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功能性 DBH 基因变异与酒精依赖风险及相关抑郁和自杀未遂表型的关联:来自大型多中心关联研究的结果。

Association of functional DBH genetic variants with alcohol dependence risk and related depression and suicide attempt phenotypes: results from a large multicenter association study.

机构信息

Department of Psychiatry, Psychotherapy, Psychosomatics, Martin-Luther-University, Halle-Wittenberg, Germany.

出版信息

Drug Alcohol Depend. 2013 Dec 1;133(2):459-67. doi: 10.1016/j.drugalcdep.2013.07.002. Epub 2013 Jul 30.

DOI:10.1016/j.drugalcdep.2013.07.002
PMID:23906995
Abstract

OBJECTIVE

Dopamine-beta-hydroxylase (DBH) metabolizes the conversion of dopamine to noradrenaline. DBH, located on chromosome 9q34.2 has variants with potential functional consequences which may be related to alterations of neurotransmitter function and several psychiatric phenotypes, including alcohol dependence (AD), depression (MD) and suicidal behavior (SA). The aim of this association study in a large multicenter sample of alcohol-dependent individuals and controls is to investigate the role of DBH SNPs and haplotypes in AD risk and associated phenotypes (AD with MD or SA).

METHOD

1606 inpatient subjects with DSM-IV AD from four addiction treatment centers and 1866 control subjects were included. Characteristics of AD, MD and SA were obtained using standardized structured interviews. After subjects were genotyped for 4 DBH polymorphisms, single SNP case-control and haplotype analyses were conducted.

RESULTS

rs1611115 (near 5') C-allele and related haplotypes were significantly associated with alcohol dependence in females. This association with female alcohol dependence also accounts for the significant relationship between this variant and comorbid conditions and traits.

CONCLUSIONS

This study presents evidence for a potentially functional DBH variant influencing the risk for alcohol dependence while other comorbid conditions are not independently influenced by this SNP. However, the study also supports the possible role of the dopamine system in the etiology of female alcohol dependence.

摘要

目的

多巴胺-β羟化酶(DBH)将多巴胺转化为去甲肾上腺素。DBH 位于 9q34.2 染色体上,具有潜在功能影响的变体,可能与神经递质功能的改变以及几种精神表型有关,包括酒精依赖(AD)、抑郁症(MD)和自杀行为(SA)。本研究旨在通过对来自四个成瘾治疗中心的大量多中心酒精依赖个体和对照个体的关联研究,探讨 DBH SNPs 和单倍型在 AD 风险和相关表型(AD 伴 MD 或 SA)中的作用。

方法

纳入 1606 名来自四个成瘾治疗中心的符合 DSM-IV AD 标准的住院患者和 1866 名对照者。使用标准化的结构化访谈获得 AD、MD 和 SA 的特征。在对 4 个 DBH 多态性进行基因分型后,进行单 SNP 病例对照和单倍型分析。

结果

rs1611115(靠近 5')C-等位基因及其相关单倍型与女性酒精依赖显著相关。这种与女性酒精依赖的关联也解释了该变体与共病状况和特征之间的显著关系。

结论

本研究为潜在的功能性 DBH 变体影响酒精依赖风险提供了证据,而其他共病状况不受该 SNP 的独立影响。然而,该研究也支持多巴胺系统在女性酒精依赖发病机制中的可能作用。

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