酒精脱氢酶基因内的基因组变异与美洲印第安人和欧洲裔美国人的酒精症状之间的关联:差异与趋同。
Associations Between Genomic Variants in Alcohol Dehydrogenase Genes and Alcohol Symptomatology in American Indians and European Americans: Distinctions and Convergence.
机构信息
Department of Neuroscience, The Scripps Research Institute, La Jolla, California.
Department of Psychological Sciences, University of Missouri-Columbia, Columbia, Missouri.
出版信息
Alcohol Clin Exp Res. 2017 Oct;41(10):1695-1704. doi: 10.1111/acer.13480. Epub 2017 Sep 15.
BACKGROUND
Higher rates of alcohol use disorders (AUD) have been observed in some Native American populations than other ethnic groups such as European Americans (EAs) in the United States. Previous studies have shown that variation in the alcohol dehydrogenase (ADH) genes may affect the risk for development of AUD and that the prevalence of these variants differs depending on the ancestral origins of a population.
METHODS
In this study, we assessed sequencing variants in the ADH genomic region (ADH1-7) and tested for their associations with AUD phenotypes in 2 independent populations: an American Indian (AI) community sample and an EA cohort from the San Francisco Family Alcohol Study. Association tests were conducted for both common and rare variants using sequencing data for 2 phenotypes: the number of alcohol-related life events and the count of alcohol dependence drinking symptoms. A regularized regression method was used to select the best set of ADH variants associated with phenotypes. Variance component model was incorporated in all analyses to leverage the admixture and relatedness.
RESULTS
Two variants near ADH4 and 2 near ADH1C exhibited significant associations with AUD in AIs; no variant was significant in EAs. Common risk variants in AIs were either absent from or much less frequent in EAs. The feature selection method selected mostly distinct yet often colocated subsets of ADH variants to be associated with AUD phenotypes between the 2 cohorts. In the rare-variant analyses, the only association was observed between the whole region and the alcohol-related life events in AIs.
CONCLUSIONS
Our results suggest that ADH variants, both common and rare, are more likely to impact risk for alcohol-related symptomatology in this AI population than in this EA sample, and ADH variants that might affect AUD are likely different but convergent on similar regions between the 2 populations.
背景
在美国,一些美洲原住民群体的酗酒障碍(AUD)发生率高于其他族裔,如欧洲裔美国人(EAs)。先前的研究表明,乙醇脱氢酶(ADH)基因的变异可能会影响 AUD 的发病风险,而且这些变体的流行程度取决于人群的祖先起源。
方法
在这项研究中,我们评估了 ADH 基因组区域(ADH1-7)中的测序变体,并在两个独立的群体中测试了它们与 AUD 表型的关联:一个美洲印第安人(AI)社区样本和一个来自旧金山家庭酒精研究的 EA 队列。使用两种表型的测序数据(与酒精相关的生活事件数量和酒精依赖饮酒症状的计数)对常见和罕见变体进行了关联测试。使用正则化回归方法选择与表型关联的最佳 ADH 变体集。在所有分析中都纳入了方差分量模型,以利用混合和相关性。
结果
ADH4 附近的两个变体和 ADH1C 附近的两个变体在 AI 中与 AUD 显著相关;在 EA 中没有变体显著。AI 中的常见风险变体要么不存在,要么在 EA 中频率要低得多。特征选择方法选择了大多数不同但通常位于同一位置的 ADH 变体子集,以与两个队列之间的 AUD 表型相关联。在稀有变体分析中,仅在 AI 中观察到整个区域与与酒精相关的生活事件之间存在关联。
结论
我们的结果表明,ADH 变体,无论是常见的还是罕见的,都更有可能影响这个 AI 人群的酒精相关症状的风险,而在这个 EA 样本中则不太可能,并且可能影响 AUD 的 ADH 变体可能不同,但在这两个群体之间的相似区域上趋同。
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