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日本人和高加索人群肝脏微粒体中细胞色素P4502J2表达及催化活性的个体间差异。

Inter-individual variation of cytochrome P4502J2 expression and catalytic activities in liver microsomes from Japanese and Caucasian populations.

作者信息

Yamazaki H, Okayama A, Imai N, Guengerich F P, Shimizu M

机构信息

Laboratory of Drug Metabolism and Pharmacokinetics, Showa Pharmaceutical University, Machida, Tokyo, Japan.

出版信息

Xenobiotica. 2006 Dec;36(12):1201-9. doi: 10.1080/00498250600944318.

Abstract

The aim of this study was to investigate the inter-individual variations in cytochrome P4502J2 (CYP2J2) and its typical drug oxidation activities in human liver microsomes in both Japanese and Caucasian populations. CYP2J2 contents were determined immunochemically in liver microsomes from 20 Japanese and 29 Caucasian samples using recombinant CYP2J2 commercially available as a standard. Ebastine hydroxylation and astemizole O-demethylation activities were compared. The CYP2J2 genotype was determined by direct sequencing of liver genomic DNA. The mean expression levels of CYP2J2 determined immunochemically in liver microsomes from Japanese and Caucasian samples were 2.0 +/- 1.5 and 1.2 +/- 2.1 pmol CYP2J2 mg-1 protein (mean +/- standard deviation), respectively, accounting for 1.8 +/- 1.1% and 0.52 +/- 0.65% of the total hepatic P450 content (0.15 +/- 0.19 and 0.27 +/- 0.14 nmol P450 mg-1 protein, respectively). The individual variation of the two marker drug oxidation activities could not be fully accounted for by the CYP2J2 contents or currently known CYP2J2 genotypes. The amounts of CYP2J2 in liver microsomes with the CYP2J2*7 allele (-76G>T) were decreased to 39% compared with those of liver microsomes from other individuals. The results indicate that CYP2J2 accounts for approximately 1-2% of total P450 in human liver microsomes. The information about large inter-individual variation of the CYP2J2 suggests that this enzyme plays a significant role in the metabolism of xenobiotics and may be useful in in-silico simulations of drug disposition.

摘要

本研究旨在调查日本人和高加索人群中细胞色素P4502J2(CYP2J2)的个体间差异及其在人肝微粒体中的典型药物氧化活性。使用市售重组CYP2J2作为标准品,通过免疫化学方法测定了20份日本人和29份高加索人样本肝微粒体中的CYP2J2含量。比较了依巴斯汀羟基化和阿司咪唑O-去甲基化活性。通过对肝脏基因组DNA进行直接测序确定CYP2J2基因型。通过免疫化学方法测定的日本人和高加索人样本肝微粒体中CYP2J2的平均表达水平分别为2.0±1.5和1.2±2.1 pmol CYP2J2 mg-1蛋白(平均值±标准差),分别占肝脏总P450含量的1.8±1.1%和0.52±0.65%(分别为0.15±0.19和0.27±0.14 nmol P450 mg-1蛋白)。两种标记药物氧化活性的个体差异不能完全由CYP2J2含量或目前已知的CYP2J2基因型来解释。与其他个体的肝微粒体相比,携带CYP2J2*7等位基因(-76G>T)的肝微粒体中CYP2J2的含量降低至39%。结果表明,CYP2J2约占人肝微粒体总P450的1-2%。关于CYP2J2个体间差异较大的信息表明,该酶在异源生物代谢中起重要作用,可能有助于药物处置的计算机模拟。

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