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爱尔兰酒精依赖症患病同胞对研究中谷氨酸脱羧酶基因与酒精依赖初始敏感性及发病年龄的关联

Associations of glutamate decarboxylase genes with initial sensitivity and age-at-onset of alcohol dependence in the Irish Affected Sib Pair Study of Alcohol Dependence.

作者信息

Kuo Po-Hsiu, Kalsi Gursharan, Prescott Carol A, Hodgkinson Colin A, Goldman David, Alexander Jeffry, van den Oord Edwin J, Chen Xiangning, Sullivan Patrick F, Patterson Diana G, Walsh Dermot, Kendler Kenneth S, Riley Brien P

机构信息

Institute of Clinical Medicine, College of Medicine, National Cheng Kung University, Taiwan.

出版信息

Drug Alcohol Depend. 2009 Apr 1;101(1-2):80-7. doi: 10.1016/j.drugalcdep.2008.11.009. Epub 2008 Dec 25.

DOI:10.1016/j.drugalcdep.2008.11.009
PMID:19111404
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2844896/
Abstract

BACKGROUND

The relation of gamma-aminobutyric acid (GABA) to alcohol dependence (AD) has been widely studied. Several previous studies suggest that GABA may be involved in alcohol withdrawal, tolerance, and the symptoms that form an AD diagnosis. The genes coding for glutamate decarboxylase (GAD), the rate-limiting enzyme in GABA synthesis, are of potential interest for their association to ethanol consumption and AD. There are two isoforms of GAD, GAD1 and GAD2, which were reported to be associated with AD in males of Han Taiwanese (GAD1) and Russian (GAD2) ancestry. The present study examined the association of the two GAD isoforms with AD and relevant alcohol-related traits in the Irish Affected Sib Pair Study of Alcohol Dependence [Prescott, C.A., Sullivan, P.F., Myers, J.M., Patterson, D.G., Devitt, M., Halberstadt, L.J., Walsh, D., Kendler, K.S., 2005. The Irish Affected Sib Pair Study of Alcohol Dependence: study methodology and validation of diagnosis by interview and family history. Alcohol.-Clin. Exp. Res. 29 (3) 417-429].

METHODS

Participants were recruited in Ireland, including 575 independent cases who met DSM-IV AD criteria and 530 controls, screened for heavy drinking. We first conducted case-control analyses of the GAD genes with AD and, within the cases, examined associations with age at onset of AD, withdrawal symptoms, and two quantitative measures: initial sensitivity and tolerance (based on scales from the Self-Rating of the Effects of Ethanol) [Schuckit, M.A., Smith, T.L., Tipp, J.E., 1997. The self-rating of the effects of alcohol (SRE) form as a retrospective measure of the risk for alcoholism. Addiction 92, 979-988]. A total of 29 SNPs were genotyped for GAD1 and GAD2 using the Illumina GoldenGate protocols. Statistical procedures were implemented to control for false discovery rates (FDR).

RESULTS

Nine of 29 markers with minor allele frequencies less than 0.01 were removed from standard analysis; the remaining 20 markers were all in Hardy-Weinberg equilibrium. Three markers in the intronic regions of GAD1 were associated with initial sensitivity to alcohol (P=0.002); the associations remained significant after a FDR based correction for multiple testing. In addition, one marker located 3kb upstream of GAD1 exhibited association with age at onset of AD (P=0.0001). Gender specific effects were observed in results of both single marker and haplotype analyses.

CONCLUSION

We found no evidence for the association of GAD genes with AD but significant association of GAD1 with initial sensitivity and age at onset of AD. Our findings suggest that the underlying pathophysiology regulated by genes like GAD1 may be more directly related to the component processes that form AD than to the clinical disorder.

摘要
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4b53/2844896/eb279ed7061f/nihms140527f1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4b53/2844896/eb279ed7061f/nihms140527f1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4b53/2844896/eb279ed7061f/nihms140527f1.jpg

背景

γ-氨基丁酸(GABA)与酒精依赖(AD)的关系已得到广泛研究。先前的多项研究表明,GABA可能参与酒精戒断、耐受性以及构成AD诊断的症状。编码谷氨酸脱羧酶(GAD,GABA合成中的限速酶)的基因因其与乙醇消耗和AD的关联而具有潜在研究价值。GAD有两种同工型,即GAD1和GAD2,据报道它们分别与台湾汉族男性(GAD1)和俄罗斯男性(GAD2)的AD相关。本研究在爱尔兰酒精依赖患病同胞对研究中[普雷斯科特,C.A.,沙利文,P.F.,迈尔斯,J.M.,帕特森,D.G.,德维特,M.,哈尔伯施塔特,L.J.,沃尔什,D.,肯德勒,K.S.,2005年。爱尔兰酒精依赖患病同胞对研究:研究方法以及通过访谈和家族史进行诊断的验证。《酒精 - 临床与实验研究》29(3)417 - 429],检验了这两种GAD同工型与AD及相关酒精相关特征之间的关联。

方法

在爱尔兰招募参与者,包括575例符合《精神疾病诊断与统计手册》第四版(DSM - IV)AD标准的独立病例以及530名对照,这些对照经过重度饮酒筛查。我们首先对GAD基因与AD进行病例对照分析,并在病例中研究其与AD发病年龄、戒断症状以及两项定量指标的关联:初始敏感性和耐受性(基于乙醇效应自评量表)[舒基特,M.A.,史密斯,T.L.,蒂普,J.E.,1997年。酒精效应自评量表(SRE)作为酒精中毒风险的回顾性测量方法。《成瘾》92,979 - 988]。使用Illumina GoldenGate技术对GAD1和GAD2总共29个单核苷酸多态性(SNP)进行基因分型。实施统计程序以控制错误发现率(FDR)。

结果

在标准分析中,29个次要等位基因频率小于0.01的标记中有9个被剔除;其余20个标记均处于哈迪 - 温伯格平衡。GAD1内含子区域的3个标记与酒精初始敏感性相关(P = 0.002);在基于FDR的多重检验校正后,这些关联仍然显著。此外,位于GAD1上游3kb处的一个标记与AD发病年龄相关(P = 0.0001)。在单标记和单倍型分析结果中均观察到性别特异性效应。

结论

我们未发现GAD基因与AD相关的证据,但发现GAD1与初始敏感性和AD发病年龄显著相关。我们的研究结果表明,由GAD1等基因调控的潜在病理生理学可能与构成AD的组成过程更直接相关,而非与临床疾病直接相关。

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