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Distribution of CYP2D6 and CYP2C19 Polymorphisms Associated with Poor Metabolizer Phenotype in Five Amerindian Groups and Western Mestizos from Mexico

机译:CYP2D6和CYP2C19基因多态性与不良代谢者表型相关的分布在墨西哥的五个美洲印第安人群体和西方混血儿中

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摘要

Background: The distribution of polymorphisms in the CYP2D6 and CYP2C19 genes allows inferring the potential risk for specific adverse drug reactions and lack of therapeutic effects in humans. This variability shows differences among human populations. The aim of this study was to analyze single-nucleotide polymorphisms related to a poor metabolizer (PM) phenotype in nonpreviously studied Amerindian groups and Mestizos (general admixed population) from Mexico. Methods: We detected by SNaPshot® different polymorphisms located in CYP2D6 (*3, *4, *6, *7, and *8) and CYP2C19 (*2, *3, *4 and *5) in western Mestizos (n=145) and five Amerindian groups from Mexico: Tarahumaras from the North (n=88); Purépechas from the Center (n=101); and Tojolabales (n=68), Tzotziles (n=88), and Tzeltales (n=20) from the Southeast. Genotypes were observed by capillary electrophoresis. The genetic relationships among these populations were estimated based on these genes. Results and Discussion: The wild-type allele (*1) of both genes was predominant in the Mexican populations studied. The most widely observed alleles were CYP2C19*2 (range, 0%–31%) and CYP2D6*4 (range, 1.2%–7.3%), whereas CYP2D6*3 was exclusively detected in Mestizos. Conversely, CYP2C19*4 and *5, as well as CYP2D6*3, *6, *7, and *8, were not observed in the majority of the Mexican populations. The Tarahumaras presented a high frequency of the allele CYP2C19*2 (31%) and of homozygotes *2/*2 (10.7%), which represent a high frequency of potentially PM phenotypes in this Amerindian group. The genetic distances showed high differentiation of Tarahumaras (principally for CYP2C19 gene). In general, a relative proximity was observed between most of the Amerindian, Mexican-Mestizo, and Latin-American populations. Conclusion: In general, the wild-type allele (*1) predominates in Mexican populations, outlining a relatively homogeneous distribution for CYP2C19 and CYP2D6. The exception is the Tarahumara group that displays a potentially increased risk for adverse reactions to CYP2C19-metabolized drugs.
机译:背景:CYP2D6和CYP2C19基因中的多态性分布可推断出特定药物不良反应的潜在风险以及对人类缺乏治疗作用。这种变异性显示了人类之间的差异。这项研究的目的是分析与墨西哥以前未曾研究过的美洲印第安人群体和混血儿(一般混血人群)的不良代谢者(PM)表型有关的单核苷酸多态性。方法:我们通过SNaPshot ®检测到位于CYP2D6(* 3,* 4,* 6,* 7和* 8)和CYP2C19(* 2,* 3,* 4和* 5)的不同多态性)在西部Mestizos(n = 145)和来自墨西哥的五个美洲印第安人群体:来自北部的Tarahumaras(n = 88);来自中心的Purépechas(n = 101);和东南部的托霍拉巴列斯(n = 68),Tzotziles(n = 88)和Tzeltales(n = 20)。通过毛细管电泳观察基因型。基于这些基因估计了这些种群之间的遗传关系。结果与讨论:在研究的墨西哥人群中,这两个基因的野生型等位基因(* 1)占主导地位。观察到最广泛的等位基因为 CYP2C19 * 2 (范围为0%–31%)和 CYP2D6 * 4 (范围为1.2%–7.3%),而 CYP2D6 * 3 仅在Mestizos中发现。相反, CYP2C19 * 4 * 5 以及 CYP2D6 * 3,* 6,* 7, * 8 < / em>,在大多数墨西哥人口中均未观察到。 Tarahumaras表现出高频率的等位基因 CYP2C19 * 2 (31%)和纯合子 * 2 / * 2 (10.7%),这代表了潜在的高频率该美洲印第安人组中的PM表型。遗传距离显示出Tarahumaras的高度分化(主要是 CYP2C19 基因)。通常,在大多数美洲印第安人,墨西哥混血儿和拉丁美洲人口之间观察到相对亲近。 结论:通常,野生型等位基因(* 1)在墨西哥人群中占主导地位,概述了 CYP2C19 CYP2D6 相对均匀的分布。 Tarahumara组除外,它对CYP2C19代谢药物产生不良反应的风险可能增加。

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