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潜在有害的功能变异体含黄素单加氧酶2*1在撒哈拉以南非洲地区的出现频率很高。

The potentially deleterious functional variant flavin-containing monooxygenase 2*1 is at high frequency throughout sub-Saharan Africa.

作者信息

Veeramah Krishna R, Thomas Mark G, Weale Michael E, Zeitlyn David, Tarekegn Ayele, Bekele Endashaw, Mendell Nancy R, Shephard Elizabeth A, Bradman Neil, Phillips Ian R

机构信息

The Centre for Genetic Anthropology, Research Department of Genetics, University College, London, UK.

出版信息

Pharmacogenet Genomics. 2008 Oct;18(10):877-86. doi: 10.1097/FPC.0b013e3283097311.

Abstract

BACKGROUND

The drug-metabolizing enzyme flavin-containing monooxygenase 2 (FMO2) is the predominant FMO isoform present in the lung of most mammals, including non-human primates. All Europeans and Asians tested have been shown to be homozygous for a non-functional variant, FMO22A, which contains a premature stop codon due to a single-nucleotide change in exon 9 (g.23238C>T). The ancestral allele, FMO21, encodes a functionally active protein and has been found in African-Americans (26%) and Hispanics (2% to 7%). Possessing this variant increases the risk of pulmonary toxicity when exposed to thioureas, a widely used class of industrial compounds. FMO2 may also be involved in the metabolism of drugs that are used to treat diseases that are prevalent in Africa.

RESULTS AND CONCLUSION

We conducted a survey of g.23238C>T variation across Africa that revealed that the distribution of this SNP is relatively homogeneous across sub-Saharan Africa, with approximately one third of individuals possessing at least one FMO2*1 allele, though in some populations the incidence of these individuals approached 50%. Thus many sub-Saharan Africans may be at substantially increased health risk when encountering thiourea-containing substrates of FMO2. Analysis of HapMap data with the Long-Range Haplotype test found no evidence for positive selection of either 23238C>T allele and maximum-likelihood coalescent analysis indicated that this mutation occurred some 500,000 years before present. This study demonstrates the value of performing genetic surveys in Africa, a continent in which human genetic diversity is thought to be greatest, but where studies of the distribution of this diversity are few.

摘要

背景

药物代谢酶含黄素单加氧酶2(FMO2)是包括非人灵长类动物在内的大多数哺乳动物肺中存在的主要FMO亚型。所有接受检测的欧洲人和亚洲人都被证明是无功能变异体FMO22A的纯合子,该变异体由于外显子9中的单核苷酸变化(g.23238C>T)而含有一个提前终止密码子。祖先等位基因FMO21编码一种功能活跃的蛋白质,在非裔美国人(26%)和西班牙裔(2%至7%)中被发现。拥有这种变异体会增加接触硫脲(一种广泛使用的工业化合物类别)时发生肺毒性的风险。FMO2也可能参与用于治疗非洲流行疾病的药物的代谢。

结果与结论

我们对非洲各地g.23238C>T变异进行了调查,结果显示该单核苷酸多态性(SNP)在撒哈拉以南非洲地区的分布相对均匀,约三分之一的个体至少拥有一个FMO2*1等位基因,不过在一些人群中,这些个体的发生率接近50%。因此,许多撒哈拉以南非洲人在接触含硫脲的FMO2底物时,健康风险可能会大幅增加。使用长程单倍型检验对HapMap数据进行分析,未发现对23238C>T任何一个等位基因进行正选择的证据,最大似然合并分析表明该突变发生在距今约50万年前。这项研究证明了在非洲进行基因调查的价值,非洲被认为是人类遗传多样性最大的大陆,但对这种多样性分布的研究却很少。

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