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Genome-wide association study of alcohol dependence in male Han Chinese and cross-ethnic polygenic risk score comparison

机译:雄性汉族和跨越民族风险评分比较的基因组 - 范围依赖性研究

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摘要

Alcohol-related behaviors are moderately heritable and have ethnic-specific characteristics. At present, genetic studies for alcohol dependence (AD) in Chinese populations are underrepresented. We are the first to conduct a genome-wide association study (GWAS) for AD using 533 male alcoholics and 2848 controls of Han Chinese ethnicity and replicate our findings in 146 male alcoholics and 200 male controls. We then assessed genetic effects on AD characteristics (drinking volume/age onset/Michigan Alcoholism Screening Test (MAST)/Barratt Impulsiveness Scale (BIS-11)), and compared the polygenic risk of AD in Han Chinese with other populations (Thai, European American and African American). We found and validated two significant loci, one located in 4q23, with lead SNP rs2075633*ADH1B (Psubdiscovery/sub?=?6.64?×?10sup-16/sup) and functional SNP rs1229984*ADH1B (Psubdiscovery/sub?=?3.93?×?10sup-13/sup); and the other located in 12q24.12-12q24.13, with lead SNP rs11066001*BRAP (Psubdiscovery/sub?=?1.63?×?10sup-9/sup) and functional SNP rs671*ALDH2 (Psubdiscovery/sub?=?3.44?×?10sup-9/sup). ADH1B rs1229984 was associated with MAST, BIS_total score and average drinking volume. Polygenic risk scores from the Thai AD and European American AD GWAS were significantly associated with AD in Han Chinese, which were entirely due to the top two loci, however there was no significant prediction from African Americans. This is the first case-control AD GWAS in Han Chinese. Our findings demonstrate that these variants, which were highly linked with ALDH2 rs671 and ADH1B rs1229984, were significant modulators for AD in our Han Chinese cohort. A larger replication cohort is still needed to validate our findings.
机译:与酒精相关的行为是适度的遗传性,具有种族特征。目前,中国人口中的酒精依赖(AD)的遗传学研究不足。我们是第一个使用533次父母和汉族族种族的3848种汉族族酗酒的广泛关联研究(GWAS),并在146名男性酗酒者和200名男性对照中复制我们的研究结果。然后,我们评估了对广告特征的遗传效应(饮用体积/年龄发作/密歇根酒精中毒筛查试验(桅杆)/ Barratt脉冲量表(BIS-11),并将汉族人群与其他人群(泰国,欧洲)进行了比较了广告的多基因风险(泰国美国和非裔美国人)。我们发现并验证了位于4Q23的两个重要基座,其中Lead SNP RS2075633 * ADH1B(P 发现?=?6.64?×10 -16 )和功能性SNP rs1229984 * adh1b(p 发现?=?3.93?×10 -13 );而另一个位于12Q24.12-12-1244.13,具有铅SNP RS11066001 * BRAP(P 发现?=?1.63?×10 -9 )和功能性SNP RS671 * ALDH2(P 发现?=?3.44?×10 -9 )。 ADH1B RS1229984与MAST,BIS_TOTAL分数和平均饮用量有关。泰国广告和欧洲广告GWA的多种子规风险分数与汉族中的广告显着相关,这完全是由于前两个基因座,但非洲裔美国人没有明显预测。这是汉族的第一个案例控制广告Gwas。我们的研究结果表明,与ALDH2 RS671和ADH1B RS1229984高度相关的这些变体是我们汉族队列中的广告的重要调节剂。仍需要更大的复制群体来验证我们的研究结果。

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