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GABRA2 与酒精使用障碍:意大利病例对照研究中没有关联的证据。

GABRA2 and alcohol use disorders: no evidence of an association in an Italian case-control study.

机构信息

Institute of Legal Medicine, Department of Neuroscience, Università Politecnica delle Marche, Ancona, Italy.

出版信息

Alcohol Clin Exp Res. 2010 Apr;34(4):659-68. doi: 10.1111/j.1530-0277.2009.01135.x. Epub 2010 Jan 26.

Abstract

BACKGROUND

Alcoholism is a major health and social issue, a highly frequent disease and a cause of premature death. It is also the most expensive addictive disorder being related to high morbidity and mortality, violence, accidents, and social and legal problems. It is a quantitative disorder, where the combined incidence of environmental and multiple genetic factors varies from 1 subject to another. Recent association studies have identified several genes as candidates for alcoholism, including GABAA receptor genes, due to their role in mediating several behavioral effects of alcohol, such as motor incoordination, anxiolysis, sedation, and withdrawal. The proposed association between the 3' half of the gene encoding the alpha-2 subunit of GABA receptor (3'-GABRA2) and alcohol use disorders (AUDs) has received several independent confirmations.

METHODS

In this study, 10 single nucleotide polymorphisms (SNPs) of the 3'-GABRA2 gene, previously reported to be implicated in alcohol dependence, were used to evaluate the linkage between selected SNPs and AUDs in an Italian sample and to compare findings with those of previous studies.

RESULTS

No evidence of an association was found at the allele, genotype, haplotype, or diplotype levels between the 3'-GABRA2 polymorphisms investigated and alcoholism in 149 Italian alcoholics (98 alcohol dependents and 51 alcohol abusers) and 278 controls.

CONCLUSIONS

Despite previous reports, we did not find an association between AUDs and 3'-GABRA2 polymorphisms. This is probably due to the minimal comorbidity of our Italian sample suggesting that this gene is implicated in polysubstance dependence rather than in alcoholism alone.

摘要

背景

酗酒是一个主要的健康和社会问题,是一种高发疾病,也是导致早逝的一个原因。它也是最昂贵的成瘾性疾病,与高发病率和死亡率、暴力、事故以及社会和法律问题有关。它是一种定量障碍,环境和多种遗传因素的综合发生率因个体而异。最近的关联研究已经确定了几个候选基因与酗酒有关,包括 GABA 受体基因,因为它们在介导酒精的几种行为效应中发挥作用,如运动不协调、焦虑缓解、镇静和戒断。编码 GABA 受体 α-2 亚基的基因 3'端(3'-GABRA2)与酒精使用障碍(AUD)之间的拟议关联得到了多项独立证实。

方法

在这项研究中,使用了先前报道与酒精依赖有关的 GABRA2 基因 3'端的 10 个单核苷酸多态性(SNP),以评估选定的 SNP 与意大利样本中 AUD 之间的连锁关系,并将结果与以前的研究进行比较。

结果

在所研究的 GABRA2 基因的 3'端多态性与 149 名意大利酗酒者(98 名酒精依赖者和 51 名酒精滥用者)和 278 名对照者之间的等位基因、基因型、单倍型或二倍型水平上均未发现关联。

结论

尽管有先前的报告,但我们没有发现 AUD 与 3'-GABRA2 多态性之间存在关联。这可能是由于我们的意大利样本的共病性最小,表明该基因与多种物质依赖有关,而不仅仅是酗酒。

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