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Diplotype trend regression analysis of the ADH gene cluster and the ALDH2 gene: Multiple significant associations with alcohol dependence

机译:ADH基因簇和ALDH2基因的双型趋势回归分析:与酒精依赖的多个显着关联

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The set of alcohol-metabolizing enzymes has considerable genetic and functional complexity. The relationships between some alcohol dehydrogenase (ADH) and aldehyde dehydrogenase (ALDH) genes and alcohol dependence (AD) have long been studied in many populations, but not comprehensively. In the present study, we genotyped 16 markers within the ADH gene cluster (including the ADH1A, ADH1B, ADH1C, ADH5, ADH6, and ADH7 genes), 4 markers within the ALDH2 gene, and 38 unlinked ancestry-informative markers in a case-control sample of 801 individuals. Associations between markers and disease were analyzed by a Hardy-Weinberg equilibrium (HWE) test, a conventional case-control comparison, a structured association analysis, and a novel diplotype trend regression (DTR) analysis. Finally, the disease alleles were fine mapped by a Hardy-Weinberg disequilibrium (HWD) measure (J). All markers were found to be in HWE in controls, but some markers showed HWD in cases. Genotypes of many markers were associated with AD. DTR analysis showed that ADH5 genotypes and diplotypes of ADH1A, ADH1B, ADH7, and ALDH2 were associated with AD in European Americans and/or African Americans. The risk-influencing alleles were fine mapped from among the markers studied and were found to coincide with some well-known functional variants. We demonstrated that DTR was more powerful than many other conventional association methods. We also found that several ADH genes and the ALDH2 gene were susceptibility loci for AD, and the associations were best explained by several independent risk genes.
机译:这组酒精代谢酶具有相当的遗传和功能复杂性。长期以来,在许多人群中研究了某些酒精脱氢酶(ADH)和醛脱氢酶(ALDH)基因与酒精依赖性(AD)之间的关系,但尚未全面研究。在本研究中,我们对ADH基因簇内的16个标记(包括ADH1A,ADH1B,ADH1C,ADH5,ADH6和ADH7基因)进行了基因分型,在ALDH2基因内对4个标记进行了基因分型,并在一个病例中对38个未关联的祖先信息标记进行了基因分型。对照样本为801个人。通过Hardy-Weinberg平衡(HWE)测试,常规病例对照比较,结构化关联分析和新型双型趋势回归(DTR)分析来分析标记物与疾病之间的关联。最后,通过Hardy-Weinberg不平衡(HWD)测度对疾病等位基因进行精细定位(J)。发现所有标记物均在对照组的HWE中,但某些标记物在病例中显示HWD。许多标志物的基因型与AD相关。 DTR分析显示,在欧洲裔美国人和/或非裔美国人中,ADH5基因型和ADH1A,ADH1B,ADH7和ALDH2的双型与AD相关。从研究的标记中精细地绘制了影响风险的等位基因,并发现它们与一些众所周知的功能变异相吻合。我们证明了DTR比许多其他常规关联方法更强大。我们还发现,几个ADH基因和ALDH2基因是AD的易感基因位点,并且这种关联可以通过几个独立的风险基因得到最好的解释。

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