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六种新的非同义CYP1A2基因多态性:天然存在的变异酶的催化活性

Six novel nonsynonymous CYP1A2 gene polymorphisms: catalytic activities of the naturally occurring variant enzymes.

作者信息

Murayama Norie, Soyama Akiko, Saito Yoshiro, Nakajima Yukiko, Komamura Kazuo, Ueno Kazuyuki, Kamakura Shiro, Kitakaze Masafumi, Kimura Hideo, Goto Yu-ichi, Saitoh Osamu, Katoh Masaaki, Ohnuma Teiichi, Kawai Mitsuru, Sugai Kenji, Ohtsuki Taisuke, Suzuki Chieko, Minami Narihiro, Ozawa Shogo, Sawada Jun-ichi

机构信息

Project Team for Pharmacogenetics, National Institute of Health Sciences, Tokyo, Japan.

出版信息

J Pharmacol Exp Ther. 2004 Jan;308(1):300-6. doi: 10.1124/jpet.103.055798. Epub 2003 Oct 16.

Abstract

Six novel nonsynonymous nucleotide alterations were found in the cytochrome P450 1A2 gene in a Japanese population, which resulted in the following amino acid substitutions: T83M, E168Q, F186L, S212C, G299A, and T438I. These individuals were heterozygous for the amino acid substitutions. The potential functional alterations caused by the amino acid substitutions were characterized by a cDNA-mediated expression system using Chinese hamster V79 cells. Among the six CYP1A2 variants, F186L showed the most profound and statistically significant reduction in O-deethylation of phenacetin and 7-ethoxyresorufin. Kinetic analyses performed for the ethoxyresorufin O-deethylation revealed that the Vmax of the F186L variant was approximately 5% of that of the CYP1A2 wild type, despite a 5-fold lower Km value of the variant, the consequence of which was reduced enzymatic activity toward the substrate. Thus, for the first time, phenylalanine at residue 186 is suggested to be a critical amino acid for catalytic activity.

摘要

在日本人群的细胞色素P450 1A2基因中发现了6种新的非同义核苷酸改变,这些改变导致了以下氨基酸替换:T83M、E168Q、F186L、S212C、G299A和T438I。这些个体的氨基酸替换为杂合状态。利用中国仓鼠V79细胞的cDNA介导表达系统对氨基酸替换引起的潜在功能改变进行了表征。在这6种CYP1A2变体中,F186L对非那西丁和7-乙氧基试卤灵的O-脱乙基作用表现出最显著且具有统计学意义的降低。对乙氧基试卤灵O-脱乙基作用进行的动力学分析表明,尽管F186L变体的Km值低5倍,但其Vmax约为CYP1A2野生型的5%,其结果是对底物的酶活性降低。因此,首次表明186位残基的苯丙氨酸是催化活性的关键氨基酸。

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