首页> 外文期刊>Biochemical Pharmacology >Human CYP2C-mediated stereoselective phenytoin hydroxylation in Japanese: difference in chiral preference of CYP2C9 and CYP2C19.
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Human CYP2C-mediated stereoselective phenytoin hydroxylation in Japanese: difference in chiral preference of CYP2C9 and CYP2C19.

机译:日语中人CYP2C介导的立体选择性苯妥英羟化:CYP2C9和CYP2C19手性偏好的差异。

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摘要

Regio- and stereoselective hydroxylation of phenytoin was determined in liver microsomes of nine extensive (EM) and three poor metabolizers (PM) of mephenytoin. Hydroxyphenytoins (HPPH) were isolated and quantified after separation into four regio- and stereoisomers. The total rates of microsomal phenytoin 4'- hydroxylation were approximately 3-fold higher than those of 3'-hydroxylation, and not significantly different in EM and PM. Formation of 4'-(R)-HPPH was 4.4-fold higher in EM than in PM, whereas no clear differences between EM and PM were detected in the formation of 4'-(S)-, 3'-(R)-, and 3'-(S)-HPPH. Cytochrome P450 (CYP)2C9, expressed in a fission yeast, Schizosaccharomyces pombe, catalyzed the formation of 4'-(R)- and 4'-(S)-HPPH stereoselectively, as observed with EM, in which predominantly 4'-(S)-HPPH was formed. Recombinant CYP2C19 was more stereoselective for 4'-(R)-HPPH formation. These results, in addition to inhibition experiments with anti-human CYP2C antibody, indicate that phenytoin hydroxylation is mainly catalyzed by CYP2C9. Furthermore, CYP2C19 showed limited contribution to phenytoin 4'-hydroxylation with a different chiral preference from CYP2C9.
机译:在苯妥英的9种广泛(EM)和3种不良代谢者(PM)的肝微粒体中测定了苯妥英的区域和立体选择性羟基化。将羟苯妥英(HPPH)分离并分离为四个区域和立体异构体后进行定量。微粒体苯妥英4'-羟基化的总速率比3'-羟基化的总速率高约3倍,并且在EM和PM中无显着差异。 EM中4'-(R)-HPPH的形成比PM高4.4倍,而在4'-(S)-,3'-(R)-的形成中未检测到EM和PM之间的明显差异。 ,和3'-(S)-HPPH。在裂殖酵母粟酒裂殖酵母中表达的细胞色素P450(CYP)2C9选择性催化4'-(R)-和4'-(S)-HPPH的形成,如EM观察到的,其中主要是4'-(( S)-HPPH形成。重组CYP2C19对4'-(R)-HPPH形成更具立体选择性。这些结果,除了用抗人CYP2C抗体进行抑制实验外,还表明苯妥英羟化反应主要由CYP2C9催化。此外,CYP2C19对苯妥英4'-羟基化的贡献有限,具有与CYP2C9不同的手性偏好。

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