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首页> 外文期刊>BMC Genetics >Increased genetic diversity of ADME genes in African Americans compared with their putative ancestral source populations and implications for Pharmacogenomics
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Increased genetic diversity of ADME genes in African Americans compared with their putative ancestral source populations and implications for Pharmacogenomics

机译:与假定的祖传来源种群相比,非洲裔美国人ADME基因的遗传多样性增加,并且对药物基因组学的影响

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Background African Americans have been treated as a representative population for African ancestry for many purposes, including pharmacogenomic studies. However, the contribution of European ancestry is expected to result in considerable differences in the genetic architecture of African American individuals compared with an African genome. In particular, the genetic admixture influences the genomic diversity of drug metabolism-related genes, and may cause high heterogeneity of drug responses in admixed populations such as African Americans. Results The genomic ancestry information of African-American (ASW) samples was obtained from data of the 1000 Genomes Project, and local ancestral components were also extracted for 32 core genes and 252 extended genes, which are associated with drug absorption, distribution, metabolism, and excretion (ADME) genes. As expected, the global genetic diversity pattern in ASW was determined by the contributions of its putative ancestral source populations, and the whole profiles of ADME genes in ASW are much closer to those in YRI than in CEU. However, we observed much higher diversity in some functionally important ADME genes in ASW than either CEU or YRI, which could be a result of either genetic drift or natural selection, and we identified some signatures of the latter. We analyzed the clinically relevant polymorphic alleles and haplotypes, and found that 28 functional mutations (including 3 missense, 3 splice, and 22 regulator sites) exhibited significantly higher differentiation between the three populations. Conclusions Analysis of the genetic diversity of ADME genes showed differentiation between admixed population and its ancestral source populations. In particular, the different genetic diversity between ASW and YRI indicated that the ethnic differences in pharmacogenomic studies are broadly existed despite that African ancestry is dominant in Africans Americans. This study should advance our understanding of the genetic basis of the drug response heterogeneity between populations, especially in the case of population admixture, and have significant implications for evaluating potential inter-population heterogeneity in drug treatment effects.
机译:背景技术出于许多目的,包括药物基因组学研究,非裔美国人被视为非洲血统的代表人群。但是,与非洲基因组相比,欧洲血统的贡献有望导致非裔美国人个体的遗传结构发生巨大差异。特别地,遗传混合物影响药物代谢相关基因的基因组多样性,并可能在诸如非洲裔美国人这样的混合人群中引起药物反应的高度异质性。结果从1000个基因组计划的数据中获得了非裔美国人(ASW)样品的基因组祖先信息,还提取了32个核心基因和252个扩展基因的本地祖先成分,这些成分与药物的吸收,分布,代谢,和排泄(ADME)基因。不出所料,ASW中的全球遗传多样性模式是由其推测的祖先种群的贡献所决定的,ASW中ADME基因的整体概况与YRI中的相似,而与CEU中的相似。但是,我们观察到ASW中某些功能重要的ADME基因比CEU或YRI具有更高的多样性,这可能是遗传漂移或自然选择的结果,我们发现了后者的一些特征。我们分析了临床相关的多态性等位基因和单倍型,发现28个功能性突变(包括3个错义,3个剪接和22个调控位点)在这三个种群之间表现出明显更高的分化。结论对ADME基因遗传多样性的分析表明,混合种群与其祖传种群之间存在差异。特别是,ASW和YRI之间不同的遗传多样性表明,尽管非洲裔在非洲裔美国人中占主导地位,但在药物基因组学研究中种族差异仍然存在。这项研究应增进我们对人群之间药物反应异质性的遗传基础的理解,尤其是在人群混合的情况下,并且对评估药物治疗效果中潜在的种群间异质性具有重要意义。

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