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确认 ALDH2 是饮酒行为的主要基因座,并确认其变异体在日本人群中调节多种代谢表型。

Confirmation of ALDH2 as a Major locus of drinking behavior and of its variants regulating multiple metabolic phenotypes in a Japanese population.

机构信息

Department of Gene Diagnostics and Therapeutics, Research Institute, National Center for Global Health and Medicine, Tokyo, Japan.

出版信息

Circ J. 2011;75(4):911-8. doi: 10.1253/circj.cj-10-0774. Epub 2011 Mar 1.

Abstract

BACKGROUND

Normative alcohol use (or drinking behavior) influences the risk of cardiovascular disease in a multi-faceted manner. To identify susceptibility gene variants for drinking behavior, a 2-staged genome-wide association study was performed in a Japanese population.

METHODS AND RESULTS

In the stage-1 scan, 733 cases and 729 controls were genotyped with 456,827 SNP markers. The associated loci without redundancy of linkage disequilibrium were further examined in the stage-2 general population panel comprising 2,794 drinkers (≥ once per week), 1,521 chance drinkers (< once per week), and 1,351 non-drinkers. Along with genome-wide exploration, we aimed to replicate the trait association of a candidate gene SNP previously reported (rs1229984 in ADH1B). A cluster of 12 SNPs on 12q24 were found to significantly (P<5×10(-8)) associate with drinking behavior in stage 1, among which rs671 (a Glu-to-Lys substitution at position 504) in the ALDH2 gene showed the strongest association (odds ratio (OR)=0.16, P=3.6×10(-211) in the joint analysis). The association was also replicated for rs1229984 (OR=1.20, P<3.6×10(-4)). Furthermore, ALDH2 504Lys was associated with several metabolic traits, eg, lower levels of high-density lipoprotein cholesterol and liver enzymes-AST, ALT, and γGTP-by interacting with alcohol intake.

CONCLUSIONS

Our results confirm ALDH2 as a major locus regulating drinking behavior in the Japanese, indicating that the ALDH2 504Lys variant exerts pleiotropic effects on risk factors of cardiovascular disease among drinkers.

摘要

背景

规范的饮酒行为(或饮酒行为)以多方面的方式影响心血管疾病的风险。为了确定饮酒行为的易感基因变异体,对日本人群进行了两阶段全基因组关联研究。

方法和结果

在第一阶段扫描中,733 例病例和 729 例对照使用 456827 个 SNP 标记进行了基因分型。没有连锁不平衡冗余的相关基因座在第二阶段的一般人群面板中进一步进行了检查,该面板包括 2794 名饮酒者(≥每周一次)、1521 名偶然饮酒者(<每周一次)和 1351 名不饮酒者。我们的目标是在全基因组探索的基础上,复制先前报道的候选基因 SNP (rs1229984 在 ADH1B 中的)的特征关联。在第一阶段,发现 12q24 上的 12 个 SNP 簇与饮酒行为显著相关(P<5×10(-8)),其中 ALDH2 基因中的 rs671(位置 504 处的 Glu 到 Lys 取代)显示出最强的相关性(联合分析中的优势比(OR)=0.16,P=3.6×10(-211))。rs1229984 的关联也得到了复制(OR=1.20,P<3.6×10(-4))。此外,ALDH2 504Lys 与几种代谢特征相关,例如,高密度脂蛋白胆固醇和肝酶-AST、ALT 和γGTP 的水平较低,这与饮酒相互作用。

结论

我们的结果证实 ALDH2 是调节日本人饮酒行为的主要基因座,表明 ALDH2 504Lys 变异体对饮酒者心血管疾病危险因素具有多效性影响。

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