Dopamine Genes and Nicotine Dependence in Treatment-Seeking and Community Smokers

被引:0
|
作者
Andrew W Bergen
David V Conti
David Van Den Berg
Wonho Lee
Jinghua Liu
Dalin Li
Nan Guo
Huaiyu Mi
Paul D Thomas
Christina N Lessov-Schlaggar
Ruth Krasnow
Yungang He
Denise Nishita
Ruhong Jiang
Jennifer B McClure
Elizabeth Tildesley
Hyman Hops
Rachel F Tyndale
Neal L Benowitz
Caryn Lerman
Gary E Swan
机构
[1] Center for Health Sciences,Department of Preventative Medicine
[2] SRI International,Department of Psychiatry
[3] University of Southern California,Department of Neuroscience, Centre for Addiction and Mental Health and Department of Pharmacology
[4] Artificial Intelligence Center,Departments of Medicine
[5] SRI International Menlo Park,Department of Psychiatry
[6] Washington University,undefined
[7] Center for Health Studies,undefined
[8] Group Health Cooperative,undefined
[9] Oregon Research Institute,undefined
[10] University of Toronto,undefined
[11] Psychiatry and BioPharmaceutical Sciences,undefined
[12] University of California at San Francisco,undefined
[13] University of Pennsylvania,undefined
来源
Neuropsychopharmacology | 2009年 / 34卷
关键词
dopamine transporter; Fagerström Test for Nicotine Dependence; single nucleotide polymorphism; candidate gene; gene–gene interaction;
D O I
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中图分类号
学科分类号
摘要
We utilized a cohort of 828 treatment-seeking self-identified white cigarette smokers (50% female) to rank candidate gene single nucleotide polymorphisms (SNPs) associated with the Fagerström Test for Nicotine Dependence (FTND), a measure of nicotine dependence which assesses quantity of cigarettes smoked and time- and place-dependent characteristics of the respondent's smoking behavior. A total of 1123 SNPs at 55 autosomal candidate genes, nicotinic acetylcholine receptors and genes involved in dopaminergic function, were tested for association to baseline FTND scores adjusted for age, depression, education, sex, and study site. SNP P-values were adjusted for the number of transmission models, the number of SNPs tested per candidate gene, and their intragenic correlation. DRD2, SLC6A3, and NR4A2 SNPs with adjusted P-values <0.10 were considered sufficiently noteworthy to justify further genetic, bioinformatic, and literature analyses. Each independent signal among the top-ranked SNPs accounted for ∼1% of the FTND variance in this sample. The DRD2 SNP appears to represent a novel association with nicotine dependence. The SLC6A3 SNPs have previously been shown to be associated with SLC6A3 transcription or dopamine transporter density in vitro, in vivo, and ex vivo. Analysis of SLC6A3 and NR4A2 SNPs identified a statistically significant gene–gene interaction (P=0.001), consistent with in vitro evidence that the NR4A2 protein product (NURR1) regulates SLC6A3 transcription. A community cohort of N=175 multiplex ever-smoking pedigrees (N=423 ever smokers) provided nominal evidence for association with the FTND at these top ranked SNPs, uncorrected for multiple comparisons.
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页码:2252 / 2264
页数:12
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