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一种GABRA2变体与饮酒后增强的刺激感和“兴奋感”相关。

A GABRA2 variant is associated with increased stimulation and 'high' following alcohol administration.

作者信息

Arias Albert J, Covault Jonathan, Feinn Richard, Pond Timothy, Yang Bao-Zhu, Ge Wenjing, Oncken Cheryl, Kranzler Henry R

机构信息

Corresponding author: Department of Psychiatry, University of Connecticut Health Center, 263 Farmington Avenue, Farmington, CT 06030-1410, USA.

出版信息

Alcohol Alcohol. 2014 Jan-Feb;49(1):1-9. doi: 10.1093/alcalc/agt163. Epub 2013 Oct 27.

Abstract

AIMS

Variation in genes encoding GABAA receptor subunits has been implicated in the risk of alcohol dependence (AD). We sought to replicate and extend previous findings of a moderating effect of single nucleotide polymorphisms (SNPs) in GABRA2 (which encodes the GABAA α-2 subunit) on the subjective effects of alcohol by examining SNPs in this and the adjacent GABRG1 gene on chromosome 4.

METHODS

Fifty-two European-Americans (22 males, 28 light drinkers and 24 heavy drinkers) completed 3 laboratory sessions, during which they drank low-dose, high-dose, or placebo alcohol prior to undergoing periodic assessments of stimulation, sedation and drug enjoyment. We genotyped subjects for three SNPs previously associated with AD: rs279858 in GABRA2, and rs7654165 and rs6447493 in GABRG1.

RESULTS

Two SNPs were associated with altered stimulatory effects of alcohol as measured on the Biphasic Alcohol Effects Scale, (rs279858: P = 0.0046; rs6447493: P = 0.0023); both effects were in the opposite direction of previous findings. Carriers of the rs279858 C allele experienced greater stimulation from alcohol. Further inspection of the rs6447493 interaction did not support a pharmacogenetic effect. The effects of rs279858 (but not the other two SNPs) on items from a secondary outcome measure, the Drug Effects Questionnaire (DEQ), were significant. Higher ratings by individuals with the C allele were observed on the DEQ items 'feel the alcohol effect' (P < 0.001), 'like the alcohol effect' (P < 0.001) and feel 'high' (P < 0.001).

CONCLUSION

We did not find that the GABRG1 SNPs rs7654165 and rs6447493 moderated the effects of alcohol. Greater stimulatory and euphoric effects of alcohol in carriers of the rs279858 C allele may, in part, explain the previously reported association of this allele with AD.

摘要

目的

编码γ-氨基丁酸A(GABAA)受体亚基的基因变异与酒精依赖(AD)风险有关。我们试图通过检测4号染色体上该基因及相邻的GABRG1基因中的单核苷酸多态性(SNP),来复制和扩展先前关于GABRA2(编码GABAAα-2亚基)中SNP对酒精主观效应的调节作用的研究结果。

方法

52名欧裔美国人(22名男性,28名轻度饮酒者和24名重度饮酒者)完成了3次实验室实验,期间他们在接受刺激、镇静和药物愉悦感的定期评估之前,饮用了低剂量、高剂量或安慰剂酒精。我们对受试者进行了3个先前与AD相关的SNP基因分型:GABRA2中的rs279858,以及GABRG1中的rs7654165和rs6447493。

结果

根据双相酒精效应量表测量,有2个SNP与酒精刺激效应的改变有关(rs279858:P = 0.0046;rs6447493:P = 0.0023);这两种效应与先前的研究结果方向相反。rs279858 C等位基因携带者从酒精中获得的刺激更大。对rs6447493相互作用的进一步检查不支持药物遗传学效应。rs279858(但不是其他两个SNP)对次要结果测量指标药物效应问卷(DEQ)各项的影响是显著的。C等位基因个体在DEQ项目“感觉到酒精作用”(P < 0.001)、“喜欢酒精作用”(P < 0.001)和感觉“兴奋”(P < 0.001)上的评分更高。

结论

我们没有发现GABRG1的SNP rs7654165和rs6447493对酒精效应有调节作用。rs279858 C等位基因携带者对酒精有更大的刺激和欣快感,这可能部分解释了先前报道的该等位基因与AD的关联。

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