against F4/80 revealed that while TLR4(+/+) microglia were activated the low concentration of 1 ng/ml of LPS, TLR4(-/-) microglia exhibit activated morphology in response to LPS only at higher concentrations (100-1,000 ng/ml). Additionally, tumor necrosis factor-alpha (TNF-alpha) was only produced from higher concentrations (100-1,000 ng/ml) of LPS in TLR4(-/-) enriched microglia cultures. Diphenylene iodonium (DPI), an inhibitor of NADPH oxidase, reduced TNF-alpha production from TLR4(-/-) microglia. The influence of TLR4 on LPS-induced superoxide production was tested in rat enriched microglia cultures, where the presence or absence of serum failed to show any effect on the superoxide production. Further, both TLR4(-/-) and TLR4(+/+) microglia showed a similar increase in extracellular superoxide production when exposed to LPS (1-1,000 ng/ml). These data indicate that LPS-induced superoxide production in microglia is independent of TLR4 and that ROS derived from the production of extracellular superoxide in microglia mediates the LPS-induced TNF-alpha response of both the TLR4-dependent and independent pathway.
          (c) 2005 Wiley-Liss, Inc.
JF  - Glia
AU  - Qin, Liya
AU  - Li, Guorong
AU  - Qian, Xun
AU  - Liu, Yuxin
AU  - Wu, Xuefei
AU  - Liu, Bin
AU  - Hong, Jau-Shyong
AU  - Block, Michelle L
AD  - Neuropharmacology Section, Laboratory of Pharmacology and Chemistry, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 78
EP  - 84
VL  - 52
IS  - 1
SN  - 0894-1491, 0894-1491
KW  - Enzyme Inhibitors
KW  - 0
KW  - Inflammation Mediators
KW  - Lipopolysaccharides
KW  - Reactive Oxygen Species
KW  - Tlr4 protein, mouse
KW  - Toll-Like Receptor 4
KW  - Tumor Necrosis Factor-alpha
KW  - Superoxides
KW  - 11062-77-4
KW  - NADPH Oxidase
KW  - EC 1.6.3.1
KW  - Index Medicus
KW  - Neurodegenerative Diseases -- physiopathology
KW  - Animals
KW  - Coculture Techniques
KW  - Dose-Response Relationship, Drug
KW  - Lipopolysaccharides -- pharmacology
KW  - Mice
KW  - Mice, Knockout
KW  - Rats
KW  - Animals, Newborn
KW  - Superoxides -- metabolism
KW  - Rats, Inbred F344
KW  - Oxidative Stress -- physiology
KW  - Cells, Cultured
KW  - Neurodegenerative Diseases -- metabolism
KW  - Oxidative Stress -- drug effects
KW  - Inflammation Mediators -- pharmacology
KW  - Mice, Inbred C3H
KW  - Mice, Inbred C57BL
KW  - Enzyme Inhibitors -- pharmacology
KW  - Tumor Necrosis Factor-alpha -- metabolism
KW  - Female
KW  - NADPH Oxidase -- metabolism
KW  - Reactive Oxygen Species -- metabolism
KW  - Gliosis -- metabolism
KW  - Gliosis -- physiopathology
KW  - Encephalitis -- physiopathology
KW  - NADPH Oxidase -- antagonists & inhibitors
KW  - Toll-Like Receptor 4 -- genetics
KW  - Gliosis -- genetics
KW  - Encephalitis -- chemically induced
KW  - Encephalitis -- genetics
KW  - Gliosis -- chemically induced
KW  - Encephalitis -- metabolism
KW  - Microglia -- drug effects
KW  - Microglia -- metabolism
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68501361?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Glia&rft.atitle=Interactive+role+of+the+toll-like+receptor+4+and+reactive+oxygen+species+in+LPS-induced+microglia+activation.&rft.au=Qin%2C+Liya%3BLi%2C+Guorong%3BQian%2C+Xun%3BLiu%2C+Yuxin%3BWu%2C+Xuefei%3BLiu%2C+Bin%3BHong%2C+Jau-Shyong%3BBlock%2C+Michelle+L&rft.aulast=Qin&rft.aufirst=Liya&rft.date=2005-10-01&rft.volume=52&rft.issue=1&rft.spage=78&rft.isbn=&rft.btitle=&rft.title=Glia&rft.issn=08941491&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-08-09
N1  - Date created - 2005-08-22
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Expression pattern of four membrane-type matrix metalloproteinases in the normal and diseased mouse mammary gland.
AN  - 68436278; 15895410
AB  - Both mammary gland development and mammary carcinogenesis involve extensive remodeling of the mammary gland extracellular matrix. The expression of four membrane-type matrix metalloproteinases (MT-MMPs) with matrix remodeling potential in development and tumorigenesis was evaluated by in-situ hybridization on mouse mammary gland sections. MT1-MMP and MT3-MMP were found in the mammary stroma mainly around epithelial structures in both developing and mature mammary gland. In contrast, MT2-MMP was found exclusively in the mammary epithelium. Lactating gland expressed none of the examined MT-MMPs. Mammary gland tumors expressed MT1-MMP, MT2-MMP, and MT3-MMP while MT4-MMP was not expressed in any developmental or cancerous stage analyzed here. Our results suggest that MT1-MMP, MT2-MMP, and MT3-MMP may be involved in remodeling of both the normal and diseased mammary gland either directly or indirectly by activation of other MMPs.
JF  - Journal of cellular physiology
AU  - Szabova, Ludmila
AU  - Yamada, Susan S
AU  - Birkedal-Hansen, Henning
AU  - Holmbeck, Kenn
AD  - Craniofacial and Skeletal Diseases Branch, Matrix Metalloproteinase Unit, National Institute of Dental and Craniofacial Research, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 123
EP  - 132
VL  - 205
IS  - 1
SN  - 0021-9541, 0021-9541
KW  - Mmp14 protein, mouse
KW  - 0
KW  - Mmp15 protein, mouse
KW  - Mmp16 protein, mouse
KW  - Matrix Metalloproteinase 15
KW  - EC 3.4.24.-
KW  - Matrix Metalloproteinase 16
KW  - Matrix Metalloproteinases, Membrane-Associated
KW  - Metalloendopeptidases
KW  - Matrix Metalloproteinase 14
KW  - EC 3.4.24.80
KW  - Index Medicus
KW  - Aging -- physiology
KW  - Animals
KW  - Lactation -- genetics
KW  - Lactation -- metabolism
KW  - Mice
KW  - Health
KW  - Female
KW  - Pregnancy
KW  - Gene Expression Profiling
KW  - Gene Expression Regulation, Enzymologic -- genetics
KW  - Mammary Neoplasms, Animal -- pathology
KW  - Mammary Glands, Animal -- cytology
KW  - Mammary Neoplasms, Animal -- genetics
KW  - Mammary Glands, Animal -- pathology
KW  - Mammary Neoplasms, Animal -- enzymology
KW  - Mammary Glands, Animal -- enzymology
KW  - Metalloendopeptidases -- metabolism
KW  - Metalloendopeptidases -- genetics
KW  - Metalloendopeptidases -- chemistry
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+cellular+physiology&rft.atitle=Expression+pattern+of+four+membrane-type+matrix+metalloproteinases+in+the+normal+and+diseased+mouse+mammary+gland.&rft.au=Szabova%2C+Ludmila%3BYamada%2C+Susan+S%3BBirkedal-Hansen%2C+Henning%3BHolmbeck%2C+Kenn&rft.aulast=Szabova&rft.aufirst=Ludmila&rft.date=2005-10-01&rft.volume=205&rft.issue=1&rft.spage=123&rft.isbn=&rft.btitle=&rft.title=Journal+of+cellular+physiology&rft.issn=00219541&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-04
N1  - Date created - 2005-08-02
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Comorbidity between DSM-IV Alcohol and Specific Drug Use Disorders in the United States: Results from the National Epidemiologic Survey on Alcohol and Related Conditions
AN  - 57082474; 200600826
AB  - Background: To date, there have been no published data on 12-month comorbidity of DSM-IV alcohol and drug use disorders in the general U.S. population. The purposes of the present study were to examine the prevalence and comorbidity of alcohol and specific drug use disorders, and to identify sociodemographic and psychopathologic correlates and treatment seeking among three groups of respondents: (1) those with alcohol use disorders only; (2) those with drug use disorders only; (3) those with comorbid alcohol and drug use disorders. Methods: Information on 12-month alcohol and specific drug use disorders in the United States was derived from face-to-face interviews in the National Institute on Alcohol Abuse and Alcoholism's (NIAAA) 2001-2002 National Epidemiologic Survey on Alcohol and Related Conditions (NESARC: n = 43,093). Results: Prevalences were 7.35% for alcohol use disorders only, 0.90% for drug use disorder only and 1.10% for comorbid alcohol and drug use disorders. Sociodemographic and psychopathologic correlates of these three groups were quite different, with the drug use disorder and comorbid groups significantly more likely to be young, male, never married and of lower socioeconomic status than the alcohol use disorder only group. Associations between current alcohol use disorders and 25 specific drug use disorders were generally positive and statistically significant. The 12-month prevalence of treatment seeking significantly increased from 6.06% for those with an alcohol use disorder only to 15.63% for those with a drug use disorder only, and to 21.76% for those with comorbid alcohol and drug use disorders. Conclusions: This study provides detailed data on the homotypic comorbidity of alcohol use disorders and 25 different drug use disorders and confirms the high levels of association seen in previous studies based on lifetime measures. Implications of this study are discussed in terms of integrating alcohol and drug treatment services and refining prevention and intervention efforts. Tables, References. [Copyright 2005 Elsevier Ireland Ltd.]
JF  - Drug and Alcohol Dependence
AU  - Stinson, Frederick S
AU  - Grant, Bridget F
AU  - Dawson, Deborah A
AU  - Ruan, W June
AU  - Huang, Boji
AU  - Saha, Tulshi
AD  - Laboratory Epidemiology & Biometry, Division Intramural Clinical & Biological Research, National Instit Alco fstinson@mail.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 105
EP  - 116
VL  - 80
IS  - 1
SN  - 0376-8716, 0376-8716
KW  - DSM-IV alcohol abuse
KW  - DSM-IV alcohol dependence
KW  - Epidemiology
KW  - Comorbidity
KW  - Socioeconomic factors
KW  - Diagnostic and Statistical Manual IV
KW  - Alcohol abuse
KW  - Alcohol dependence
KW  - article
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/57082474?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aassia&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Drug+and+Alcohol+Dependence&rft.atitle=Comorbidity+between+DSM-IV+Alcohol+and+Specific+Drug+Use+Disorders+in+the+United+States%3A+Results+from+the+National+Epidemiologic+Survey+on+Alcohol+and+Related+Conditions&rft.au=Stinson%2C+Frederick+S%3BGrant%2C+Bridget+F%3BDawson%2C+Deborah+A%3BRuan%2C+W+June%3BHuang%2C+Boji%3BSaha%2C+Tulshi&rft.aulast=Stinson&rft.aufirst=Frederick&rft.date=2005-10-01&rft.volume=80&rft.issue=1&rft.spage=105&rft.isbn=&rft.btitle=&rft.title=Drug+and+Alcohol+Dependence&rft.issn=03768716&rft_id=info:doi/10.1016%2Fj.drugalcdep.2005.03.009
LA  - English
DB  - Applied Social Sciences Index & Abstracts (ASSIA)
N1  - Date revised - 2006-04-07
N1  - Last updated - 2016-09-27
N1  - CODEN - DADEDV
N1  - SubjectsTermNotLitGenreText - Alcohol abuse; Alcohol dependence; Diagnostic and Statistical Manual IV; Socioeconomic factors; Epidemiology; Comorbidity
DO  - http://dx.doi.org/10.1016/j.drugalcdep.2005.03.009
ER  - 



TY  - JOUR
T1  - Co-Occurring DSM-IV Drug Abuse in DSM-IV Drug Dependence: Results from the National Epidemiologic Survey on Alcohol and Related Conditions
AN  - 57081008; 200600358
AB  - The extent to which dependence occurs with or without abuse is important because of the potential for underestimation and biased estimates of drug dependence in surveys that rely on abuse as a screening method for dependence. The purpose of this paper was to present the prevalence of DSM-IV drug dependence with and without drug abuse in a nationally representative sample, as well as in subgroups defined by sex, age and race/ethnicity. Among all respondents with current drug dependence, 22.0% did not additionally meet criteria for abuse (19.5% among males and 27.8% among females). Current drug dependence without abuse was especially common among females age 45-64 (52.6% of all cases). Among those with lifetime diagnoses of drug dependence, a small proportion overall, 5.0% had no symptoms of abuse, with the highest proportion again found among females aged 45-64 (19.5% of all cases). The use of drug abuse as a screening method for drug dependence in large epidemiologic studies will differentially underestimate the prevalence of dependence by subgroup, affecting many types of research. Dependence with and without abuse may represent heterogeneous phenotypes for genetic and gene-environment research, which should be explored. Tables, References. [Copyright 2005 Elsevier Ireland Ltd.]
JF  - Drug and Alcohol Dependence
AU  - Hasin, Deborah S
AU  - Hatzenbueler, Mark
AU  - Smith, Sharon
AU  - Grant, Bridget F
AD  - Laboratory Epidemiology & Biometry, Division Clinical & Biological Intramural Research, National Instit Alco
Y1  - 2005/10//
PY  - 2005
DA  - October 2005
SP  - 117
EP  - 123
VL  - 80
IS  - 1
SN  - 0376-8716, 0376-8716
KW  - Alcohol abuse
KW  - Drug abuse
KW  - Alcohol dependence
KW  - Drug dependence
KW  - Epidemiology
KW  - Drug dependency
KW  - article
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aassia&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Drug+and+Alcohol+Dependence&rft.atitle=Co-Occurring+DSM-IV+Drug+Abuse+in+DSM-IV+Drug+Dependence%3A+Results+from+the+National+Epidemiologic+Survey+on+Alcohol+and+Related+Conditions&rft.au=Hasin%2C+Deborah+S%3BHatzenbueler%2C+Mark%3BSmith%2C+Sharon%3BGrant%2C+Bridget+F&rft.aulast=Hasin&rft.aufirst=Deborah&rft.date=2005-10-01&rft.volume=80&rft.issue=1&rft.spage=117&rft.isbn=&rft.btitle=&rft.title=Drug+and+Alcohol+Dependence&rft.issn=03768716&rft_id=info:doi/10.1016%2Fj.drugalcdep.2005.03.010
LA  - English
DB  - Applied Social Sciences Index & Abstracts (ASSIA)
N1  - Date revised - 2006-04-07
N1  - Last updated - 2016-09-27
N1  - CODEN - DADEDV
N1  - SubjectsTermNotLitGenreText - Alcohol abuse; Drug abuse; Alcohol dependence; Epidemiology; Drug dependency
DO  - http://dx.doi.org/10.1016/j.drugalcdep.2005.03.010
ER  - 



TY  - JOUR
T1  - Hypnotic disgust makes moral judgments more severe
AN  - 37718111; 3264474
AB  - Highly hypnotizable participants were given a posthypnotic suggestion to feel a flash of disgust whenever they read an arbitrary word. They were then asked to rate moral transgressions described in vignettes that either did or did not include the disgust-inducing word. Two studies show that moral judgments can be made more severe by the presence of a flash of disgust. These findings suggest that moral judgments may be grounded in affectively laden moral intuitions. Reprinted by permission of Sage Publications
JF  - Psychological science
AU  - Wheatley, Thalia
AU  - Haidt, Jonathan
AD  - National Institutes of Health ; University of Virginia
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 780
EP  - 784
VL  - 16
IS  - 10
SN  - 0956-7976, 0956-7976
KW  - Sociology
KW  - Morals
KW  - Sight
KW  - Psychology
KW  - Regression analysis
KW  - Empirical research
KW  - Judgement
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Psychological+science&rft.atitle=Hypnotic+disgust+makes+moral+judgments+more+severe&rft.au=Wheatley%2C+Thalia%3BHaidt%2C+Jonathan&rft.aulast=Wheatley&rft.aufirst=Thalia&rft.date=2005-10-01&rft.volume=16&rft.issue=10&rft.spage=780&rft.isbn=&rft.btitle=&rft.title=Psychological+science&rft.issn=09567976&rft_id=info:doi/
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 10404; 8282 8281 6085; 7007 3322 6071 1542 11325 4551; 4200 10902; 10739 12228 10919; 11650 11505 1678
ER  - 



TY  - JOUR
T1  - A new tool to assess treatment fidelity and evaluation of treatment fidelity across 10 years of health behavior research
AN  - 36494664; 3305211
AB  - A. Bellg, B. Borrelli, et al. (2004) previously developed a framework that consisted of strategies to enhance treatment fidelity of health behavior interventions. The present study used this framework to (a) develop a measure of treatment fidelity and (b) use the measure to evaluate treatment fidelity in articles published in 5 journals over 10 years. Three hundred forty-two articles met inclusion criteria: 22% reported strategies to maintain provider skills, 27% reported checking adherence to protocol, 35% reported using a treatment manual. 54% reported using none of these strategies, and 12% reported using all 3 strategies. The mean proportion adherence to treatment fidelity strategies was 55; 15.5% of articles achieved greater than or equal to .80. This tool may be useful for researchers, grant reviewers, and editors planning and evaluating trials. Reprinted by permission of the American Psychological Association
JF  - Journal of consulting and clinical psychology
AU  - Borrelli, Belinda
AU  - Sepinwall, Deborah
AU  - Ernst, Denise
AU  - Bellg, Albert J
AU  - Czajkowski, Susan
AU  - Breger, Rosemary
AU  - DeFrancesco, Carol
AU  - Levesque, Chantal
AU  - Sharp, Daryl L
AU  - Ogedegbe, Gbenga
AU  - Resnick, Barbara
AU  - Orwig, Denise
AD  - Brown University ; University of New Mexico ; Appleton Heart Institute ; National Institutes of Health ; University of Oregon ; Southwest Missouri State University ; University of Rochester ; Columbia University ; University of Maryland
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 852
EP  - 860
VL  - 73
IS  - 5
SN  - 0022-006X, 0022-006X
KW  - Sociology
KW  - Evaluation
KW  - Conceptualization
KW  - Medical treatment
KW  - Clinical psychology
KW  - Methodology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/36494664?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+consulting+and+clinical+psychology&rft.atitle=A+new+tool+to+assess+treatment+fidelity+and+evaluation+of+treatment+fidelity+across+10+years+of+health+behavior+research&rft.au=Borrelli%2C+Belinda%3BSepinwall%2C+Deborah%3BErnst%2C+Denise%3BBellg%2C+Albert+J%3BCzajkowski%2C+Susan%3BBreger%2C+Rosemary%3BDeFrancesco%2C+Carol%3BLevesque%2C+Chantal%3BSharp%2C+Daryl+L%3BOgedegbe%2C+Gbenga%3BResnick%2C+Barbara%3BOrwig%2C+Denise&rft.aulast=Borrelli&rft.aufirst=Belinda&rft.date=2005-10-01&rft.volume=73&rft.issue=5&rft.spage=852&rft.isbn=&rft.btitle=&rft.title=Journal+of+consulting+and+clinical+psychology&rft.issn=0022006X&rft_id=info:doi/10.1037%2F0022-006X.73.5.852
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 4551; 7994; 7890 5792 10484; 2688 2449 10404; 2388 10404
DO  - http://dx.doi.org/10.1037/0022-006X.73.5.852
ER  - 



TY  - JOUR
T1  - Epidemiology of HIV/AIDS among Asians and Pacific islanders in the United States
AN  - 36440010; 3331506
AB  - Although the percentage of overall AIDS diagnoses remains low among Asian and Pacific Islanders (APIs) in the United States compared with other racial/ethnic groups, research on API risk behaviors and health status suggest that the low number of AIDS cases may not provide a full picture of the epidemic and issues faced by this understudied and underserved population. Data from national HIV/AIDS surveillance systems and the Behavioral Risk Factor Surveillance System (BRFSS) were examined to delineate the magnitude and course of the HIV/AIDS epidemic among APIs in the United States. Same-sex sexual activity is the main HIV risk for API men, whereas heterosexual contact is for API women. APIs are significantly less likely to report being tested for HIV despite the fact that a similar proportion of APIs and other racial/ethnic groups reported having HIV risk in the past 12 months. Given the enormous diversity among APIs in the United States it is important to collect detailed demographic information to improve race/ethnicity and HIV risk classification, conduct better behavioral and disease monitoring for informing prevention planning, and addressing cultural, linguistic, economic and legal barriers to HIV prevention among APIs. Reprinted by permission of Guilford Publications Inc., New York City
JF  - AIDS education and prevention
AU  - Zaidi, Irum F
AU  - Crepaz, Nicole
AU  - Song, Ruiguang
AU  - Wan, Choi K
AU  - Lin, Lillian S
AU  - Hu, Dale J
AU  - Sy, Francisco S
AD  - Centers for Disease Control and Prevention ; National Institutes of Health
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 405
EP  - 417
VL  - 17
IS  - 5
SN  - 0899-9546, 0899-9546
KW  - Sociology
KW  - Epidemiology
KW  - AIDS
KW  - Health
KW  - Diseases
KW  - U.S.A.
KW  - HIV
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/36440010?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=AIDS+education+and+prevention&rft.atitle=Epidemiology+of+HIV%2FAIDS+among+Asians+and+Pacific+islanders+in+the+United+States&rft.au=Zaidi%2C+Irum+F%3BCrepaz%2C+Nicole%3BSong%2C+Ruiguang%3BWan%2C+Choi+K%3BLin%2C+Lillian+S%3BHu%2C+Dale+J%3BSy%2C+Francisco+S&rft.aulast=Zaidi&rft.aufirst=Irum&rft.date=2005-10-01&rft.volume=17&rft.issue=5&rft.spage=405&rft.isbn=&rft.btitle=&rft.title=AIDS+education+and+prevention&rft.issn=08999546&rft_id=info:doi/
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 4357 7894; 3617 6220; 482 3617 6220; 5703 3617 6220; 5772; 433 293 14
ER  - 



TY  - JOUR
T1  - HIV/AIDS among Asians and Pacific islanders in the United States
AN  - 36438819; 3331559
JF  - AIDS education and prevention
AU  - Choi, Kyung-Hee
AU  - Wong, Frank
AU  - Zaidi, Irum F
AU  - Crepaz, Nicole
AU  - Song, Ruiguang
AU  - Wan, Choi K
AU  - Lin, Lillian S
AU  - Hu, Dale J
AU  - Sy, Francisco S
AU  - Operario, Don
AU  - Gregorich, Steven E
AU  - McFarland, Willi
AU  - MacKellar, Duncan
AU  - Valleroy, Linda
AU  - Nemoto, Tooru
AU  - Iwamoto, Mariko
AU  - Oh, Hyun Joo
AU  - Wong, Serena
AU  - Nguyen, Hongmai
AU  - So, Dominicus W
AU  - DeLeon, Jordana M
AU  - Lin, Peter
AU  - Simoni, Jane M
AU  - Zemon, Vance
AU  - Chin, John J
AU  - Mantell, Joanne
AU  - Weiss, Linda
AU  - Bhagavan, Mamatha
AU  - Luo, Xiaoting
AD  - University of California ; Georgetown University ; Centers for Disease Control and Prevention ; National Institutes of Health ; University California ; San Francisco Department of Public Health ; Howard University ; Columbia University ; University of Washington ; Yeshiva University ; New York Academy of Medicine
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 405
EP  - 502
VL  - 17
IS  - 5
SN  - 0899-9546, 0899-9546
KW  - Sociology
KW  - Sexual behaviour
KW  - AIDS
KW  - Immigrants
KW  - Health
KW  - Homosexuality
KW  - U.S.A.
KW  - Students
KW  - Models
KW  - Risk
KW  - Prevention
KW  - Sex workers
KW  - Epidemiology
KW  - Transsexuality
KW  - Religious institutions
KW  - Drug use
KW  - HIV
KW  - Sexual intercourse
KW  - Sex
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/36438819?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aibss&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=AIDS+education+and+prevention&rft.atitle=HIV%2FAIDS+among+Asians+and+Pacific+islanders+in+the+United+States&rft.au=Choi%2C+Kyung-Hee%3BWong%2C+Frank%3BZaidi%2C+Irum+F%3BCrepaz%2C+Nicole%3BSong%2C+Ruiguang%3BWan%2C+Choi+K%3BLin%2C+Lillian+S%3BHu%2C+Dale+J%3BSy%2C+Francisco+S%3BOperario%2C+Don%3BGregorich%2C+Steven+E%3BMcFarland%2C+Willi%3BMacKellar%2C+Duncan%3BValleroy%2C+Linda%3BNemoto%2C+Tooru%3BIwamoto%2C+Mariko%3BOh%2C+Hyun+Joo%3BWong%2C+Serena%3BNguyen%2C+Hongmai%3BSo%2C+Dominicus+W%3BDeLeon%2C+Jordana+M%3BLin%2C+Peter%3BSimoni%2C+Jane+M%3BZemon%2C+Vance%3BChin%2C+John+J%3BMantell%2C+Joanne%3BWeiss%2C+Linda%3BBhagavan%2C+Mamatha%3BLuo%2C+Xiaoting&rft.aulast=Choi&rft.aufirst=Kyung-Hee&rft.date=2005-10-01&rft.volume=17&rft.issue=5&rft.spage=405&rft.isbn=&rft.btitle=&rft.title=AIDS+education+and+prevention&rft.issn=08999546&rft_id=info:doi/
LA  - English
DB  - International Bibliography of the Social Sciences (IBSS)
N1  - Date revised - 2013-06-12
N1  - SuppNotes - Collection of 7 articles
N1  - Last updated - 2013-09-16
N1  - SubjectsTermNotLitGenreText - 4357 7894; 3753 3755; 5969 11579 11538; 11567 11563 1025 1542 11325 6071; 11035; 11563 1025 1542 11325 6071; 12947 11579 11538; 11556 13682; 11538; 12334 4049; 8163; 6232 8037; 10072; 10813 6590; 482 3617 6220; 5703 3617 6220; 5772; 433 293 14
ER  - 



TY  - JOUR
T1  - Prolonged Hospital Stay for Extremely Premature Infants: Risk Factors, Center Differences, and the Impact of Mortality on Selecting a Best-Performing Center
AN  - 220439406; 16079906
AB  - The first objective was to identify factors associated with prolonged hospital stay (PHS: hospitalized >42 weeks postmenstrual age) in extremely premature (EP: born less than or equal to 28 weeks gestation) infants. The second objective was to identify a PHS best-performing benchmark center.  
This study was a retrospective cohort analysis of infants born < or =28 weeks gestation and admitted to one of 12 tertiary centers between January 1998 and October 2001. Risk-adjusted odds of PHS, defined as hospitalization beyond 42 weeks postmenstrual age, and the competing outcome, mortality, were assessed using logistic regression models.  
Among 3892 EP survivors who had complete data for multivariable analysis, 685 (18%) had PHS. Variables contributing to PHS included chronic lung disease (oxygen use at discharge home or 36 week postmenstrual age) (OR 6.75; 95% CI: 5.04 to 9.03), necrotizing enterocolitis requiring surgery (OR 13.83; 95% CI: 8.05 to 23.76), and >two episodes of late-onset sepsis (OR 2.39; 95% CI: 1.66 to 3.44). Centers' risk-adjusted PHS odds differed from the reference center, which had the lowest incidence of PHS and mortality (overall P-value <0.0001). Mortality contributed to PHS, but in an opposite direction compared to other factors. Centers with lowest PHS odds were among those with highest mortality.  
These findings suggest that reduction of CLD, surgical NEC, and late onset sepsis could reduce PHS in EP infants. Risk adjusted odds of PHS and mortality are both crucial for selecting a PHS best-performing center.
JF  - Journal of Perinatology
AU  - Cotten, C Michael
AU  - Oh, William
AU  - McDonald, Scott
AU  - Carlo, Waldemar
AU  - Fanaroff, Avroy A
AU  - Duara, Shahnaz
AU  - Stoll, Barbara
AU  - Abbot Laptook
AU  - Poole, Kenneth
AU  - Wright, Linda L
AU  - Goldberg, Ronald N
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 650
EP  - 5
CY  - New York
PB  - Nature Publishing Group
VL  - 25
IS  - 10
SN  - 07438346
KW  - Medical Sciences--Pediatrics
KW  - Logistic Models
KW  - Risk Factors
KW  - Humans
KW  - Treatment Outcome
KW  - Retrospective Studies
KW  - Infant, Newborn
KW  - Length of Stay
KW  - Infant Mortality
KW  - Health Facilities -- classification
KW  - Infant, Premature
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/220439406?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ahealthcompleteshell&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Perinatology&rft.atitle=Prolonged+Hospital+Stay+for+Extremely+Premature+Infants%3A+Risk+Factors%2C+Center+Differences%2C+and+the+Impact+of+Mortality+on+Selecting+a+Best-Performing+Center&rft.au=Cotten%2C+C+Michael%3BOh%2C+William%3BMcDonald%2C+Scott%3BCarlo%2C+Waldemar%3BFanaroff%2C+Avroy+A%3BDuara%2C+Shahnaz%3BStoll%2C+Barbara%3BAbbot+Laptook%3BPoole%2C+Kenneth%3BWright%2C+Linda+L%3BGoldberg%2C+Ronald+N&rft.aulast=Cotten&rft.aufirst=C&rft.date=2005-10-01&rft.volume=25&rft.issue=10&rft.spage=650&rft.isbn=&rft.btitle=&rft.title=Journal+of+Perinatology&rft.issn=07438346&rft_id=info:doi/10.1038%2Fsj.jp.7211369
LA  - English
DB  - ProQuest Central
N1  - Copyright - Copyright Nature Publishing Group Oct 2005
N1  - Last updated - 2014-04-30
DO  - http://dx.doi.org/10.1038/sj.jp.7211369
ER  - 



TY  - JOUR
T1  - Rehospitalization of Extremely Low Birth Weight (ELBW) Infants: Are There Racial/Ethnic Disparities?
AN  - 220407556; 16107873
AB  - Premature infants are at increased risk for rehospitalization after discharge from the hospital. Racial disparities are known to exist in pediatric health care.  
To evaluate whether racial disparities exist in the proportion of extremely low birth weight (ELBW) infants rehospitalized prior to 18 months corrected age and the causes of rehospitalization.  
The National Institute of Child Health and Human Development Neonatal Research Network database was used to identify all ELBW infants (n=2446) who were born between November 1, 1998 and May 31, 2000 at the 14 participating centers and discharged alive (n=1591). Infants were seen at 18-22 months corrected age for followup. Data related to maternal variables, race, socioeconomic status, medical morbidities, insurance, and rehospitalizations were recorded from the medical record and parent interview. Logistic regression analyses were used to examine the relationship of race/ethnicity and rehospitalization while controlling for gestational age, gender, center, maternal education, family income, bronchopulmonary dysplasia (BPD), necrotizing enterocolitis, ventriculoperitoneal (VP) shunt, respiratory syncytial virus (RSV) prophylaxis, and insurance type.  
In all, 1405 (88%) infants were evaluated at followup. The racial distribution of infants admitted, discharged, seen at followup, and rehospitalized were similar. Rehospitalization occurred at least once in 49% of the infants. In the logistic regression analyses, race was not a significant predictor for rehospitalization. The odds of rehospitalization were related to low family income, type of insurance, BPD, VP shunt, RSV prophylaxis, and center.  
Race was not a predominant variable in the risk of rehospitalization in this cohort of ELBW infants. Medical morbidities and low family income appear to be the major risk factors for rehospitalization.
JF  - Journal of Perinatology
AU  - Morris, Brenda H
AU  - Gard, Charlotte C
AU  - Kennedy, Kathleen
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 656
EP  - 63
CY  - New York
PB  - Nature Publishing Group
VL  - 25
IS  - 10
SN  - 07438346
KW  - Medical Sciences--Pediatrics
KW  - United States
KW  - Regression Analysis
KW  - Humans
KW  - Infant, Newborn
KW  - African Americans
KW  - Morbidity
KW  - Income
KW  - Socioeconomic Factors
KW  - Infant
KW  - Hispanic Americans
KW  - Insurance, Health
KW  - Databases, Factual
KW  - Female
KW  - Male
KW  - Patient Readmission -- statistics & numerical data
KW  - Infant, Very Low Birth Weight
KW  - Continental Population Groups
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/220407556?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ahealthcompleteshell&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Perinatology&rft.atitle=Rehospitalization+of+Extremely+Low+Birth+Weight+%28ELBW%29+Infants%3A+Are+There+Racial%2FEthnic+Disparities%3F&rft.au=Morris%2C+Brenda+H%3BGard%2C+Charlotte+C%3BKennedy%2C+Kathleen&rft.aulast=Morris&rft.aufirst=Brenda&rft.date=2005-10-01&rft.volume=25&rft.issue=10&rft.spage=656&rft.isbn=&rft.btitle=&rft.title=Journal+of+Perinatology&rft.issn=07438346&rft_id=info:doi/10.1038%2Fsj.jp.7211361
LA  - English
DB  - ProQuest Central
N1  - Copyright - Copyright Nature Publishing Group Oct 2005
N1  - Last updated - 2014-04-30
DO  - http://dx.doi.org/10.1038/sj.jp.7211361
ER  - 



TY  - JOUR
T1  - Summary Report: Early Reproductive Events and Breast Cancer Workshop
AN  - 215288747; 16419725
AB  - A summary report on Reproductive Events and Breast Cancer Workshop is presented. The Workshop was established to provide an integrated scientific assessment of the association between reproductive events and the risk of breast cancer.
JF  - Issues in Law & Medicine
AU  - Anonymous
Y1  - 2005///Fall
PY  - 2005
DA  - Fall 2005
SP  - 161
EP  - 5
CY  - Terre Haute
PB  - National Legal Center for the Medically Dependent and Disabled Inc.
VL  - 21
IS  - 2
SN  - 87568160
KW  - Medical Sciences
KW  - Workshops
KW  - Breast cancer
KW  - Health risk assessment
KW  - Pregnancy
KW  - United States
KW  - Education
KW  - Humans
KW  - Health Knowledge, Attitudes, Practice
KW  - Female
KW  - Reproductive Behavior
KW  - Breast Neoplasms -- etiology
KW  - Risk Assessment
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/215288747?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acriminaljusticeperiodicals&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Issues+in+Law+%26+Medicine&rft.atitle=Summary+Report%3A+Early+Reproductive+Events+and+Breast+Cancer+Workshop&rft.au=Anonymous&rft.aulast=Anonymous&rft.aufirst=&rft.date=2005-10-01&rft.volume=21&rft.issue=2&rft.spage=161&rft.isbn=&rft.btitle=&rft.title=Issues+in+Law+%26+Medicine&rft.issn=87568160&rft_id=info:doi/
LA  - English
DB  - ProQuest Central
N1  - Copyright - Copyright National Legal Center for the Medically Dependent & Disabled Inc. Fall 2005
N1  - Last updated - 2014-12-13
ER  - 



TY  - JOUR
T1  - Cancer Facts: Abortion, Miscarriage, and Breast Cancer Risk
AN  - 215288670; 16419724
AB  - A woman's hormone levels normally change throughout her life for a variety of reasons, and these hormonal change can lead to changes in her breasts. Here, several extensive research on the relationship between induced and spontaneous abortion and breast cancer risk later in life are described.
JF  - Issues in Law & Medicine
AU  - Anonymous
Y1  - 2005///Fall
PY  - 2005
DA  - Fall 2005
SP  - 159
EP  - 60
CY  - Terre Haute
PB  - National Legal Center for the Medically Dependent and Disabled Inc.
VL  - 21
IS  - 2
SN  - 87568160
KW  - Medical Sciences
KW  - Medical research
KW  - Abortion
KW  - Miscarriage
KW  - Breast cancer
KW  - Women
KW  - Health risk assessment
KW  - United States
KW  - Risk Factors
KW  - Humans
KW  - Female
KW  - Abortion, Induced
KW  - Breast Neoplasms -- etiology
KW  - Abortion, Spontaneous
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/215288670?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acriminaljusticeperiodicals&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Issues+in+Law+%26+Medicine&rft.atitle=Cancer+Facts%3A+Abortion%2C+Miscarriage%2C+and+Breast+Cancer+Risk&rft.au=Anonymous&rft.aulast=Anonymous&rft.aufirst=&rft.date=2005-10-01&rft.volume=21&rft.issue=2&rft.spage=159&rft.isbn=&rft.btitle=&rft.title=Issues+in+Law+%26+Medicine&rft.issn=87568160&rft_id=info:doi/
LA  - English
DB  - ProQuest Central
N1  - Copyright - Copyright National Legal Center for the Medically Dependent & Disabled Inc. Fall 2005
N1  - Last updated - 2014-12-13
ER  - 



TY  - JOUR
T1  - A model of lysosomal metabolism of dextran coated superparamagnetic iron oxide (SPIO) nanoparticles: implications for cellular magnetic resonance imaging
AN  - 21067493; 8632077
AB  - Ferumoxides, dextran-coated superparamagnetic iron oxide (SPIO) particles, form ferumoxide-transfection agent (FE-TA) complexes that are internalized into endosomes/lysosomes and have been used to label cells for in vivo MRI tracking and localization studies. A better understanding of the physical state of the FE-TA complexes during endocytosis could improve their use. The purpose of this study was to measure the rate of the degradation of iron particles under varying physiological conditions. FE-TA complexes were incubated in seven different buffers containing different chelates with different pH. Reducible iron concentrations, T2 relaxation rates and gradient echo (GRE) magnetic resonance images (MRI) were obtained from each condition immediately after incubation and at 6, 24, 48, 72 and 96h and days 7, 14 and 21. The dynamics of FE-TA in the endosome/lysomes within the cells were visualized with electron microscopy. Sodium citrate buffer at pH 4.5 rapidly dissolved FE-TA complexes. However, FE-TA complexes were less soluble in the same buffer at pH 5.5. Similarly, FE-TA complexes were not readily soluble in any of the other buffers with or without chelates, regardless of pH. Electron microscopic images showed degraded FE-TA in some intracellular endosome/lysosomes between days 3 and 5. In the cellular environment, some of the FE-TA-containing endosomes were found to fuse with lysosomes, causing rapid dissociation at low pH and exposing the iron core to chelates that resulted in soluble Fe(III) within the lysosomes. The studies presented represent a first step in identifying the important cellular environmental parameters affecting the integrity of FE-TA complexes. Published in 2005 by John Wiley & Sons, Ltd.
JF  - NMR in Biomedicine
AU  - Arbab, Ali S
AU  - Wilson, Lindsey B
AU  - Ashari, Parwana
AU  - Jordan, Elaine K
AU  - Lewis, Bobbi K
AU  - Frank, Joseph A
AD  - Experimental Neuroimaging Section, Laboratory of Diagnostic Radiology Research, National Institutes of Health, Bethesda, Maryland, USA, Saali@rad.hfh.edu
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 383
EP  - 389
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 18
IS  - 6
SN  - 0952-3480, 0952-3480
KW  - Biotechnology and Bioengineering Abstracts
KW  - sodium citrate
KW  - Dextran
KW  - iron oxides
KW  - Magnetic resonance imaging
KW  - Endocytosis
KW  - endosomes
KW  - N.M.R.
KW  - Chelates
KW  - nanoparticles
KW  - Iron
KW  - pH effects
KW  - Electron microscopy
KW  - Metabolism
KW  - Lysosomes
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/21067493?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=NMR+in+Biomedicine&rft.atitle=A+model+of+lysosomal+metabolism+of+dextran+coated+superparamagnetic+iron+oxide+%28SPIO%29+nanoparticles%3A+implications+for+cellular+magnetic+resonance+imaging&rft.au=Arbab%2C+Ali+S%3BWilson%2C+Lindsey+B%3BAshari%2C+Parwana%3BJordan%2C+Elaine+K%3BLewis%2C+Bobbi+K%3BFrank%2C+Joseph+A&rft.aulast=Arbab&rft.aufirst=Ali&rft.date=2005-10-01&rft.volume=18&rft.issue=6&rft.spage=383&rft.isbn=&rft.btitle=&rft.title=NMR+in+Biomedicine&rft.issn=09523480&rft_id=info:doi/10.1002%2Fnbm.970
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-12-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - pH effects; Lysosomes; endosomes; Magnetic resonance imaging; Iron; Chelates; iron oxides; nanoparticles; N.M.R.; Metabolism; Dextran; Endocytosis; Electron microscopy; sodium citrate
DO  - http://dx.doi.org/10.1002/nbm.970
ER  - 



TY  - JOUR
T1  - Normal and Cystic Fibrosis Airway Surface Liquid Homeostasis: THE EFFECTS OF PHASIC SHEAR STRESS AND VIRAL INFECTIONS
AN  - 21044834; 6503552
AB  - Mammalian airways normally regulate the volume of a thin liquid layer, the periciliary liquid (PCL), to facilitate the mucus clearance component of lung defense. Studies under standard (static) culture conditions revealed that normal airway epithelia possess an adenosine-regulated pathway that blends Na super(+) absorption and Cl super(-) secretion to optimize PCL volume. In cystic fibrosis (CF), the absence of CF transmembrane conductance regulator results in a failure of adenosine regulation of PCL volume, which is predicted to initiate mucus stasis and infection. However, under conditions that mimic the phasic motion of the lung in vivo, ATP release into PCL was increased, CF ion transport was rebalanced, and PCL volume was restored to levels adequate for lung defense. This ATP signaling system was vulnerable, however, to insults that trigger CF bacterial infections, such as viral (respiratory syncitial virus) infections, which up-regulated extracellular ATPase activity and abolished motion-dependent ATP regulation of CF PCL height. These studies demonstrate (i) how the normal coordination of opposing ion transport pathways to maintain PCL volume is disrupted in CF, (ii) the hitherto unknown role of phasic motion in regulating key aspects of normal and CF innate airways defense, and (iii) that maneuvers directed at increasing motion-induced nucleotide release may be therapeutic in CF patients.
JF  - Journal of Biological Chemistry
AU  - Tarran, Robert
AU  - Button, Brian
AU  - Picher, Maryse
AU  - Paradiso, Anthony M
AU  - Ribeiro, Carla M
AU  - Lazarowski, Eduardo R
AU  - Zhang, Liqun
AU  - Collins, Peter L
AU  - Pickles, Raymond J
AU  - Fredberg, Jeffrey J
AU  - Boucher, Richard C
AD  - Cystic Fibrosis/Pulmonary Research and Treatment Center, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599-7248, Laboratory of Infectious Diseases, NIAID, National Institutes of Health, Bethesda, Maryland 20892-0720, and School of Public Health, Harvard University, Boston, Massachusetts 02115
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 35751
EP  - 35759
PB  - American Society for Biochemistry and Molecular Biology, 9650 Rockville Pike Bethesda MD 20814-3996 USA, [mailto:asbmb@asbmb.faseb.org], [URL:http://www.jbc.org]
VL  - 280
IS  - 42
SN  - 0021-9258, 0021-9258
KW  - Microbiology Abstracts B: Bacteriology; Virology & AIDS Abstracts
KW  - Adenosinetriphosphatase
KW  - Secretion
KW  - ATP
KW  - Chloride
KW  - Mucus
KW  - Homeostasis
KW  - Infection
KW  - Nucleotides
KW  - Mechanical stimuli
KW  - Lung
KW  - Adenosine
KW  - Cystic fibrosis
KW  - Signal transduction
KW  - Respiratory tract
KW  - J 02410:Animal Diseases
KW  - V 22320:Replication
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/21044834?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Biological+Chemistry&rft.atitle=Normal+and+Cystic+Fibrosis+Airway+Surface+Liquid+Homeostasis%3A+THE+EFFECTS+OF+PHASIC+SHEAR+STRESS+AND+VIRAL+INFECTIONS&rft.au=Tarran%2C+Robert%3BButton%2C+Brian%3BPicher%2C+Maryse%3BParadiso%2C+Anthony+M%3BRibeiro%2C+Carla+M%3BLazarowski%2C+Eduardo+R%3BZhang%2C+Liqun%3BCollins%2C+Peter+L%3BPickles%2C+Raymond+J%3BFredberg%2C+Jeffrey+J%3BBoucher%2C+Richard+C&rft.aulast=Tarran&rft.aufirst=Robert&rft.date=2005-10-01&rft.volume=280&rft.issue=42&rft.spage=35751&rft.isbn=&rft.btitle=&rft.title=Journal+of+Biological+Chemistry&rft.issn=00219258&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-12-01
N1  - Last updated - 2015-03-27
N1  - SubjectsTermNotLitGenreText - Adenosinetriphosphatase; Secretion; ATP; Mucus; Chloride; Homeostasis; Infection; Nucleotides; Mechanical stimuli; Lung; Cystic fibrosis; Adenosine; Respiratory tract; Signal transduction
ER  - 



TY  - JOUR
T1  - Variable Tick Protein in Two Genomic Groups of the Relapsing Fever Spirochete Borrelia hermsii in Western North America
AN  - 20983771; 6527448
AB  - Borrelia hermsii is the primary cause of tick-borne relapsing fever in North America. When its tick vector, Ornithodoros hermsi, acquires these spirochetes from the blood of an infected mammal, the bacteria switch their outer surface from one of many bloodstream variable major proteins (Vmps) to a unique protein, Vtp (Vsp33). Vtp may be critical for successful tick transmission of B. hermsii; however, the gene encoding this protein has been described previously in only one isolate. Here we identified and sequenced the vtp gene in 31 isolates of B. hermsii collected over 40 years from localities throughout much of its known geographic distribution. Seven major Vtp types were found. Little or no sequence variation existed within types, but between them significant variation was observed, similar to the pattern of diversity described for the outer surface protein C (OspC) gene in Lyme disease spirochetes. The pattern of sequence relatedness among the Vtp types was incongruent in two branches compared to two genomic groups identified among the isolates by multilocus sequence typing of the 16S rRNA, flaB, gyrB, and glpQ genes. Therefore, both horizontal transfer and recombination within and between the two genomic groups were responsible for some of the variation observed in the vtp gene. O. hermsi ticks were capable of transmitting spirochetes in the newly identified genomic group. Therefore, given the longevity of the tick vector and persistent infection of spirochetes in ticks, these arthropods rather than mammals may be the likely host where the exchange of spirochetal DNA occurs.
JF  - Infection and Immunity
AU  - Porcella, Stephen F
AU  - Raffel, Sandra J
AU  - Anderson, Donald EJr
AU  - Gilk, Stacey D
AU  - Bono, James L
AU  - Schrumpf, Merry E
AU  - Schwan, Tom G
AD  - Laboratory of Human Bacterial Pathogenesis, Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, National Institutes of Health, 903 South 4th Street, Hamilton, Montana. Sacred Heart Medical Center, Spokane, Washington
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 6647
EP  - 6658
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 73
IS  - 10
SN  - 0019-9567, 0019-9567
KW  - Genetics Abstracts; Entomology Abstracts; Immunology Abstracts; Microbiology Abstracts B: Bacteriology
KW  - Borrelia hermsii
KW  - Geographical distribution
KW  - Relapsing fever
KW  - Persistent infection
KW  - Disease transmission
KW  - Recombination
KW  - outer surface protein C
KW  - tick-borne diseases
KW  - ospC gene
KW  - genomics
KW  - Lyme disease
KW  - North America
KW  - tick-borne relapsing fever
KW  - Ixodidae
KW  - DNA topoisomerase
KW  - Vectors
KW  - Horizontal transfer
KW  - Longevity
KW  - multilocus sequence typing
KW  - Blood
KW  - Spirochetes
KW  - Arthropoda
KW  - DNA
KW  - rRNA 16S
KW  - Ornithodoros
KW  - J 02870:Invertebrate bacteriology
KW  - Z 05350:Medical, Veterinary, and Agricultural Entomology
KW  - F 06910:Microorganisms & Parasites
KW  - G 07770:Bacteria
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20983771?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Infection+and+Immunity&rft.atitle=Variable+Tick+Protein+in+Two+Genomic+Groups+of+the+Relapsing+Fever+Spirochete+Borrelia+hermsii+in+Western+North+America&rft.au=Porcella%2C+Stephen+F%3BRaffel%2C+Sandra+J%3BAnderson%2C+Donald+EJr%3BGilk%2C+Stacey+D%3BBono%2C+James+L%3BSchrumpf%2C+Merry+E%3BSchwan%2C+Tom+G&rft.aulast=Porcella&rft.aufirst=Stephen&rft.date=2005-10-01&rft.volume=73&rft.issue=10&rft.spage=6647&rft.isbn=&rft.btitle=&rft.title=Infection+and+Immunity&rft.issn=00199567&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Geographical distribution; tick-borne relapsing fever; Relapsing fever; DNA topoisomerase; Vectors; Persistent infection; Longevity; Horizontal transfer; multilocus sequence typing; Disease transmission; Spirochetes; Blood; Recombination; outer surface protein C; tick-borne diseases; DNA; ospC gene; genomics; rRNA 16S; Lyme disease; Borrelia hermsii; Arthropoda; Ixodidae; Ornithodoros; North America
ER  - 



TY  - JOUR
T1  - S5FP: Spectrally selective suppression with steady state free precession
AN  - 20855769; 8367905
AB  - A method is presented that employs the inherent spectral selectivity of the Steady-State Free Precession (SSFP) pulse sequence to provide a spectral band of suppression. At TE = TR/2, SSFP partitions the magnetization into two phase-opposed spectral components. Z-storing one of these components simultaneously further excites the other, which is then suppressed by gradient crushing and RF spoiling. The Spectrally Selective Suppression with SSFP (S5FP) method is shown to provide significant attenuation of fat signals, while the water signals are essentially unaffected and provide the normal SSFP contrast. Fat suppression is achieved with relatively little temporal overhead (less than 10% reduction in temporal resolution). S5FP was validated using simulations, phantoms, and human studies.
JF  - Magnetic Resonance in Medicine
AU  - Derbyshire, J A
AU  - Herzka, D A
AU  - McVeigh, E R
AD  - Laboratory of Cardiac Energetics, National Heart, Lung and Blood Institute, National Institutes of Health, DHHS, Bethesda, MD 20892-1061, USA, jad11@nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 918
EP  - 928
PB  - John Wiley & Sons, Baffins Lane Chichester W. Sussex PO19 1UD UK, [mailto:customer@wiley.co.uk], [URL:http://www.wiley.com/]
VL  - 54
IS  - 4
SN  - 0740-3194, 0740-3194
KW  - Biotechnology and Bioengineering Abstracts
KW  - N.M.R.
KW  - W 30910:Imaging
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20855769?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Magnetic+Resonance+in+Medicine&rft.atitle=S5FP%3A+Spectrally+selective+suppression+with+steady+state+free+precession&rft.au=Derbyshire%2C+J+A%3BHerzka%2C+D+A%3BMcVeigh%2C+E+R&rft.aulast=Derbyshire&rft.aufirst=J&rft.date=2005-10-01&rft.volume=54&rft.issue=4&rft.spage=918&rft.isbn=&rft.btitle=&rft.title=Magnetic+Resonance+in+Medicine&rft.issn=07403194&rft_id=info:doi/10.1002%2Fmrm.20633
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-08-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - N.M.R.
DO  - http://dx.doi.org/10.1002/mrm.20633
ER  - 



TY  - JOUR
T1  - Evolutionary and functional genomics of the Archaea
AN  - 20851273; 8336564
AB  - In the past two years, archaeal genomics has achieved several breakthroughs. On the evolutionary front the most exciting development was the sequencing and analysis of the genome of Nanoarchaeum equitans, a tiny parasitic organism that has only 540 genes. The genome of Nanoarchaeum shows signs of extreme rearrangement including the virtual absence of conserved operons and the presence of several split genes. Nanoarchaeum is distantly related to other archaea, and it has been proposed to represent a deep archaeal branch that is distinct from Euryarchaeota and Crenarchaeota. This would imply that many features of its gene repertoire and genome organization might be ancestral. However, additional genome analysis has provided a more conservative suggestion - that Nanoarchaeum is a highly derived euryarchaeon. Also there have been substantial developments in functional genomics, including the discovery of the elusive aminoacyl-tRNA synthetase that is involved in both the biosynthesis of cysteine and its incorporation into proteins in methanogens, and the first experimental validation of the predicted archaeal exosome.
JF  - Current Opinion in Microbiology
AU  - Makarova, Kira S
AU  - Koonin, Eugene V
AD  - National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health, Bethesda, MD 20894, USA, koonin@ncbi.nlm.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 586
EP  - 594
PB  - Elsevier Science, The Boulevard Langford Lane Kidlington Oxford OX5 1GB UK, [mailto:usinfo-f@elsevier.com], [URL:http://www.elsevier.nl]
VL  - 8
IS  - 5
SN  - 1369-5274, 1369-5274
KW  - Microbiology Abstracts B: Bacteriology; Genetics Abstracts; Biochemistry Abstracts 2: Nucleic Acids
KW  - Archaea
KW  - exosomes
KW  - Nanoarchaeum equitans
KW  - Methanogenic bacteria
KW  - Crenarchaeota
KW  - Cysteine
KW  - Reviews
KW  - Euryarchaeota
KW  - genomics
KW  - Aminoacyl-tRNA ligase
KW  - Operons
KW  - Evolution
KW  - J 02310:Genetics & Taxonomy
KW  - N 14845:Miscellaneous
KW  - G 07770:Bacteria
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20851273?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Current+Opinion+in+Microbiology&rft.atitle=Evolutionary+and+functional+genomics+of+the+Archaea&rft.au=Makarova%2C+Kira+S%3BKoonin%2C+Eugene+V&rft.aulast=Makarova&rft.aufirst=Kira&rft.date=2005-10-01&rft.volume=8&rft.issue=5&rft.spage=586&rft.isbn=&rft.btitle=&rft.title=Current+Opinion+in+Microbiology&rft.issn=13695274&rft_id=info:doi/10.1016%2Fj.mib.2005.08.003
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-07-01
N1  - Last updated - 2015-03-27
N1  - SubjectsTermNotLitGenreText - exosomes; Cysteine; Reviews; Aminoacyl-tRNA ligase; genomics; Operons; Methanogenic bacteria; Evolution; Crenarchaeota; Archaea; Nanoarchaeum equitans; Euryarchaeota
DO  - http://dx.doi.org/10.1016/j.mib.2005.08.003
ER  - 



TY  - JOUR
T1  - Radiosyntheses and reactivities of novel [ super(18)F]2-fluoroethyl arylsulfonates
AN  - 20796092; 6462915
AB  - [ super(18)F]2-Fluoroethyl tosylate ([ super(18)F]FEOX, X=Ts) is widely used for labeling radiotracers for positron emission tomography (PET). Little work has been reported on syntheses of other [ super(18)F]2-fluoroethyl arylsulfonates ([ super(18)F]FEOX) that bear a less electron-rich aryl group, even though these might offer enhanced reactivities. Thus, a series of novel [ super(18)F]FEOX (X=benzenesulfonyl, brosyl, nosyl, 3,4-dibromobenzenesulfonyl) were synthesized and reactivities compared to [ super(18)F]FEOTs. Precursors for radiolabeling (bis- ethylene glycol arylsulfonates) and reference FEOX were synthesized (alcohol+arylsulfonyl chloride+KOSiMe sub(3) in THF). Regardless of substitution pattern, [ super(18)F]FEOX (110 degree C, 5 min, acetonitrile) were obtained in similar decay-corrected isolated radiochemical yields (RCY; 47-53%). All [ super(18)F]FEOX gave excellent RCYs (64-87%) of the dopamine uptake radioligand, [ super(18)F]FECNT (130 degree C, 10 min, acetonitrile). The 3,4-dibromobenzensulfonate gave the highest RCY of [ super(18)F]FECNT (87%) and this HPLC-purified labeling agent was used directly for efficient [ super(18)F]FECNT production. When the secondary aniline of an amyloid probe (HM-IMPY) or p-nitrophenol was reacted with [ super(18)F]FEOX, RCYs were appreciably higher for brosylate and nosylate than for tosylate, while 3,4- dibromobenzenesulfonate again gave the highest RCY. Owing to the high reactivity of the new [ super(18)F]FEOX and their ease of syntheses via stable precursors, such agents (particularly 3,4-dibromobenzenesulfonate) should be considered as alternatives to [ super(18)F]FEOTs.
JF  - Journal of Labelled Compounds and Radiopharmaceuticals
AU  - Musachio, John L
AU  - Shah, Jay
AU  - Pike, Victor W
AD  - PET Radiopharmaceutical Sciences, Molecular Imaging Branch, National Institute of Mental Health, National Institutes of Health, Building 10, Room B3 C346, 10 Center Drive, Bethesda, MD 20892-1003, USA, john.musachio@nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 735
EP  - 747
PB  - John Wiley & Sons, Inc., 111 River Street Hoboken NJ 07030 USA, [mailto:custserv@wiley.com], [URL:http://www.wiley.com/]
VL  - 48
IS  - 10
SN  - 0362-4803, 0362-4803
KW  - Biotechnology and Bioengineering Abstracts
KW  - Dopamine
KW  - Probes
KW  - Positron emission tomography
KW  - p-Nitrophenol
KW  - Ethylene glycol
KW  - Acetonitrile
KW  - Aniline
KW  - Amyloid
KW  - W 30940:Products
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20796092?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Labelled+Compounds+and+Radiopharmaceuticals&rft.atitle=Radiosyntheses+and+reactivities+of+novel+%5B+super%2818%29F%5D2-fluoroethyl+arylsulfonates&rft.au=Musachio%2C+John+L%3BShah%2C+Jay%3BPike%2C+Victor+W&rft.aulast=Musachio&rft.aufirst=John&rft.date=2005-10-01&rft.volume=48&rft.issue=10&rft.spage=735&rft.isbn=&rft.btitle=&rft.title=Journal+of+Labelled+Compounds+and+Radiopharmaceuticals&rft.issn=03624803&rft_id=info:doi/10.1002%2Fjlcr.991
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-08-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - Acetonitrile; Positron emission tomography; Probes; Amyloid; Aniline; Ethylene glycol; p-Nitrophenol; Dopamine
DO  - http://dx.doi.org/10.1002/jlcr.991
ER  - 



TY  - JOUR
T1  - Radiation Sensitivity of Human Carcinoma Cells Transfected with Small Interfering RNA Targeted against Cyclooxygenase-2
AN  - 20715213; 6508654
AB  - PURPOSE: Cyclooxygenase-2 (COX-2) is considered a potential target for cancer therapy, because COX-2 levels are elevated in the majority of human tumors compared with the normal tissues. COX-2 inhibitors inhibit tumor growth and enhance radiation response in vitro as well as in vivo. However, the precise role of COX-2 in radiation response is not clear. The purpose of the present study was to investigate the in vitro radiosensitivity of tumor cells as a function of COX-2 expression. Experimental Design and Results: PC3 and HeLa cells express COX-2 protein constitutively. We silenced the COX-2 gene in these cells using small interfering RNA (siRNA). Transfection of PC3 cells with 100 nmol/L siRNA targeted against COX-2 resulted in reduction of COX-2 protein by 75% and inhibition of arachidonic acid-induced prostaglandin E sub(2) synthesis by similar to 50% compared with the vehicle control. In HeLa cells, 100 nmol/L COX-2 siRNA inhibited COX-2 protein expression by 80%. Cell cycle analysis showed that transfection with COX-2 siRNA did not alter the cell cycle distribution. Radiosensitivity was determined by clonogenic cell survival assay. There was no significant difference in the radiosensitivity of cells in which COX-2 was silenced compared with the cells transfected vehicle or with negative control siRNAs (enhancement ratio = 1.1). CONCLUSIONS: These data indicate that the in vitro radiosensitivity of tumor cells is minimally dependent on the cellular COX-2 status. Given that a number of potential mechanisms are attributed to COX-2 inhibitors for radiosensitization, specific intervention of COX-2 by RNA interference could help elucidate the precise role of COX-2 in cancer therapy and to optimize strategies for COX-2 inhibition.
JF  - Clinical Cancer Research
AU  - Palayoor, Sanjeewani T
AU  - Arayankalayil, Moly J
AU  - Shoaibi, Azadeh
AU  - Coleman, CNorman
AD  - Radiation Oncology Branch, Center for Cancer Research, National Cancer Institute, NIH, Bethesda, Maryland
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 6980
EP  - 6986
PB  - American Association for Cancer Research, 615 Chestnut St., 17th Floor Philadelphia PA 19106-4404 USA, [URL:http://www.aacr.org/]
VL  - 11
IS  - 19
SN  - 1078-0432, 1078-0432
KW  - Biochemistry Abstracts 2: Nucleic Acids; Biotechnology and Bioengineering Abstracts
KW  - Cell survival
KW  - Cyclooxygenase-2
KW  - Data processing
KW  - Cell cycle
KW  - Radiosensitization
KW  - Prostaglandin E2
KW  - Tumors
KW  - Tumor cells
KW  - Cancer
KW  - Carcinoma
KW  - Radiation
KW  - siRNA
KW  - Transfection
KW  - RNA-mediated interference
KW  - Radiosensitivity
KW  - Gene silencing
KW  - N 14830:RNA
KW  - W 30915:Pharmaceuticals & Vaccines
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20715213?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+Cancer+Research&rft.atitle=Radiation+Sensitivity+of+Human+Carcinoma+Cells+Transfected+with+Small+Interfering+RNA+Targeted+against+Cyclooxygenase-2&rft.au=Palayoor%2C+Sanjeewani+T%3BArayankalayil%2C+Moly+J%3BShoaibi%2C+Azadeh%3BColeman%2C+CNorman&rft.aulast=Palayoor&rft.aufirst=Sanjeewani&rft.date=2005-10-01&rft.volume=11&rft.issue=19&rft.spage=6980&rft.isbn=&rft.btitle=&rft.title=Clinical+Cancer+Research&rft.issn=10780432&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-09-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Cyclooxygenase-2; Cell survival; Data processing; Cell cycle; Radiosensitization; Tumors; Prostaglandin E2; Tumor cells; Cancer; Carcinoma; siRNA; Radiation; Transfection; Radiosensitivity; RNA-mediated interference; Gene silencing
ER  - 



TY  - JOUR
T1  - Rational Development of Histone Deacetylase Inhibitors as Anticancer Agents: A Review
AN  - 20220856; 6528637
AB  - The epigenome is defined by DNA methylation patterns and the associated post-translational modifications of histones. This histone code determines the expression status of individual genes dependent upon their localization on the chromatin. The histone deacetylases (HDACs) play a major role in keeping the balance between the acetylated and deacetylated states of chromatin and eventually regulate gene expression. Recent developments in understanding the cancer cell cycle, specifically the interplay with chromatin control, are providing opportunities for developing mechanism-based therapeutic drugs. Inhibitors of HDACs are under considerable exploration, in part because of their potential roles in reversing the silenced genes in transformed tumor cells by modulating transcriptional processes. This review is an effort to summarize the nonclinical and clinical status of HDAC inhibitors currently under development in anticancer therapy.
JF  - Molecular Pharmacology
AU  - Acharya, Milin R
AU  - Sparreboom, Alex
AU  - Venitz, Juergen
AU  - Figg, William D
AD  - Clinical Pharmacology Research Core, National Cancer Institute, National Institutes of Health, Bethesda, Maryland (M.R.A., A.S., W.D.F.)
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 917
EP  - 932
PB  - Williams & Wilkins, 351 W. Camden St. Baltimore MD 21201 USA, [URL:http://www.lww.com/]
VL  - 68
IS  - 4
SN  - 0026-895X, 0026-895X
KW  - Biotechnology and Bioengineering Abstracts
KW  - Histone deacetylase
KW  - Chromatin
KW  - Post-translation
KW  - Reviews
KW  - Cell cycle
KW  - DNA methylation
KW  - Transcription
KW  - Antitumor agents
KW  - Tumor cells
KW  - Cancer
KW  - Gene silencing
KW  - W 30915:Pharmaceuticals & Vaccines
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/20220856?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Molecular+Pharmacology&rft.atitle=Rational+Development+of+Histone+Deacetylase+Inhibitors+as+Anticancer+Agents%3A+A+Review&rft.au=Acharya%2C+Milin+R%3BSparreboom%2C+Alex%3BVenitz%2C+Juergen%3BFigg%2C+William+D&rft.aulast=Acharya&rft.aufirst=Milin&rft.date=2005-10-01&rft.volume=68&rft.issue=4&rft.spage=917&rft.isbn=&rft.btitle=&rft.title=Molecular+Pharmacology&rft.issn=0026895X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Histone deacetylase; Post-translation; Chromatin; Reviews; Cell cycle; DNA methylation; Transcription; Tumor cells; Antitumor agents; Cancer; Gene silencing
ER  - 



TY  - JOUR
T1  - Diminished Lipoxin Biosynthesis in Severe Asthma
AN  - 199579013; 15961693
AB  - Severe asthma is characterized by increased airway inflammation that persists despite therapy with corticosteroids. It is not, however, merely an exaggeration of the eosinophilic inflammation that characterizes mild to moderate asthma; rather, severe asthma presents unique features. Although arachidonic acid metabolism is well appreciated to regulate airway inflammation and reactivity, alterations in the biosynthetic capacity for both pro- and antiinflammatory eicosanoids in severe asthma have not been determined.  
Patients with severe asthma were identified according to National Heart, Lung, and Blood Institute Severe Asthma Research Program criteria. Samples of whole blood from individuals with severe or moderate asthma were assayed for biosynthesis of lipoxygenase-derived eicosanoids.  
The counterregulatory mediator lipoxin A4 was detectable in low picogram amounts, using a novel fluorescence-based detection system. In activated whole blood, mean lipoxin A4 levels were decreased in severe compared with moderate asthma (0.4 [SD 0.4] ng/ml vs. 1.8 [SD 0.8] ng/ml, p=0.001). In sharp contrast, mean levels of prophlogistic cysteinyl leukotrienes were increased in samples from severe compared with moderate asthma (112.5 [SD 53.7] pg/ml vs. 64.4 [SD 24.8] pg/ml, p=0.03). Basal circulating levels of lipoxin A4 were also decreased in severe relative to moderate asthma. The marked imbalance in lipoxygenase-derived eicosanoid biosynthesis correlated with the degree of airflow obstruction.  
Mechanisms underlying airway responses in severe asthma include underproduction of lipoxins. This is the first report of a defect in lipoxin biosynthesis in severe asthma, and suggests an alternative therapeutic strategy that emphasizes natural counterregulatory pathways in the airways.
JF  - American Journal of Respiratory and Critical Care Medicine
AU  - Levy, Bruce D
AU  - Bonnans, Caroline
AU  - Silverman, Eric S
AU  - Palmer, Lyle J
AU  - et al
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 824
EP  - 30
CY  - New York
PB  - American Thoracic Society
VL  - 172
IS  - 7
SN  - 1073449X
KW  - Medical Sciences--Respiratory Diseases
KW  - Lipoxins
KW  - Membrane Proteins
KW  - Receptors, Leukotriene
KW  - leukotriene D4 receptor
KW  - lipoxin A4
KW  - Sputum -- chemistry
KW  - Membrane Proteins -- metabolism
KW  - Humans
KW  - Adult
KW  - Chromatography, High Pressure Liquid -- methods
KW  - Receptors, Leukotriene -- metabolism
KW  - Forced Expiratory Volume
KW  - Male
KW  - Female
KW  - Asthma -- physiopathology
KW  - Asthma -- metabolism
KW  - Lipoxins -- biosynthesis
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LA  - English
DB  - ProQuest Central
N1  - Copyright - Copyright American Thoracic Society Oct 1, 2005
N1  - Last updated - 2017-01-07
ER  - 



TY  - JOUR
T1  - Transvenous Access to the Pericardial Space: An Approach to Epicardial Lead Implantation for Cardiac Resynchronization Therapy
AN  - 19929413; 6563776
AB  - Background: Percutaneous access to the pericardial space (PS) may be useful for a number of therapeutic modalities including implantation of epicardial pacing leads. We have developed a catheter-based transvenous method to access the PS for implanting chronic medical devices. Methods: In eight pigs, a transseptal Mullins sheath and Brockenbrough needle were introduced into the right atrium (RA) from the jugular vein under fluoroscopic guidance. The PS was entered through a controlled puncture of the terminal anterior superior vena cava (SVC) (n = 7) or right atrial appendage (n = 1). A guidewire was advanced through the transseptal sheath, which was then removed leaving the wire in PS. The guidewire was used to direct both passive and active fixation pacing leads into the PS. Pacing was attempted and lead position was confirmed by cine fluoroscopy. Animals were sacrificed acutely and at 2 and 6 weeks. Results: All animals survived the procedure. Pericardial effusion (PE) during the procedure was hemodynamically significant in four of the eight animals. At necropsy, lead exit sites appeared to heal without complication at 2 and 6 weeks. Volume of pericardial fluid was 10.8 plus or minus 6.2 mL and appeared normal in four of the six chronic animals. Moderate fibrinous deposition was observed in two animals, which had exhibited significant over-procedural PE. Conclusions: Access to the PS via a transvenous approach is feasible. Pacing leads can be negotiated into this region. The puncture site heals with the lead in place. Further development should focus on eliminating PE and performing this technique in appropriate heart failure models.
JF  - Pacing and Clinical Electrophysiology
AU  - Mickelsen, Steven R
AU  - Ashikaga, Hiroshi
AU  - Desilva, Ranil
AU  - Raval, Amish N
AU  - Mcveigh, Elliot
AU  - Kusumoto, Fred
AD  - Address for reprints: Steven R. Mickelsen, B.A., Laboratory of Cardiac Energetics, National Heart Lung and Blood Institute Bldg. 10 Rm. B1D412 10 Center Drive, Bethesda, MD 20892, smickelsen@salud.unm.edu
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 1018
EP  - 1024
PB  - Blackwell Publishing Ltd., 9600 Garsington Road Oxford OX4 2DQ UK, [URL:http://www.blackwellpublishing.com]
VL  - 28
IS  - 10
SN  - 0147-8389, 0147-8389
KW  - Biotechnology and Bioengineering Abstracts
KW  - Heart
KW  - Autopsy
KW  - Effusion
KW  - Jugular vein
KW  - Sheaths
KW  - Electrophysiology
KW  - Development
KW  - Appendages
KW  - Models
KW  - fluoroscopy
KW  - Atrium
KW  - Heart diseases
KW  - W 30965:Miscellaneous, Reviews
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-07-01
N1  - SuppNotes - Figures, 5; references, 21.
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Heart; Autopsy; Effusion; Jugular vein; fluoroscopy; Appendages; Development; Electrophysiology; Sheaths; Atrium; Models; Heart diseases
DO  - http://dx.doi.org/10.1111/j.1540-8159.2005.00236.x
ER  - 



TY  - JOUR
T1  - Craniospinal Reduced Dose Radiotherapy After Myeoablative Chemotherapy with Peripheral Blood Stem Cells Rescue, in High Risk Medulloblastoma: Results of a Mono-Institutional Study in Italy
AN  - 19898561; 8067651
JF  - International Journal of Radiation Oncology, Biology, & Physics
AU  - Barra, S
AU  - Vitale, V
AU  - Dallorso, S
AU  - Milanaccio, C
AU  - Foppiano, F
AU  - Guenzi, M
AU  - Rossi, A
AU  - Pavanello, M
AU  - Nozza, P
AU  - Cama, A
AU  - Garre', M
AD  - Radiotherapy, National Cancer Institute, Genova, Italy
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 1
PB  - Elsevier Science, Box 882 New York NY 10159 USA, [mailto:usinfo-f@elsevier.com]
VL  - 63
SN  - 0360-3016, 0360-3016
KW  - Biotechnology and Bioengineering Abstracts
KW  - Stem cells
KW  - Chemotherapy
KW  - Risk factors
KW  - Medulloblastoma
KW  - Radiotherapy
KW  - Peripheral blood
KW  - W 30965:Miscellaneous, Reviews
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19898561?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=International+Journal+of+Radiation+Oncology%2C+Biology%2C+%26+Physics&rft.atitle=Craniospinal+Reduced+Dose+Radiotherapy+After+Myeoablative+Chemotherapy+with+Peripheral+Blood+Stem+Cells+Rescue%2C+in+High+Risk+Medulloblastoma%3A+Results+of+a+Mono-Institutional+Study+in+Italy&rft.au=Barra%2C+S%3BVitale%2C+V%3BDallorso%2C+S%3BMilanaccio%2C+C%3BFoppiano%2C+F%3BGuenzi%2C+M%3BRossi%2C+A%3BPavanello%2C+M%3BNozza%2C+P%3BCama%2C+A%3BGarre%27%2C+M&rft.aulast=Barra&rft.aufirst=S&rft.date=2005-10-01&rft.volume=63&rft.issue=&rft.spage=S25&rft.isbn=&rft.btitle=&rft.title=International+Journal+of+Radiation+Oncology%2C+Biology%2C+%26+Physics&rft.issn=03603016&rft_id=info:doi/10.1016%2Fj.ijrobp.2005.07.050
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-05-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Stem cells; Risk factors; Chemotherapy; Medulloblastoma; Radiotherapy; Peripheral blood
DO  - http://dx.doi.org/10.1016/j.ijrobp.2005.07.050
ER  - 



TY  - JOUR
T1  - Lymphomatoid Granulomatosis: Abnormalities of the Brain at MR Imaging
AN  - 19896219; 6529004
AB  - PURPOSE: To retrospectively evaluate the magnetic resonance (MR) imaging features of lymphomatoid granulomatosis in the brain. MATERIALS AND METHODS: The study, including retrospective analysis of data, was approved by the institutional review board of the National Cancer Institute and complied with Health Insurance Portability and Accountability Act. All patients gave written informed consent. Thirty-one patients with pathologically confirmed lymphomatoid granulomatosis were enrolled in a natural history and treatment study at the National Institutes of Health. Twenty-five patients (median age, 50 years; range, 18-62 years; 18 men, seven women) were evaluated with MR imaging of the brain at study entry for the presence of brain lesions and enhancing characteristics. Patients with abnormal findings were reexamined at intervals ranging from 2 to 19 months, as medically indicated. Cytologic analysis and flow cytometry of cerebrospinal fluid (CSF) were performed. Statistical analysis was performed to compare neurologic and CSF findings in patients with brain MR imaging abnormalities and in patients without abnormalities. The sensitivity of brain MR imaging was compared with that of CSF studies. RESULTS: Thirteen (52%) of 25 patients evaluated with MR imaging had a variety of brain abnormalities. Multiple focal intraparenchymal lesions, which exhibited T2 prolongation and commonly punctate or linear enhancement, were the most frequent abnormalities, and they were encountered in seven patients. The second most common finding was involvement of leptomeninges and cranial nerves, which manifested as abnormal enhancement on MR images obtained after contrast agent administration. This abnormality was seen in six patients. Involvement of dura mater was noted in another. Four patients had brain masses. Two had abnormal engorgement and intense enhancement of the choroid plexus. Most lesions resolved after treatment, but seven resulted in lacunar infarctions. Abnormal B cells were detected in the CSF with either cytologic techniques or flow cytometry in five patients. CONCLUSION: Lymphomatoid granulomatosis has a high rate of central nervous system involvement and a variable spectrum of lesions at MR imaging. Findings in this study suggest that MR imaging is more sensitive than CSF cytologic analysis or flow cytometry for detection of central nervous system involvement from lymphomatoid granulomatosis. [copy ] RSNA, 2005
JF  - Radiology
AU  - Patsalides, Athos D
AU  - Atac, Gokce
AU  - Hedge, Upendra
AU  - Janik, John
AU  - Grant, Nicole
AU  - Jaffe, Elaine S
AU  - Dwyer, Andrew
AU  - Patronas, Nicholas J
AU  - Wilson, Wyndham H
AD  - Department of Diagnostic Radiology, Warren Grant Magnuson Clinical Center, National Institutes of Health, Bldg 10, Room 1C660, 9000 Rockville Pike, Bethesda, MD 20892-1182 (A.D.P., G.A., A.D., N.J.P.)
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 265
EP  - 273
PB  - Radiological Society of North America, 820 Jorie Blvd. Oak Brook Illinois 60523-2251 USA
VL  - 237
IS  - 1
SN  - 0033-8419, 0033-8419
KW  - Immunology Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Central nervous system
KW  - Age
KW  - Neuroimaging
KW  - Magnetic resonance imaging
KW  - Statistical analysis
KW  - Flow cytometry
KW  - Cerebrospinal fluid
KW  - Contrast media
KW  - Dura mater
KW  - Cranial nerves
KW  - Granulomatosis
KW  - Data processing
KW  - Lymphocytes B
KW  - Brain
KW  - Choroid plexus
KW  - Cancer
KW  - Infarction
KW  - Engorgement
KW  - W 30910:Imaging
KW  - F 06915:Cancer Immunology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Radiology&rft.atitle=Lymphomatoid+Granulomatosis%3A+Abnormalities+of+the+Brain+at+MR+Imaging&rft.au=Patsalides%2C+Athos+D%3BAtac%2C+Gokce%3BHedge%2C+Upendra%3BJanik%2C+John%3BGrant%2C+Nicole%3BJaffe%2C+Elaine+S%3BDwyer%2C+Andrew%3BPatronas%2C+Nicholas+J%3BWilson%2C+Wyndham+H&rft.aulast=Patsalides&rft.aufirst=Athos&rft.date=2005-10-01&rft.volume=237&rft.issue=1&rft.spage=265&rft.isbn=&rft.btitle=&rft.title=Radiology&rft.issn=00338419&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-14
N1  - SubjectsTermNotLitGenreText - Magnetic resonance imaging; Cerebrospinal fluid; Granulomatosis; Neuroimaging; Brain; Flow cytometry; Central nervous system; Choroid plexus; Data processing; Contrast media; Statistical analysis; Cranial nerves; Lymphocytes B; Engorgement; Dura mater; Age; Infarction; Cancer
ER  - 



TY  - JOUR
T1  - Viral and cellular RNA helicases as antiviral targets
AN  - 19890946; 7964374
AB  - Although there has been considerable progress in the development of antiviral agents in recent years, there is still a pressing need for new drugs both to improve on the properties of existing agents and to combat the problem of viral resistance. Helicases, both viral and human, have recently emerged as novel targets for the treatment of viral infections. Here, we discuss the role of these enzymes, factors affecting their potential as drug targets and progress in the development of agents that inhibit their activity using the hepatitis C virus-encoded helicase NS3 and the cellular helicase DDX3 adopted for use by HIV-1 as examples.
JF  - Nature Reviews: Drug Discovery
AU  - Kwong, Ann D
AU  - Rao, BGovinda
AU  - Jeang, Kuan-Teh
AD  - Vertex Pharmaceuticals Inc., 130 Waverly Street, Cambridge, Massachusetts 02139, USA., kj7e@nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 845
EP  - 853
PB  - Nature Publishing Group, The Macmillan Building 4 Crinan Street London N1 9XW UK, [mailto:feedback@nature.com], [URL:http://www.nature.com/]
VL  - 4
IS  - 10
SN  - 1474-1784, 1474-1784
KW  - Microbiology Abstracts A: Industrial & Applied Microbiology; Virology & AIDS Abstracts; Biochemistry Abstracts 2: Nucleic Acids
KW  - RNA helicase
KW  - Antiviral agents
KW  - Human immunodeficiency virus 1
KW  - Enzymes
KW  - Drug development
KW  - Hepatitis C
KW  - Infection
KW  - DNA helicase
KW  - A 01340:Antibiotics & Antimicrobials
KW  - V 22360:AIDS and HIV
KW  - N 14830:RNA
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologya&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Nature+Reviews%3A+Drug+Discovery&rft.atitle=Viral+and+cellular+RNA+helicases+as+antiviral+targets&rft.au=Kwong%2C+Ann+D%3BRao%2C+BGovinda%3BJeang%2C+Kuan-Teh&rft.aulast=Kwong&rft.aufirst=Ann&rft.date=2005-10-01&rft.volume=4&rft.issue=10&rft.spage=845&rft.isbn=&rft.btitle=&rft.title=Nature+Reviews%3A+Drug+Discovery&rft.issn=14741784&rft_id=info:doi/10.1038%2Fnrd1853
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-03-01
N1  - Last updated - 2015-03-27
N1  - SubjectsTermNotLitGenreText - RNA helicase; Antiviral agents; Enzymes; Drug development; Hepatitis C; Infection; DNA helicase; Human immunodeficiency virus 1
DO  - http://dx.doi.org/10.1038/nrd1853
ER  - 



TY  - JOUR
T1  - HLA-A*0201, HLA-A*1101, and HLA-B*0702 Transgenic Mice Recognize Numerous Poxvirus Determinants from a Wide Variety of Viral Gene Products
AN  - 19818419; 6504277
AB  - In virus models explored in detail in mice, CTL typically focus on a few immunodominant determinants. In this study we use a multipronged approach to understand the diversity of CTL responses to vaccinia virus, a prototypic poxvirus with a genome similar to 20-fold larger than that of the model RNA viruses typically studied in mice. Based on predictive computational algorithms for peptide binding to HLA supertypes, we synthesized a panel of 2889 peptides to begin to create an immunomic map of human CTL responses to poxviruses. Using this panel in conjunction with CTLs from vaccinia virus-infected HLA transgenic mice, we identified 14 HLA-A*0201-, 4 HLA-A*1101-, and 3 HLA-B*0702-restricted CD8 super(+) T cell determinants distributed over 20 distinct proteins. These peptides were capable of binding one or multiple A2, A3, and B7 supertype molecules with affinities typical of viral determinants. Surprisingly, many of the viral proteins recognized are predicted to be late gene products, in addition to the early intermediate gene products expected. Nearly all of the determinants identified have identical counterparts encoded by modified vaccinia virus Ankara as well as variola virus, the agent of smallpox. These findings have implications for the design of new smallpox vaccines and the understanding of immune responses to large DNA viruses in general.
JF  - Journal of Immunology
AU  - Pasquetto, Valerie
AU  - Bui, Huynh-Hoa
AU  - Giannino, Rielle
AU  - Mirza, Fareed
AU  - Sidney, John
AU  - Oseroff, Carla
AU  - Tscharke, David C
AU  - Irvine, Kari
AU  - Bennink, Jack R
AU  - Peters, Bjoern
AU  - Southwood, Scott
AU  - Cerundolo, Vincenzo
AU  - Grey, Howard
AU  - Yewdell, Jonathan W
AU  - Sette, Alessandro
AD  - La Jolla Institute for Allergy and Immunology, San Diego, CA 92109. Tumor Immunology Unit, Weatherall Institute of Molecular Medicine, Oxford University, Oxford, United Kingdom. Epimmune Incorporated, San Diego, CA 92121. Laboratory of Viral Diseases, National Institutes of Health, Bethesda, MD 20892. Division of Immunology and Infectious Diseases, Queensland Institute of Medical Research, Herston, Queensland, Australia
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 5504
EP  - 5515
PB  - American Association of Immunologists, 9650 Rockville Pike Bethesda MD 20814-3998 USA, [URL:http://www.jimmunol.org/]
VL  - 175
IS  - 8
SN  - 0022-1767, 0022-1767
KW  - smallpox virus
KW  - Genetics Abstracts; Biotechnology and Bioengineering Abstracts; Virology & AIDS Abstracts; Immunology Abstracts
KW  - Genomes
KW  - Histocompatibility antigen HLA
KW  - Vaccinia
KW  - Algorithms
KW  - RNA viruses
KW  - CD8 antigen
KW  - Transgenic mice
KW  - Computer applications
KW  - DNA viruses
KW  - B7 antigen
KW  - Smallpox
KW  - Cytotoxicity
KW  - Vaccinia virus
KW  - Poxvirus
KW  - Antigenic determinants
KW  - Lymphocytes T
KW  - Vaccines
KW  - Immune response
KW  - Variola virus
KW  - V 22099:Immune response & immune mechanisms
KW  - F 06100:Vaccines - active immunity
KW  - G 07730:Development & Cell Cycle
KW  - W 30960:Bioinformatics & Computer Applications
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Immunology&rft.atitle=HLA-A*0201%2C+HLA-A*1101%2C+and+HLA-B*0702+Transgenic+Mice+Recognize+Numerous+Poxvirus+Determinants+from+a+Wide+Variety+of+Viral+Gene+Products&rft.au=Pasquetto%2C+Valerie%3BBui%2C+Huynh-Hoa%3BGiannino%2C+Rielle%3BMirza%2C+Fareed%3BSidney%2C+John%3BOseroff%2C+Carla%3BTscharke%2C+David+C%3BIrvine%2C+Kari%3BBennink%2C+Jack+R%3BPeters%2C+Bjoern%3BSouthwood%2C+Scott%3BCerundolo%2C+Vincenzo%3BGrey%2C+Howard%3BYewdell%2C+Jonathan+W%3BSette%2C+Alessandro&rft.aulast=Pasquetto&rft.aufirst=Valerie&rft.date=2005-10-01&rft.volume=175&rft.issue=8&rft.spage=5504&rft.isbn=&rft.btitle=&rft.title=Journal+of+Immunology&rft.issn=00221767&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Histocompatibility antigen HLA; Genomes; Vaccinia; Algorithms; RNA viruses; CD8 antigen; Computer applications; Transgenic mice; DNA viruses; B7 antigen; Smallpox; Cytotoxicity; Antigenic determinants; Lymphocytes T; Immune response; Vaccines; Vaccinia virus; Poxvirus; Variola virus
ER  - 



TY  - JOUR
T1  - Unravelling the structure of the pneumococcal autolytic lysozyme
AN  - 19792538; 7195779
AB  - The LytC lysozyme of Streptococcus pneumoniae forms part of the autolytic system of this important pathogen. This enzyme is composed of a C-terminal CM (catalytic module), belonging to the GH25 family of glycosyl hydrolases, and an N-terminal CBM (choline-binding module), made of eleven homologous repeats, that specifically recognizes the choline residues that are present in pneumococcal teichoic and lipoteichoic acids. This arrangement inverts the general assembly pattern of the major pneumococcal autolysin, LytA, and the lytic enzymes encoded by pneumococcal bacteriophages that place the CBM (made of six repeats) at the C-terminus. In the present paper, a three-dimensional model of LytC built by homology modelling of each module and consistent with spectroscopic and hydrodynamic studies is shown. In addition, the putative catalytic-pair residues are identified. Despite the inversion in the modular arrangement, LytC and the bacteriophage-encoded Cpl-1 lysozyme most probably adopt a similar global fold. However, the distinct choline-binding ability and their substrate-binding surfaces may reflect a divergent evolution directed by the different roles played by them in the host (LytC) or in the bacteriophage (Cpl-1). The tight binding of LytC to the pneumococcal envelope, mediated by the acquisition of additional choline-binding repeats, could facilitate the regulation of the potentially suicidal activity of this autolysin. In contrast, a looser attachment of Cpl-1 to the cell wall and the establishment of more favourable interactions between its highly negatively charged catalytic surface and the positively charged chains of pneumococcal murein could enhance the lytic activity of the parasite-encoded enzyme and therefore liberation of the phage progeny.
JF  - Biochemical Journal
AU  - Monterroso, B
AU  - Lopez-Zumel, C
AU  - Garcia, J L
AU  - Salz, J L
AU  - Garcia, P
AU  - Campillo, N E
AU  - Menendez, M
AD  - Section on Physical Biochemistry, Laboratory of Biochemistry and Genetics, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892, USA, nuria@suricata.iqm.csic.es
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 41
EP  - 49
VL  - 391
IS  - 1
SN  - 0264-6021, 0264-6021
KW  - Virology & AIDS Abstracts; Microbiology Abstracts B: Bacteriology
KW  - Phages
KW  - Lysozyme
KW  - Choline
KW  - Murein
KW  - Hydrodynamics
KW  - C-Terminus
KW  - Enzymes
KW  - Pathogens
KW  - Lipoteichoic acid
KW  - Lytic enzymes
KW  - Autolysins
KW  - Streptococcus pneumoniae
KW  - Envelopes
KW  - Homology
KW  - Inversion
KW  - Glycosyl hydrolase
KW  - Progeny
KW  - Evolution
KW  - Cell walls
KW  - V 22320:Replication
KW  - J 02320:Cell Biology
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19792538?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Biochemical+Journal&rft.atitle=Unravelling+the+structure+of+the+pneumococcal+autolytic+lysozyme&rft.au=Monterroso%2C+B%3BLopez-Zumel%2C+C%3BGarcia%2C+J+L%3BSalz%2C+J+L%3BGarcia%2C+P%3BCampillo%2C+N+E%3BMenendez%2C+M&rft.aulast=Monterroso&rft.aufirst=B&rft.date=2005-10-01&rft.volume=391&rft.issue=1&rft.spage=41&rft.isbn=&rft.btitle=&rft.title=Biochemical+Journal&rft.issn=02646021&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-01-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Phages; Lysozyme; Choline; Murein; Hydrodynamics; C-Terminus; Enzymes; Pathogens; Lytic enzymes; Lipoteichoic acid; Autolysins; Envelopes; Homology; Inversion; Progeny; Glycosyl hydrolase; Evolution; Cell walls; Streptococcus pneumoniae
ER  - 



TY  - JOUR
T1  - An assessment of hepatitis C virus infection among health-care workers of the National Cancer Institute of Naples, Southern Italy
AN  - 19774150; 6734928
AB  - As many people with chronic hepatitis C virus (HCV) infection are asymptomatic, HCV infection could spread easily among the health-care workers of the National Cancer Institute of Naples (especially before the identification of HCV and in the absence of good, effective preventative measures, e.g. sterile syringe use, gloves, protective glasses). In order to determine whether there is a transmission risk for HCV infection from patient to health-care worker, we carried out a cross-sectional study of a cohort of National Cancer Institute health-care workers in Naples, Southern Italy. The chi super(2)-test was not significant; we did not find any significant risk for HCV in the 'other untrained staff group [odds ratio (OR) 2.2; 95% confidence interval (CI) 0.4-10.9] or in the health-care workers group (OR 1.6; 95% CI 0.4-7.0). In the health-care worker subgroups, doctors were the reference category because of the low prevalence of HCV in this subgroup (3.3%). A non-significant association was found in the professional nurses group (OR 2.7; 95% CI 0.8-8.8), as well as in the categories of technicians and biologists. No excessive risk was found among the health-care workers as a whole or among the different categories of personnel, confirming that health-care employees have benefited sufficiently from preventative measures.
JF  - European Journal of Public Health
AU  - Montella, M
AU  - Crispo, A
AU  - Grimaldi, M
AU  - Ruffolo, P
AU  - Ronga, D
AU  - Izzo, F
AU  - Mastro, A A
AD  - Epidemiology Unit, National Cancer Institute, Via Mariano Semmola, 80131 Naples, Italy, epidemiologia.int@tin.it
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 467
EP  - 469
VL  - 15
IS  - 5
SN  - 1101-1262, 1101-1262
KW  - Virology & AIDS Abstracts; Health & Safety Science Abstracts; Risk Abstracts
KW  - needles
KW  - Medical personnel
KW  - Public health
KW  - Protective clothing
KW  - Prevention
KW  - Hepatitis C virus
KW  - Personnel
KW  - Italy, Naples
KW  - Chronic infection
KW  - Gloves
KW  - Syringes
KW  - Hepatitis C
KW  - Occupational exposure
KW  - R2 23080:Industrial and labor
KW  - H 1000:Occupational Safety and Health
KW  - V 22400:Human Diseases
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Ariskabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=European+Journal+of+Public+Health&rft.atitle=An+assessment+of+hepatitis+C+virus+infection+among+health-care+workers+of+the+National+Cancer+Institute+of+Naples%2C+Southern+Italy&rft.au=Montella%2C+M%3BCrispo%2C+A%3BGrimaldi%2C+M%3BRuffolo%2C+P%3BRonga%2C+D%3BIzzo%2C+F%3BMastro%2C+A+A&rft.aulast=Montella&rft.aufirst=M&rft.date=2005-10-01&rft.volume=15&rft.issue=5&rft.spage=467&rft.isbn=&rft.btitle=&rft.title=European+Journal+of+Public+Health&rft.issn=11011262&rft_id=info:doi/10.1093%2Feurpub%2Fcki032
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Personnel; Chronic infection; Syringes; Gloves; Public health; Prevention; Protective clothing; needles; Hepatitis C; Occupational exposure; Medical personnel; Hepatitis C virus; Italy, Naples
DO  - http://dx.doi.org/10.1093/eurpub/cki032
ER  - 



TY  - JOUR
T1  - Monitoring Differentiation of Human Embryonic Stem Cells Using Real-Time PCR
AN  - 19772258; 7145383
AB  - There is a general lack of rapid, sensitive, and quantitative methods for the detection of differentiating human embryonic stem cells (hESCs). Using light microscopy and immunohistochemistry, we observed that morphological changes of differentiating hESCs precede any major alterations in the expression of several commonly used hESC markers (SSEA-3, SSEA-4, TRA-1-60, TRA-1-81, Oct-4, and Nanog). In an attempt to quantify the changes during stochastic differentiation of hESCs, we developed a robust and sensitive multi-marker quantitative real-time polymerase chain reaction (QPCR) method. To maximize the sensitivity of the method, we measured the expression of up- and downregulated genes before and after differentiation of the hESCs. Out of the 12 genes assayed, we found it clearly sufficient to determine the relative differentiation state of the cells by calculating a collective expression index based on the mRNA levels of Oct-4, Nanog, Cripto, and alpha -fetoprotein. We evaluated the method using different hESC lines maintained in either feeder-dependent or feeder-free culture conditions. The QPCR method is very flexible, and by appropriately selecting reporter genes, the method can be designed for various applications. The combination of QPCR with hESC-based technologies opens novel avenues for high-throughput analysis of hESCs in, for example, pharmacological and cytotoxicity screening.
JF  - Stem Cells
AU  - Noaksson, Karin
AU  - Zoric, Neven
AU  - Zeng, Xianmin
AU  - Rao, Mahendra S
AU  - Hyllner, Johan
AU  - Semb, Henrik
AU  - Kubista, Mikael
AU  - Sartipy, Peter
AD  - Cellartis AB, Goeteborg, Sweden. TATAA Biocenter, Lundberg Laboratory, Goeteborg, Sweden. Cellular Neurobiology Branch, National Institute on Drug Abuse, Department of Health and Human Services, Baltimore, Maryland, USA. Laboratory of Neurosciences, National Institute of Aging, Department of Health and Human Services, Baltimore, Maryland, USA. Section of Endocrinology, Lund University, Lund, Sweden
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 1460
EP  - 1467
PB  - AlphaMed Press, Inc., One Prestige Pl, Ste 290 Miamisburg OH 45342-3758 USA
VL  - 23
IS  - 10
SN  - 1066-5099, 1066-5099
KW  - Genetics Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Differentiation
KW  - Stem cells
KW  - Cytotoxicity
KW  - Embryo cells
KW  - alpha -fetoprotein
KW  - Polymerase chain reaction
KW  - Cell culture
KW  - Oct-4 protein
KW  - Immunohistochemistry
KW  - Stochasticity
KW  - mRNA
KW  - G 07720:Immunogenetics
KW  - W 30945:Fermentation & Cell Culture
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19772258?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Stem+Cells&rft.atitle=Monitoring+Differentiation+of+Human+Embryonic+Stem+Cells+Using+Real-Time+PCR&rft.au=Noaksson%2C+Karin%3BZoric%2C+Neven%3BZeng%2C+Xianmin%3BRao%2C+Mahendra+S%3BHyllner%2C+Johan%3BSemb%2C+Henrik%3BKubista%2C+Mikael%3BSartipy%2C+Peter&rft.aulast=Noaksson&rft.aufirst=Karin&rft.date=2005-10-01&rft.volume=23&rft.issue=10&rft.spage=1460&rft.isbn=&rft.btitle=&rft.title=Stem+Cells&rft.issn=10665099&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-05-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Differentiation; Cytotoxicity; Stem cells; Embryo cells; alpha -fetoprotein; Polymerase chain reaction; Cell culture; Oct-4 protein; Stochasticity; Immunohistochemistry; mRNA
ER  - 



TY  - JOUR
T1  - Expression of human peripheral cannabinoid receptor for structural studies
AN  - 19766983; 6508261
AB  - Human peripheral-type cannabinoid receptor (CB2) was expressed in Escherichia coli as a fusion with the maltose-binding protein, thioredoxin, and a deca-histidine tag. Functional activity and structural integrity of the receptor in bacterial protoplast membranes was confirmed by extensive binding studies with a variety of natural and synthetic cannabinoid ligands. E. coli membranes expressing CB2 also activated cognate G-proteins in an in vitro coupled assay. Detergent-solubilized receptor was purified to 80%-90% homogeneity by affinity chromatography followed by ion-exchange chromatography. By high-resolution NMR on the receptor in DPC micelles, it was determined that purified CB2 forms 1:1 complexes with the ligands CP-55,940 and anandamide. The receptor was successfully reconstituted into phosphatidylcholine bilayers and the membranes were deposited into a porous substrate as tubular lipid bilayers for structural studies by NMR and scattering techniques.
JF  - Protein Science
AU  - Yeliseev, Alexei A
AU  - Wong, Karen K
AU  - Soubias, Olivier
AU  - Gawrisch, Klaus
AD  - Laboratory of Membrane Biochemistry and Biophysics, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Bethesda, Maryland 20892, USA
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 2638
EP  - 2653
PB  - Cold Spring Harbor Laboratory Press, [mailto:cshpress@cshl.org], [URL:http://www.cshl.org/]
VL  - 14
IS  - 10
SN  - 0961-8368, 0961-8368
KW  - Microbiology Abstracts B: Bacteriology
KW  - Thioredoxin
KW  - Lipid bilayers
KW  - Anandamide
KW  - Ion-exchange chromatography
KW  - Lecithin
KW  - Guanine nucleotide-binding protein
KW  - Affinity chromatography
KW  - Micelles
KW  - Structure-function relationships
KW  - Cannabinoid CB2 receptors
KW  - Escherichia coli
KW  - Protoplasts
KW  - N.M.R.
KW  - maltose-binding protein
KW  - J 02330:Biochemistry
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19766983?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Protein+Science&rft.atitle=Expression+of+human+peripheral+cannabinoid+receptor+for+structural+studies&rft.au=Yeliseev%2C+Alexei+A%3BWong%2C+Karen+K%3BSoubias%2C+Olivier%3BGawrisch%2C+Klaus&rft.aulast=Yeliseev&rft.aufirst=Alexei&rft.date=2005-10-01&rft.volume=14&rft.issue=10&rft.spage=2638&rft.isbn=&rft.btitle=&rft.title=Protein+Science&rft.issn=09618368&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2009-05-01
N1  - Last updated - 2015-03-30
N1  - SubjectsTermNotLitGenreText - Thioredoxin; Lipid bilayers; Anandamide; Lecithin; Ion-exchange chromatography; Guanine nucleotide-binding protein; Affinity chromatography; Structure-function relationships; Micelles; Cannabinoid CB2 receptors; Protoplasts; N.M.R.; maltose-binding protein; Escherichia coli
ER  - 



TY  - JOUR
T1  - Nuclear Magnetic Resonance Solution Structure of the Escherichia coli DNA Polymerase III theta Subunit
AN  - 19762664; 6503228
AB  - The catalytic core of Escherichia coli DNA polymerase III holoenzyme contains three subunits: alpha , epsilon , and theta . The alpha subunit contains the polymerase, and the epsilon subunit contains the exonucleolytic proofreading function. The small (8-kDa) theta subunit binds only to epsilon . Its function is not well understood, although it was shown to exert a small stabilizing effect on the epsilon proofreading function. In order to help elucidate its function, we undertook a determination of its solution structure. In aqueous solution, theta yielded poor-quality nuclear magnetic resonance spectra, presumably due to conformational exchange and/or protein aggregation. Based on our recently determined structure of the theta homolog from bacteriophage P1, named HOT, we constructed a homology model of theta . This model suggested that the unfavorable behavior of theta might arise from exposed hydrophobic residues, particularly toward the end of alpha -helix 3. In gel filtration studies, theta elutes later than expected, indicating that aggregation is potentially responsible for these problems. To address this issue, we recorded super(1)H- super(15)N heteronuclear single quantum correlation (HSQC) spectra in water-alcohol mixed solvents and observed substantially improved dispersion and uniformity of peak intensities, facilitating a structural determination under these conditions. The structure of theta in 60/40 (vol/vol) water-methanol is similar to that of HOT but differs significantly from a previously reported theta structure. The new theta structure is expected to provide additional insight into its physiological role and its effect on the epsilon proofreading subunit.
JF  - Journal of Bacteriology
AU  - Mueller, Geoffrey A
AU  - Kirby, Thomas W
AU  - DeRose, Eugene F
AU  - Li, Dawei
AU  - Schaaper, Roel M
AU  - London, Robert E
AD  - Laboratory of Structural Biology. Laboratory of Molecular Genetics, National Institute of Environmental Health Sciences, Box 12233, Research Triangle Park, North Carolina 27709
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 7081
EP  - 7089
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 187
IS  - 20
SN  - 0021-9193, 0021-9193
KW  - Virology & AIDS Abstracts; Microbiology Abstracts B: Bacteriology; Biochemistry Abstracts 2: Nucleic Acids
KW  - Phages
KW  - Filtration
KW  - Homology
KW  - DNA-directed DNA polymerase
KW  - Escherichia coli
KW  - Solvents
KW  - N.M.R.
KW  - Hydrophobicity
KW  - Protein interaction
KW  - Proofreading
KW  - Models
KW  - J 02725:DNA
KW  - N 14085:DNA: Transcription factors, repressors, nucleoproteins & DNA-binding proteins
KW  - V 22320:Replication
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19762664?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Bacteriology&rft.atitle=Nuclear+Magnetic+Resonance+Solution+Structure+of+the+Escherichia+coli+DNA+Polymerase+III+theta+Subunit&rft.au=Mueller%2C+Geoffrey+A%3BKirby%2C+Thomas+W%3BDeRose%2C+Eugene+F%3BLi%2C+Dawei%3BSchaaper%2C+Roel+M%3BLondon%2C+Robert+E&rft.aulast=Mueller&rft.aufirst=Geoffrey&rft.date=2005-10-01&rft.volume=187&rft.issue=20&rft.spage=7081&rft.isbn=&rft.btitle=&rft.title=Journal+of+Bacteriology&rft.issn=00219193&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Phages; Filtration; Homology; DNA-directed DNA polymerase; Solvents; Hydrophobicity; N.M.R.; Protein interaction; Models; Proofreading; Escherichia coli
ER  - 



TY  - JOUR
T1  - Enduring representational plasticity after somatosensory stimulation
AN  - 19437509; 6676548
AB  - Somatosensory stimulation (SS), leading to increases in motor cortical excitability, influences motor performance in patients with brain lesions like stroke. The mechanisms by which SS modulates motor function are incompletely understood. Here, we used functional magnetic resonance imaging (fMRI, blood- oxygenation-level-dependent (BOLD), and perfusion imagings simultaneously acquired in a 3 T magnet) to assess the effects of SS on thumb-movement-related activation in three regions of interest (ROI) in the motor network: primary motor cortex (M1), primary somatosensory cortex (S1), and dorsal premotor cortex (PMd) in healthy volunteers. Scans were obtained in different sessions before and after 2-h electrical stimulation applied to the median nerve at the wrist (MNS), to the skin overlying the shoulder deltoid muscle (DMS), and in the absence of stimulation (NOSTIM) in a counterbalanced design. We found that baseline perfusion intensity was comparable within and across sessions. MNS but not DMS nor NOSTIM led to an increase in signal intensity and number of voxels activated by performance of median nerve-innervated thumb movements in M1, S1, and PMd for up to 60 min. Task-related fMRI activation changes were most prominent in M1 followed by S1 and to a lesser extent in PMd. MNS elicited a displacement of the center of gravity for the thumb movement representation towards the other finger representations within S1. These results indicate that MNS leads to an expansion of the thumb representation towards other finger representations within S1, a form of plasticity that may underlie the influence of SS on motor cortical function, possibly supporting beneficial effects on motor control.
JF  - NeuroImage
AU  - Wu, Carolyn W-H
AU  - Van Gelderen, Peter
AU  - Hanakawa, Takashi
AU  - Yaseen, Zaneb
AU  - Cohen, Leonardo G
AD  - Human Cortical Physiology Section, NINDS, NIH, Bethesda, MD 20892, USA, wuwh@ninds.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 872
EP  - 884
PB  - Elsevier Science Ltd., The Boulevard Langford Lane Kidlington Oxford OX5 1GB UK, [mailto:usinfo-f@elsevier.com], [URL:http://www.elsevier.nl]
VL  - 27
IS  - 4
SN  - 1053-8119, 1053-8119
KW  - CSA Neurosciences Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Neuroimaging
KW  - Functional magnetic resonance imaging
KW  - Wrist
KW  - Excitability
KW  - Electrical stimuli
KW  - Cortex
KW  - Cortex (premotor)
KW  - Shoulder
KW  - Cortex (motor)
KW  - Perfusion
KW  - Skin
KW  - median nerve
KW  - Plasticity (cortical)
KW  - Stroke
KW  - Motor task performance
KW  - Muscles
KW  - Brain
KW  - Finger
KW  - Cortex (somatosensory)
KW  - W 30910:Imaging
KW  - N3 11004:Motor & sensory systems
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19437509?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=NeuroImage&rft.atitle=Enduring+representational+plasticity+after+somatosensory+stimulation&rft.au=Wu%2C+Carolyn+W-H%3BVan+Gelderen%2C+Peter%3BHanakawa%2C+Takashi%3BYaseen%2C+Zaneb%3BCohen%2C+Leonardo+G&rft.aulast=Wu&rft.aufirst=Carolyn&rft.date=2005-10-01&rft.volume=27&rft.issue=4&rft.spage=872&rft.isbn=&rft.btitle=&rft.title=NeuroImage&rft.issn=10538119&rft_id=info:doi/10.1016%2Fj.neuroimage.2005.05.055ZZ%3A
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-01-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Functional magnetic resonance imaging; Cortex (somatosensory); Finger; Cortex (premotor); Motor task performance; Cortex (motor); Neuroimaging; Stroke; Shoulder; Wrist; Plasticity (cortical); Excitability; median nerve; Electrical stimuli; Brain; Muscles; Skin; Cortex; Perfusion
DO  - http://dx.doi.org/10.1016/j.neuroimage.2005.05.055ZZ:
ER  - 



TY  - JOUR
T1  - High-resolution cDNA microarray-based comparative genomic hybridization analysis in neuroblastoma
AN  - 19418528; 6676642
AB  - Neuroblastoma (NB) is one of the most common pediatric solid tumors and displays a broad variety of genomic alterations. Array-based comparative genomic hybridization (A-CGH) is a novel technology enabling the high-resolution detection of DNA copy number aberrations. In this article, we outline features of this new technology and approaches of data analysis. We focus on stage specific DNA copy number variations in neuroblastoma detected by cDNA array- based comparative genomic hybridization (A-CGH). We also discuss hypothetic evolutionary models of neuroblastoma progression that can be derived from A-CGH data.
JF  - Cancer Letters
AU  - Chen, Qing-Rong
AU  - Bilke, Sven
AU  - Khan, Javed
AD  - Oncogenomics Section, Pediatric Oncology Branch, Advanced Technology Center, National Cancer Institute, 8717 Government Circle, Gaithersburg, MD 20877, USA, chenqi@mail.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 71
EP  - 81
PB  - Elsevier Science Ltd., The Boulevard Langford Lane Kidlington Oxford OX5 1GB UK, [mailto:usinfo-f@elsevier.com], [URL:http://www.elsevier.nl]
VL  - 228
IS  - 1-2
SN  - 0304-3835, 0304-3835
KW  - Genetics Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Neuroblastoma
KW  - Array CGH
KW  - Microarray
KW  - Tumor evolution
KW  - DNA copy number
KW  - Genomic alteration
KW  - Amplification
KW  - MYCN
KW  - Data processing
KW  - Pediatrics
KW  - Solid tumors
KW  - DNA
KW  - genomics
KW  - DNA microarrays
KW  - Evolution
KW  - Hybridization analysis
KW  - copy number
KW  - W 30900:Methods
KW  - G 07700:Molecular Genetics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19418528?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cancer+Letters&rft.atitle=High-resolution+cDNA+microarray-based+comparative+genomic+hybridization+analysis+in+neuroblastoma&rft.au=Chen%2C+Qing-Rong%3BBilke%2C+Sven%3BKhan%2C+Javed&rft.aulast=Chen&rft.aufirst=Qing-Rong&rft.date=2005-10-01&rft.volume=228&rft.issue=1-2&rft.spage=71&rft.isbn=&rft.btitle=&rft.title=Cancer+Letters&rft.issn=03043835&rft_id=info:doi/10.1016%2Fj.canlet.2004.12.056
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Data processing; Solid tumors; Pediatrics; DNA; genomics; DNA microarrays; Hybridization analysis; Evolution; Neuroblastoma; copy number
DO  - http://dx.doi.org/10.1016/j.canlet.2004.12.056
ER  - 



TY  - JOUR
T1  - Recovery of Stem Cells from Cryopreserved Periodontal Ligament
AN  - 19418044; 6492151
AB  - Human post-natal stem cells possess a great potential to be utilized in stem-cell-mediated clinical therapies and tissue engineering. It is not known whether cryopreserved human tissues contain functional post-natal stem cells. In this study, we utilized human periodontal ligament to test the hypothesis that cryopreserved human periodontal ligament contains retrievable post-natal stem cells. These cryopreserved periodontal ligament stem cells maintained normal periodontal ligament stem cell characteristics, including expression of the mesenchymal stem cell surface molecule STRO-1, single-colony-strain generation, multipotential differentiation, cementum/periodontal-ligament-like tissue regeneration, and a normal diploid karyotype. Collectively, this study provides valuable evidence demonstrating a practical approach to the preservation of solid-frozen human tissues for subsequent post-natal stem cell isolation and tissue regeneration. The present study demonstrates that human post-natal stem cells can be recovered from cryopreserved human periodontal ligament, thereby providing a practical clinical approach for the utilization of frozen tissues for stem cell isolation.
JF  - Journal of Dental Research
AU  - Seo, B-M
AU  - Miura, M
AU  - Sonoyama, W
AU  - Coppe, C
AU  - Stanyon, R
AU  - Shi, S
AD  - Craniofacial and Skeletal Diseases Branch, National Institute of Dental and Craniofacial Research, Building 30, Room 131, 30 Convent Drive MSC-4320, and Comparative Molecular Cytogenetics Core, Genetics Branch, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA, sshi@dir.nidcr.nih.gov
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 907
EP  - 912
VL  - 84
IS  - 10
SN  - 0022-0345, 0022-0345
KW  - Biotechnology and Bioengineering Abstracts
KW  - Differentiation
KW  - Cell surface
KW  - Stem cells
KW  - Diploids
KW  - periodontal ligament
KW  - Cementum
KW  - Preservation
KW  - Tissue engineering
KW  - Mesenchyme
KW  - Karyotypes
KW  - W 30945:Fermentation & Cell Culture
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19418044?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Dental+Research&rft.atitle=Recovery+of+Stem+Cells+from+Cryopreserved+Periodontal+Ligament&rft.au=Seo%2C+B-M%3BMiura%2C+M%3BSonoyama%2C+W%3BCoppe%2C+C%3BStanyon%2C+R%3BShi%2C+S&rft.aulast=Seo&rft.aufirst=B-M&rft.date=2005-10-01&rft.volume=84&rft.issue=10&rft.spage=907&rft.isbn=&rft.btitle=&rft.title=Journal+of+Dental+Research&rft.issn=00220345&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Stem cells; periodontal ligament; Cell surface; Mesenchyme; Tissue engineering; Cementum; Karyotypes; Differentiation; Diploids; Preservation
ER  - 



TY  - JOUR
T1  - SNPdetector: A Software Tool for Sensitive and Accurate SNP Detection
AN  - 19417191; 6514396
AB  - Identification of single nucleotide polymorphisms (SNPs) and mutations is important for the discovery of genetic predisposition to complex diseases. PCR resequencing is the method of choice for de novo SNP discovery. However, manual curation of putative SNPs has been a major bottleneck in the application of this method to high-throughput screening. Therefore it is critical to develop a more sensitive and accurate computational method for automated SNP detection. We developed a software tool, SNPdetector, for automated identification of SNPs and mutations in fluorescence-based resequencing reads. SNPdetector was designed to model the process of human visual inspection and has a very low false positive and false negative rate. We demonstrate the superior performance of SNPdetector in SNP and mutation analysis by comparing its results with those derived by human inspection, PolyPhred (a popular SNP detection tool), and independent genotype assays in three large-scale investigations. The first study identified and validated inter- and intra-subspecies variations in 4,650 traces of 25 inbred mouse strains that belong to either the Mus musculus species or the M. spretus species. Unexpected heterozgyosity in CAST/Ei strain was observed in two out of 1,167 mouse SNPs. The second study identified 11,241 candidate SNPs in five ENCODE regions of the human genome covering 2.5 Mb of genomic sequence. Approximately 50% of the candidate SNPs were selected for experimental genotyping; the validation rate exceeded 95%. The third study detected ENU- induced mutations (at 0.04% allele frequency) in 64,896 traces of 1,236 zebra fish. Our analysis of three large and diverse test datasets demonstrated that SNPdetector is an effective tool for genome-scale research and for large-sample clinical studies. SNPdetector runs on Unix/Linux platform and is available publicly (http://lpg.nci.nih.gov
JF  - PLoS Computational Biology
AU  - Zhang, Jinghui
AU  - Wheeler, David A
AU  - Yakub, Imtiaz
AU  - Wei, Sharon
AU  - Sood, Raman
AU  - Rowe, William
AU  - Liu, Paul P
AU  - Gibbs, Richard A
AU  - Buetow, Kenneth H
AD  - Laboratory of Population Genetics, National Cancer Institute, National Institutes of Health, Bethesda, Maryland, United States of America, jinghuiz@mail.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
PB  - Public Library of Science, 185 Berry Street Suite 1300 San Francisco CA 94107 USA, [mailto:plos@plos.org], [URL:http://www.plos.org]
VL  - 1
IS  - 5
SN  - 1553-734X, 1553-734X
KW  - Biotechnology and Bioengineering Abstracts
KW  - Genomes
KW  - Nucleotide sequence
KW  - Genotyping
KW  - Animal models
KW  - Computer applications
KW  - Mus musculus
KW  - Models
KW  - Computer programs
KW  - Danio rerio
KW  - software
KW  - Single-nucleotide polymorphism
KW  - Polymerase chain reaction
KW  - high-throughput screening
KW  - genomics
KW  - Mutation
KW  - W 30960:Bioinformatics & Computer Applications
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19417191?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=PLoS+Computational+Biology&rft.atitle=SNPdetector%3A+A+Software+Tool+for+Sensitive+and+Accurate+SNP+Detection&rft.au=Zhang%2C+Jinghui%3BWheeler%2C+David+A%3BYakub%2C+Imtiaz%3BWei%2C+Sharon%3BSood%2C+Raman%3BRowe%2C+William%3BLiu%2C+Paul+P%3BGibbs%2C+Richard+A%3BBuetow%2C+Kenneth+H&rft.aulast=Zhang&rft.aufirst=Jinghui&rft.date=2005-10-01&rft.volume=1&rft.issue=5&rft.spage=&rft.isbn=&rft.btitle=&rft.title=PLoS+Computational+Biology&rft.issn=1553734X&rft_id=info:doi/10.1371%2Fjournal.pcbi.0010053
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Danio rerio; Mus musculus; Single-nucleotide polymorphism; Mutation; Computer programs; software; Computer applications; genomics; Genotyping; Models; Animal models; Genomes; Nucleotide sequence; high-throughput screening; Polymerase chain reaction
DO  - http://dx.doi.org/10.1371/journal.pcbi.0010053
ER  - 



TY  - JOUR
T1  - ORIOGEN: order restricted inference for ordered gene expression data
AN  - 19414738; 6509121
AB  - SUMMARY: ORIOGEN is a user-friendly Java-based software package for selecting and clustering genes according to their profiles across various treatment groups. In particular, ORIOGEN is useful for analyzing data obtained from time-course or dose-response type experiments. AVAILABILITY: The ORIOGEN software can be downloaded freely from http://dir.niehs.nih.gov/dirbb/oriogen/index.cfm. Supplementary information: ORIOGEN has a full set of help files. Also, an example input file is provided with the download.
JF  - Bioinformatics
AU  - Peddada, S
AU  - Harris, S
AU  - Zajd, J
AU  - Harvey, E
AD  - Biostatistics Branch, National Institute of Environmental Health Sciences Durham, NC 27713, USA. Constella Group, LLC Durham, NC 27713, USA, peddada@niehs.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 3933
EP  - 3934
PB  - Oxford University Press, Oxford Journals, Great Clarendon Street Oxford OX2 6DP UK, [mailto:jnl.samples@oup.co.uk], [URL:http://www3.oup.co.uk/jnls/]
VL  - 21
IS  - 20
SN  - 1367-4803, 1367-4803
KW  - Genetics Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Gene expression
KW  - Computer programs
KW  - software
KW  - Data processing
KW  - Statistics
KW  - Bioinformatics
KW  - G 07880:Human Genetics
KW  - W 30960:Bioinformatics & Computer Applications
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19414738?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Bioinformatics&rft.atitle=ORIOGEN%3A+order+restricted+inference+for+ordered+gene+expression+data&rft.au=Peddada%2C+S%3BHarris%2C+S%3BZajd%2C+J%3BHarvey%2C+E&rft.aulast=Peddada&rft.aufirst=S&rft.date=2005-10-01&rft.volume=21&rft.issue=20&rft.spage=3933&rft.isbn=&rft.btitle=&rft.title=Bioinformatics&rft.issn=13674803&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2015-04-01
N1  - SubjectsTermNotLitGenreText - Gene expression; Computer programs; software; Statistics; Data processing; Bioinformatics
ER  - 



TY  - JOUR
T1  - Robust accurate identification of peptides (RAId): deciphering MS super(2) data using a structured library search with de novo based statistics
AN  - 19413408; 6509088
AB  - MOTIVATION: The key to MS -based proteomics is peptide sequencing. The major challenge in peptide sequencing, whether library search or de novo, is to better infer statistical significance and better attain noise reduction. Since the noise in a spectrum depends on experimental conditions, the instrument used and many other factors, it cannot be predicted even if the peptide sequence is known. The characteristics of the noise can only be uncovered once a spectrum is given. We wish to overcome such issues. RESULTS: We designed RAId to identify peptides from their associated tandem mass spectrometry data. RAId performs a novel de novo sequencing followed by a search in a peptide library that we created. Through de novo sequencing, we establish the spectrum-specific background score statistics for the library search. When the database search fails to return significant hits, the top-ranking de novo sequences become potential candidates for new peptides that are not yet in the database. The use of spectrum-specific background statistics seems to enable RAId to perform well even when the spectral quality is marginal. Other important features of RAId include its potential in de novo sequencing alone and the ease of incorporating post-translational modifications. AVAILABILITY: Programs implementing the methods described are available from the authors on request. CONTACT: yyucbi.nlm.nih.gov Supplementary information: ftp://ftp.ncbi.nih.gov/pub/yyu/Proteomics/MSMS/RAId/MSMS_bioinfo_s u pp.pdf
JF  - Bioinformatics
AU  - Alves, Gelio
AU  - Yu, Yi-Kuo
AD  - National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health Bethesda, MD 20894, USA
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 3726
EP  - 3732
PB  - Oxford University Press, Oxford Journals, Great Clarendon Street Oxford OX2 6DP UK, [mailto:jnl.samples@oup.co.uk], [URL:http://www3.oup.co.uk/jnls/]
VL  - 21
IS  - 19
SN  - 1367-4803, 1367-4803
KW  - Biotechnology and Bioengineering Abstracts
KW  - Computer programs
KW  - Databases
KW  - Statistics
KW  - Post-translation
KW  - Bioinformatics
KW  - proteomics
KW  - Peptide libraries
KW  - Mass spectroscopy
KW  - W 30960:Bioinformatics & Computer Applications
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19413408?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Bioinformatics&rft.atitle=Robust+accurate+identification+of+peptides+%28RAId%29%3A+deciphering+MS+super%282%29+data+using+a+structured+library+search+with+de+novo+based+statistics&rft.au=Alves%2C+Gelio%3BYu%2C+Yi-Kuo&rft.aulast=Alves&rft.aufirst=Gelio&rft.date=2005-10-01&rft.volume=21&rft.issue=19&rft.spage=3726&rft.isbn=&rft.btitle=&rft.title=Bioinformatics&rft.issn=13674803&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Statistics; proteomics; Databases; Peptide libraries; Mass spectroscopy; Post-translation; Computer programs; Bioinformatics
ER  - 



TY  - JOUR
T1  - Immunoassay Interference by a Commonly Used Blood Collection Tube Additive, the Organosilicone Surfactant Silwet L-720
AN  - 19412133; 6502826
AB  - BACKGROUND: A small number of immunoassays on several different types of analyzers were recently adversely affected by tube additives in Becton Dickinson (BD) Vacutainer registered SST super(TM), SST II, and Microtainer super(TM) blood collection tubes. We examined the effect of a commonly used tube surfactant, Silwet super(TM) L-720, on immunoassays and the mechanism for the interference. METHODS: Immunoassays were performed on serum supplemented with Silwet L-720 on the IMMULITE super(TM) 2500 and AxSYM super(TM) analyzers. Direct effects of the surfactant on the chemiluminescent detection step of immunoassays and on antibody immobilization on the solid phase were examined. RESULTS: Increasing the final surfactant concentration from 0 to 400 mg/L in serum significantly increased ( similar to 51%) the apparent total triiodothyronine (TT sub(3)) concentrations measured on the IMMULITE 2500 but not the AxSYM analyzer. Several other competitive, but not noncompetitive, assays were also significantly affected by the surfactant on the IMMULITE 2500 analyzer. The effect was independent of serum components, and the surfactant had no direct effect on chemiluminescence reactions. The capture antibody, however, was displaced from the solid phase by incubation with solutions containing surfactant under conditions similar to the IMMULITE TT sub(3) assay. CONCLUSIONS: The Silwet L-720 surfactant, which is used to coat the inner surfaces of tubes, appears to account for previously reported immunoassay interference by BD Vacutainer SST blood collection tubes. One of the mechanisms for the interference is the desorption of antibodies from the solid phase by the surfactant. The results identify an important factor in the selection of suitable blood collection tube surfactants and provide an approach for solving similar tube-assay interference problems in the future.
JF  - Clinical Chemistry
AU  - Bowen, Raffick AR
AU  - Chan, Yung
AU  - Ruddel, Mark E
AU  - Hortin, Glen L
AU  - Csako, Gyorgy
AU  - Demosky, Stephen JJr
AU  - Remaley, Alan T
AD  - Department of Laboratory Medicine, Warren Grant Magnuson Clinical Center, and Molecular Disease Section, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, MD
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 1874
EP  - 1882
PB  - American Association for Clinical Chemistry, Inc.
VL  - 51
IS  - 10
SN  - 0009-9147, 0009-9147
KW  - Biotechnology and Bioengineering Abstracts
KW  - Thyroid hormones
KW  - Blood
KW  - Antibodies
KW  - Desorption
KW  - Triiodothyronine
KW  - Chemiluminescence
KW  - Immunoassays
KW  - Surfactants
KW  - Immobilization
KW  - W 30900:Methods
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19412133?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+Chemistry&rft.atitle=Immunoassay+Interference+by+a+Commonly+Used+Blood+Collection+Tube+Additive%2C+the+Organosilicone+Surfactant+Silwet+L-720&rft.au=Bowen%2C+Raffick+AR%3BChan%2C+Yung%3BRuddel%2C+Mark+E%3BHortin%2C+Glen+L%3BCsako%2C+Gyorgy%3BDemosky%2C+Stephen+JJr%3BRemaley%2C+Alan+T&rft.aulast=Bowen&rft.aufirst=Raffick&rft.date=2005-10-01&rft.volume=51&rft.issue=10&rft.spage=1874&rft.isbn=&rft.btitle=&rft.title=Clinical+Chemistry&rft.issn=00099147&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Surfactants; Immunoassays; Blood; Antibodies; Chemiluminescence; Thyroid hormones; Triiodothyronine; Desorption; Immobilization
ER  - 



TY  - JOUR
T1  - Matrigel: Basement membrane matrix with biological activity
AN  - 19410407; 6501529
AB  - The basement membrane extracellular matrix contacts epithelial, endothelial, fat and smooth muscle cells. Because this extracellular matrix is so thin, it had been hard to study its composition, structure, and function. An extract of a tumor was found to contain all of the components present in basement and to be very biologically active. This extract, termed Matrigel, Cultrex, or EHS matrix, promotes cell differentiation, and is used to measure the invasive activity of tumor cells. In vivo, it is used for measuring angiogenic inhibitors and stimulators, to improve graft survival, repair damaged tissues, and increase tumor growth.
JF  - Seminars in Cancer Biology
AU  - Kleinman, H K
AU  - Martin, G R
AD  - NIDCR, 30/433, 30 Convent Dr. MSC 4370, Bethesda, MD 20892-4370, USA, hkleinman@dir.nidcr.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 378
EP  - 386
VL  - 15
IS  - 5
SN  - 1044-579X, 1044-579X
KW  - Biotechnology and Bioengineering Abstracts
KW  - Smooth muscle
KW  - Differentiation
KW  - Basement membranes
KW  - Structure-function relationships
KW  - Extracellular matrix
KW  - Angiogenesis
KW  - Tumors
KW  - Tumor cells
KW  - W 30920:Tissue Engineering
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/19410407?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Seminars+in+Cancer+Biology&rft.atitle=Matrigel%3A+Basement+membrane+matrix+with+biological+activity&rft.au=Kleinman%2C+H+K%3BMartin%2C+G+R&rft.aulast=Kleinman&rft.aufirst=H&rft.date=2005-10-01&rft.volume=15&rft.issue=5&rft.spage=378&rft.isbn=&rft.btitle=&rft.title=Seminars+in+Cancer+Biology&rft.issn=1044579X&rft_id=info:doi/10.1016%2Fj.semcancer.2005.05.004
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Tumors; Extracellular matrix; Basement membranes; Tumor cells; Structure-function relationships; Differentiation; Angiogenesis; Smooth muscle
DO  - http://dx.doi.org/10.1016/j.semcancer.2005.05.004
ER  - 



TY  - JOUR
T1  - Cnu, a Novel oriC-Binding Protein of Escherichia coli
AN  - 17663358; 6503219
AB  - We have found, using a newly developed genetic method, a protein (named Cnu, for oriC-binding nucleoid-associated) that binds to a specific 26-base-pair sequence (named cnb) in the origin of replication of Escherichia coli, oriC. Cnu is composed of 71 amino acids (8.4 kDa) and shows extensive amino acid identity to a group of proteins belonging to the Hha/YmoA family. Cnu was previously discovered as a protein that, like Hha, complexes with H-NS in vitro. Our in vivo and in vitro assays confirm the results and further suggest that the complex formation with H-NS is involved in Cnu/Hha binding to cnb. Unlike the hns mutants, elimination of either the cnu or hha gene did not disturb the growth rate, origin content, and synchrony of DNA replication initiation of the mutants compared to the wild-type cells. However, the cnu hha double mutant was moderately reduced in origin content. The Cnu/Hha complex with H-NS thus could play a role in optimal activity of oriC.
JF  - Journal of Bacteriology
AU  - Kim, Myung Suk
AU  - Bae, Sung-Hun
AU  - Yun, Sang Hoon
AU  - Lee, Hee Jung
AU  - Ji, Sang Chun
AU  - Lee, Ji Hyun
AU  - Srivastava, Preeti
AU  - Lee, Seol-Hoon
AU  - Chae, Huiseok
AU  - Lee, Younghoon
AU  - Choi, Byong-Seok
AU  - Chattoraj, Dhruba K
AU  - Lim, Heon M
AD  - Department of Biology, School of Biological Sciences and Biotechnology, Chungnam National University, Taejon, 305-764 Korea. Laboratory of Biochemistry, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892-4255. Department of Chemistry, Korea Advanced Institute of Science and Technology, Taejon, 305-701, Korea
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 6998
EP  - 7008
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 187
IS  - 20
SN  - 0021-9193, 0021-9193
KW  - Cnu protein
KW  - Genetics Abstracts; Microbiology Abstracts B: Bacteriology
KW  - J 02725:DNA
KW  - G 07320:Bacterial genetics
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Bacteriology&rft.atitle=Cnu%2C+a+Novel+oriC-Binding+Protein+of+Escherichia+coli&rft.au=Kim%2C+Myung+Suk%3BBae%2C+Sung-Hun%3BYun%2C+Sang+Hoon%3BLee%2C+Hee+Jung%3BJi%2C+Sang+Chun%3BLee%2C+Ji+Hyun%3BSrivastava%2C+Preeti%3BLee%2C+Seol-Hoon%3BChae%2C+Huiseok%3BLee%2C+Younghoon%3BChoi%2C+Byong-Seok%3BChattoraj%2C+Dhruba+K%3BLim%2C+Heon+M&rft.aulast=Kim&rft.aufirst=Myung&rft.date=2005-10-01&rft.volume=187&rft.issue=20&rft.spage=6998&rft.isbn=&rft.btitle=&rft.title=Journal+of+Bacteriology&rft.issn=00219193&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2005-12-01
N1  - Last updated - 2011-12-13
ER  - 



TY  - JOUR
T1  - Factors associated with bicycle helmet use among young adolescents in a multinational sample
AN  - 17660447; 6508890
AB  - OBJECTIVE: To determine factors associated with variation in bicycle helmet use by youth of different industrialized countries. DESIGN: A multinational cross sectional nationally representative survey of health behaviors including symptoms, risk taking, school setting, and family context. SETTING: School based survey of 26 countries. SUBJECTS: School students, ages 11, 13, and 15 years totaling 112 843. OUTCOME MEASURES: Reported frequency of bicycle helmet use among bicycle riders. RESULTS: Reported helmet use varied greatly by country from 39.2% to 1.9%, with 12 countries reporting less than 10% of the bicycle riders as frequent helmet users and 14 countries more than 10%. Reported helmet use was highest at 11 years and decreased as children's age increased. Use was positively associated with other healthy behaviors, with parental involvement, and with per capita gross domestic product of the country. It is negatively associated with risk taking behaviors. Countries reported to have interventions promoting helmet use, exemplified by helmet giveaway programmes, had greater frequency of reported helmet use than those without programmes. CONCLUSIONS: Bicycle helmet use among young adolescents varies greatly between countries; however, helmet use does not reach 50% in any country. Age is the most significant individual factor associated with helmet for helmet using countries. The observation that some helmet promotion programmes are reported for countries with relatively higher student helmet use and no programmes reported for the lowest helmet use countries, suggests the possibility of a relation and the need for objective evaluation of programme effectiveness.
JF  - Injury Prevention
AU  - Klein, K S
AU  - Thompson, D
AU  - Scheidt, P C
AU  - Overpeck, M D
AU  - Gross, L A
AD  - National Institute of Child Health and Human Development, NIH, Bethesda, MD, USA
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 288
EP  - 293
PB  - B M J Publishing Group, B.M.A. House Tavistock Sq. London WC1H 9JR UK
VL  - 11
IS  - 5
SN  - 1353-8047, 1353-8047
KW  - Physical Education Index; Health & Safety Science Abstracts
KW  - H 11000:Diseases/Injuries/Trauma
KW  - PE 030:Exercise, Health & Physical Fitness
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17660447?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aphysicaleducation&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Injury+Prevention&rft.atitle=Factors+associated+with+bicycle+helmet+use+among+young+adolescents+in+a+multinational+sample&rft.au=Klein%2C+K+S%3BThompson%2C+D%3BScheidt%2C+P+C%3BOverpeck%2C+M+D%3BGross%2C+L+A&rft.aulast=Klein&rft.aufirst=K&rft.date=2005-10-01&rft.volume=11&rft.issue=5&rft.spage=288&rft.isbn=&rft.btitle=&rft.title=Injury+Prevention&rft.issn=13538047&rft_id=info:doi/
LA  - English
DB  - Physical Education Index; ProQuest Environmental Science Collection
N1  - Date revised - 2005-12-01
N1  - Last updated - 2011-12-13
ER  - 



TY  - JOUR
T1  - Cancer Mortality among Men Occupationally Exposed to Dichlorodiphenyltrichloroethane
AN  - 17657043; 6502512
AB  - Several studies have evaluated cancer risk associated with occupational and environmental exposure to dichlorodiphenyltrichloroethane (DDT). Results are mixed. To further inquire into human carcinogenicity of DDT, we conducted a mortality follow-up study of 4,552 male workers, exposed to DDT during antimalarial operations in Sardinia, Italy, conducted in 1946 to 1950. Detailed information on DDT use during the operations provided the opportunity to develop individual estimates of average and cumulative exposure. Mortality of the cohort was first compared with that of the Sardinian population. Overall mortality in the cohort was about as expected, but there was a deficit for death from cardiovascular disease and a slight excess for nonmalignant respiratory diseases and lymphatic cancer among the unexposed subcohort. For internal comparisons, we used Poisson regression analysis to calculate relative risks of selected malignant and nonmalignant diseases with the unexposed subcohort as the reference. Cancer mortality was decreased among DDT-exposed workers, mainly due to a reduction in lung cancer deaths. Birth outside from the study area was a strong predictor of mortality from leukemia. Mortality from stomach cancer increased up to 2-fold in the highest quartile of cumulative exposure (relative risk, 2.0; 95% confidence interval, 0.9-4.4), but no exposure-response trend was observed. Risks of liver cancer, pancreatic cancer, and leukemia were not elevated among DDT-exposed workers. No effect of latency on risk estimates was observed over the 45 years of follow-up and within selected time windows. Adjusting risks by possible exposure to chlordane in the second part of the antimalarial operations did not change the results. In conclusion, we found little evidence for a link between occupational exposure to DDT and mortality from any of the cancers previously suggested to be associated.
JF  - Cancer Research
AU  - Cocco, Pierluigi
AU  - Fadda, Domenica
AU  - Billai, Beatrice
AU  - D'Atri, Mario
AU  - Melis, Massimo
AU  - Blair, Aaron
AD  - Occupational Health Section, Department of Public Health, University of Cagliari, Cagliari, Italy and Occupational and Environmental Epidemiology Branch, Division of Cancer Epidemiology and Genetics, National Cancer Institute, NIH, Department of Health and Human Services, Bethesda, Maryland
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 9588
EP  - 9594
PB  - American Association for Cancer Research, 615 Chestnut St., 17th Floor Philadelphia PA 19106-4404 USA, [URL:http://www.aacr.org/]
VL  - 65
IS  - 20
SN  - 0008-5472, 0008-5472
KW  - Toxicology Abstracts
KW  - X 24136:Environmental impact
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxicologyabstracts&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cancer+Research&rft.atitle=Cancer+Mortality+among+Men+Occupationally+Exposed+to+Dichlorodiphenyltrichloroethane&rft.au=Cocco%2C+Pierluigi%3BFadda%2C+Domenica%3BBillai%2C+Beatrice%3BD%27Atri%2C+Mario%3BMelis%2C+Massimo%3BBlair%2C+Aaron&rft.aulast=Cocco&rft.aufirst=Pierluigi&rft.date=2005-10-01&rft.volume=65&rft.issue=20&rft.spage=9588&rft.isbn=&rft.btitle=&rft.title=Cancer+Research&rft.issn=00085472&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2005-11-01
N1  - Last updated - 2011-12-13
ER  - 



TY  - JOUR
T1  - An updated catalogue of salivary gland transcripts in the adult female mosquito, Anopheles gambiae
AN  - 17647012; 6504104
AB  - Salivary glands of blood-sucking arthropods contain a variety of compounds that prevent platelet and clotting functions and modify inflammatory and immunological reactions in the vertebrate host. In mosquitoes, only the adult female takes blood meals, while both sexes take sugar meals. With the recent description of the Anopheles gambiae genome, and with a set of similar to 3000 expressed sequence tags from a salivary gland cDNA library from adult female mosquitoes, we attempted a comprehensive description of the salivary transcriptome of this most important vector of malaria transmission. In addition to many transcripts associated with housekeeping functions, we found an active transposable element, a set of Wolbachia-like proteins, several transcription factors, including Forkhead, Hairy and doublesex, extracellular matrix components and 71 genes coding for putative secreted proteins. Fourteen of these 71 proteins had matching Edman degradation sequences obtained from SDS-PAGE experiments. Overall, 33 transcripts are reported for the first time as coding for salivary proteins. The tissue and sex specificity of these protein-coding transcripts were analyzed by RT-PCR and microarray experiments for insight into their possible function. Notably, two gene products appeared to be differentially spliced in the adult female salivary glands, whereas 13 contigs matched predicted intronic regions and may include additional alternatively spliced transcripts. Most An. gambiae salivary proteins represent novel protein families of unknown function, potentially coding for pharmacologically or microbiologically active substances. Supplemental data to this work can be found at http://www.ncbi.nlm.nih.gov/projects/omes/index.html#Ag2.
JF  - Journal of Experimental Biology
AU  - Arca, Bruno
AU  - Lombardo, Fabrizio
AU  - Valenzuela, Jesus G
AU  - Francischetti, Ivo MB
AU  - Marinotti, Osvaldo
AU  - Coluzzi, Mario
AU  - Ribeiro, Jose MC
AD  - Department of Structural and Functional Biology, University "Federico II", 80126 Naples, Italy Parasitology Section, Department of Public Health, University "La Sapienza", 00185 Rome, Italy Medical Entomology Section, Laboratory of Malaria and Vector Research, National Institute of Allergy and Infectious Diseases, National Institutes of Health, 12735 Twinbrook Parkway, Rockville, MD 20852, USA Department of Molecular Biology and Biochemistry and Department of Biological Chemistry, University of California, Irvine, CA 92697, USA
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 3971
EP  - 3986
PB  - Company of Biologists, 140 Cowley Road Cambridge CB4 0DL UK, [URL:http://www.biologists.com/web/index.html]
VL  - 208
IS  - 20
SN  - 0022-0949, 0022-0949
KW  - Mosquitoes
KW  - Salivary glands
KW  - ASFA 1: Biological Sciences & Living Resources; ASFA 3: Aquatic Pollution & Environmental Quality; Entomology Abstracts
KW  - Q5 01524:Public health, medicines, dangerous organisms
KW  - Z 05206:Medical & veterinary entomology
KW  - Q1 01305:Genetics and evolution
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-07-01
N1  - Last updated - 2011-12-13
ER  - 



TY  - JOUR
T1  - The association between stress and drinking: Modifying effects of gender and vulnerability
AN  - 17597655; 6509958
AB  - To assess the relationship between number and type of past-year stressful experiences and alcohol consumption, with a focus on how gender, poverty, and psychological vulnerability moderate this association. Data from 26 946 US past-year drinkers 18 years of age and over, interviewed in the 2001-2002 National Epidemiologic Survey on Alcohol and Related Conditions (NESARC), were used to construct multivariate linear regression models predicting six measures of drinking pattern and volume. There was a consistent positive relationship between number of past-year Stressors experienced and all measures of heavy drinking. Frequency of heavy (5+ drinks for men; 4+ drinks for women) drinking increased by 24% with each additional Stressor reported by men and by 13% with each additional Stressor reported by women. In contrast, the frequency of moderate drinking (<5 drinks for men; <4 drinks for women) decreased as stress levels increased. Job-related and legal sources of stress were more strongly associated with alcohol consumption than were social and health-related stress. Men showed a stronger association than women between the number of Stressors and the most consumption measures; they also responded more strongly to the presence of any legal and job-related stress. Having an income below the poverty level intensified the effects of job-related stress, but having a mood or anxiety disorder did not affect any of the associations between stress and consumption. Stress does not so much lead individuals to drink more often as to substitute larger quantities of alcohol on the days when they do drink. Treatment and brief interventions aimed at problem drinkers might benefit from addressing the issue of tension alleviation and the development of alternative coping mechanisms.
JF  - Alcohol and Alcoholism
AU  - Dawson, DA
AU  - Grant, B F
AU  - Ruan, W J
AD  - NIAAA/LEB Room 3083, 5635 Fishers Lane MSC 9304, Bethesda, MD 20892-9304, USA, ddawson@mail.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 453
EP  - 460
VL  - 40
IS  - 5
SN  - 0735-0414, 0735-0414
KW  - Risk Abstracts
KW  - Alcohol
KW  - Stress
KW  - Working conditions
KW  - Gender
KW  - Substance abuse
KW  - Occupational health
KW  - R2 23080:Industrial and labor
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-11-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Stress; Alcohol; Substance abuse; Occupational health; Gender; Working conditions
DO  - http://dx.doi.org/10.1093/alcalc/agh176
ER  - 



TY  - JOUR
T1  - The potential for gene-targeted radiation therapy of cancers
AN  - 17589493; 6513230
AB  - Targeted cancer therapy is the mantra now chanted by oncologists of all types. Everyone hopes that the rapid expansion in the knowledge of cancer cell genetics, signaling, regulatory factors and other changes that underlie malignant transformation and metastasis will lead to innovative approaches for the treatment of cancers. To date, successful targeted therapies have been derived from pharmaceutical chemistry - designing chemical compounds intended to disrupt a crucial pathway for malignant cells to survive, grow and metastasize. Radiotherapy also has a goal of more-selective targeting of therapeutic radiation effects to only tumor cells. In this review, we describe our efforts to create a form of gene-targeted radiation therapy by using the unique radiation effects of radionuclides that decay by the Auger process attached to oligonucleotide carrier-molecules that are capable of forming triplex DNA structures with target sequences in the genome of the human cancer cell.
JF  - Trends in Biotechnology
AU  - Panyutin, I G
AU  - Neumann, R D
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 492
EP  - 496
PB  - Elsevier Ltd
VL  - 23
IS  - 10
SN  - 0167-7799, 0167-7799
KW  - Biotechnology and Bioengineering Abstracts; Medical and Pharmaceutical Biotechnology Abstracts
KW  - Metastases
KW  - Transformation
KW  - DNA structure
KW  - Gene therapy
KW  - Reviews
KW  - Radioisotopes
KW  - Radiotherapy
KW  - Tumor cells
KW  - Oligonucleotides
KW  - Cancer
KW  - Signal transduction
KW  - W 30965:Miscellaneous, Reviews
KW  - W3 33180:Gene based (protocols, clinical trials, and animal models)
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-11-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Cancer; Reviews; Oligonucleotides; Gene therapy; Signal transduction; Transformation; DNA structure; Tumor cells; Metastases; Radiotherapy; Radioisotopes
DO  - http://dx.doi.org/10.1016/j.tibtech.2005.08.001
ER  - 



TY  - JOUR
T1  - Green fluorescent protein tagging: A novel tool in biomedical research
AN  - 17425428; 6549508
AB  - In recent years, the green fluorescent protein (GFP) isolated from the jellyfish, Aequorea victoria, has become a novel tool in biomedical research. The tagging of GFP to proteins of interest has widely been used in studies involving various biological events both in vitro and in vivo. In this report, the authors demonstrate the utility of GFP tagging for studying localization of protein kinase C (PKC alpha ), and pleckstrin homology (PH) domains of phospholipase C (PLC delta 1), and Akt in mouse neuroblastoma (Neuro 2A) cells. The authors also show the real time translocation of PKC alpha and Akt-PH-EGFP to the membrane upon stimulation with either 12-phorbal myristate acetate (PMA) or insulin growth factor (IGF). Pretreatment of cells expressing PKC alpha -EGFP or Akt-PH-EGFP with staurosporine (a protein kinase inhibitor) or wortmanin (a phosphatidylinositol 3-kinase inhibitor), prevented the translocation of these proteins to the membrane. These data demonstrate that, GFP tagging could be employed as a tool to study sub cellular localization and distribution of signaling proteins in response to external stimuli in real time.
JF  - Indian Journal of Biotechnology
AU  - Akbar, M
AU  - Kim, Hee Yong
AD  - Section of Mass Spectrometry, Laboratory of Membrane Biochemistry and Biophysics NIAAA, NIH, Rockville, MD 20852, USA, akbarm@exchange.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 466
EP  - 470
VL  - 4
IS  - 4
SN  - 0972-5849, 0972-5849
KW  - Water jellyfish
KW  - Biotechnology and Bioengineering Abstracts; Medical and Pharmaceutical Biotechnology Abstracts
KW  - Protein kinase C
KW  - Phorbol esters
KW  - Phospholipase C
KW  - Green fluorescent protein
KW  - pleckstrin
KW  - Acetic acid
KW  - Neuroblastoma
KW  - Insulin
KW  - 1-Phosphatidylinositol 3-kinase
KW  - Staurosporine
KW  - Insulin-like growth factors
KW  - AKT protein
KW  - Aequorea victoria
KW  - W3 33340:Other proteins, peptides, amino acids
KW  - W 30965:Miscellaneous, Reviews
KW  - W3 33250:Methods: Others
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Aequorea victoria; Protein kinase C; Green fluorescent protein; Phospholipase C; pleckstrin; Phorbol esters; AKT protein; Acetic acid; Insulin-like growth factors; Insulin; Neuroblastoma; Staurosporine; 1-Phosphatidylinositol 3-kinase
ER  - 



TY  - JOUR
T1  - Mutator Phenotype Resulting from DNA Polymerase IV Overproduction in Escherichia coli: Preferential Mutagenesis on the Lagging Strand
AN  - 17423722; 6527578
AB  - We investigated the mutator effect resulting from overproduction of Escherichia coli DNA polymerase IV. Using lac mutational targets in the two possible orientations on the chromosome, we observed preferential mutagenesis during lagging strand synthesis. The mutator activity likely results from extension of mismatches produced by polymerase III holoenzyme.
JF  - Journal of Bacteriology
AU  - Kuban, Wojciech
AU  - Banach-Orlowska, Magdalena
AU  - Bialoskorska, Malgorzata
AU  - Lipowska, Aleksandra
AU  - Schaaper, Roel M
AU  - Jonczyk, Piotr
AU  - Fijalkowska, Iwona J
AD  - Institute of Biochemistry and Biophysics, Polish Academy of Sciences, 02 106 Warsaw, Poland. Laboratory of Molecular Genetics, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina 27709
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 6862
EP  - 6866
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 187
IS  - 19
SN  - 0021-9193, 0021-9193
KW  - Biochemistry Abstracts 2: Nucleic Acids; Microbiology Abstracts B: Bacteriology
KW  - Chromosomes
KW  - DNA-directed DNA polymerase
KW  - Escherichia coli
KW  - Mutagenesis
KW  - N 14835:Protein-Nucleic Acids Association
KW  - J 02740:Genetics and evolution
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17423722?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Bacteriology&rft.atitle=Mutator+Phenotype+Resulting+from+DNA+Polymerase+IV+Overproduction+in+Escherichia+coli%3A+Preferential+Mutagenesis+on+the+Lagging+Strand&rft.au=Kuban%2C+Wojciech%3BBanach-Orlowska%2C+Magdalena%3BBialoskorska%2C+Malgorzata%3BLipowska%2C+Aleksandra%3BSchaaper%2C+Roel+M%3BJonczyk%2C+Piotr%3BFijalkowska%2C+Iwona+J&rft.aulast=Kuban&rft.aufirst=Wojciech&rft.date=2005-10-01&rft.volume=187&rft.issue=19&rft.spage=6862&rft.isbn=&rft.btitle=&rft.title=Journal+of+Bacteriology&rft.issn=00219193&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Chromosomes; DNA-directed DNA polymerase; Mutagenesis; Escherichia coli
ER  - 



TY  - JOUR
T1  - Role of RcsF in Signaling to the Rcs Phosphorelay Pathway in Escherichia coli
AN  - 17419839; 6527566
AB  - The rcs phosphorelay pathway components were originally identified as regulators of capsule synthesis. In addition to the transmembrane sensor kinase RcsC, the RcsA coregulator, and the response regulator RcsB, two new components have been characterized, RcsD and RcsF. RcsD, the product of the yojN gene, now renamed rcsD, acts as a phosphorelay between RcsC and RcsB. Transcription of genes for capsule synthesis (cps) requires both RcsA and RcsB; transcription of other promoters, including that for the small RNA RprA, requires only RcsB. RcsF was described as an alternative sensor kinase for RcsB. We have examined the role of RcsF in the activation of both the rprA and cps promoters. We find that a number of signals that lead to activation of the phosphorelay require both RcsF and RcsC; epistasis experiments place RcsF upstream of RcsC. The RcsF sequence is characteristic of lipoproteins, consistent with a role in sensing cell surface perturbation and transmitting this signal to RcsC. Activation of RcsF does not require increased transcription of the gene, suggesting that modification of the RcsF protein may act as an activating signal. Signals from RcsC require RcsD to activate RcsB. Sequencing of an rcsC allele, rcsC137, that leads to high-level constitutive expression of both cps and rprA suggests that the response regulator domain of RcsC plays a role in negatively regulating the kinase activity of RcsC. The phosphorelay and the variation in the activation mechanism (dependent upon or independent of RcsA) provide multiple steps for modulating the output from this system.
JF  - Journal of Bacteriology
AU  - Majdalani, Nadim
AU  - Heck, Michael
AU  - Stout, Valerie
AU  - Gottesman, Susan
AD  - Laboratory of Molecular Biology, National Cancer Institute, Bethesda, Maryland 20892. School of Life Sciences, Arizona State University, Tempe, Arizona 85287-4501
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 6770
EP  - 6778
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 187
IS  - 19
SN  - 0021-9193, 0021-9193
KW  - Microbiology Abstracts B: Bacteriology
KW  - Promoters
KW  - Cell surface
KW  - RNA
KW  - Epistasis
KW  - Lipoproteins
KW  - Escherichia coli
KW  - Transcription
KW  - Signal transduction
KW  - J 02727:Amino acids, peptides and proteins
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Bacteriology&rft.atitle=Role+of+RcsF+in+Signaling+to+the+Rcs+Phosphorelay+Pathway+in+Escherichia+coli&rft.au=Majdalani%2C+Nadim%3BHeck%2C+Michael%3BStout%2C+Valerie%3BGottesman%2C+Susan&rft.aulast=Majdalani&rft.aufirst=Nadim&rft.date=2005-10-01&rft.volume=187&rft.issue=19&rft.spage=6770&rft.isbn=&rft.btitle=&rft.title=Journal+of+Bacteriology&rft.issn=00219193&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Cell surface; Promoters; RNA; Epistasis; Lipoproteins; Transcription; Signal transduction; Escherichia coli
ER  - 



TY  - JOUR
T1  - Modifying the NH sub(2) and COOH Termini of Aquaporin-5: Effects on Localization in Polarized Epithelial Cells
AN  - 17416101; 6537910
AB  - To reengineer polarized epithelial cell functions directly in situ, or ex vivo in the fabrication of an artificial organ, it is necessary to understand mechanisms that account for polarized membrane sorting. We have used the aquaporins (AQPs), a family of homotetrameric water channel proteins, as model membrane proteins for this purpose. AQP monomers contain six transmembrane-spanning domains linked by five interconnecting loops, with the NH sub(2) and COOH termini residing in the cytosol. AQP5 is localized in the apical membranes of several different epithelia in vivo, and in stably transfected MDCK-II cells grown as a polarized monolayer. We wished to identify a structural region(s) within rat AQP5 (rAQP5) important for apical localization, and to study the MDCK-II cell localization of rAQP5s modified in either their NH sub(2) or COOH terminus. We show that the NH sub(2)- terminal region does not play a major role in apical localization as deletion of the NH sub(2) terminus produced a modified rAQP5 construct (AQP5- NT sub(del)) that was stably expressed and localized primarily to the apical membranes of MDCK-II cells. Attachment of a FLAG epitope to the NH sub(2) terminus of AQP5 (AQP5 sub(flag) construct) also did not perturb apical localization. In addition, we found that the exchange of NH sub(2)-terminal regions between rAQP5 and human AQP1 (hAQP1; a nonpolarized AQP isoform) produced a modified rAQP5 construct (AQP5-1NT) and a modified hAQP1 construct (AQP1-5NT), each of which localized as the parental AQP (apically, and to both apical and basolateral membranes, respectively). In contrast, we found that deletion of the COOH terminus resulted in a modified rAQP5 construct (AQP5-CT sub(del)) that was unstably expressed and localized to intracellular site(s) in MDCK-II cells. Substitution of the COOH terminus of AQP1 with the COOH terminus of AQP5 also produced a construct (AQP1-5CT) transiently expressed in intracellular compartment(s). However, substitution of the COOH terminus of rAQP5 with the COOH terminus of hAQP1 produced a modified rAQP5 construct (AQP5-1CT) that was stably expressed and localized to basolateral membranes, suggesting the loss of an apical targeting/retention signal from rAQP5, the gain of a basolateral targeting/retention signal from hAQP1, or a combination of these two possibilities.
JF  - Tissue Engineering
AU  - Wellner, R B
AU  - Hong, Sohee
AU  - Cotrim, A P
AU  - Swaim, W D
AU  - Baum, B J
AD  - Gene Therapy and Therapeutics Branch, National Institute of Dental and Craniofacial Research, National Institutes of Health, Building 10, Room 1N113, 10 Center Drive, MSC 1190, Bethesda, MD 20892-1190, USA, bbaum@dir.nidcr.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 1449
EP  - 1458
VL  - 11
IS  - 9-10
SN  - 1076-3279, 1076-3279
KW  - Biotechnology and Bioengineering Abstracts; Bioengineering Abstracts; Medical and Pharmaceutical Biotechnology Abstracts
KW  - Epithelial cells
KW  - Clonal deletion
KW  - Aquaporin 1
KW  - aquaporins
KW  - Membrane proteins
KW  - Polarization
KW  - Tissue engineering
KW  - Monomers
KW  - Cytosol
KW  - Epitopes
KW  - artificial organs
KW  - W 30965:Miscellaneous, Reviews
KW  - W3 33220:Cell culture
KW  - W4 110:Biomedical Materials & Tissue Engineering
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Tissue+Engineering&rft.atitle=Modifying+the+NH+sub%282%29+and+COOH+Termini+of+Aquaporin-5%3A+Effects+on+Localization+in+Polarized+Epithelial+Cells&rft.au=Wellner%2C+R+B%3BHong%2C+Sohee%3BCotrim%2C+A+P%3BSwaim%2C+W+D%3BBaum%2C+B+J&rft.aulast=Wellner&rft.aufirst=R&rft.date=2005-10-01&rft.volume=11&rft.issue=9-10&rft.spage=1449&rft.isbn=&rft.btitle=&rft.title=Tissue+Engineering&rft.issn=10763279&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Clonal deletion; Aquaporin 1; Epithelial cells; artificial organs; Cytosol; Monomers; Tissue engineering; Membrane proteins; Epitopes; aquaporins; Polarization
ER  - 



TY  - JOUR
T1  - Anti-IFN- gamma Autoantibodies in Disseminated Nontuberculous Mycobacterial Infections
AN  - 17410141; 6528263
AB  - Although many patients with disseminated nontuberculous mycobacterial disease have molecular defects in the IFN- gamma /IL-12 axis, recent case reports have shown autoantibodies against IFN- gamma associated with severe nontuberculous mycobacterial infections. To check this finding in an independent population, we screened 35 patients with either disseminated or pulmonary nontuberculous mycobacterial infections for whom no molecular defect was known. We identified high-titer-neutralizing anti-IFN- gamma IgG in the plasma of six patients. All six patients were female, parous, of East Asian descent, and had disseminated infection, predominantly with rapidly growing mycobacteria. The anti-IFN- gamma IgG had in vitro biological activity on the IFN- gamma -dependent phosphorylation of STAT-1 as well as on the IFN- gamma -dependent up-regulation of TNF- alpha and IL-12. In contrast, this anti-IFN- gamma Ab had no effect on IFN- alpha -dependent STAT-1 phosphorylation. These patients confirm a novel syndrome linking autoimmunity and immunodeficiency.
JF  - Journal of Immunology
AU  - Patel, Smita Y
AU  - Ding, Li
AU  - Brown, Margaret R
AU  - Lantz, Larry
AU  - Gay, Ted
AU  - Cohen, Stuart
AU  - Martyak, Lenna A
AU  - Kubak, Bernard
AU  - Holland, Steven M
AD  - Immunopathogenesis Section, Laboratory of Clinical Infectious Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892. Department of Laboratory Medicine, National Institutes of Health, Bethesda, MD 20892. Research Technologies Branch, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892. Tri City Medical Center, Oceanside, CA 92056. University of California, Davis School of Medicine, Sacramento, CA 95817. University of California, Los Angeles School of Medicine, Los Angeles, CA 90095
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 4769
EP  - 4776
PB  - American Association of Immunologists, 9650 Rockville Pike Bethesda MD 20814-3998 USA, [URL:http://www.jimmunol.org/]
VL  - 175
IS  - 7
SN  - 0022-1767, 0022-1767
KW  - Microbiology Abstracts B: Bacteriology; Immunology Abstracts
KW  - gamma -Interferon
KW  - Disseminated infection
KW  - Immunodeficiency
KW  - Autoimmunity
KW  - Interleukin 12
KW  - Phosphorylation
KW  - Autoantibodies
KW  - Case reports
KW  - Stat1 protein
KW  - Lung
KW  - Immunoglobulin G
KW  - Tumor necrosis factor- alpha
KW  - F 06366:Respiratory System: Clinical
KW  - J 02845:Ear, nose and respiratory tract
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17410141?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Immunology&rft.atitle=Anti-IFN-+gamma+Autoantibodies+in+Disseminated+Nontuberculous+Mycobacterial+Infections&rft.au=Patel%2C+Smita+Y%3BDing%2C+Li%3BBrown%2C+Margaret+R%3BLantz%2C+Larry%3BGay%2C+Ted%3BCohen%2C+Stuart%3BMartyak%2C+Lenna+A%3BKubak%2C+Bernard%3BHolland%2C+Steven+M&rft.aulast=Patel&rft.aufirst=Smita&rft.date=2005-10-01&rft.volume=175&rft.issue=7&rft.spage=4769&rft.isbn=&rft.btitle=&rft.title=Journal+of+Immunology&rft.issn=00221767&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Interleukin 12; gamma -Interferon; Case reports; Autoantibodies; Phosphorylation; Lung; Stat1 protein; Disseminated infection; Immunodeficiency; Immunoglobulin G; Autoimmunity; Tumor necrosis factor- alpha
ER  - 



TY  - JOUR
T1  - Habitual physical activity in children: the role of genes and the environment
AN  - 17407114; 6511748
AB  - Background: Understanding the factors that contribute to physical inactivity in children is important because sedentary behavior strongly relates to metabolic disorders such as obesity and diabetes. Objective: We aimed to quantify the genetic and environmental influences on physical activity energy expenditure (PAEE) in 100 sex-concordant dizygotic (n = 38) and monozygotic (n = 62) twin pairs aged 4-10 y. Design: Resting metabolic rate (RMR) was assessed by using respiratory gas exchange, total energy expenditure (TEE) by using doubly labeled water, and body composition by using dual-energy X-ray absorptiometry. Structural equation modeling was used to partition the phenotypic variance into additive genetic (a super(2)) and common (c super(2)) and unshared (e super(2)) environmental components. Results: Because PAEE [TEE - (RMR + 0.1 x TEE)] depends on body weight, which is highly heritable, we tested several models: 1) after adjustment for age, sex, ethnicity, study date, season, and weight, a super(2) explained none of the phenotypic variance in PAEE (95% CI: 0%, 38%), whereas c super(2) and e super(2) accounted for 69% (33%, 77%; P = 0.001) and 31% (23%, 39%; P < 0.001) of the variance, respectively; 2) after adjustment for the cofactors in model 1, a super(2) explained 19% of the phenotypic variance in TEE (0%, 60%; P = 0.13), whereas c super(2) and e super(2) accounted for 59% (16%, 79%; P = 0.007) and 23% (17%, 31%; P < 0.0001) of the variance, respectively; 3) in models adjusted as above (excluding weight), a super(2) explained no variance in physical activity level (TEE/RMR) (0%, 32%; P = 0.50), whereas c super(2) and e super(2) explained 65% (34%, 60%; P = 0.001) and 35% (28%, 45%; P < 0.0001) of the variance, respectively. Conclusions: Our data suggest that the familial resemblance in physical activity in these children is explained.
JF  - American Journal of Clinical Nutrition
AU  - Franks, P W
AU  - Ravussin, E
AU  - Hanson, R L
AU  - Harper, I T
AU  - Allison, D B
AU  - Knowler, W C
AU  - Tataranni, P A
AU  - Salbe, AD
AD  - National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Phoenix, AZ, USA
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 901
EP  - 908
VL  - 82
IS  - 4
SN  - 0002-9165, 0002-9165
KW  - Genetics Abstracts; Physical Education Index
KW  - Gas exchange
KW  - Age
KW  - Physical activity
KW  - Metabolic rate
KW  - Dual energy X-ray absorptiometry
KW  - Nutrition
KW  - Water
KW  - Models
KW  - Genetics
KW  - Body weight
KW  - Weight
KW  - Body composition
KW  - Ethnic groups
KW  - Sex
KW  - Obesity
KW  - Mathematical models
KW  - Data processing
KW  - Metabolic disorders
KW  - Basal metabolic rate
KW  - Exercise
KW  - Children
KW  - Diabetes
KW  - Diabetes mellitus
KW  - Energy cost
KW  - X-Ray
KW  - Twins
KW  - Energy expenditure
KW  - Cofactors
KW  - Behavior
KW  - Modeling
KW  - G 07880:Human Genetics
KW  - PE 030:Exercise, Health & Physical Fitness
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aphysicaleducation&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=American+Journal+of+Clinical+Nutrition&rft.atitle=Habitual+physical+activity+in+children%3A+the+role+of+genes+and+the+environment&rft.au=Franks%2C+P+W%3BRavussin%2C+E%3BHanson%2C+R+L%3BHarper%2C+I+T%3BAllison%2C+D+B%3BKnowler%2C+W+C%3BTataranni%2C+P+A%3BSalbe%2C+AD&rft.aulast=Franks&rft.aufirst=P&rft.date=2005-10-01&rft.volume=82&rft.issue=4&rft.spage=901&rft.isbn=&rft.btitle=&rft.title=American+Journal+of+Clinical+Nutrition&rft.issn=00029165&rft_id=info:doi/
LA  - English
DB  - Physical Education Index
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Gas exchange; Obesity; Age; Basal metabolic rate; Exercise; Children; Nutrition; Water; Diabetes; X-Ray; Energy cost; Genetics; Weight; Behavior; Body composition; Modeling; Sex; Data processing; Mathematical models; Metabolic disorders; Physical activity; Dual energy X-ray absorptiometry; Metabolic rate; Models; Diabetes mellitus; Cofactors; Energy expenditure; Twins; Body weight; Ethnic groups
ER  - 



TY  - JOUR
T1  - Inactivation of Retroviruses with Preservation of Structural Integrity by Targeting the Hydrophobic Domain of the Viral Envelope
AN  - 17405288; 6528592
AB  - We describe a new approach for the preparation of inactivated retroviruses for vaccine application. The lipid domain of the viral envelope was selectively targeted to inactivate proteins and lipids therein and block fusion of the virus with the target cell membrane. In this way, complete elimination of the infectivity of human immunodeficiency virus (HIV) and simian immunodeficiency virus (SIV) could be achieved with preservation of antigenic determinants on the surface of the viral envelope. Inactivation was accomplished by modification of proteins and lipids in the viral envelope using the hydrophobic photoinduced alkylating probe 1,5 iodonaphthylazide (INA). Treatment of HIV and SIV isolates with INA plus light completely blocked fusion of the viral envelope and abolished infectivity. The inactivated virus remained structurally unchanged, with no detectable loss of viral proteins. Modifications to envelope and nucleocapsid proteins were detected by changes in their elution pattern on reverse-phase high-performance liquid chromatography. These modifications had no effect on primary and secondary structure epitopes as determined by monoclonal antibodies. Likewise, the inactivated HIV reacted as well as the live virus with the conformation-sensitive and broadly neutralizing anti-HIV type 1 monoclonal antibodies 2G12, b12, and 4E10. Targeting the lipid domain of biological membranes with hydrophobic alkylating compounds could be used as a general approach for inactivation of enveloped viruses and other pathogenic microorganisms for vaccine application.
JF  - Journal of Virology
AU  - Raviv, Yossef
AU  - Viard, Mathias
AU  - Bess, Julian W, Jr
AU  - Chertova, Elena
AU  - Blumenthal, Robert
AD  - Center for Cancer Research Nanobiology Program. Basic Research Program, SAIC. AIDS Vaccine Program, SAIC, National Cancer Institute, Frederick, Maryland
Y1  - 2005/10/01/
PY  - 2005
DA  - 2005 Oct 01
SP  - 12394
EP  - 12400
PB  - American Society for Microbiology, 1752 N Street N.W. Washington, DC 20036 USA, [URL:http://www.asm.org/]
VL  - 79
IS  - 19
SN  - 0022-538X, 0022-538X
KW  - HIV
KW  - SIV
KW  - Microbiology Abstracts A: Industrial & Applied Microbiology; Virology & AIDS Abstracts
KW  - High-performance liquid chromatography
KW  - Monoclonal antibodies
KW  - Lipids
KW  - Secondary structure
KW  - Probes
KW  - Hydrophobicity
KW  - Light effects
KW  - Protein structure
KW  - Infectivity
KW  - Retrovirus
KW  - Envelopes
KW  - Human immunodeficiency virus
KW  - Antigenic determinants
KW  - Nucleocapsids
KW  - Microorganisms
KW  - Vaccines
KW  - Preservation
KW  - Simian immunodeficiency virus
KW  - Epitopes
KW  - A 01340:Antibiotics & Antimicrobials
KW  - V 22002:AIDS: Molecular and in vitro aspects
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologya&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+Virology&rft.atitle=Inactivation+of+Retroviruses+with+Preservation+of+Structural+Integrity+by+Targeting+the+Hydrophobic+Domain+of+the+Viral+Envelope&rft.au=Raviv%2C+Yossef%3BViard%2C+Mathias%3BBess%2C+Julian+W%2C+Jr%3BChertova%2C+Elena%3BBlumenthal%2C+Robert&rft.aulast=Raviv&rft.aufirst=Yossef&rft.date=2005-10-01&rft.volume=79&rft.issue=19&rft.spage=12394&rft.isbn=&rft.btitle=&rft.title=Journal+of+Virology&rft.issn=0022538X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-01-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - High-performance liquid chromatography; Monoclonal antibodies; Lipids; Secondary structure; Probes; Hydrophobicity; Light effects; Protein structure; Infectivity; Envelopes; Antigenic determinants; Microorganisms; Nucleocapsids; Preservation; Vaccines; Epitopes; Retrovirus; Human immunodeficiency virus; Simian immunodeficiency virus
ER  - 



TY  - JOUR
T1  - EVOPRINTER, a multigenomic comparative tool for rapid identification of functionally important DNA
AN  - 17400084; 6505009
AB  - Here, we describe a multigenomic DNA sequence-analysis tool, EVOPRINTER, that facilitates the rapid identification of evolutionary conserved sequences within the context of a single species. The EVOPRINTER output identifies multispecies-conserved DNA sequences as they exist in a reference DNA. This identification is accomplished by superimposing multiple reference DNA vs. test-genome pairwise BLAT (BLAST-like alignment tool) readouts of the reference DNA to identify conserved nucleotides that are shared by all orthologous DNAs. EVOPRINTER analysis of well characterized genes reveals that most, if not all, of the conserved sequences are essential for gene function. For example, analysis of orthologous genes that are shared by many vertebrates identifies conserved DNA in both protein-encoding sequences and noncoding cis-regulatory regions, including enhancers and mRNA microRNA binding sites. In Drosophila, the combined mutational histories of five or more species affords near-base pair resolution of conserved transcription factor DNA-binding sites, and essential amino acids are revealed by the nucleotide flexibility of their codon-wobble position(s). Conserved small peptide-encoding genes, which had been undetected by conventional gene-prediction algorithms, are identified by the codon-wobble signatures of invariant amino acids. Also, EVOPRINTER allows one to assess the degree of evolutionary divergence between orthologous DNAs by highlighting differences between a selected species and the other test species.
JF  - Proceedings of the National Academy of Sciences, USA
AU  - Odenwald, Ward F
AU  - Rasband, Wayne
AU  - Kuzin, Alexander
AU  - Brody, Thomas
AD  - Neural Cell-Fate Determinants Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD 20892
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 14700
EP  - 14705
PB  - National Academy of Sciences, 2101 Constitution Ave. Washington DC 20418 USA
VL  - 102
IS  - 41
SN  - 0027-8424, 0027-8424
KW  - Biotechnology and Bioengineering Abstracts; Bioengineering Abstracts; Biochemistry Abstracts 2: Nucleic Acids; Entomology Abstracts
KW  - Algorithms
KW  - DNA sequencing
KW  - Amino acids
KW  - miRNA
KW  - Assays
KW  - Enhancers
KW  - Transcription factors
KW  - Bioinformatics
KW  - Drosophila
KW  - Evolution
KW  - N 14010:Physical & Computer Methods & Assays
KW  - Z 05216:Biochemical genetics
KW  - W 30965:Miscellaneous, Reviews
KW  - W4 350:Bioinformatics
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17400084?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Proceedings+of+the+National+Academy+of+Sciences%2C+USA&rft.atitle=EVOPRINTER%2C+a+multigenomic+comparative+tool+for+rapid+identification+of+functionally+important+DNA&rft.au=Odenwald%2C+Ward+F%3BRasband%2C+Wayne%3BKuzin%2C+Alexander%3BBrody%2C+Thomas&rft.aulast=Odenwald&rft.aufirst=Ward&rft.date=2005-10-01&rft.volume=102&rft.issue=41&rft.spage=14700&rft.isbn=&rft.btitle=&rft.title=Proceedings+of+the+National+Academy+of+Sciences%2C+USA&rft.issn=00278424&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-04-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Drosophila; DNA sequencing; Amino acids; Bioinformatics; Assays; Evolution; Algorithms; miRNA; Enhancers; Transcription factors
ER  - 



TY  - JOUR
T1  - Induction of Invasive Mouse Skin Carcinomas in Transgenic Mice with Mutations in Both H-ras and p53
AN  - 17400064; 6509469
AB  - Synergistic interaction between H-ras and p53 were systematically examined during skin tumorigenesis. Concurrent expression of an activated H-ras gene and a mutant p53 gene was accomplished by crossing p53 super(Val135/wt) mice with TG.AC mice. Topical application to wild-type mice with benzo(a)pyrene (BaP) alone produced similar to 26% skin tumor incidence, whereas BaP treatment of p53 super(wt/wt)Hras super(TG.AC/wt), p53 super(Val135/wt)Hras super(wt/wt), and p53 super(Val135/wt)Hras super(TG.AC/wt) mice produced a 75%, 77%, and 100% incidence of skin tumors, respectively. An average of 0.33 tumor per mouse was observed in wild-type (p53 super(wt/wt)Hras super(wt/wt)) mice, whereas similar to 1.54, 1.96, and 3.08 tumors per mouse were seen in BaP-treated p53 super(wt/wt)Hras super(TG.AC/wt), p53 super(Val135/wt)Hras super(wt/wt), and p53 super(Val135/wt)Hras super(TG.AC/wt) mice, respectively. The effects on total tumor volume were even more striking with 7-, 48-, and 588-fold increases in tumor volume compared with wild-type (p53 super(wt/wt)Hras super(wt/wt)) in p53 super(wt/wt)Hras super(TG.AC/wt), p53 super(Val135/wt)Hras super(wt/wt), and p53 super(Val135/wt)Hras super(TG.AC/wt) mice, respectively. Histopathologically, all tumors from p53 super(wt/wt)Hras super(wt/wt) mice were either papillomas or well-differentiated squamous cell carcinomas, whereas the tumors in p53 super(wt/wt)Hras super(TG.AC/wt), p53 super(Val135/wt)Hras super(wt/wt), and p53 super(Val135/wt)Hras super(TG.AC/wt) mice were principally squamous cell carcinomas with varying degree of invasiveness. Particularly, tumors in p53 super(Val135/wt)Hras super(TG.AC/wt) mice exhibited the most rapid growth and the extreme form of tumor invasion. Microarray analysis revealed that dominant-negative p53 (Val super(135)) and activated H-ras affected several cellular processes involved in tumorigenesis possibly through its effects on apoptosis, cell cycle arrest, and Ras-mitogen-activated protein kinase pathways. The present study provides the first in vivo evidence that a germ line p53 mutation and activated H-ras act synergistically to profoundly enhance tumor progression.
JF  - Molecular Cancer Research
AU  - Zhang, Zhongqiu
AU  - Yao, Ruisheng
AU  - Li, Jie
AU  - Wang, Yian
AU  - Boone, Charles W
AU  - Lubet, Ronald A
AU  - You, Ming
AD  - Department of Surgery and The Alvin J. Siteman Cancer Center, Washington University School of Medicine, St. Louis, Missouri and Chemoprevention Branch, National Cancer Institute, Bethesda, Maryland
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 563
EP  - 574
PB  - American Association for Cancer Research, 615 Chestnut St., 17th Floor Philadelphia PA 19106-4404 USA, [URL:http://www.aacr.org/]
VL  - 3
IS  - 10
SN  - 1541-7786, 1541-7786
KW  - Genetics Abstracts; Oncogenes & Growth Factors Abstracts; Biotechnology and Bioengineering Abstracts
KW  - Invasiveness
KW  - Skin
KW  - Apoptosis
KW  - H-Ras protein
KW  - Cell cycle
KW  - Tumorigenesis
KW  - squamous cell carcinoma
KW  - Transgenic mice
KW  - skin carcinoma
KW  - p53 protein
KW  - Topical application
KW  - Protein kinase
KW  - Benzo(a)pyrene
KW  - Papilloma
KW  - Mutation
KW  - Hras gene
KW  - W 30925:Genetic Engineering
KW  - B 26670:Tumor Suppressors
KW  - G 07730:Development & Cell Cycle
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17400064?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Molecular+Cancer+Research&rft.atitle=Induction+of+Invasive+Mouse+Skin+Carcinomas+in+Transgenic+Mice+with+Mutations+in+Both+H-ras+and+p53&rft.au=Zhang%2C+Zhongqiu%3BYao%2C+Ruisheng%3BLi%2C+Jie%3BWang%2C+Yian%3BBoone%2C+Charles+W%3BLubet%2C+Ronald+A%3BYou%2C+Ming&rft.aulast=Zhang&rft.aufirst=Zhongqiu&rft.date=2005-10-01&rft.volume=3&rft.issue=10&rft.spage=563&rft.isbn=&rft.btitle=&rft.title=Molecular+Cancer+Research&rft.issn=15417786&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Invasiveness; Apoptosis; Skin; H-Ras protein; Tumorigenesis; Cell cycle; squamous cell carcinoma; Transgenic mice; Topical application; p53 protein; skin carcinoma; Protein kinase; Benzo(a)pyrene; Papilloma; Mutation; Hras gene
ER  - 



TY  - JOUR
T1  - Recombination Hotspots and Population Structure in Plasmodium falciparum
AN  - 17398750; 6514407
AB  - Understanding the influences of population structure, selection, and recombination on polymorphism and linkage disequilibrium (LD) is integral to mapping genes contributing to drug resistance or virulence in Plasmodium falciparum. The parasites short generation time, coupled with a high cross-over rate, can cause rapid LD break-down. However, observations of low genetic variation have led to suggestions of effective clonality: selfing, population admixture, and selection may preserve LD in populations. Indeed, extensive LD surrounding drug-resistant genes has been observed, indicating that recombination and selection play important roles in shaping recent parasite genome evolution. These studies, however, provide only limited information about haplotype variation at local scales. Here we describe the first (to our knowledge) chromosome-wide SNP haplotype and population recombination maps for a global collection of malaria parasites, including the 3D7 isolate, whose genome has been sequenced previously. The parasites are clustered according to continental origin, but alternative groupings were obtained using SNPs at 37 putative transporter genes that are potentially under selection. Geographic isolation and highly variable multiple infection rates are the major factors affecting haplotype structure. Variation in effective recombination rates is high, both among populations and along the chromosome, with recombination hotspots conserved among populations at chromosome ends. This study supports the feasibility of genome-wide association studies in some parasite populations.
JF  - PLoS Biology
AU  - Mu, Jianbing
AU  - Awadalla, Philip
AU  - Duan, Junhui
AU  - McGee, Kate M
AU  - Joy, Deirdre A
AU  - McVean, Gilean AT
AU  - Su, Xin-Zhuan
AD  - Laboratory of Malaria and Vector Research, National Institutes of Health, Rockville, Maryland, United States of America, xsu@niaid.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
PB  - Public Library of Science, 185 Berry Street Suite 1300 San Francisco CA 94107 USA, [mailto:plos@plos.org], [URL:http://www.plos.org]
VL  - 3
IS  - 10
SN  - 1544-9173, 1544-9173
KW  - Ecology Abstracts; Microbiology Abstracts C: Algology, Mycology & Protozoology; Genetics Abstracts
KW  - Hot spots
KW  - Gene polymorphism
KW  - Drug resistance
KW  - Genetic diversity
KW  - Malaria
KW  - Plasmodium falciparum
KW  - Virulence
KW  - Linkage disequilibrium
KW  - Recombination
KW  - Chromosomes
KW  - Haplotypes
KW  - Single-nucleotide polymorphism
KW  - Population structure
KW  - Evolutionary genetics
KW  - Gene mapping
KW  - G 07361:Protozoans/slime molds
KW  - D 04655:Invertebrates - general
KW  - K 03081:Protozoa
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17398750?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Aecology&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=PLoS+Biology&rft.atitle=Recombination+Hotspots+and+Population+Structure+in+Plasmodium+falciparum&rft.au=Mu%2C+Jianbing%3BAwadalla%2C+Philip%3BDuan%2C+Junhui%3BMcGee%2C+Kate+M%3BJoy%2C+Deirdre+A%3BMcVean%2C+Gilean+AT%3BSu%2C+Xin-Zhuan&rft.aulast=Mu&rft.aufirst=Jianbing&rft.date=2005-10-01&rft.volume=3&rft.issue=10&rft.spage=&rft.isbn=&rft.btitle=&rft.title=PLoS+Biology&rft.issn=15449173&rft_id=info:doi/10.1371%2Fjournal.pbio.0030335
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-12-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Hot spots; Drug resistance; Gene polymorphism; Genetic diversity; Malaria; Virulence; Recombination; Linkage disequilibrium; Chromosomes; Haplotypes; Single-nucleotide polymorphism; Population structure; Evolutionary genetics; Gene mapping; Plasmodium falciparum
DO  - http://dx.doi.org/10.1371/journal.pbio.0030335
ER  - 



TY  - JOUR
T1  - Crystal structure of the Yersinia type III secretion protein YscE
AN  - 17392323; 6508274
AB  - The plague-causing bacterium Yersinia pestis utilizes a contact-dependent (type III) secretion system (T3SS) to transport virulence factors from the bacterial cytosol directly into the interior of mammalian cells where they interfere with signal transduction pathways that mediate phagocytosis and the inflammatory response. The type III secretion apparatus is composed of 20-25 different Yersinia secretion (Ysc) proteins. We report here the structure of YscE, the smallest Ysc protein, which is a dimer in solution. The probable mode of oligomerization is discussed.
JF  - Protein Science
AU  - Phan, Jason
AU  - Austin, Brian P
AU  - Waugh, David S
AD  - Macromolecular Crystallography Laboratory, Center for Cancer Research, National Cancer Institute at Frederick, Frederick, Maryland 21702-1201, USA
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 2759
EP  - 2763
PB  - Cold Spring Harbor Laboratory Press, [mailto:cshpress@cshl.org], [URL:http://www.cshl.org/]
VL  - 14
IS  - 10
SN  - 0961-8368, 0961-8368
KW  - YscE protein
KW  - Microbiology Abstracts B: Bacteriology
KW  - virulence factors
KW  - Mammalian cells
KW  - Secretion
KW  - Oligomerization
KW  - Cytosol
KW  - Crystal structure
KW  - Yersinia pestis
KW  - Plague
KW  - Phagocytosis
KW  - Inflammation
KW  - Signal transduction
KW  - J 02727:Amino acids, peptides and proteins
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17392323?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologyb&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Protein+Science&rft.atitle=Crystal+structure+of+the+Yersinia+type+III+secretion+protein+YscE&rft.au=Phan%2C+Jason%3BAustin%2C+Brian+P%3BWaugh%2C+David+S&rft.aulast=Phan&rft.aufirst=Jason&rft.date=2005-10-01&rft.volume=14&rft.issue=10&rft.spage=2759&rft.isbn=&rft.btitle=&rft.title=Protein+Science&rft.issn=09618368&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-04-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Mammalian cells; virulence factors; Secretion; Oligomerization; Crystal structure; Cytosol; Plague; Phagocytosis; Signal transduction; Inflammation; Yersinia pestis
ER  - 



TY  - JOUR
T1  - High-Resolution Serum Proteomic Profiling of Alzheimer Disease Samples Reveals Disease-Specific, Carrier-Protein-Bound Mass Signatures
AN  - 17385924; 6502847
AB  - BACKGROUND: Researchers typically search for disease markers using a "targeted" approach in which a hypothesis about the disease mechanism is tested and experimental results either confirm or disprove the involvement of a particular gene or protein in the disease. Recently, there has been interest in developing disease diagnostics based on unbiased quantification of differences in global patterns of protein and peptide masses, typically in blood from individuals with and without disease. We combined a suite of methods and technologies, including novel sample preparation based on carrier-protein capture and biomarker enrichment, high-resolution mass spectrometry, a unique cohort of well-characterized persons with and without Alzheimer disease (AD), and powerful bioinformatic analysis, that add statistical and procedural robustness to biomarker discovery from blood. METHODS: Carrier-protein-bound peptides were isolated from serum samples by affinity chromatography, and peptide mass spectra were acquired by a matrix-assisted laser desorption/ionization (MALDI) orthogonal time-of-flight (O-TOF) mass spectrometer capable of collecting data over a broad mass range (100 to >300 000 Da) in a single acquisition. Discriminatory analysis of mass spectra was used to process and analyze the raw mass spectral data. RESULTS: Coupled with the biomarker enrichment protocol, the high-resolution MALDI O-TOF mass spectra provided informative, reproducible peptide signatures. The raw mass spectra were analyzed and used to build discriminant disease models that were challenged with blinded samples for classification. CONCLUSIONS: Carrier-protein enrichment of disease biomarkers coupled with high-resolution mass spectrometry and discriminant pattern analysis is a powerful technology for diagnostics and population screening. The mass fingerprint model successfully classified blinded AD patient and control samples with high sensitivity and specificity.
JF  - Clinical Chemistry
AU  - Lopez, Mary F
AU  - Mikulskis, Alvydas
AU  - Kuzdzal, Scott
AU  - Bennett, David A
AU  - Kelly, Jeremiah
AU  - Golenko, Eva
AU  - DiCesare, Joseph
AU  - Denoyer, Eric
AU  - Patton, Wayne F
AU  - Ediger, Richard
AU  - Sapp, Lisa
AU  - Ziegert, Tillmann
AU  - Lynch, Christopher
AU  - Kramer, Susan
AU  - Whiteley, Gordon R
AU  - Wall, Michael R
AU  - Mannion, David P
AU  - della Cioppa, Guy
AU  - Rakitan, John S
AU  - Wolfe, Gershon M
AD  - PerkinElmer Life and Analytical Sciences, Boston, MA. PerkinElmer Life and Analytical Sciences, Shelton, CT. Rush Alzheimer's Disease Center, Rush University Medical Center, Chicago, IL. PerkinElmer Life and Analytical Sciences, Beaconsfield, Bucks, United Kingdom. Clinical Proteomics Reference Laboratory, SAIC-Frederick, Inc., NCI Frederick, Gaithersburg, MD. Predictive Diagnostics, Inc., Vacaville, CA
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 1946
EP  - 1954
PB  - American Association for Clinical Chemistry, Inc.
VL  - 51
IS  - 10
SN  - 0009-9147, 0009-9147
KW  - man
KW  - Biotechnology and Bioengineering Abstracts; Genetics Abstracts; Bioengineering Abstracts
KW  - Alzheimer's disease
KW  - Statistical analysis
KW  - biomarkers
KW  - Blood
KW  - proteomics
KW  - Bioinformatics
KW  - W4 130:General Biomedical Engineering: Tools & Techniques
KW  - G 07433:Miscellaneous
KW  - W 30965:Miscellaneous, Reviews
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17385924?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Clinical+Chemistry&rft.atitle=High-Resolution+Serum+Proteomic+Profiling+of+Alzheimer+Disease+Samples+Reveals+Disease-Specific%2C+Carrier-Protein-Bound+Mass+Signatures&rft.au=Lopez%2C+Mary+F%3BMikulskis%2C+Alvydas%3BKuzdzal%2C+Scott%3BBennett%2C+David+A%3BKelly%2C+Jeremiah%3BGolenko%2C+Eva%3BDiCesare%2C+Joseph%3BDenoyer%2C+Eric%3BPatton%2C+Wayne+F%3BEdiger%2C+Richard%3BSapp%2C+Lisa%3BZiegert%2C+Tillmann%3BLynch%2C+Christopher%3BKramer%2C+Susan%3BWhiteley%2C+Gordon+R%3BWall%2C+Michael+R%3BMannion%2C+David+P%3Bdella+Cioppa%2C+Guy%3BRakitan%2C+John+S%3BWolfe%2C+Gershon+M&rft.aulast=Lopez&rft.aufirst=Mary&rft.date=2005-10-01&rft.volume=51&rft.issue=10&rft.spage=1946&rft.isbn=&rft.btitle=&rft.title=Clinical+Chemistry&rft.issn=00099147&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-07-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - Alzheimer's disease; biomarkers; Blood; Statistical analysis; Bioinformatics; proteomics
ER  - 



TY  - JOUR
T1  - A live-cell assay to detect antigen-specific CD4 super(+) T cells with diverse cytokine profiles
AN  - 17238807; 6986618
AB  - Recently activated, but not resting, CD4 super(+) T cells express CD154, providing costimulatory signals to B cells and antigen-presenting cells (APCs). Therefore, de novo CD154 expression after stimulation identifies antigen- specific CD4 super(+) T cells. Previous assays were limited by the transient nature of surface CD154 expression; we overcame this by including fluorescently conjugated CD154-specific antibody during stimulation. Our assay is fully compatible with intracellular cytokine staining, and can be used for stimulations as long as 24 h. Notably, it is nonlethal, providing a means to purify viable antigen-specific CD4 super(+) T cells for further analysis. Using this assay, we found that stimulated cells expressing tumor necrosis factor (TNF)- [alpha], interleukin (IL)-2 or interferon (IFN)-[gamma] were predominantly CD154 super(+). Furthermore, some cells expressing none of these cytokines also expressed CD154, suggesting that CD154 marks cells with other effector functions. For vaccine- or pathogen-specific responses, we found substantial heterogeneity in expression of CD154 and cytokines, suggesting previously unrecognized diversity in abilities of responding cells to stimulate APCs through CD40.
JF  - Nature Medicine
AU  - Chattopadhyay, Pratip K
AU  - Yu, Joanne
AU  - Roederer, Mario
AD  - ImmunoTechnology Section, Vaccine Research Center, National Institute of Allergy and Infectious Disease, National Institutes of Health, 40 Convent Drive, Room 5509, Bethesda, Maryland 20892, USA., roederer@nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 1113
EP  - 1117
PB  - Nature Publishing Group, The Macmillan Building 4 Crinan Street London N1 9XW UK, [mailto:feedback@nature.com], [URL:http://www.nature.com/]
VL  - 11
IS  - 10
SN  - 1078-8956, 1078-8956
KW  - Biotechnology and Bioengineering Abstracts; Immunology Abstracts; Medical and Pharmaceutical Biotechnology Abstracts
KW  - Interleukins
KW  - CD4 antigen
KW  - adenomatous polyposis coli
KW  - Lymphocytes T
KW  - Cytokines
KW  - Antigen-presenting cells
KW  - CD40 antigen
KW  - CD154 antigen
KW  - g-Interferon
KW  - Lymphocytes B
KW  - Tumor necrosis factor-a
KW  - Effector cells
KW  - Antibodies
KW  - ^g-Interferon
KW  - Tumor necrosis factor-^a
KW  - W3 33240:Immunology
KW  - F 06704:Immunoassays
KW  - W 30965:Miscellaneous, Reviews
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17238807?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Nature+Medicine&rft.atitle=A+live-cell+assay+to+detect+antigen-specific+CD4+super%28%2B%29+T+cells+with+diverse+cytokine+profiles&rft.au=Chattopadhyay%2C+Pratip+K%3BYu%2C+Joanne%3BRoederer%2C+Mario&rft.aulast=Chattopadhyay&rft.aufirst=Pratip&rft.date=2005-10-01&rft.volume=11&rft.issue=10&rft.spage=1113&rft.isbn=&rft.btitle=&rft.title=Nature+Medicine&rft.issn=10788956&rft_id=info:doi/10.1038%2Fnm1293
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-09-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - CD154 antigen; CD40 antigen; CD4 antigen; Lymphocytes T; adenomatous polyposis coli; Effector cells; Antigen-presenting cells; Cytokines; Antibodies; Lymphocytes B; g-Interferon; Interleukins; Tumor necrosis factor-a; ^g-Interferon; Tumor necrosis factor-^a
DO  - http://dx.doi.org/10.1038/nm1293
ER  - 



TY  - JOUR
T1  - Carbohydrate-binding molecules inhibit viral fusion and entry by crosslinking membrane glycoproteins
AN  - 17082812; 6709216
AB  - Defensins are peptides that protect the host against microorganisms. Here we show that the theta-defensin retrocyclin 2 (RC2) inhibited influenza virus infection by blocking membrane fusion mediated by the viral hemagglutinin. RC2 was effective even after hemagglutinin attained a fusogenic conformation or had induced membrane hemifusion. RC2, a multivalent lectin, prevented hemagglutinin- mediated fusion by erecting a network of crosslinked and immobilized surface glycoproteins. RC2 also inhibited fusion mediated by Sindbis virus and baculovirus. Human beta-defensin 3 and mannan-binding lectin also blocked viral fusion by creating a protective barricade of immobilized surface proteins. This general mechanism might explain the broad-spectrum antiviral activity of many multivalent lectins of the innate immune system.
JF  - Nature Immunology
AU  - Leikina, Eugenia
AU  - Delanoe-Ayari, Helene
AU  - Melikov, Kamran
AU  - Cho, Myoung-Soon
AU  - Chen, Andrew
AU  - Waring, Alan J
AU  - Wang, Wei
AU  - Xie, Yongming
AU  - Loo, Joseph A
AU  - Lehrer, Robert I
AU  - Chernomordik, Leonid V
AD  - Section on Membrane Biology, Laboratory of Cellular and Molecular Biophysics, National Institute of Child Health and Human Development, Bethesda, Maryland 20892-1855, USA., chernoml@mail.nih.gov
Y1  - 2005/10//
PY  - 2005
DA  - Oct 2005
SP  - 995
EP  - 1001
PB  - Nature Publishing Group, The Macmillan Building 4 Crinan Street London N1 9XW UK, [mailto:feedback@nature.com], [URL:http://www.nature.com/]
VL  - 6
IS  - 10
SN  - 1529-2908, 1529-2908
KW  - Microbiology Abstracts A: Industrial & Applied Microbiology; Immunology Abstracts; Virology & AIDS Abstracts
KW  - Membrane fusion
KW  - Immune system
KW  - Hemagglutinins
KW  - Antiviral activity
KW  - Infection
KW  - Influenza
KW  - Mannose-binding lectin
KW  - Defensins
KW  - Influenza virus
KW  - Sindbis virus
KW  - Microorganisms
KW  - mannose-binding lectin
KW  - Glycoproteins
KW  - Baculovirus
KW  - Membrane glycoproteins
KW  - Conformation
KW  - A 01340:Antibiotics & Antimicrobials
KW  - V 22094:Hemagglutinin & neuraminidase
KW  - V 22042:Adsorption, penetration & uncoating
KW  - F 06104:Virus
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Amicrobiologya&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Nature+Immunology&rft.atitle=Carbohydrate-binding+molecules+inhibit+viral+fusion+and+entry+by+crosslinking+membrane+glycoproteins&rft.au=Leikina%2C+Eugenia%3BDelanoe-Ayari%2C+Helene%3BMelikov%2C+Kamran%3BCho%2C+Myoung-Soon%3BChen%2C+Andrew%3BWaring%2C+Alan+J%3BWang%2C+Wei%3BXie%2C+Yongming%3BLoo%2C+Joseph+A%3BLehrer%2C+Robert+I%3BChernomordik%2C+Leonid+V&rft.aulast=Leikina&rft.aufirst=Eugenia&rft.date=2005-10-01&rft.volume=6&rft.issue=10&rft.spage=995&rft.isbn=&rft.btitle=&rft.title=Nature+Immunology&rft.issn=15292908&rft_id=info:doi/10.1038%2Fni1248
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-04-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Membrane fusion; Hemagglutinins; Immune system; Infection; Antiviral activity; Influenza; Mannose-binding lectin; Defensins; Microorganisms; mannose-binding lectin; Glycoproteins; Membrane glycoproteins; Conformation; Influenza virus; Sindbis virus; Baculovirus
DO  - http://dx.doi.org/10.1038/ni1248
ER  - 



TY  - JOUR
T1  - Induction of transplantation tolerance in non-human primate preclinical models.
AN  - 68565719; 16147537
AB  - Short-term outcomes following organ transplantation have improved considerably since the availability of cyclosporine ushered in the modern era of immunosuppression. In spite of this, many of the current limitations to progress in the field are directly related to the existing practice of relatively non-specific immunosuppression. These include increased risks of opportunistic infection and cancer, and toxicity associated with long-term immunosuppressive drug exposure. In addition, long-term graft loss continues to result in part from a failure to adequately control the anti-donor immune response. The development of a safe and reliable means of inducing tolerance would ameliorate these issues and improve the lives of transplant recipients, yet given the improving clinical standard of care, the translation of new therapies has become appropriately more cautious and dependent on increasingly predictive preclinical models. While convenient and easy to use, rodent tolerance models have not to date been reliably capable of predicting a therapy's potential efficacy in humans. Non-human primates possess an immune system that more closely approximates that found in humans, and have served as a more rigorous preclinical testing ground for novel therapies. Prior to clinical adaptation therefore, tolerance regimens should be vetted in non-human primates to ensure that there is sufficient potential for efficacy to justify the risk of its application.
JF  - Philosophical transactions of the Royal Society of London. Series B, Biological sciences
AU  - Hale, Douglas A
AU  - Dhanireddy, Kiran
AU  - Bruno, David
AU  - Kirk, Allan D
AD  - Digestive and Kidney Diseases, National Institute of Diabetes, NIH, Transplantation Branch, Bethesda, MD 20892, USA. douglash@intra.niddk.nih.gov
Y1  - 2005/09/29/
PY  - 2005
DA  - 2005 Sep 29
SP  - 1723
EP  - 1737
VL  - 360
IS  - 1461
SN  - 0962-8436, 0962-8436
KW  - Antibodies, Monoclonal
KW  - 0
KW  - Antilymphocyte Serum
KW  - Index Medicus
KW  - Animals
KW  - Transplantation Chimera -- immunology
KW  - Primates
KW  - Antilymphocyte Serum -- therapeutic use
KW  - Antibodies, Monoclonal -- therapeutic use
KW  - Transplantation Tolerance -- immunology
KW  - Models, Animal
KW  - Models, Immunological
KW  - Signal Transduction -- immunology
KW  - Immunosuppression -- methods
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68565719?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Philosophical+transactions+of+the+Royal+Society+of+London.+Series+B%2C+Biological+sciences&rft.atitle=Induction+of+transplantation+tolerance+in+non-human+primate+preclinical+models.&rft.au=Hale%2C+Douglas+A%3BDhanireddy%2C+Kiran%3BBruno%2C+David%3BKirk%2C+Allan+D&rft.aulast=Hale&rft.aufirst=Douglas&rft.date=2005-09-29&rft.volume=360&rft.issue=1461&rft.spage=1723&rft.isbn=&rft.btitle=&rft.title=Philosophical+transactions+of+the+Royal+Society+of+London.+Series+B%2C+Biological+sciences&rft.issn=09628436&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-06
N1  - Date created - 2005-09-08
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Am J Transplant. 2004 Sep;4(9):1391-8 [15307826]
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Transplantation. 1971 Sep;12(3):202-10 [4105459]
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JPEN J Parenter Enteral Nutr. 1998 May-Jun;22(3):152-5 [9586793]
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Nat Med. 1999 Nov;5(11):1303-7 [10545998]
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J Immunol. 2000 Jan 1;164(1):512-21 [10605049]
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N Engl J Med. 2000 Mar 2;342(9):605-12 [10699159]
J Exp Med. 2000 Feb 21;191(4):651-60 [10684857]
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J Rheumatol. 2001 Jan;28(1):95-101 [11196549]
Transplant Proc. 2001 Feb-Mar;33(1-2):116-7 [11266735]
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Philos Trans R Soc Lond B Biol Sci. 2001 May 29;356(1409):681-9 [11375071]
Immunol Res. 2001;23(2-3):253-62 [11444390]
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J Immunol. 2001 Aug 15;167(4):1945-53 [11489974]
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Transplantation. 2001 Nov 15;72(9):1473-8 [11707732]
Immunol Rev. 2001 Oct;183:214-22 [11782259]
Immunol Rev. 2001 Oct;183:223-33 [11782260]
J Immunol. 2002 Feb 1;168(3):1123-30 [11801646]
Diabetes. 2002 Feb;51(2):265-70 [11812731]
Transplantation. 2002 Mar 27;73(6):862-6 [11923684]
Transplantation. 2002 Jun 15;73(11):1757-64 [12084998]
Am J Transplant. 2002 Apr;2(4):381-5 [12118862]
Am J Transplant. 2002 Sep;2(8):745-57 [12243495]
Transplantation. 2002 Oct 15;74(7):933-40 [12394833]
Transplantation. 2002 Nov 27;74(10):1365-9 [12451232]
Transplantation. 2002 Nov 27;74(10):1405-9 [12451240]
J Immunol. 2003 Mar 1;170(5):2776-82 [12594309]
Am J Transplant. 2003 Jun;3(6):722-30 [12780564]
J Clin Invest. 2003 Jun;111(12):1887-95 [12813024]
Transplantation. 2003 Jun 27;75(12):2106-13 [12829920]
Transplantation. 2003 Jul 15;76(1):120-9 [12865797]
Transplantation. 2003 Aug 15;76(3):524-30 [12923438]
Am J Transplant. 2003 Nov;3(11):1350-4 [14525594]
Transpl Immunol. 2003 Oct-Nov;12(1):41-8 [14551031]
Transplant Proc. 2003 Nov;35(7):2477-8 [14611990]
Immunol Rev. 2003 Dec;196:147-60 [14617203]
Immunol Rev. 2003 Dec;196:176-96 [14617205]
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Transplantation. 2004 Feb 15;77(3):460-2 [14966427]
Transplantation. 2004 Mar 27;77(6):936-9 [15077042]
J Immunol. 2004 May 1;172(9):5753-64 [15100322]
Transplantation. 1999 Jan 15;67(1):18-30 [9921791]
J Am Soc Nephrol. 1999 Feb;10(2):374-81 [10215338]
Transplant Proc. 1999 Feb-Mar;31(1-2):680 [10083292]
Transplant Proc. 1999 May;31(3B Suppl):27S-28S [10330966]
Nat Med. 1999 Jun;5(6):686-93 [10371508]
Diabetes. 1999 Jul;48(7):1473-81 [10389857]
Proc Natl Acad Sci U S A. 1999 Jul 6;96(14):8132-7 [10393960]
Transplantation. 1999 Aug 27;68(4):459-67 [10480398]
Am J Transplant. 2005 May;5(5):1032-41 [15816883]
Transplantation. 2005 Oct 27;80(8):1051-9 [16278585]
Transplant Proc. 2003 Dec;35(8):3156-9 [14698002]
Transplant Proc. 1997 Sep;29(6):2546-7 [9290735]
Transplant Proc. 1979 Mar;11(1):923-7 [109974]
Transplantation. 1979 Oct;28(4):347-50 [116401]
Surg Forum. 1979;30:282-3 [120017]
Transplantation. 1980 May;29(5):401-4 [6769184]
Transplantation. 1980 May;29(5):405-8 [6769185]
Transplant Proc. 1981 Mar;13(1 Pt 1):434-8 [7022867]
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Transplantation. 1983 Jul;36(1):104-6 [6346606]
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Ann Surg. 1983 Sep;198(3):370-8 [6351775]
J Immunol. 1984 Feb;132(2):1019-25 [6228586]
J Immunol. 1986 Aug 15;137(4):1127-32 [3090139]
Transplantation. 1989 Feb;47(2):209-15 [2645699]
Immunol Today. 1988 Jan;9(1):23-7 [3076756]
Transplantation. 1989 Nov;48(5):732-41 [2573179]
Surgery. 1990 Aug;108(2):406-13; discussion 413-4 [2382234]
Science. 1990 Sep 14;249(4974):1293-5 [2119056]
Transplantation. 1991 Jan;51(1):198-207 [1824804]
Crit Rev Immunol. 1990;10(2):113-30 [1981679]
Semin Immunol. 1990 Nov;2(6):401-17 [2104278]
Proc Natl Acad Sci U S A. 1992 Apr 1;89(7):2585-9 [1372981]
Science. 1992 Aug 7;257(5071):789-92 [1323143]
Ann Surg. 1992 Oct;216(4):409-14; discussion 414-6 [1417190]
Immunol Res. 1993;12(1):48-64 [8099942]
Proc Natl Acad Sci U S A. 1993 Jul 15;90(14):6586-90 [7688125]
Ann Surg. 1993 Oct;218(4):492-501; discussion 501-3 [8215640]
Br J Surg. 1993 Nov;80(11):1389-92 [8252344]
Transplantation. 1994 Jan;57(1):101-15 [8291095]
Transplantation. 1994 Mar 27;57(6):788-93 [7908767]
Transplantation. 1994 Apr 15;57(7):1103-10 [8165709]
Transplantation. 1994 Jul 27;58(2):261-4 [7913778]
Immunol Today. 1994 Jul;15(7):321-31 [7522010]
Transplantation. 1995 Jan 27;59(2):256-62 [7839449]
Transplantation. 1995 Jul 15;60(1):71-6 [7624946]
Proc Natl Acad Sci U S A. 1995 Oct 10;92(21):9560-4 [7568172]
J Urol. 1995 Dec;154(6):2197-202 [7500488]
Transplantation. 1995 Nov 27;60(10):1171-8 [7482727]
Nature. 1996 May 30;381(6581):434-8 [8632801]
Transplantation. 1996 Jul 15;62(1):117-22 [8693525]
Exp Clin Endocrinol Diabetes. 1995;103 Suppl 2:129-32 [8839269]
Immunogenetics. 1997;45(3):171-9 [8995183]
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Transplant Proc. 1997 Sep;29(6):2624-5 [9290767]
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Transplantation. 1997 Oct 27;64(8):1181-7 [9355837]
Tissue Antigens. 1997 Dec;50(6):657-61 [9458122]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Involvement of poly(ADP-ribose) polymerase activity in regulating Chk1-dependent apoptotic cell death.
AN  - 68592903; 16002346
AB  - The activity of poly(ADP-ribose) polymerase (PARP) is highly stimulated following DNA damage resulting in formation of DNA nicks and strand breaks. This leads to modification of numerous proteins, including itself, using NAD(+) as substrate and to exhaustion of intracellular ATP. A highly cytotoxic concentration of the DNA methylating agent methyl methanesulfonate (MMS) results in cellular ATP depletion and cell death primarily by necrosis in both wild-type and DNA polymerase beta null mouse fibroblasts. The loss of ATP can be prevented by the PARP inhibitor 4-amino-1,8-naphthalimide (4-AN), and now cells die by an energy-dependent apoptotic pathway. We find that inhibition of PARP activity transforms a sub-lethal exposure to MMS into a highly cytotoxic event. Under this condition, ATP is not depleted and cell death is by apoptosis. The caspase inhibitor, Z-VAD, shifts the mechanism of cell death to necrosis indicating a caspase-dependent component of the apoptotic cell death. Co-exposure to the Chk1 inhibitor UCN-01 also produces a decrease in apoptotic cell death, but now there is an increase in viable cells and an enhancement in long-term survival. Taken together, our results suggest that inhibition of PARP activity, induced as a result of low dose MMS exposure, signals via a Chk1-dependent pathway for cell death by apoptosis.
JF  - DNA repair
AU  - Horton, Julie K
AU  - Stefanick, Donna F
AU  - Wilson, Samuel H
AD  - Laboratory of Structural Biology, National Institute of Environmental Health Sciences, National Institutes of Health, Research Triangle Park, NC 27709, USA.
Y1  - 2005/09/28/
PY  - 2005
DA  - 2005 Sep 28
SP  - 1111
EP  - 1120
VL  - 4
IS  - 10
SN  - 1568-7864, 1568-7864
KW  - Amino Acid Chloromethyl Ketones
KW  - 0
KW  - Caspase Inhibitors
KW  - Poly(ADP-ribose) Polymerase Inhibitors
KW  - benzyloxycarbonylvalyl-alanyl-aspartyl fluoromethyl ketone
KW  - Adenosine Triphosphate
KW  - 8L70Q75FXE
KW  - DNA
KW  - 9007-49-2
KW  - Methyl Methanesulfonate
KW  - AT5C31J09G
KW  - Poly(ADP-ribose) Polymerases
KW  - EC 2.4.2.30
KW  - Protein Kinases
KW  - EC 2.7.-
KW  - Checkpoint Kinase 1
KW  - EC 2.7.11.1
KW  - Chek1 protein, mouse
KW  - Index Medicus
KW  - Animals
KW  - Fibroblasts -- drug effects
KW  - Fibroblasts -- enzymology
KW  - Mice
KW  - DNA -- drug effects
KW  - Necrosis
KW  - Methyl Methanesulfonate -- toxicity
KW  - Cells, Cultured
KW  - Adenosine Triphosphate -- metabolism
KW  - Amino Acid Chloromethyl Ketones -- pharmacology
KW  - Mutation
KW  - Protein Kinases -- metabolism
KW  - Poly(ADP-ribose) Polymerases -- genetics
KW  - Apoptosis
KW  - Poly(ADP-ribose) Polymerases -- metabolism
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68592903?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=DNA+repair&rft.atitle=Involvement+of+poly%28ADP-ribose%29+polymerase+activity+in+regulating+Chk1-dependent+apoptotic+cell+death.&rft.au=Horton%2C+Julie+K%3BStefanick%2C+Donna+F%3BWilson%2C+Samuel+H&rft.aulast=Horton&rft.aufirst=Julie&rft.date=2005-09-28&rft.volume=4&rft.issue=10&rft.spage=1111&rft.isbn=&rft.btitle=&rft.title=DNA+repair&rft.issn=15687864&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-04
N1  - Date created - 2005-09-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - REV1 mediated mutagenesis in base excision repair deficient mouse fibroblast.
AN  - 68592824; 15950550
AB  - The DNA polymerase beta (Pol beta) null background renders mouse embryonic fibroblast (MEF) cells base excision repair deficient and hyper-mutagenic upon treatment with the monofunctional alkylating agent, methyl methanesulfonate (MMS). This effect involves an increase in all types of base substitutions, with a modest predominance of G to A transitions. In the present study, we examined the hypothesis that the MMS-induced mutagenesis in the Pol beta null MEF system is due to a lesion bypass mechanism. We studied the effect of RNAi mediated down-regulation of the lesion bypass factor REV1. The steady-state level of REV1 protein was reduced by more than 95% using stable expression of a siRNA construct in a Pol beta null cell line. We found that REV1 expression is required for the MMS-induced mutagenesis phenotype of Pol beta null MEF cells. In contrast, cell survival after MMS treatment is not reduced in the absence of REV1.
JF  - DNA repair
AU  - Poltoratsky, Vladimir
AU  - Horton, Julie K
AU  - Prasad, Rajendra
AU  - Wilson, Samuel H
AD  - Laboratory of Structural Biology, NIEHS, National Institutes of Health, Research Triangle Park, NC 27709, USA.
Y1  - 2005/09/28/
PY  - 2005
DA  - 2005 Sep 28
SP  - 1182
EP  - 1188
VL  - 4
IS  - 10
SN  - 1568-7864, 1568-7864
KW  - RNA, Small Interfering
KW  - 0
KW  - Methyl Methanesulfonate
KW  - AT5C31J09G
KW  - DNA Polymerase beta
KW  - EC 2.7.7.-
KW  - Nucleotidyltransferases
KW  - Rev1l protein, mouse
KW  - Index Medicus
KW  - Fibroblasts -- drug effects
KW  - Animals
KW  - Methyl Methanesulfonate -- toxicity
KW  - Down-Regulation
KW  - RNA, Small Interfering -- genetics
KW  - Mice
KW  - Mutation
KW  - Fibroblasts -- metabolism
KW  - DNA Repair -- genetics
KW  - Nucleotidyltransferases -- metabolism
KW  - Nucleotidyltransferases -- genetics
KW  - DNA Polymerase beta -- genetics
KW  - Mutagenesis
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68592824?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=DNA+repair&rft.atitle=REV1+mediated+mutagenesis+in+base+excision+repair+deficient+mouse+fibroblast.&rft.au=Poltoratsky%2C+Vladimir%3BHorton%2C+Julie+K%3BPrasad%2C+Rajendra%3BWilson%2C+Samuel+H&rft.aulast=Poltoratsky&rft.aufirst=Vladimir&rft.date=2005-09-28&rft.volume=4&rft.issue=10&rft.spage=1182&rft.isbn=&rft.btitle=&rft.title=DNA+repair&rft.issn=15687864&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-01-04
N1  - Date created - 2005-09-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Probing Specific Lipid-Protein Interaction by Saturation Transfer Difference NMR Spectroscopy
AN  - 17421563; 6538465
AB  - We studied the interaction of mono- and polyunsaturated phosphatidylcholines with rhodopsin by super(1)H NMR saturation transfer difference spectroscopy with magic angle spinning (STD-MAS NMR). The results indicate a strong preference for interaction of rhodopsin with the polyunsaturated docosahexaenoic acid.
JF  - Journal of the American Chemical Society
AU  - Soubias, O
AU  - Gawrisch, K
AD  - Laboratory of Membrane Biochemistry and Biophysics, NIAAA, National Institutes of Health, Bethesda, Maryland 20892, USA, gawrisch@helix.nih.gov
Y1  - 2005/09/28/
PY  - 2005
DA  - 2005 Sep 28
SP  - 13110
EP  - 13111
VL  - 127
IS  - 38
SN  - 1272-7863, 1272-7863
KW  - phosphatidylcholines
KW  - Biotechnology and Bioengineering Abstracts; Bioengineering Abstracts
KW  - Docosahexaenoic acid
KW  - Rhodopsin
KW  - Lipids
KW  - Magnetic resonance spectroscopy
KW  - Lecithin
KW  - Proteins
KW  - N.M.R.
KW  - Spectroscopy
KW  - Spinning
KW  - W4 150:Medical Imaging
KW  - W 30965:Miscellaneous, Reviews
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/17421563?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Abiotechresearch&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+the+American+Chemical+Society&rft.atitle=Probing+Specific+Lipid-Protein+Interaction+by+Saturation+Transfer+Difference+NMR+Spectroscopy&rft.au=Soubias%2C+O%3BGawrisch%2C+K&rft.aulast=Soubias&rft.aufirst=O&rft.date=2005-09-28&rft.volume=127&rft.issue=38&rft.spage=13110&rft.isbn=&rft.btitle=&rft.title=Journal+of+the+American+Chemical+Society&rft.issn=12727863&rft_id=info:doi/10.1021%2Fja0538942
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-03-01
N1  - Last updated - 2011-12-13
N1  - SubjectsTermNotLitGenreText - N.M.R.; Rhodopsin; Spinning; Lecithin; Spectroscopy; Docosahexaenoic acid; Magnetic resonance spectroscopy; Lipids; Proteins
DO  - http://dx.doi.org/10.1021/ja0538942
ER  - 



TY  - JOUR
T1  - LRP 1 B functions as a receptor for Pseudomonas exotoxin.
AN  - 68621362; 16095885
AB  - Pseudomonas aeruginosa is an opportunistic pathogen that produces several virulence factors, among them Pseudomonas Exotoxin A (PE). Previously, low-density lipoprotein receptor-related protein 1 (LRP 1) was shown to be the primary receptor for PE. In this report, we show that a close family member, LRP 1B, can also function as a receptor.
JF  - Biochimica et biophysica acta
AU  - Pastrana, Diana V
AU  - Hanson, Alison J
AU  - Knisely, Jane
AU  - Bu, Guojun
AU  - Fitzgerald, David J
AD  - Laboratory of Molecular Biology, CCR, National Cancer Institute, Bethesda, MD 20892-4263, USA.
Y1  - 2005/09/25/
PY  - 2005
DA  - 2005 Sep 25
SP  - 234
EP  - 239
VL  - 1741
IS  - 3
SN  - 0006-3002, 0006-3002
KW  - Bacterial Proteins
KW  - 0
KW  - LRP1B protein, human
KW  - Membranes, Artificial
KW  - Polyvinyls
KW  - Protein Synthesis Inhibitors
KW  - Receptors, LDL
KW  - pseudomonas exoprotein A protein, Pseudomonas aeruginosa
KW  - polyvinylidene fluoride
KW  - 24937-79-9
KW  - Index Medicus
KW  - Animals
KW  - Gene Transfer Techniques
KW  - Cricetulus
KW  - Electrophoresis, Polyacrylamide Gel
KW  - Protein Binding -- drug effects
KW  - Toxicity Tests
KW  - Mutation -- genetics
KW  - CHO Cells
KW  - Cricetinae
KW  - Bacterial Proteins -- toxicity
KW  - Protein Synthesis Inhibitors -- metabolism
KW  - Protein Synthesis Inhibitors -- toxicity
KW  - Bacterial Proteins -- genetics
KW  - Bacterial Proteins -- metabolism
KW  - Receptors, LDL -- metabolism
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/68621362?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Biochimica+et+biophysica+acta&rft.atitle=LRP+1+B+functions+as+a+receptor+for+Pseudomonas+exotoxin.&rft.au=Pastrana%2C+Diana+V%3BHanson%2C+Alison+J%3BKnisely%2C+Jane%3BBu%2C+Guojun%3BFitzgerald%2C+David+J&rft.aulast=Pastrana&rft.aufirst=Diana&rft.date=2005-09-25&rft.volume=1741&rft.issue=3&rft.spage=234&rft.isbn=&rft.btitle=&rft.title=Biochimica+et+biophysica+acta&rft.issn=00063002&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-03-13
N1  - Date created - 2005-09-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Age and Results of Treatment of Atypical Glandular Cells
T2  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AN  - 39804247; 3987527
JF  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AU  - Figueiredo, E.M.A.
AU  - Giorgi, R
AU  - Magalhaes, C.M.G.
AU  - Moralez, G M
Y1  - 2005/09/25/
PY  - 2005
DA  - 2005 Sep 25
KW  - Oncology
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39804247?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=14th+International+Meeting+of+the+European+Society+of+Gynaecological+Oncology+%28ESGO+14%29&rft.atitle=Age+and+Results+of+Treatment+of+Atypical+Glandular+Cells&rft.au=Figueiredo%2C+E.M.A.%3BGiorgi%2C+R%3BMagalhaes%2C+C.M.G.%3BMoralez%2C+G+M&rft.aulast=Figueiredo&rft.aufirst=E.M.A.&rft.date=2005-09-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=14th+International+Meeting+of+the+European+Society+of+Gynaecological+Oncology+%28ESGO+14%29&rft.issn=&rft_id=info:doi/
L2  - http://www.kenes.com/esgo14prog/program/SessionIndex.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Gynecology Oncology Subspecialty Training in Brazil
T2  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AN  - 39742215; 3987594
JF  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AU  - Figueiredo, E.M.A.
AU  - Koch, H A
AU  - Moralez, G M
Y1  - 2005/09/25/
PY  - 2005
DA  - 2005 Sep 25
KW  - Brazil
KW  - Gynecology
KW  - Oncology
KW  - Training
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39742215?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=14th+International+Meeting+of+the+European+Society+of+Gynaecological+Oncology+%28ESGO+14%29&rft.atitle=Gynecology+Oncology+Subspecialty+Training+in+Brazil&rft.au=Figueiredo%2C+E.M.A.%3BKoch%2C+H+A%3BMoralez%2C+G+M&rft.aulast=Figueiredo&rft.aufirst=E.M.A.&rft.date=2005-09-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=14th+International+Meeting+of+the+European+Society+of+Gynaecological+Oncology+%28ESGO+14%29&rft.issn=&rft_id=info:doi/
L2  - http://www.kenes.com/esgo14prog/program/SessionIndex.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - En Block Laparoscopic Pelvic and Aortic Lymphadenectomy in Gynaecologic oncology: Experience with 90 Patients
T2  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AN  - 39694315; 3987833
JF  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AU  - Vizza, E
AU  - Corrado, G
AU  - Diotallevi, F
AU  - Vincenzoni, C
AU  - Grasso, M
AU  - Costaggini, I
AU  - Sbiroli, C
Y1  - 2005/09/25/
PY  - 2005
DA  - 2005 Sep 25
KW  - Laparoscopy
KW  - Oncology
KW  - Pelvis
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39694315?accountid=14244
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L2  - http://www.kenes.com/esgo14prog/program/SessionIndex.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Piver II Versus Piver III Nerve Sparing Radical Hysterectomy: Comparison of Lower Urinary Tract Dysfunctions and Morbidity
T2  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AN  - 39671908; 3987378
JF  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AU  - Raspagliesi, F
AU  - Ditto, A
AU  - Fontanelli, R
AU  - Hanozet, F
AU  - Zanaboni, F
AU  - Solima, E
AU  - Spatti, G
AU  - Vecchione, F
AU  - Rossi, G
AU  - Kusamura, S
Y1  - 2005/09/25/
PY  - 2005
DA  - 2005 Sep 25
KW  - Urine
KW  - Urinary tract
KW  - Morbidity
KW  - Nerves
KW  - Radicals
KW  - Hysterectomy
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39671908?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=14th+International+Meeting+of+the+European+Society+of+Gynaecological+Oncology+%28ESGO+14%29&rft.atitle=Piver+II+Versus+Piver+III+Nerve+Sparing+Radical+Hysterectomy%3A+Comparison+of+Lower+Urinary+Tract+Dysfunctions+and+Morbidity&rft.au=Raspagliesi%2C+F%3BDitto%2C+A%3BFontanelli%2C+R%3BHanozet%2C+F%3BZanaboni%2C+F%3BSolima%2C+E%3BSpatti%2C+G%3BVecchione%2C+F%3BRossi%2C+G%3BKusamura%2C+S&rft.aulast=Raspagliesi&rft.aufirst=F&rft.date=2005-09-25&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=14th+International+Meeting+of+the+European+Society+of+Gynaecological+Oncology+%28ESGO+14%29&rft.issn=&rft_id=info:doi/
L2  - http://www.kenes.com/esgo14prog/program/SessionIndex.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Neoadjuvant Chemotherapy with Paclitaxel, Ifosfamide and Cisplatin in Locally Advanced Cervical Cancer: Phase Ii Trial
T2  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AN  - 39668547; 3987520
JF  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AU  - Raspagliesi, F
AU  - Zanaboni, F
AU  - Vecchione , F.
AU  - Ditto, A
AU  - Hanozet, F
AU  - Anghileri, C
AU  - Kusamura, S
Y1  - 2005/09/25/
PY  - 2005
DA  - 2005 Sep 25
KW  - Cervical cancer
KW  - Cisplatin
KW  - Ifosfamide
KW  - Paclitaxel
KW  - Chemotherapy
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39668547?accountid=14244
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L2  - http://www.kenes.com/esgo14prog/program/SessionIndex.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Sentinel Node Detection in Endometrial Cancer
T2  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AN  - 39667580; 3987741
JF  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AU  - Raspagliesi, F
AU  - Solima, E
AU  - Ditto, A
AU  - Hanozet, F
AU  - Vecchione, F
AU  - Anghileri, C
AU  - Kusamura, S
Y1  - 2005/09/25/
PY  - 2005
DA  - 2005 Sep 25
KW  - Cancer
KW  - Nodes
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39667580?accountid=14244
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L2  - http://www.kenes.com/esgo14prog/program/SessionIndex.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Photodynamic Therapy in Recurrent Vulvar Paget Disease: a Pilot Study
T2  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AN  - 39661434; 3987432
JF  - 14th International Meeting of the European Society of Gynaecological Oncology (ESGO 14)
AU  - Raspagliesi, F
AU  - Fontanelli, R
AU  - Di Naro, E
AU  - Ditto, A
AU  - Solima, E
AU  - Vecchione, F
AU  - Hanozet, F
AU  - Rossi, G
Y1  - 2005/09/25/
PY  - 2005
DA  - 2005 Sep 25
KW  - Photodynamic therapy
KW  - U 2000:Biological Sciences
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L2  - http://www.kenes.com/esgo14prog/program/SessionIndex.asp
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Mechanistic link between PKR dimerization, autophosphorylation, and eIF2alpha substrate recognition.
AN  - 68614337; 16179259
AB  - The antiviral protein kinase PKR inhibits protein synthesis by phosphorylating the translation initiation factor eIF2alpha on Ser51. Binding of double-stranded RNA to the regulatory domains of PKR promotes dimerization, autophosphorylation, and the functional activation of the kinase. Herein, we identify mutations that activate PKR in the absence of its regulatory domains and map the mutations to a recently identified dimerization surface on the kinase catalytic domain. Mutations of other residues on this surface block PKR autophosphorylation and eIF2alpha phosphorylation, while mutating Thr446, an autophosphorylation site within the catalytic-domain activation segment, impairs eIF2alpha phosphorylation and viral pseudosubstrate binding. Mutational analysis of catalytic-domain residues preferentially conserved in the eIF2alpha kinase family identifies helix alphaG as critical for the specific recognition of eIF2alpha. We propose an ordered mechanism of PKR activation in which catalytic-domain dimerization triggers Thr446 autophosphorylation and specific eIF2alpha substrate recognition.
JF  - Cell
AU  - Dey, Madhusudan
AU  - Cao, Chune
AU  - Dar, Arvin C
AU  - Tamura, Tomohiko
AU  - Ozato, Keiko
AU  - Sicheri, Frank
AU  - Dever, Thomas E
AD  - Laboratory of Gene Regulation and Development, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892, USA.
Y1  - 2005/09/23/
PY  - 2005
DA  - 2005 Sep 23
SP  - 901
EP  - 913
VL  - 122
IS  - 6
SN  - 0092-8674, 0092-8674
KW  - Eukaryotic Initiation Factor-2
KW  - 0
KW  - RNA, Double-Stranded
KW  - eIF-2 Kinase
KW  - EC 2.7.11.1
KW  - Index Medicus
KW  - Mutagenesis, Site-Directed
KW  - Protein Structure, Secondary
KW  - Saccharomyces cerevisiae -- metabolism
KW  - RNA, Double-Stranded -- chemistry
KW  - Phosphorylation
KW  - Dimerization
KW  - Protein Binding
KW  - RNA, Double-Stranded -- metabolism
KW  - Protein Conformation
KW  - Catalysis
KW  - eIF-2 Kinase -- metabolism
KW  - Eukaryotic Initiation Factor-2 -- metabolism
KW  - Eukaryotic Initiation Factor-2 -- genetics
KW  - eIF-2 Kinase -- genetics
KW  - Eukaryotic Initiation Factor-2 -- chemistry
KW  - eIF-2 Kinase -- chemistry
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cell&rft.atitle=Mechanistic+link+between+PKR+dimerization%2C+autophosphorylation%2C+and+eIF2alpha+substrate+recognition.&rft.au=Dey%2C+Madhusudan%3BCao%2C+Chune%3BDar%2C+Arvin+C%3BTamura%2C+Tomohiko%3BOzato%2C+Keiko%3BSicheri%2C+Frank%3BDever%2C+Thomas+E&rft.aulast=Dey&rft.aufirst=Madhusudan&rft.date=2005-09-23&rft.volume=122&rft.issue=6&rft.spage=901&rft.isbn=&rft.btitle=&rft.title=Cell&rft.issn=00928674&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-22
N1  - Date created - 2005-09-23
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Comment In:
Cell. 2005 Sep 23;122(6):823-5 [16179248]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Second cancers among 40,576 testicular cancer patients: focus on long-term survivors.
AN  - 68611677; 16174857
AB  - Although second primary cancers are a leading cause of death among men with testicular cancer, few studies have quantified risks among long-term survivors.
          Within 14 population-based tumor registries in Europe and North America (1943-2001), we identified 40,576 1-year survivors of testicular cancer and ascertained data on any new incident solid tumors among these patients. We used Poisson regression analysis to model relative risks (RRs) and excess absolute risks (EARs) of second solid cancers. All statistical tests were two-sided. A total of 2,285 second solid cancers were reported in the cohort. The relative risk and EAR decreased with increasing age at testicular cancer diagnosis (P < .001); the EAR increased with attained age (P < .001) but the excess RR decreased. Among 10-year survivors diagnosed with testicular cancer at age 35 years, the risk of developing a second solid tumor was increased (RR = 1.9, 95% confidence interval [CI] = 1.8 to 2.1). Risk remained statistically significantly elevated for 35 years (RR = 1.7, 95% CI = 1.5 to 2.0; P < .001). We observed statistically significantly elevated risks, for the first time, for cancers of the pleura (malignant mesothelioma; RR = 3.4, 95% CI = 1.7 to 5.9) and esophagus (RR = 1.7, 95% CI = 1.0 to 2.6). Cancers of the lung (RR = 1.5, 95% CI = 1.2 to 1.7), colon (RR = 2.0, 95% CI = 1.7 to 2.5), bladder (RR = 2.7, 95% CI = 2.2 to 3.1), pancreas (RR = 3.6, 95% CI = 2.8 to 4.6), and stomach (RR = 4.0, 95% CI = 3.2 to 4.8) accounted for almost 60% of the total excess. Overall patterns were similar for seminoma and nonseminoma patients, with lower risks observed for nonseminoma patients treated after 1975. Statistically significantly increased risks of solid cancers were observed among patients treated with radiotherapy alone (RR = 2.0, 95% CI = 1.9 to 2.2), chemotherapy alone (RR = 1.8, 95% CI = 1.3 to 2.5), and both (RR = 2.9, 95% CI = 1.9 to 4.2). For patients diagnosed with seminomas or nonseminomatous tumors at age 35 years, cumulative risks of solid cancer 40 years later (i.e., to age 75 years) were 36% and 31%, respectively, compared with 23% for the general population.
          Testicular cancer survivors are at statistically significantly increased risk of solid tumors for at least 35 years after treatment. Young patients may experience high levels of risk as they reach older ages. The statistically significantly increased risk of malignant mesothelioma in testicular cancer survivors has, to our knowledge, not been observed previously in a cohort of patients treated with radiotherapy.
JF  - Journal of the National Cancer Institute
AU  - Travis, Lois B
AU  - Fosså, Sophie D
AU  - Schonfeld, Sara J
AU  - McMaster, Mary L
AU  - Lynch, Charles F
AU  - Storm, Hans
AU  - Hall, Per
AU  - Holowaty, Eric
AU  - Andersen, Aage
AU  - Pukkala, Eero
AU  - Andersson, Michael
AU  - Kaijser, Magnus
AU  - Gospodarowicz, Mary
AU  - Joensuu, Timo
AU  - Cohen, Randi J
AU  - Boice, John D
AU  - Dores, Graça M
AU  - Gilbert, Ethel S
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA. travisl@mail.nih.gov
Y1  - 2005/09/21/
PY  - 2005
DA  - 2005 Sep 21
SP  - 1354
EP  - 1365
VL  - 97
IS  - 18
KW  - Antineoplastic Agents
KW  - 0
KW  - Index Medicus
KW  - Mesothelioma -- epidemiology
KW  - Odds Ratio
KW  - Urinary Bladder Neoplasms -- epidemiology
KW  - Humans
KW  - Pleural Neoplasms -- epidemiology
KW  - Aged
KW  - Poisson Distribution
KW  - Esophageal Neoplasms -- epidemiology
KW  - Antineoplastic Agents -- adverse effects
KW  - Risk Assessment
KW  - Lung Neoplasms -- epidemiology
KW  - North America -- epidemiology
KW  - Adult
KW  - Pancreatic Neoplasms -- epidemiology
KW  - Stomach Neoplasms -- epidemiology
KW  - Male
KW  - Kidney Neoplasms -- epidemiology
KW  - Europe -- epidemiology
KW  - Radiotherapy, Adjuvant -- adverse effects
KW  - Chemotherapy, Adjuvant -- adverse effects
KW  - Radiotherapy -- adverse effects
KW  - Registries
KW  - Colonic Neoplasms -- epidemiology
KW  - Incidence
KW  - Confidence Intervals
KW  - Middle Aged
KW  - Survivors -- statistics & numerical data
KW  - Testicular Neoplasms -- drug therapy
KW  - Testicular Neoplasms -- radiotherapy
KW  - Neoplasms, Second Primary -- epidemiology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Journal+of+the+National+Cancer+Institute&rft.atitle=Second+cancers+among+40%2C576+testicular+cancer+patients%3A+focus+on+long-term+survivors.&rft.au=Travis%2C+Lois+B%3BFoss%C3%A5%2C+Sophie+D%3BSchonfeld%2C+Sara+J%3BMcMaster%2C+Mary+L%3BLynch%2C+Charles+F%3BStorm%2C+Hans%3BHall%2C+Per%3BHolowaty%2C+Eric%3BAndersen%2C+Aage%3BPukkala%2C+Eero%3BAndersson%2C+Michael%3BKaijser%2C+Magnus%3BGospodarowicz%2C+Mary%3BJoensuu%2C+Timo%3BCohen%2C+Randi+J%3BBoice%2C+John+D%3BDores%2C+Gra%C3%A7a+M%3BGilbert%2C+Ethel+S&rft.aulast=Travis&rft.aufirst=Lois&rft.date=2005-09-21&rft.volume=97&rft.issue=18&rft.spage=1354&rft.isbn=&rft.btitle=&rft.title=Journal+of+the+National+Cancer+Institute&rft.issn=1460-2105&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-09-30
N1  - Date created - 2005-09-21
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Applied Proteomics in HCV/HIV co-infection: Differential Expression of Serum Proteins Prior to Treatment is Associated with Response to HCV Therapy in HIV Co-infected individuals.
T2  - 45th Interscience Conference on Antimicrobial Agents and Chemotherapy
AN  - 40078585; 3986993
JF  - 45th Interscience Conference on Antimicrobial Agents and Chemotherapy
AU  - Kottilil
Y1  - 2005/09/21/
PY  - 2005
DA  - 2005 Sep 21
KW  - Therapy
KW  - proteomics
KW  - Serum proteins
KW  - Hepatitis C virus
KW  - Human immunodeficiency virus
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40078585?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Interscience+Conference+on+Antimicrobial+Agents+and+Chemotherapy&rft.atitle=Applied+Proteomics+in+HCV%2FHIV+co-infection%3A+Differential+Expression+of+Serum+Proteins+Prior+to+Treatment+is+Associated+with+Response+to+HCV+Therapy+in+HIV+Co-infected+individuals.&rft.au=Kottilil&rft.aulast=Kottilil&rft.aufirst=&rft.date=2005-09-21&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Interscience+Conference+on+Antimicrobial+Agents+and+Chemotherapy&rft.issn=&rft_id=info:doi/
L2  - http://www.icaac.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Selective Suppression by Synthetic siRNA Duplexes of Human Papillomavirus 16 and 18 E6 and E7 Oncogene Expression
T2  - 45th Interscience Conference on Antimicrobial Agents and Chemotherapy
AN  - 40078529; 3986979
JF  - 45th Interscience Conference on Antimicrobial Agents and Chemotherapy
AU  - Zheng
Y1  - 2005/09/21/
PY  - 2005
DA  - 2005 Sep 21
KW  - siRNA
KW  - Oncogenes
KW  - Human papillomavirus 16
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40078529?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Interscience+Conference+on+Antimicrobial+Agents+and+Chemotherapy&rft.atitle=Selective+Suppression+by+Synthetic+siRNA+Duplexes+of+Human+Papillomavirus+16+and+18+E6+and+E7+Oncogene+Expression&rft.au=Zheng&rft.aulast=Zheng&rft.aufirst=&rft.date=2005-09-21&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Interscience+Conference+on+Antimicrobial+Agents+and+Chemotherapy&rft.issn=&rft_id=info:doi/
L2  - http://www.icaac.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Antagonistic Interaction Between Amphotericin B (AB) and Ravuconazole (RAV) Using the Bliss Independence Drug Interaction (BIDI) Model: In Vitro and In Vivo Correlations
T2  - 45th Interscience Conference on Antimicrobial Agents and Chemotherapy
AN  - 40055304; 3987021
JF  - 45th Interscience Conference on Antimicrobial Agents and Chemotherapy
AU  - Meletiadis
Y1  - 2005/09/21/
PY  - 2005
DA  - 2005 Sep 21
KW  - Models
KW  - Amphotericin B
KW  - Drug interaction
KW  - ravuconazole
KW  - Antibodies
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=45th+Interscience+Conference+on+Antimicrobial+Agents+and+Chemotherapy&rft.atitle=Antagonistic+Interaction+Between+Amphotericin+B+%28AB%29+and+Ravuconazole+%28RAV%29+Using+the+Bliss+Independence+Drug+Interaction+%28BIDI%29+Model%3A+In+Vitro+and+In+Vivo+Correlations&rft.au=Meletiadis&rft.aulast=Meletiadis&rft.aufirst=&rft.date=2005-09-21&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=45th+Interscience+Conference+on+Antimicrobial+Agents+and+Chemotherapy&rft.issn=&rft_id=info:doi/
L2  - http://www.icaac.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Multi-dimensional Volumetric Imaging Method (MDVIM) in Assessment of Pulmonary Infiltrates in Response to Antifungal Therapy in Experimental Invasive Pulmonary Aspergillosis (IPA)
T2  - 45th Interscience Conference on Antimicrobial Agents and Chemotherapy
AN  - 40045662; 3987012
JF  - 45th Interscience Conference on Antimicrobial Agents and Chemotherapy
AU  - Petraitis
Y1  - 2005/09/21/
PY  - 2005
DA  - 2005 Sep 21
KW  - Therapy
KW  - Fungicides
KW  - Lung
KW  - Aspergillosis
KW  - Imaging techniques
KW  - U 2000:Biological Sciences
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L2  - http://www.icaac.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Sympathetic Noradrenergic Denervation in Parkinson Disease
T2  - 59th Annual Fall Conference and Scientific Sessions of the Council for High Blood Pressure Research in association with the Council on the Kidney in Cardiovascular Disease
AN  - 39710148; 4023271
JF  - 59th Annual Fall Conference and Scientific Sessions of the Council for High Blood Pressure Research in association with the Council on the Kidney in Cardiovascular Disease
AU  - Goldstein, David S
AU  - Holmes, Courtney
AU  - Sharabi, Yehonatan
Y1  - 2005/09/21/
PY  - 2005
DA  - 2005 Sep 21
KW  - Parkinson's disease
KW  - Movement disorders
KW  - Neurodegenerative diseases
KW  - Norepinephrine
KW  - Denervation
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39710148?accountid=14244
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L2  - http://www.americanheart.org/downloadable/heart/1126889314397Final%20Progra m.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Hypokalemia in Thiazide-Sensitive Na-Cl Cotransporter Knockout Mice
T2  - 59th Annual Fall Conference and Scientific Sessions of the Council for High Blood Pressure Research in association with the Council on the Kidney in Cardiovascular Disease
AN  - 39666364; 4023356
JF  - 59th Annual Fall Conference and Scientific Sessions of the Council for High Blood Pressure Research in association with the Council on the Kidney in Cardiovascular Disease
AU  - Morris, Ryan G
AU  - Hoorn, Ewout J
AU  - Knepper, Mark A
Y1  - 2005/09/21/
PY  - 2005
DA  - 2005 Sep 21
KW  - Mice
KW  - Hypokalemia
KW  - U 2000:Biological Sciences
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L2  - http://www.americanheart.org/downloadable/heart/1126889314397Final%20Progra m.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Phase I trial of recombinant immunotoxin RFB4(dsFv)-PE38 (BL22) in patients with B-cell malignancies.
AN  - 68594802; 16061911
AB  - To conduct a phase I trial of recombinant immunotoxin BL22, an anti-CD22 Fv fragment fused to truncated Pseudomonas exotoxin.
          Forty-six pretreated patients with CD22+ non-Hodgkin's lymphoma (NHL; n = 4), chronic lymphocytic leukemia (CLL; n = 11), and hairy cell leukemia (HCL; n = 31) received 265 cycles at 3 to 50 microg/Kg every other day x 3 doses. BL22 was active in HCL, with 19 complete remissions (CRs; 61%) and six partial responses (PRs; 19%) in 31 patients. Of 19 CRs, 11 were achieved after one cycle and eight after two to 14 cycles. All 25 responders benefited clinically with one cycle. The CR rate was 86% in patients enrolled at > or = 40 microg/Kg every other day x 3, and 41% at lower doses (P = .011). The median duration for CR was 36 months (range, 5 to 66 months), and eight patients remain in CR at 45 months (range, 29 to 66 months). Lower but significant activity occurred in CLL. Neutralizing antibodies occurred in 11 (24%) of 46 patients (all HCL). A reversible hemolytic uremic syndrome requiring plasmapheresis was observed in one patient with NHL during cycle 1 and in four patients with HCL during cycle 2 or 3. The maximum-tolerated dose (MTD) evaluated at cycle 1 was 40 microg/Kg IV. QOD x 3. The most common toxicities at 30 to 50 microg/Kg every other day x 3 included hypoalbuminemia, transaminase elevations, fatigue, and edema. BL22 was well tolerated and highly effective in HCL, even after one cycle. Phase II testing is underway to define the efficacy with one cycle and to study safety when additional cycles are needed for optimal response.
JF  - Journal of clinical oncology : official journal of the American Society of Clinical Oncology
AU  - Kreitman, Robert J
AU  - Squires, David R
AU  - Stetler-Stevenson, Maryalice
AU  - Noel, Pierre
AU  - FitzGerald, David J P
AU  - Wilson, Wyndham H
AU  - Pastan, Ira
AD  - Laboratory of Molecular Biology, National Cancer Institute, National Institutes of Health, Bldg 5124b, 9000 Rockville Pike, Bethesda, MD 20892, USA. kreitmar@mail.nih.gov
Y1  - 2005/09/20/
PY  - 2005
DA  - 2005 Sep 20
SP  - 6719
EP  - 6729
VL  - 23
IS  - 27
SN  - 0732-183X, 0732-183X
KW  - Antibodies
KW  - 0
KW  - Enterotoxins
KW  - Immunotoxins
KW  - RFB4(dsFv)-PE38 recombinant immunotoxin
KW  - Index Medicus
KW  - Severity of Illness Index
KW  - Drug Administration Schedule
KW  - Infusions, Intravenous
KW  - Dose-Response Relationship, Drug
KW  - Humans
KW  - Aged
KW  - Risk Assessment
KW  - Aged, 80 and over
KW  - Adult
KW  - Treatment Outcome
KW  - Middle Aged
KW  - Follow-Up Studies
KW  - Maximum Tolerated Dose
KW  - Female
KW  - Male
KW  - Survival Analysis
KW  - Lymphoma, Non-Hodgkin -- drug therapy
KW  - Lymphoma, Non-Hodgkin -- diagnosis
KW  - Leukemia, Lymphocytic, Chronic, B-Cell -- diagnosis
KW  - Leukemia, Hairy Cell -- mortality
KW  - Lymphoma, Non-Hodgkin -- mortality
KW  - Leukemia, Lymphocytic, Chronic, B-Cell -- drug therapy
KW  - Leukemia, Hairy Cell -- drug therapy
KW  - Immunotoxins -- therapeutic use
KW  - Leukemia, Lymphocytic, Chronic, B-Cell -- mortality
KW  - Leukemia, Hairy Cell -- diagnosis
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-10-27
N1  - Date created - 2005-09-19
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Cardiac-specific Nkx2.5 homeodomain: conformational stability and specific DNA binding of Nkx2.5(C56S).
AN  - 68584227; 16156660
AB  - The cardiac-specific Nkx2.5 homeodomain has been expressed as a 79-residue protein with the oxidizable Cys(56) replaced with Ser. The Nkx2.5 or Nkx2.5(C56S) homeodomain is 73% identical in sequence to and has the same NMR structure as the vnd (ventral nervous system defective)/NK-2 homeodomain of Drosophila when bound to the same specific DNA. The thermal unfolding of Nkx2.5(C56S) at pH 6.0 or 7.4 is a reversible, two-state process with unit cooperativity, as measured by differential scanning calorimetry (DSC) and far-UV circular dichroism. Adding 100 mM NaCl to Nkx2.5(C56S) at pH 7.4 increases T(m) from 44 to 54 +/- 0.2 degrees C and DeltaH from 34 to 45 +/- 2 kcal/mol (giving a DeltaC(p) of approximately 1.2 kcal K(-)(1) mol(-)(1) for homeodomain unfolding). DSC profiles of Nkx2.5 indicate fluctuating nativelike structures at <37 degrees C. Titrations of specific 18 bp DNA with Nkx2.5(C56S) in buffer at pH 7.4 with 100 mM NaCl yield binding constants of 2-6 x 10(8) M(-)(1) from 10 to 37 degrees C and a stoichiometry of 1:1 for homeodomain binding DNA, using isothermal titration calorimetry. The DNA binding reaction of Nkx2.5 is enthalpically controlled, and the temperature dependence of DeltaH gives a DeltaC(p) of -0.18 +/- 0.01 kcal K(-)(1) mol(-)(1). This corresponds to 648 +/- 36 A(2) of buried apolar surface upon Nkx2.5(C56S) binding duplex B-DNA. Thermodynamic parameters differ for Nkx2.5 and vnd/NK-2 homeodomains binding specific DNA. Unbound NK-2 is more flexible than Nkx2.5.
JF  - Biochemistry
AU  - Fodor, Elfrieda
AU  - Mack, James W
AU  - Maeng, Jin-Soo
AU  - Ju, Jeong-Ho
AU  - Lee, Hyun Sook
AU  - Gruschus, James M
AU  - Ferretti, James A
AU  - Ginsburg, Ann
AD  - Section on Protein Chemistry, Laboratory of Biochemistry, National Heart, Lung and Blood Institute, National Institutes of Health, Bethesda, Maryland 20892-8012, USA.
Y1  - 2005/09/20/
PY  - 2005
DA  - 2005 Sep 20
SP  - 12480
EP  - 12490
VL  - 44
IS  - 37
SN  - 0006-2960, 0006-2960
KW  - Drosophila Proteins
KW  - 0
KW  - Homeodomain Proteins
KW  - Recombinant Proteins
KW  - Transcription Factors
KW  - vnd protein, Drosophila
KW  - DNA
KW  - 9007-49-2
KW  - Index Medicus
KW  - Mutagenesis, Site-Directed
KW  - Animals
KW  - Protein Structure, Secondary
KW  - Thermodynamics
KW  - Recombinant Proteins -- metabolism
KW  - Restriction Mapping
KW  - Protein Denaturation
KW  - Molecular Sequence Data
KW  - Calorimetry
KW  - Mice
KW  - Amino Acid Sequence
KW  - Recombinant Proteins -- chemistry
KW  - Drosophila
KW  - Myocardium -- metabolism
KW  - Amino Acid Substitution
KW  - Protein Conformation
KW  - Binding Sites
KW  - Drosophila Proteins -- chemistry
KW  - Transcription Factors -- metabolism
KW  - DNA -- metabolism
KW  - Transcription Factors -- chemistry
KW  - Homeodomain Proteins -- metabolism
KW  - Drosophila Proteins -- metabolism
KW  - Homeodomain Proteins -- chemistry
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-14
N1  - Date created - 2005-09-13
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Barium potentiates the conditioned aversion to, but not the somatic signs of, morphine withdrawal in mice.
AN  - 68582210; 16122731
AB  - The effect of barium, a putative blocker of G-protein-activated inwardly rectifying potassium (GIRK) channels, on naltrexone-precipitated withdrawal signs in morphine-dependent mice was investigated. Mice were chronically treated with morphine (8-45 mg/kg) for 6 days. The morphine-dependent mice were then given naltrexone (1 and 3 mg/kg), after which they showed several somatic signs of withdrawal, as well as conditioned aversion, increased cortical noradrenaline turnover, and decreased dopamine turnover in the limbic forebrain. Pretreatment with barium (1.25 and 2.5 nmol) significantly potentiated the naltrexone-precipitated conditioned aversion and augmented the decrease in dopamine turnover in the limbic forebrain. However, barium pretreatment did not affect the naltrexone-precipitated somatic signs of withdrawal and increased cortical noradrenaline turnover. These findings suggest that modification of GIRK channels may be involved in the expression of aversion to morphine withdrawal mediated through the dopaminergic system but it is not involved in the somatic signs of morphine withdrawal mediated through the noradrenergic system.
JF  - European journal of pharmacology
AU  - Sato, Mio
AU  - Wada, Kiyoshi
AU  - Funada, Masahiko
AD  - Section of Additive Drugs Research, Department of Drug Dependence Research, National Institute of Mental Health, National Center of Neurology and Psychiatry, 4-1-1 Ogawa-higashi, Kodaira, Tokyo 187-8502, Japan.
Y1  - 2005/09/20/
PY  - 2005
DA  - 2005 Sep 20
SP  - 215
EP  - 222
VL  - 519
IS  - 3
SN  - 0014-2999, 0014-2999
KW  - Narcotic Antagonists
KW  - 0
KW  - Barium
KW  - 24GP945V5T
KW  - Naltrexone
KW  - 5S6W795CQM
KW  - Morphine
KW  - 76I7G6D29C
KW  - Dopamine
KW  - VTD58H1Z2X
KW  - Norepinephrine
KW  - X4W3ENH1CV
KW  - Index Medicus
KW  - Animals
KW  - Cerebral Cortex -- drug effects
KW  - Mice, Inbred ICR
KW  - Substance Withdrawal Syndrome -- physiopathology
KW  - Prosencephalon -- metabolism
KW  - Cerebral Cortex -- metabolism
KW  - Substance Withdrawal Syndrome -- prevention & control
KW  - Dose-Response Relationship, Drug
KW  - Dopamine -- metabolism
KW  - Mice
KW  - Behavior, Animal -- drug effects
KW  - Norepinephrine -- metabolism
KW  - Prosencephalon -- drug effects
KW  - Naltrexone -- pharmacology
KW  - Drug Synergism
KW  - Narcotic Antagonists -- pharmacology
KW  - Male
KW  - Conditioning, Operant -- drug effects
KW  - Morphine -- toxicity
KW  - Barium -- pharmacology
KW  - Morphine -- pharmacology
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=European+journal+of+pharmacology&rft.atitle=Barium+potentiates+the+conditioned+aversion+to%2C+but+not+the+somatic+signs+of%2C+morphine+withdrawal+in+mice.&rft.au=Sato%2C+Mio%3BWada%2C+Kiyoshi%3BFunada%2C+Masahiko&rft.aulast=Sato&rft.aufirst=Mio&rft.date=2005-09-20&rft.volume=519&rft.issue=3&rft.spage=215&rft.isbn=&rft.btitle=&rft.title=European+journal+of+pharmacology&rft.issn=00142999&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-10-25
N1  - Date created - 2005-09-13
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Polymorphisms in the DNA nucleotide excision repair genes and lung cancer risk in Xuan Wei, China.
AN  - 68070858; 15849729
AB  - The lung cancer mortality rate in Xuan Wei County is among the highest in China and has been attributed to exposure to indoor smoky coal emissions that contain very high levels of polycyclic aromatic hydrocarbons (PAHs). Nucleotide excision repair (NER) plays a key role in reversing DNA damage from exposure to environmental carcinogens, such as PAHs, that form bulky DNA adducts. We studied single nucleotide polymorphisms (SNPs) and their corresponding haplotypes in 6 genes (ERCC1, ERCC2/XPD, ERCC4/XPF, ERCC5/XPG, RAD23B and XPC) involved in NER in a population-based case-control study of lung cancer in Xuan Wei. A total of 122 incident primary lung cancer cases and 122 individually matched controls were enrolled. Three linked SNPs in ERCC2 were associated with lung cancer with similar ORs; e.g., persons with the Gln allele at codon 751 had a 60% reduction of lung cancer (OR = 0.40, 95% CI 0.18-0.89). Moreover, one haplotype in ERCC2 was associated with a decreased risk of lung cancer (OR = 0.40, 95% CI 0.19-0.85) compared to the most common haplotype. In addition, subjects with one or 2 copies of the Val allele at codon 249 of RAD23B had a 2-fold increased risk of lung cancer (OR = 1.91, 95% CI 1.12-3.24). In summary, our results suggest that genetic variants in genes involved in the NER pathway may play a role in lung cancer susceptibility in Xuan Wei. However, due to the small sample size, additional studies are needed to evaluate these associations within Xuan Wei and in other populations with substantial environmental exposure to PAHs. (c) 2005 Wiley-Liss, Inc.
JF  - International journal of cancer
AU  - Shen, Min
AU  - Berndt, Sonja I
AU  - Rothman, Nathaniel
AU  - Demarini, David M
AU  - Mumford, Judy L
AU  - He, Xingzhou
AU  - Bonner, Matthew R
AU  - Tian, Linwei
AU  - Yeager, Meredith
AU  - Welch, Robert
AU  - Chanock, Stephen
AU  - Zheng, Tongzhang
AU  - Caporaso, Neil
AU  - Lan, Qing
AD  - Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892-7240, USA. shenmi@mail.nih.gov
Y1  - 2005/09/20/
PY  - 2005
DA  - 2005 Sep 20
SP  - 768
EP  - 773
VL  - 116
IS  - 5
SN  - 0020-7136, 0020-7136
KW  - DNA excision repair protein ERCC-5
KW  - 0
KW  - DNA-Binding Proteins
KW  - Nuclear Proteins
KW  - RAD23B protein, human
KW  - Transcription Factors
KW  - xeroderma pigmentosum group F protein
KW  - RAD23A protein, human
KW  - 156533-33-4
KW  - XPC protein, human
KW  - 156533-34-5
KW  - ERCC1 protein, human
KW  - EC 3.1.-
KW  - Endonucleases
KW  - DNA Helicases
KW  - EC 3.6.4.-
KW  - Xeroderma Pigmentosum Group D Protein
KW  - EC 3.6.4.12
KW  - ERCC2 protein, human
KW  - EC 5.99.-
KW  - DNA Repair Enzymes
KW  - EC 6.5.1.-
KW  - Index Medicus
KW  - Nuclear Proteins -- genetics
KW  - Humans
KW  - DNA-Binding Proteins -- genetics
KW  - Aged
KW  - Endonucleases -- genetics
KW  - Transcription Factors -- genetics
KW  - Linkage Disequilibrium
KW  - Risk
KW  - Adult
KW  - Case-Control Studies
KW  - DNA Helicases -- genetics
KW  - Middle Aged
KW  - Female
KW  - Male
KW  - DNA Repair -- genetics
KW  - Polymorphism, Single Nucleotide
KW  - Lung Neoplasms -- etiology
KW  - Lung Neoplasms -- genetics
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=International+journal+of+cancer&rft.atitle=Polymorphisms+in+the+DNA+nucleotide+excision+repair+genes+and+lung+cancer+risk+in+Xuan+Wei%2C+China.&rft.au=Shen%2C+Min%3BBerndt%2C+Sonja+I%3BRothman%2C+Nathaniel%3BDemarini%2C+David+M%3BMumford%2C+Judy+L%3BHe%2C+Xingzhou%3BBonner%2C+Matthew+R%3BTian%2C+Linwei%3BYeager%2C+Meredith%3BWelch%2C+Robert%3BChanock%2C+Stephen%3BZheng%2C+Tongzhang%3BCaporaso%2C+Neil%3BLan%2C+Qing&rft.aulast=Shen&rft.aufirst=Min&rft.date=2005-09-20&rft.volume=116&rft.issue=5&rft.spage=768&rft.isbn=&rft.btitle=&rft.title=International+journal+of+cancer&rft.issn=00207136&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-09-01
N1  - Date created - 2005-07-26
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Frontiers in Research with Bioactive Food Components, the Omics and Cancer: Perspectives from the National Cancer Institute
T2  - 18th International Nutrition Congress (NUTRITION SAFARI 2005)
AN  - 39732042; 3985902
JF  - 18th International Nutrition Congress (NUTRITION SAFARI 2005)
AU  - Milner, John
Y1  - 2005/09/19/
PY  - 2005
DA  - 2005 Sep 19
KW  - Food
KW  - Cancer
KW  - U 2000:Biological Sciences
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L2  - http://www.puk.ac.za/fakulteite/voeding/iuns/scientific%20programme.htm
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Opportunities for International Research Collaboration in Maternal and Child Health: NICHD International Nutrition Interests, Mechanisms, and Capacity Building
T2  - 18th International Nutrition Congress (NUTRITION SAFARI 2005)
AN  - 39672340; 3985903
JF  - 18th International Nutrition Congress (NUTRITION SAFARI 2005)
AU  - Raiten, Dan
Y1  - 2005/09/19/
PY  - 2005
DA  - 2005 Sep 19
KW  - Nutrition
KW  - U 2000:Biological Sciences
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L2  - http://www.puk.ac.za/fakulteite/voeding/iuns/scientific%20programme.htm
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Differential Metabolism of 2-Amino-1-methyl-6-phenylimidazo [4,5-b]pyridine (PhlP) in Mice Humanized for CYP1A1 and CYP1A2
AN  - 17471971; 6674237
AB  - The procarcinogen 2-amino-1-methyl-6-phenylimidazo[4,5-b]pyridine (PhIP) is the most abundant heterocyclic amine formed during the cooking of foods. Metabolism of PhIP by CYP1A2 differs substantially between humans and rodents, with more N super(2)-hydroxylation (activation) and less 4'-hydroxylation (detoxication) in humans. Therefore, the human response to PhIP and other heterocyclic amine exposure may not be accurately reflected in the laboratory rodent. By generating mouse models expressing the human genes, species differences in heterocyclic amine metabolism can be addressed. Two transgenic mouse lines were developed, one expressing the human CYP1A1 CYP1A2 transgene in a mouse Cyplal-null background (hCYPlAl) and another expressing human CYP1A1 CYP1A2 in a mouse Cypla2-null background (hCYPIA2). Expression of human CYP1A2 protein was detected in the liver and also at considerably lower levels in extrahepatic tissues such as lung, kidney, colon, and heart. In the hCYPlAl and HCYP1A2 mice, 3-methylcholanthrene (3-MC) induced both human CYP1A1 and CYP1A2 protein in the liver. Differences in the metabolism of the heterocyclic amine PhIP were observed between wild-type and hCYPlA2 mice. PhIP was preferentially metabolized by N super(2)-hydroxylation in hCYPlA2 mice, whereas in wild-type mice, 4'-hydroxylation was the predominant pathway. Since the N super(2)-hydroxylation pathway for PhIP metabolism has been reported to be predominant in humans, these results illustrate the potential effectiveness of using these transgenic, humanized mice as models for determining human health risks to PhIP and other heterocyclic amines instead of wild-type mice.
JF  - Chemical Research in Toxicology
AU  - Cheung, C
AU  - Ma, X
AU  - Krausz, K W
AU  - Kimura, S
AU  - Feigenbaum, L
AU  - Dalton, T P
AU  - Nebert, D W
AU  - Idle, J R
AU  - Gonzalez, F J
AD  - Laboratory of Metabolism, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892, USA
Y1  - 2005/09/19/
PY  - 2005
DA  - 2005 Sep 19
SP  - 1471
EP  - 1478
VL  - 18
IS  - 9
SN  - 0893-228X, 0893-228X
KW  - Toxicology Abstracts
KW  - Heart
KW  - Heterocyclic amines
KW  - CYP1A2 protein
KW  - 3-Methylcholanthrene
KW  - Transgenic mice
KW  - Colon
KW  - Lung
KW  - Cooking
KW  - Liver
KW  - Kidney
KW  - Cytochrome P450
KW  - Metabolism
KW  - X 24153:Metabolism
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2006-02-01
N1  - Last updated - 2015-03-25
N1  - SubjectsTermNotLitGenreText - Heart; Heterocyclic amines; CYP1A2 protein; Colon; Lung; Cooking; Kidney; 3-Methylcholanthrene; Liver; Cytochrome P450; Transgenic mice; Metabolism
DO  - http://dx.doi.org/10.1021/tx050136g
ER  - 



TY  - CPAPER
T1  - Understanding the Simple Complexities of Drug Resistance
T2  - Second International Meeting on Tumor Progression and Therapeutic Resistance (TPTR 2005)
AN  - 39704401; 4016892
JF  - Second International Meeting on Tumor Progression and Therapeutic Resistance (TPTR 2005)
AU  - Fojo, Tito
Y1  - 2005/09/18/
PY  - 2005
DA  - 2005 Sep 18
KW  - Drug resistance
KW  - U 2000:Biological Sciences
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L2  - http://gtcbio.com/ebrochure/tptr.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Biomarkers and Imaging Endpoints to Accelerate Oncologic Drug Development
T2  - Second International Meeting on Tumor Progression and Therapeutic Resistance (TPTR 2005)
AN  - 39644004; 4016906
JF  - Second International Meeting on Tumor Progression and Therapeutic Resistance (TPTR 2005)
AU  - Kelloff, Gary
Y1  - 2005/09/18/
PY  - 2005
DA  - 2005 Sep 18
KW  - Biomarkers
KW  - Drug development
KW  - Bioindicators
KW  - Imaging techniques
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/39644004?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=Second+International+Meeting+on+Tumor+Progression+and+Therapeutic+Resistance+%28TPTR+2005%29&rft.atitle=Biomarkers+and+Imaging+Endpoints+to+Accelerate+Oncologic+Drug+Development&rft.au=Kelloff%2C+Gary&rft.aulast=Kelloff&rft.aufirst=Gary&rft.date=2005-09-18&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=Second+International+Meeting+on+Tumor+Progression+and+Therapeutic+Resistance+%28TPTR+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://gtcbio.com/ebrochure/tptr.pdf
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - JOUR
T1  - Survey of oxaliplatin-associated neurotoxicity using an interview-based questionnaire in patients with metastatic colorectal cancer.
AN  - 68725793; 16168057
AB  - New chemotherapy regimens for patients with colorectal cancer have improved survival, but at the cost of clinical toxicity. Oxaliplatin, an agent used in first-line therapy for metastatic colorectal cancer, causes acute and chronic neurotoxicity. This study was performed to carefully assess the incidence, type and duration of oxaliplatin neurotoxicity.
          A detailed questionnaire was completed after each chemotherapy cycle for patients with metastatic colorectal cancer enrolled in a phase I trial of oxaliplatin and capecitabine. An oxaliplatin specific neurotoxicity scale was used to grade toxicity. Eighty-six adult patients with colorectal cancer were evaluated. Acute neuropathy symptoms included voice changes, visual alterations, pharyngo-laryngeal dysesthesia (lack of awareness of breathing); peri-oral or oral numbness, pain and symptoms due to muscle contraction (spasm, cramps, tremors). When the worst neurotoxicity per patient was considered, grade 1/2/3/4 dysesthesias and paresthesias were seen in 71/12/5/0 and 66/20/7/1 percent of patients. By cycles 3, 6, 9, and 12, oxaliplatin dose reduction or discontinuation was needed in 2.7%, 20%, 37.5% and 62.5% of patients.
          Oxaliplatin-associated acute neuropathy causes a variety of distressing, but transient, symptoms due to peripheral sensory and motor nerve hyperexcitability. Chronic neuropathy may be debilitating and often necessitates dose reductions or discontinuation of oxaliplatin. Patients should be warned of the possible spectrum of symptoms and re-assured about the transient nature of acute neurotoxicity. Ongoing studies are addressing the treatment and prophylaxis of oxaliplatin neurotoxicity.
JF  - BMC cancer
AU  - Leonard, Gregory D
AU  - Wright, Maurice A
AU  - Quinn, Mary G
AU  - Fioravanti, Suzanne
AU  - Harold, Nancy
AU  - Schuler, Barbara
AU  - Thomas, Rebecca R
AU  - Grem, Jean L
AD  - Cancer Therapeutics Branch, Center for Cancer Research, National Cancer Institute, National Naval Medical Center, Bethesda, MD 20889-5105, USA. LeonardG@Sehb.ie
Y1  - 2005/09/16/
PY  - 2005
DA  - 2005 Sep 16
SP  - 116
VL  - 5
KW  - Antimetabolites, Antineoplastic
KW  - 0
KW  - Antineoplastic Agents
KW  - Organoplatinum Compounds
KW  - oxaliplatin
KW  - 04ZR38536J
KW  - Deoxycytidine
KW  - 0W860991D6
KW  - Capecitabine
KW  - 6804DJ8Z9U
KW  - Fluorouracil
KW  - U3P01618RT
KW  - Index Medicus
KW  - Antimetabolites, Antineoplastic -- adverse effects
KW  - Humans
KW  - Paresthesia -- chemically induced
KW  - Clinical Trials as Topic
KW  - Aged
KW  - Antimetabolites, Antineoplastic -- pharmacology
KW  - Antineoplastic Agents -- adverse effects
KW  - Adult
KW  - Fluorouracil -- analogs & derivatives
KW  - Treatment Outcome
KW  - Surveys and Questionnaires
KW  - Neoplasm Metastasis
KW  - Middle Aged
KW  - Time Factors
KW  - Antineoplastic Agents -- pharmacology
KW  - Neurotoxicity Syndromes -- pathology
KW  - Female
KW  - Male
KW  - Organoplatinum Compounds -- adverse effects
KW  - Organoplatinum Compounds -- pharmacology
KW  - Deoxycytidine -- adverse effects
KW  - Colorectal Neoplasms -- pathology
KW  - Deoxycytidine -- analogs & derivatives
KW  - Deoxycytidine -- pharmacology
KW  - Colorectal Neoplasms -- drug therapy
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2006-02-27
N1  - Date created - 2005-10-25
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Clin Colorectal Cancer. 2002 May;2(1):54-8 [12453338]
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N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - The synaptic localization of NR2B-containing NMDA receptors is controlled by interactions with PDZ proteins and AP-2.
AN  - 68583684; 16157279
AB  - The NMDA receptor (NMDAR) is a component of excitatory synapses and a key participant in synaptic plasticity. We investigated the role of two domains in the C terminus of the NR2B subunit--the PDZ binding domain and the clathrin adaptor protein (AP-2) binding motif--in the synaptic localization of NMDA receptors. NR2B subunits lacking functional PDZ binding are excluded from the synapse. Mutations in the AP-2 binding motif, YEKL, significantly increase the number of synaptic receptors and allow the synaptic localization of NR2B subunits lacking PDZ binding. Peptides corresponding to YEKL increase the synaptic response within minutes. In contrast, the NR2A subunit localizes to the synapse in the absence of PDZ binding and is not altered by mutations in its motif corresponding to YEKL of NR2B. This study identifies a dynamic regulation of synaptic NR2B-containing NMDARs through PDZ protein-mediated stabilization and AP-2-mediated internalization that is modulated by phosphorylation by Fyn kinase.
JF  - Neuron
AU  - Prybylowski, Kate
AU  - Chang, Kai
AU  - Sans, Nathalie
AU  - Kan, Lilly
AU  - Vicini, Stefano
AU  - Wenthold, Robert J
AD  - Laboratory of Neurochemistry, National Institute on Deafness and Other Communication Disorders, Room 4148/Bldg. 50, National Institutes of Health, Bethesda Maryland 20892, USA. prybylow@nidcd.nih.gov
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
SP  - 845
EP  - 857
VL  - 47
IS  - 6
SN  - 0896-6273, 0896-6273
KW  - DNA Probes
KW  - 0
KW  - NR2B NMDA receptor
KW  - Nerve Tissue Proteins
KW  - Receptors, N-Methyl-D-Aspartate
KW  - Tyrosine
KW  - 42HK56048U
KW  - Index Medicus
KW  - Animals
KW  - Fluorescent Antibody Technique -- methods
KW  - Two-Hybrid System Techniques
KW  - Mutagenesis -- physiology
KW  - Amino Acid Sequence
KW  - Blotting, Western -- methods
KW  - Rats
KW  - Animals, Newborn
KW  - Cerebellum -- cytology
KW  - Amino Acid Motifs -- physiology
KW  - Transfection
KW  - Mutation -- physiology
KW  - Cells, Cultured
KW  - DNA Probes -- physiology
KW  - Immunoprecipitation -- methods
KW  - Tyrosine -- metabolism
KW  - Models, Neurological
KW  - Time Factors
KW  - Excitatory Postsynaptic Potentials -- physiology
KW  - Neurons -- physiology
KW  - Nerve Tissue Proteins -- metabolism
KW  - Receptors, N-Methyl-D-Aspartate -- metabolism
KW  - Synapses -- metabolism
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Neuron&rft.atitle=The+synaptic+localization+of+NR2B-containing+NMDA+receptors+is+controlled+by+interactions+with+PDZ+proteins+and+AP-2.&rft.au=Prybylowski%2C+Kate%3BChang%2C+Kai%3BSans%2C+Nathalie%3BKan%2C+Lilly%3BVicini%2C+Stefano%3BWenthold%2C+Robert+J&rft.aulast=Prybylowski&rft.aufirst=Kate&rft.date=2005-09-15&rft.volume=47&rft.issue=6&rft.spage=845&rft.isbn=&rft.btitle=&rft.title=Neuron&rft.issn=08966273&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-12-07
N1  - Date created - 2005-09-13
N1  - Date revised - 2017-01-13
N1  - SuppNotes - Cited By:
Neuron. 2002 Oct 24;36(3):435-49 [12408846]
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Science. 2002 Jan 18;295(5554):491-5 [11799243]
J Neurochem. 2002 Feb;80(4):589-97 [11841566]
J Biol Chem. 2002 Feb 22;277(8):5699-702 [11741967]
Neuron. 2002 Feb 28;33(5):765-77 [11879653]
Neuron. 2002 Apr 11;34(2):255-64 [11970867]
Annu Rev Neurosci. 2002;25:103-26 [12052905]
J Biol Chem. 2002 Jun 14;277(24):21697-711 [11937501]
J Neurosci. 2002 Jul 15;22(14):6208-17 [12122079]
Neuron. 2002 Jul 18;35(2):345-53 [12160751]
Nat Neurosci. 2002 Sep;5(9):833-4 [12195433]
Neuron. 2002 Nov 14;36(4):661-74 [12441055]
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Fixed dose-rate gemcitabine infusion as first-line treatment for advanced-stage carcinoma of the pancreas and biliary tree.
AN  - 68556690; 16078261
AB  - Gemcitabine infusion at the fixed dose rate of 10 mg/m(2) per minute (FDR-gemcitabine) has pharmacokinetic advantages and may result in improved therapeutic efficacy.
          Between April 2002 and September 2003, 40 patients with advanced-stage pancreatic adenocarcinoma (PDAC; n = 27) or biliary tree carcinoma (BTC; n = 13) were treated with weekly FDR-gemcitabine (1000 mg/m(2)). The primary end point was the response rate. The secondary end points were progression-free and overall survival (PFS and OS), tumor marker response, and clinical benefit response (CBR). The overall response rate (ORR) on an intent-to-treat basis was 15% (95% confidence interval [95% CI], 4-26%). A positive CBR was obtained in 14 of 29 (48%) patients. Seventeen of 25 (68%) patients had a reduction in carbohydrate antigen 19-9 (CA 19-9) of > 25%. The median time to treatment failure and the median PFS were 17 weeks (95% CI, 13-22 weeks) and 19 weeks (95% CI, 15-23 weeks), respectively. The median OS was 40 weeks (95% CI, 36-45 weeks) and the 1-year actuarial survival rate was 25.8%. Multivariate analysis showed that a performance status score of 0-1 at study entry and locally advanced disease were the only independent predictors of longer PFS and OS, whereas a reduction in CA 19-9 serum levels > 75% was an independent predictor of longer PFS, but had no impact on OS. Toxicity was mild with Grade 3-4 neutropenia (according to the National Cancer Institute-Common Toxicity Criteria [version 2.0]) in 18 of 427 treatment weeks (4.2%), and Grade 3 anemia and thrombocytopenia in 6 of 427 treatment weeks (1.4%) and 9 of 427 treatment weeks (2.1%), respectively, and asymptomatic Grade 3-4 transaminase elevation in 21 of 427 treatment weeks (4.9%). FDR-gemcitabine at the weekly dose of 1000 mg/m(2) demonstrated promising activity, despite negligible toxicity, in patients with advanced-stage PDAC and BTC.
          Copyright 2005 American Cancer Society.
JF  - Cancer
AU  - Gelibter, Alain
AU  - Malaguti, Paola
AU  - Di Cosimo, Serena
AU  - Bria, Emilio
AU  - Ruggeri, Enzo Maria
AU  - Carlini, Paolo
AU  - Carboni, Fabio
AU  - Ettorre, Giuseppe Maria
AU  - Pellicciotta, Mario
AU  - Giannarelli, Diana
AU  - Terzoli, Edmondo
AU  - Cognetti, Francesco
AU  - Milella, Michele
AD  - Division of Medical Oncology A, Regina Elena National Cancer Institute, Rome, Italy.
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
SP  - 1237
EP  - 1245
VL  - 104
IS  - 6
SN  - 0008-543X, 0008-543X
KW  - CA-19-9 Antigen
KW  - 0
KW  - Deoxycytidine
KW  - 0W860991D6
KW  - gemcitabine
KW  - B76N6SBZ8R
KW  - Abridged Index Medicus
KW  - Index Medicus
KW  - CA-19-9 Antigen -- blood
KW  - Survival Rate
KW  - Humans
KW  - Male
KW  - Female
KW  - Pancreatic Neoplasms -- mortality
KW  - Deoxycytidine -- adverse effects
KW  - Deoxycytidine -- analogs & derivatives
KW  - Deoxycytidine -- therapeutic use
KW  - Deoxycytidine -- administration & dosage
KW  - Pancreatic Neoplasms -- drug therapy
KW  - Biliary Tract Neoplasms -- mortality
KW  - Adenocarcinoma -- drug therapy
KW  - Biliary Tract Neoplasms -- drug therapy
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Cancer&rft.atitle=Fixed+dose-rate+gemcitabine+infusion+as+first-line+treatment+for+advanced-stage+carcinoma+of+the+pancreas+and+biliary+tree.&rft.au=Gelibter%2C+Alain%3BMalaguti%2C+Paola%3BDi+Cosimo%2C+Serena%3BBria%2C+Emilio%3BRuggeri%2C+Enzo+Maria%3BCarlini%2C+Paolo%3BCarboni%2C+Fabio%3BEttorre%2C+Giuseppe+Maria%3BPellicciotta%2C+Mario%3BGiannarelli%2C+Diana%3BTerzoli%2C+Edmondo%3BCognetti%2C+Francesco%3BMilella%2C+Michele&rft.aulast=Gelibter&rft.aufirst=Alain&rft.date=2005-09-15&rft.volume=104&rft.issue=6&rft.spage=1237&rft.isbn=&rft.btitle=&rft.title=Cancer&rft.issn=0008543X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-10-27
N1  - Date created - 2005-09-06
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Maternal serum levels of polychlorinated biphenyls and 1,1-dichloro-2,2-bis(p-chlorophenyl)ethylene (DDE) and time to pregnancy.
AN  - 68538714; 16093292
AB  - Polychlorinated biphenyls (PCBs), once used widely in transformers and other applications, and 1,1-dichloro-2,2-bis(p-chlorophenyl)ethylene (DDE), the main metabolite of the pesticide 1,1,1-trichloro-2,2-bis(p-chlorophenyl)ethane (DDT), are hormonally active agents. Changes in menstrual cycle functioning associated with PCBs and DDE, and increased odds of spontaneous abortion associated with DDE, suggest that these compounds could affect fertility. The authors investigated the association between PCB and DDE exposure and time to pregnancy by using serum levels measured in 390 pregnant women in the Collaborative Perinatal Project enrolled at 12 study centers in the United States from 1959 to 1965. They estimated adjusted fecundability odds ratios by using Cox proportional hazards modeling for discrete time data. Compared with time to pregnancy for women in the lowest exposure category (PCBs  or = 5.00 microg/liter = 0.65, 95% confidence interval: 0.36, 1.18) and DDE (fecundability odds ratio for DDE > or = 60 microg/liter = 0.65, 95% confidence interval: 0.32, 1.31). Overall, time to pregnancy increased with increasing serum PCB levels but was less suggestive of an association with DDE. Both trends were imprecise and attenuated when expressed on a lipid basis. Overall, evidence of an association between PCB or DDE exposure and time to pregnancy was weak and inconclusive.
JF  - American journal of epidemiology
AU  - Law, Dionne C Gesink
AU  - Klebanoff, Mark A
AU  - Brock, John W
AU  - Dunson, David B
AU  - Longnecker, Matthew P
AD  - Epidemiology Branch, National Institute of Environmental Health Sciences, National Institutes of Health, Department of Health and Human Services, Research Triangle Park, NC 27709, USA.
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
SP  - 523
EP  - 532
VL  - 162
IS  - 6
SN  - 0002-9262, 0002-9262
KW  - Dichlorodiphenyl Dichloroethylene
KW  - 4M7FS82U08
KW  - Polychlorinated Biphenyls
KW  - DFC2HB4I0K
KW  - Index Medicus
KW  - United States
KW  - Prospective Studies
KW  - Humans
KW  - Adult
KW  - Follow-Up Studies
KW  - Time Factors
KW  - Female
KW  - Pregnancy
KW  - Pregnancy Trimester, Third -- blood
KW  - Polychlorinated Biphenyls -- blood
KW  - Maternal Exposure
KW  - Fertility -- physiology
KW  - Dichlorodiphenyl Dichloroethylene -- blood
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-10-20
N1  - Date created - 2005-09-01
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - JOUR
T1  - Synthesis of tripeptides as potent Yersinia protein tyrosine phosphatase inhibitors.
AN  - 68473349; 16039123
AB  - We report the synthesis of a series of monoanionic phosphotyrosyl (pTyr) mimetic-containing tripeptides based on 'Fmoc-Glu(OBn)-Xxx-Leu-amide' (where Xxx = pTyr mimetic) and their N-terminally modified derivatives. The inhibitory potencies of compounds were tested against YopH and human PTP1B enzymes. Several compounds exhibited noteworthy activity against both YopH and PTP1B. Among the N-terminally modified analogues, 5-methylindole derivative 30 was found to be the best moiety to replace base-labile Fmoc group. A mode of binding with YopH is proposed for tripeptides 21, 30, and 31.
JF  - Bioorganic & medicinal chemistry letters
AU  - Lee, Kyeong
AU  - Boovanahalli, Shanthaveerappa K
AU  - Nam, Ky-Youb
AU  - Kang, Sang-Uk
AU  - Lee, Mijeoung
AU  - Phan, Jason
AU  - Wu, Li
AU  - Waugh, David S
AU  - Zhang, Zhong-Yin
AU  - No, Kyoung Tai
AU  - Lee, Jung Jun
AU  - Burke, Terrence R
AD  - Laboratory of Medicinal Chemistry, NCI, NIH, NCI-Frederick, Frederick, MD 21702, USA.
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
SP  - 4037
EP  - 4042
VL  - 15
IS  - 18
SN  - 0960-894X, 0960-894X
KW  - Bacterial Outer Membrane Proteins
KW  - 0
KW  - Enzyme Inhibitors
KW  - Oligopeptides
KW  - PTPN1 protein, human
KW  - EC 3.1.3.48
KW  - Protein Tyrosine Phosphatase, Non-Receptor Type 1
KW  - Protein Tyrosine Phosphatases
KW  - yopH protein, Yersinia
KW  - Index Medicus
KW  - Molecular Structure
KW  - Models, Molecular
KW  - Humans
KW  - Inhibitory Concentration 50
KW  - Protein Structure, Tertiary
KW  - Protein Binding
KW  - Structure-Activity Relationship
KW  - Binding Sites
KW  - Protein Tyrosine Phosphatases -- metabolism
KW  - Enzyme Inhibitors -- chemistry
KW  - Oligopeptides -- chemistry
KW  - Bacterial Outer Membrane Proteins -- metabolism
KW  - Bacterial Outer Membrane Proteins -- chemistry
KW  - Oligopeptides -- chemical synthesis
KW  - Bacterial Outer Membrane Proteins -- antagonists & inhibitors
KW  - Enzyme Inhibitors -- pharmacology
KW  - Enzyme Inhibitors -- chemical synthesis
KW  - Oligopeptides -- pharmacology
KW  - Yersinia -- enzymology
KW  - Protein Tyrosine Phosphatases -- chemistry
KW  - Protein Tyrosine Phosphatases -- antagonists & inhibitors
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Atoxline&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.jtitle=Bioorganic+%26+medicinal+chemistry+letters&rft.atitle=Synthesis+of+tripeptides+as+potent+Yersinia+protein+tyrosine+phosphatase+inhibitors.&rft.au=Lee%2C+Kyeong%3BBoovanahalli%2C+Shanthaveerappa+K%3BNam%2C+Ky-Youb%3BKang%2C+Sang-Uk%3BLee%2C+Mijeoung%3BPhan%2C+Jason%3BWu%2C+Li%3BWaugh%2C+David+S%3BZhang%2C+Zhong-Yin%3BNo%2C+Kyoung+Tai%3BLee%2C+Jung+Jun%3BBurke%2C+Terrence+R&rft.aulast=Lee&rft.aufirst=Kyeong&rft.date=2005-09-15&rft.volume=15&rft.issue=18&rft.spage=4037&rft.isbn=&rft.btitle=&rft.title=Bioorganic+%26+medicinal+chemistry+letters&rft.issn=0960894X&rft_id=info:doi/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date completed - 2005-11-21
N1  - Date created - 2005-08-15
N1  - Date revised - 2017-01-13
N1  - Last updated - 2017-01-18
ER  - 



TY  - CPAPER
T1  - Detection of Myocardial Capillary Orientation with Intravascular Nano Iron-Oxide Particles in Spin-echo MRI: R2 Tensor Imaging
T2  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AN  - 40094591; 4000876
JF  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AU  - Vignaud, A C
AU  - Rodriguez, I
AU  - Ennis, D B
AU  - DeSilva, R
AU  - Kellman, P
AU  - Taylor, J
AU  - Bennett, E
AU  - Wen, H
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
KW  - Particulates
KW  - Magnetic resonance imaging
KW  - U 2000:Biological Sciences
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L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=22nd+Annual+Scientific+Meeting+of+the+European+Society+for+Magnetic+Resonance+in+Medicine+and+Biology+%28ESMRMB+2005%29&rft.atitle=Detection+of+Myocardial+Capillary+Orientation+with+Intravascular+Nano+Iron-Oxide+Particles+in+Spin-echo+MRI%3A+R2+Tensor+Imaging&rft.au=Vignaud%2C+A+C%3BRodriguez%2C+I%3BEnnis%2C+D+B%3BDeSilva%2C+R%3BKellman%2C+P%3BTaylor%2C+J%3BBennett%2C+E%3BWen%2C+H&rft.aulast=Vignaud&rft.aufirst=A&rft.date=2005-09-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=22nd+Annual+Scientific+Meeting+of+the+European+Society+for+Magnetic+Resonance+in+Medicine+and+Biology+%28ESMRMB+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.esmrmb.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Carbon-13 Magnetization Transfer Spectroscopy: Detection of Aspartate Aminotransferase reaction in vivo
T2  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AN  - 40094475; 4000846
JF  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AU  - Shen, J
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
KW  - Aspartate aminotransferase
KW  - Spectroscopy
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40094475?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=22nd+Annual+Scientific+Meeting+of+the+European+Society+for+Magnetic+Resonance+in+Medicine+and+Biology+%28ESMRMB+2005%29&rft.atitle=Carbon-13+Magnetization+Transfer+Spectroscopy%3A+Detection+of+Aspartate+Aminotransferase+reaction+in+vivo&rft.au=Shen%2C+J&rft.aulast=Shen&rft.aufirst=J&rft.date=2005-09-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=22nd+Annual+Scientific+Meeting+of+the+European+Society+for+Magnetic+Resonance+in+Medicine+and+Biology+%28ESMRMB+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.esmrmb.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Regional Strain Mapping of the Carotid Artery Wall in Humans Using DENSE
T2  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AN  - 40059112; 4000845
JF  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AU  - Wen, H
AU  - Vignaud, A
AU  - Rodriguez, I
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
KW  - Mapping
KW  - Carotid artery
KW  - Strains
KW  - U 2000:Biological Sciences
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L2  - http://www.esmrmb.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Anatomically Guided Shaped Smoothing in Myocardial Strain Data Analysis
T2  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AN  - 40054062; 4000650
JF  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AU  - Wen, H
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
KW  - Data processing
KW  - Strains
KW  - U 2000:Biological Sciences
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L2  - http://www.esmrmb.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - TAX, an Element for Increased Receive Array Population Density
T2  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AN  - 40053473; 4000947
JF  - 22nd Annual Scientific Meeting of the European Society for Magnetic Resonance in Medicine and Biology (ESMRMB 2005)
AU  - Merkle, H
AU  - Li, T.
AU  - Wang, S
AU  - van Gelderen, P
AU  - Koretsky, A P
AU  - Duyn, J H
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
KW  - Population density
KW  - U 2000:Biological Sciences
UR  - http://libproxy.lib.unc.edu/login?url=http://search.proquest.com/docview/40053473?accountid=14244
L2  - http://vb3lk7eb4t.search.serialssolutions.com/?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&rfr_id=info:sid/ProQ%3Acpi&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=conference&rft.jtitle=22nd+Annual+Scientific+Meeting+of+the+European+Society+for+Magnetic+Resonance+in+Medicine+and+Biology+%28ESMRMB+2005%29&rft.atitle=TAX%2C+an+Element+for+Increased+Receive+Array+Population+Density&rft.au=Merkle%2C+H%3BLi%2C+T.%3BWang%2C+S%3Bvan+Gelderen%2C+P%3BKoretsky%2C+A+P%3BDuyn%2C+J+H&rft.aulast=Merkle&rft.aufirst=H&rft.date=2005-09-15&rft.volume=&rft.issue=&rft.spage=&rft.isbn=&rft.btitle=&rft.title=22nd+Annual+Scientific+Meeting+of+the+European+Society+for+Magnetic+Resonance+in+Medicine+and+Biology+%28ESMRMB+2005%29&rft.issn=&rft_id=info:doi/
L2  - http://www.esmrmb.org/
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2007-09-05
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Induction of a Graft-Versus-Host-Like Skin Disease by Intradermal Injection of Ovalbumin-Peptide-Specific CD8+ (OT-I) T Cells into Keratin 14-Ovalbumin-Expressing Transgenic Mice
T2  - 9th International Workshop on Langerhans Cells (LC 2005)
AN  - 39704185; 4016116
JF  - 9th International Workshop on Langerhans Cells (LC 2005)
AU  - Kim, B S
AU  - Miyagawa, F
AU  - Katz, S I
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
KW  - Mice
KW  - Skin diseases
KW  - Ovalbumin
KW  - Lymphocytes T
KW  - Transgenic mice
KW  - CD8 antigen
KW  - Keratin
KW  - U 2000:Biological Sciences
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ER  - 



TY  - CPAPER
T1  - Oncostatin M Enhances CCL21 Expression by Microvascular Endothelial Cells in Vitro and Increases the Efficiency of Dendritic Cell Trafficking in Vivo
T2  - 9th International Workshop on Langerhans Cells (LC 2005)
AN  - 39704022; 4016078
JF  - 9th International Workshop on Langerhans Cells (LC 2005)
AU  - Cardones, Adela R
AU  - Sugaya, Makoto
AU  - Blauvelt, Andrew
AU  - Hwang, Sam T
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
KW  - Endothelial cells
KW  - CCL21 protein
KW  - Microvasculature
KW  - Oncostatin M
KW  - Dendritic cells
KW  - U 2000:Biological Sciences
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LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  - 



TY  - CPAPER
T1  - Exogenous Administration of IL-15 Breaks Peripheral Tolerance Towards Low Dose Antigen in Experimental Graft VS. Host Disease
T2  - 9th International Workshop on Langerhans Cells (LC 2005)
AN  - 39643924; 4016141
JF  - 9th International Workshop on Langerhans Cells (LC 2005)
AU  - Miyagawa, Fumi
AU  - Kim, B S
AU  - Patel, H
AU  - Tagaya, Y
AU  - Waldmann, T A
AU  - Katz, Stephen I
Y1  - 2005/09/15/
PY  - 2005
DA  - 2005 Sep 15
KW  - Hosts
KW  - Immunological tolerance
KW  - Interleukin 15
KW  - Antigens
KW  - U 2000:Biological Sciences
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L2  - http://www.lc2005.at/index.php?open=program
LA  - English
DB  - ProQuest Environmental Science Collection
N1  - Date revised - 2008-05-21
N1  - Last updated - 2010-05-03
ER  -