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中国人群中S-美芬妥英多态性的遗传分析。

Genetic analysis of the S-mephenytoin polymorphism in a Chinese population.

作者信息

de Morais S M, Goldstein J A, Xie H G, Huang S L, Lu Y Q, Xia H, Xiao Z S, Ile N, Zhou H H

机构信息

Laboratory of Biochemical Risk Analysis, National Institute of Environmental Health Sciences, Research Triangle Park 27709, USA.

出版信息

Clin Pharmacol Ther. 1995 Oct;58(4):404-11. doi: 10.1016/0009-9236(95)90053-5.

Abstract

The 4'-hydroxylation of S-mephenytoin exhibits a polymorphism in humans, with the poor metabolizer phenotype exhibiting a lower frequency in white (3% to 5%) than in Oriental populations (13% to 23%). Two mutations in CYP2C19 (CYP2C19m1 and CYP2C19m2) have recently been described that account for approximately 85% of white and 100% of Japanese poor metabolizers. This study examines whether these mutations account for the poor metabolizer phenotype in the Chinese population. The metabolism of S-mephenytoin exhibited a bimodal distribution in 244 unrelated Chinese subjects, although the distribution of the two phenotypes overlapped. In 75 selected Chinese subjects, CYP2C19 genotype analysis predicted the phenotype with 100% accuracy. The frequency of the poor metabolizer phenotype was approximately 11% (95% confidence interval 7% to 15%). The frequency of the CYP2C19m1 allele was 0.289, whereas that of CYP2C19m2 was 0.044. Homozygous extensive metabolizers had slightly lower ratios of S/R-mephenytoin compared with heterozygous extensive metabolizers, showing a gene-dosage effect. These data show the advantages of genotype analysis in investigations of the mephenytoin phenotype in Oriental subjects.

摘要

S-美芬妥因的4'-羟化在人类中表现出多态性,慢代谢者表型在白种人中的频率(3%至5%)低于东方人群(13%至23%)。最近描述了CYP2C19中的两种突变(CYP2C19m1和CYP2C19m2),它们约占白种人慢代谢者的85%,占日本慢代谢者的100%。本研究探讨这些突变是否可解释中国人群中的慢代谢者表型。S-美芬妥因的代谢在244名无亲缘关系的中国受试者中呈双峰分布,尽管两种表型的分布有重叠。在75名选定的中国受试者中,CYP2C19基因型分析对表型的预测准确率为100%。慢代谢者表型的频率约为11%(95%置信区间为7%至15%)。CYP2C19m1等位基因的频率为0.289,而CYP2C19m2的频率为0.044。与杂合子快代谢者相比,纯合子快代谢者的S/R-美芬妥因比值略低,显示出基因剂量效应。这些数据显示了基因型分析在东方受试者美芬妥因表型研究中的优势。

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