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在肝脏和小肠组织中表达的狨猴细胞色素P450 3A4直系同源物可有效代谢咪达唑仑、阿普唑仑、硝苯地平和睾酮。

Marmoset Cytochrome P450 3A4 Ortholog Expressed in Liver and Small-Intestine Tissues Efficiently Metabolizes Midazolam, Alprazolam, Nifedipine, and Testosterone.

作者信息

Uehara Shotaro, Uno Yasuhiro, Nakanishi Kazuyuki, Ishii Sakura, Inoue Takashi, Sasaki Erika, Yamazaki Hiroshi

机构信息

Laboratory of Drug Metabolism and Pharmacokinetics, Showa Pharmaceutical University, Machida, Tokyo, Japan (S.U., K.N., S.I., H.Y.); Pharmacokinetics and Bioanalysis Center, Shin Nippon Biomedical Laboratories, Ltd., Kainan, Wakayama, Japan (Y.U.); Department of Applied Developmental Biology (T.I.), and Center of Applied Developmental Biology (E.S.), Central Institute for Experimental Animals, Kawasaki, Japan; and Keio Advanced Research Center, Keio University, Minato-ku, Tokyo, Japan (E.S.).

Laboratory of Drug Metabolism and Pharmacokinetics, Showa Pharmaceutical University, Machida, Tokyo, Japan (S.U., K.N., S.I., H.Y.); Pharmacokinetics and Bioanalysis Center, Shin Nippon Biomedical Laboratories, Ltd., Kainan, Wakayama, Japan (Y.U.); Department of Applied Developmental Biology (T.I.), and Center of Applied Developmental Biology (E.S.), Central Institute for Experimental Animals, Kawasaki, Japan; and Keio Advanced Research Center, Keio University, Minato-ku, Tokyo, Japan (E.S.)

出版信息

Drug Metab Dispos. 2017 May;45(5):457-467. doi: 10.1124/dmd.116.074898. Epub 2017 Feb 14.

Abstract

Common marmosets (), small New World primates, are increasingly attracting attention as potentially useful animal models for drug development. However, characterization of cytochrome P450 (P450) 3A enzymes involved in the metabolism of a wide variety of drugs has not investigated in marmosets. In this study, sequence homology, tissue distribution, and enzymatic properties of marmoset P450 3A4 ortholog, 3A5 ortholog, and 3A90 were investigated. Marmoset P450 3A forms exhibited high amino acid sequence identities (88-90%) to the human and cynomolgus monkey P450 3A orthologs and evolutionary closeness to human and cynomolgus monkey P450 3A orthologs compared with other P450 3A enzymes. Among the five marmoset tissues examined, P450 3A4 ortholog mRNA was abundant in livers and small intestines where P450 3A4 ortholog proteins were immunologically detected. Three marmoset P450 3A proteins heterologously expressed in membranes catalyzed midazolam 1'- and 4-hydroxylation, alprazolam 4-hydroxylation, nifedipine oxidation, and testosterone 6-hydroxylation, similar to cynomolgus monkey and human P450 3A enzymes. Among the marmoset P450 3A enzymes, P450 3A4 ortholog effectively catalyzed midazolam 1'-hydroxylation, comparable to microsomes from marmoset livers and small intestines. Correlation analyses with 23 individual marmoset liver microsomes suggested contributions of P450 3A enzymes to 1'-hydroxylation of both midazolam (human P450 3A probe) and bufuralol (human P450 2D6 probe), similar to cynomolgus monkey P450 3A enzymes. These results indicated that marmoset P450 3A forms had functional characteristics roughly similar to cynomolgus monkeys and humans in terms of tissue expression patterns and catalytic activities, suggesting marmosets as suitable animal models for P450 3A-dependent drug metabolism.

摘要

普通狨猴是一种小型新大陆灵长类动物,作为药物开发潜在的有用动物模型,正越来越受到关注。然而,普通狨猴中参与多种药物代谢的细胞色素P450(P450)3A酶的特性尚未得到研究。在本研究中,对普通狨猴P450 3A4直系同源物、3A5直系同源物和3A90的序列同源性、组织分布及酶学性质进行了研究。普通狨猴P450 3A形式与人类和食蟹猴P450 3A直系同源物表现出较高的氨基酸序列同一性(88 - 90%),与其他P450 3A酶相比,与人类和食蟹猴P450 3A直系同源物在进化上更为接近。在所检测的普通狨猴的五种组织中,P450 3A4直系同源物mRNA在肝脏和小肠中含量丰富,且在这些组织中通过免疫检测到了P450 3A4直系同源物蛋白。在细胞膜中异源表达的三种普通狨猴P450 3A蛋白催化咪达唑仑1'-和4-羟基化、阿普唑仑4-羟基化、硝苯地平氧化以及睾酮6-羟基化,类似于食蟹猴和人类P450 3A酶。在普通狨猴P450 3A酶中,P450 3A4直系同源物有效地催化咪达唑仑1'-羟基化,与普通狨猴肝脏和小肠的微粒体相当。对23个普通狨猴肝脏微粒体进行的相关性分析表明,P450 3A酶对咪达唑仑(人类P450 3A探针)和布非洛尔(人类P450 2D6探针)的1'-羟基化均有贡献,类似于食蟹猴P450 3A酶。这些结果表明,普通狨猴P450 3A形式在组织表达模式和催化活性方面具有与食蟹猴和人类大致相似的功能特征,这表明普通狨猴是P450 3A依赖性药物代谢的合适动物模型。

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