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GABRA2 单核苷酸多态性与酒精依赖的脑电图遗传关联研究。

Genetic association study of GABRA2 single nucleotide polymorphisms and electroencephalography in alcohol dependence.

机构信息

Molecular Psychiatry Laboratory, Windeyer Institute of Medical Sciences, Department of Psychiatry and Behavioural Sciences, Royal Free and University College London, London Medical School, 46 Cleveland Street, London W1T 4JF, UK.

出版信息

Neurosci Lett. 2011 Aug 18;500(3):162-6. doi: 10.1016/j.neulet.2011.05.240. Epub 2011 Jun 12.

Abstract

The gamma aminobutyric acid (GABA) system has been implicated in the susceptibility to develop alcohol dependence and in determining electroencephalogram (EEG) beta activity. The role of the GABA receptor alpha-2 gene (GABRA2) in human alcohol dependence was determined in a genetic and electrophysiological study. The study population comprised 586 white UK individuals with alcohol dependence but a very low prevalence of co-morbid drug dependence, and 603 ancestrally matched healthy controls. Genotyping for seven GABRA2 single nucleotide polymorphisms (SNPs), identified from the literature as positively associated with alcohol dependence, was performed with success rates of 90% or greater. EEGs were available in 32 selected patients who had been abstinent from alcohol for a minimum of 24 months and in 138 ancestrally matched healthy controls. None of the SNPs showed allelic or haplotypic association with alcohol dependence. All markers were in Hardy Weinberg equilibrium (HWE) in the controls. HWE for marker rs279841 in the alcohol dependent sample was p=0.0199 and combined p=0.0166. Linkage disequilibrium patterns appear to be very similar to that observed in the HapMap CEU data. A significantly higher prevalence of excess EEG fast activity was found in the patients (31 vs. 14%, p=0.018). A significant relationship was found between the presence of excess EEG fast activity and GABRA2 SNPs rs548583, rs279871 and rs279841. This allelic association study provides no evidence for an association between GABRA2 polymorphisms and alcohol dependence. However, a significant relationship was identified between GABRA2 and excess EEG fast activity. This dissociation of effect may reflect the fact that the EEG is a more direct marker of phenotypic GABRA2 expression than the more heterogeneous alcohol dependence phenotype.

摘要

γ-氨基丁酸(GABA)系统被认为与易患酒精依赖和决定脑电图(EEG)β活动有关。在一项遗传和电生理研究中,确定了 GABA 受体α-2 基因(GABRA2)在人类酒精依赖中的作用。研究人群包括 586 名英国白人酒精依赖患者,但合并药物依赖的患病率非常低,以及 603 名祖先匹配的健康对照者。从文献中确定的与酒精依赖呈正相关的 GABRA2 七个单核苷酸多态性(SNP)进行基因分型,成功率达到 90%或更高。在至少 24 个月未饮酒的 32 名选定患者和 138 名祖先匹配的健康对照者中获得了 EEG。没有 SNP 显示与酒精依赖具有等位基因或单体型关联。所有标记在对照中均符合 Hardy Weinberg 平衡(HWE)。在酒精依赖样本中,标记 rs279841 的 HWE 为 p=0.0199,合并 p=0.0166。与 HapMap CEU 数据观察到的连锁不平衡模式非常相似。在患者中发现了明显更高的过量 EEG 快活动发生率(31%比 14%,p=0.018)。发现 EEG 快活动的存在与 GABRA2 SNPs rs548583、rs279871 和 rs279841 之间存在显著关系。该等位基因关联研究未提供 GABRA2 多态性与酒精依赖之间存在关联的证据。然而,在 GABRA2 和过量 EEG 快活动之间发现了显著关系。这种效应的分离可能反映了这样一个事实,即 EEG 是表型 GABRA2 表达的更直接标记,而不是更具异质性的酒精依赖表型。

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