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非洲人群的药物遗传学多样性模式:古代和近代历史的作用

Patterns of pharmacogenetic diversity in African populations: role of ancient and recent history.

作者信息

Oliveira Elisabete, Pereira Rui, Amorim António, McLeod Howard, Prata Maria João

机构信息

Faculty of Sciences, University of Porto and IPATIMUP, 4200-465 Porto, Portugal.

出版信息

Pharmacogenomics. 2009 Sep;10(9):1413-22. doi: 10.2217/pgs.09.74.

Abstract

AIMS

The knowledge that genetic variation influencing drug response is clearly structured among human populations has prompted many studies aimed at obtaining pharmacogenetic profiles in specific populations. While large amounts of data are being produced for populations from developed countries, the African continent still remains very poorly studied. To help to fill this gap, this work characterized three previously uncharacterized African populations for a set of pharmacogenetically relevant polymorphisms.

MATERIALS & METHODS: Seven polymorphic variations in four genes that encode enzymes from phase I (CYP2C9, CYP3A4 and CYP3A5) or phase III (ABCB1) of drug metabolism were analyzed in population samples from Cabinda (n = 107), Mozambique (n = 109) and São Tomé e Príncipe (n = 126). All three populations shared strong recent historical links with Portugal.

RESULTS

The majority of the screened variations displayed large contrasts in allele frequencies between European and African populations, and this study identified a substantial higher European influence in São Tomé e Príncipe than in Cabinda or Mozambique. Admixture analysis demonstrated that the European contribution to the population of São Tomé e Príncipe amounted to 13.3 +/- 3.3%. Furthermore, the proportion of African or European pharmacogenetic ancestry varied widely across each São Tomean individual.

DISCUSSION & CONCLUSION: This implies that genetic association studies conducted in São Tomé e Príncipe should take into account the confounding factor of admixture to avoid spurious positive or negative results. Our findings also indicate that drug dosage requirements may be different in São Tomé e Príncipe than in other African populations. Thus, the search for pharmacogenetic risk factors should be assessed at an individual level, therefore fulfilling the perspective of personalized medicine. This study further indicates that the common notion of 'African population' might hide a pattern of pharmacogenetic heterogeneity whose real extent still needs to be evaluated by means of a refined sampling of the entire continent.

摘要

目的

已知影响药物反应的基因变异在人类群体中具有明显的结构差异,这促使许多研究致力于获取特定群体的药物遗传学特征。虽然发达国家群体已产生大量数据,但非洲大陆的研究仍非常匮乏。为填补这一空白,本研究对三个此前未被描述的非洲群体的一组与药物遗传学相关的多态性进行了特征分析。

材料与方法

在来自卡宾达(n = 107)、莫桑比克(n = 109)和圣多美和普林西比(n = 126)的群体样本中,分析了四个基因中的七个多态性变异,这些基因编码药物代谢I期(CYP2C9、CYP3A4和CYP3A5)或III期(ABCB1)的酶。这三个群体都与葡萄牙有着密切的近代历史联系。

结果

大多数筛选出的变异在欧洲和非洲群体的等位基因频率上表现出巨大差异,并且本研究发现圣多美和普林西比受欧洲的影响明显高于卡宾达或莫桑比克。混合分析表明,欧洲对圣多美和普林西比群体的贡献为13.3±3.3%。此外,每个圣多美个体的非洲或欧洲药物遗传学血统比例差异很大。

讨论与结论

这意味着在圣多美和普林西比进行的基因关联研究应考虑混合的混杂因素,以避免出现虚假的阳性或阴性结果。我们的研究结果还表明,圣多美和普林西比的药物剂量需求可能与其他非洲群体不同。因此,应在个体水平上评估药物遗传学风险因素,从而实现个性化医疗的目标。本研究进一步表明,“非洲群体”这一普遍概念可能掩盖了药物遗传学异质性模式,其实际程度仍需通过对整个非洲大陆进行精细抽样来评估。

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