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Molecular population genetics of human CYP3A locus: signatures of positive selection and implications for evolutionary environmental medicine.

机译:人类CYP3A基因座的分子群体遗传学:阳性选择的标志及其对进化环境医学的影响。

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BACKGROUND: The human CYP3A gene cluster codes for cytochrome P450 (CYP) subfamily enzymes that catalyze the metabolism of various exogenous and endogenous chemicals and is an obvious candidate for evolutionary and environmental genomic study. Functional variants in the CYP3A locus may have undergone a selective sweep in response to various environmental conditions. OBJECTIVE: The goal of this study was to profile the allelic structure across the human CYP3A locus and investigate natural selection on that locus. METHODS: From the CYP3A locus spanning 231 kb, we resequenced 54 genomic DNA fragments (a total of 43,675 bases) spanning four genes (CYP3A4, CYP3A5, CYP3A7, and CYP3A43) and two pseudogenes (CYP3AP1 and CYP3AP2), and randomly selected intergenic regions at the CYP3A locus in Africans (24 individuals), Caucasians (24 individuals), and Chinese (29 individuals). We comprehensively investigated the nucleotide diversity and haplotype structure and examined the possible role of natural selection in shaping the sequence variation throughout the gene cluster. RESULTS: Neutrality tests with Tajima's D, Fu and Li's D* and F*, and Fay and Wu's H indicated possible roles of positive selection on the entire CYP3A locus in non-Africans. Sliding-window analyses of nucleotide diversity and frequency spectrum, as well as haplotype diversity and phylogenetically inferred haplotype structure, revealed that CYP3A4 and CYP3A7 had recently undergone or were undergoing a selective sweep in all three populations, whereas CYP3A43 and CYP3A5 were undergoing a selective sweep in non-Africans and Caucasians, respectively. CONCLUSION: The refined allelic architecture and selection spectrum for the human CYP3A locus highlight that evolutionary dynamics of molecular adaptation may underlie the phenotypic variation of the xenobiotic disposition system and varied predisposition to complex disorders in which xenobiotics play a role.
机译:背景:人类CYP3A基因簇编码细胞色素P450(CYP)亚家族酶,可催化各种外源和内源化学物质的代谢,并且是进行进化和环境基因组研究的明显候选者。 CYP3A基因座中的功能变体可能已响应各种环境条件进行了选择性清除。目的:本研究的目的是分析整个人CYP3A基因座的等位基因结构,并研究该基因座上的自然选择。方法:从跨越231 kb的CYP3A基因座,我们重新测序了54个基因组DNA片段(共43,675个碱基),跨越了四个基因(CYP3A4,CYP3A5,CYP3A7和CYP3A43)和两个假基因(CYP3AP1和CYP3AP2),并随机选择了基因间区域CYP3A基因座位点在非洲人(24人),白种人(24人)和中国人(29人)中。我们全面研究了核苷酸多样性和单倍型结构,并检查了自然选择在塑造整个基因簇的序列变异中的可能作用。结果:用田岛D,Fu和Li的D *和F *以及Fay和Wu的H进行的中性测试表明,在非非洲人群中,对整个CYP3A基因座进行阳性选择可能具有积极作用。对核苷酸多样性和频谱以及单倍型多样性和系统发育推断的单倍型结构的滑动窗口分析显示,CYP3A4和CYP3A7最近在所有三个族群中经历或正在进行选择性扫描,而CYP3A43和CYP3A5正在进行选择性扫描分别在非非洲人和高加索人中。结论:人类CYP3A基因座的精细等位基因结构和选择光谱突出表明,分子适应性的进化动力学可能是异种生物素配置系统的表型变异的基础,并且是易受异种生物素影响的复杂疾病的易感性。

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