Allelic, genotypic and phenotypic distributions of S-mephenytoin 4'-hydroxylase (CYP2C19) in healthy Caucasian populations of European descent throughout the world.

Xie HG; Stein CM; Kim RB; Wilkinson GR; Flockhart DA; Wood AJ

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Allelic, genotypic and phenotypic distributions of S-mephenytoin 4'-hydroxylase (CYP2C19) in healthy Caucasian populations of European descent throughout the world.

机译：S-美芬妥英4'-羟化酶（CYP2C19）在欧洲人的欧洲后裔的健康高加索人群中的等位基因，基因型和表型分布。

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Impaired S-mephenytoin 4'-hydroxylation is a well-described genetic polymorphism affecting drug metabolism in humans. The reported population prevalence of the CYP2C19 poor metabolizer phenotype in Caucasians of European descent has been described as ranging from 0.9% to 7.7%. To address the question of whether the difference in the frequency of poor metabolizers represents an ethnic genetic microheterogeneity in the structure and expression of the CYP2C19 gene in Caucasian individuals, we performed a pooled analysis of available studies. Combined data from the 22 homogeneous studies showed that the frequency of poor metabolizers in healthy unrelated Caucasians determined by phenotyping was 2.8% (110 of 3990; 95% confidence interval 2.3-3.3). Data obtained from eight homogeneous studies that determined the frequency of poor metabolizers by genotyping showed that the genotypic frequency of poor metabolizers was 2.1% (28 of 1356; 95% confidence interval 1.3-2.8), consistent with the poor metabolizer frequency determined by phenotyping. In the extensive metabolizers, 26% (471 of 1786; 95% confidence interval 24.4-28.4) were heterozygotes. The observed frequencies of the three Mendelian genotypes were 73% for wt/wt, 26% for wt/m, and 2.1% for m/m. Based on the overall phenotypic poor metabolizer frequency of 2.8%, the expected genotypic frequencies were 69% for wt/wt, 28% for wt/m and 2.8% for m/m, which are in good agreement to the observed values. However, in the 84 Caucasian phenotyped and genotyped poor metabolizers, approximately 10% of the putative poor metabolizer alleles (17 of 168) were unknown. This study provides a systematic overview of the population distribution of the CYP2C19 poor metabolizer phenotype and CYP2C19 alleles and genotypes in healthy Caucasians living in different geographical areas, and shows a similar polymorphic pattern in the structure and expression of the CYP2C19 gene in the worldwide Caucasian populations.

机译：S-美芬妥英4'-羟基化受损是一种众所周知的影响人类药物代谢的遗传多态性。据报道，欧洲血统的白种人中CYP2C19弱代谢者表型的人群患病率在0.9％至7.7％之间。为了解决低级代谢者频率差异是否代表白种人个体中CYP2C19基因的结构和表达中的种族遗传微异质性的问题，我们对现有研究进行了汇总分析。来自22项同类研究的综合数据显示，通过表型分析确定的健康无亲缘关系的高加索人中不良代谢者的发生率为2.8％（3990的110; 95％的置信区间2.3-3.3）。从八项通过基因分型确定不良代谢物频率的同类研究中获得的数据表明，不良代谢物的基因型频率为2.1％（1356年为28; 95％置信区间1.3-2.8），与通过表型确定的不良代谢物频率一致。在广泛的代谢者中，杂合子占26％（1786年的471; 95％的置信区间24.4-28.4）。三种孟德尔基因型的观察频率分别为wt / wt的73％，wt / m的26％和m / m的2.1％。基于2.8％的总体表型不良代谢频率，预期的基因型频率为wt / wt为69％，wt / m为28％和m / m为2.8％，这与观察值非常吻合。但是，在84个白种人的表型和基因型不良代谢者中，大约10％的假定不良代谢者等位基因（168个中的17个）是未知的。这项研究为生活在不同地理区域的健康白种人中CYP2C19弱代谢者表型和CYP2C19等位基因和基因型的人群分布提供了系统的概述，并显示了在全球白种人人群中CYP2C19基因的结构和表达具有相似的多态性模式。。

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《Pharmacogenetics》 |1999年第5期|共11页
作者
Xie HG; Stein CM; Kim RB; Wilkinson GR; Flockhart DA; Wood AJ;
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正文语种 eng
中图分类生药学（天然药物学）;
关键词
Caucasoid Race; Cytochrome P-450; Hydroxylases; mephenytoin-4-hydroxylase; 高加索人种; 细胞色素P-450; 羟化酶类;

机译：Caucasoid Race;Cytochrome P-450;Hydroxylases;mephenytoin-4-hydroxylase;高加索人种;细胞色素P-450;羟化酶类;

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1. Allelic, genotypic and phenotypic distributions of S-mephenytoin 4'-hydroxylase (CYP2C19) in healthy Caucasian populations of European descent throughout the world. [J] . Xie HG, Stein CM, Kim RB, Pharmacogenetics . 1999,第5期

机译：S-美芬妥英4'-羟化酶（CYP2C19）在欧洲人的欧洲后裔的健康高加索人群中的等位基因，基因型和表型分布。
2. An additional defective allele, CYP2C19*5, contributes to the S-mephenytoin poor metabolizer phenotype in Caucasians. [J] . Ibeanu GC, Blaisdell J, Ghanayem BI, Pharmacogenetics . 1998,第2期

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Allelic, genotypic and phenotypic distributions of S-mephenytoin 4'-hydroxylase (CYP2C19) in healthy Caucasian populations of European descent throughout the world.

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