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红霉素在内质网中与细胞色素P450 3A1/2的差异相互作用:一项CO闪光光解研究。

Differential interaction of erythromycin with cytochromes P450 3A1/2 in the endoplasmic reticulum: a CO flash photolysis study.

作者信息

Koley A P, Dai R, Robinson R C, Markowitz A, Friedman F K

机构信息

Laboratory of Molecular Carcinogenesis, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

Biochemistry. 1997 Mar 18;36(11):3237-41. doi: 10.1021/bi962110h.

Abstract

The kinetics of CO binding to cytochromes P450, measured by the flash photolysis technique, were used to probe the interaction of erythromycin with cytochromes P450 in rat liver microsomes. Addition of erythromycin generates substrate difference spectra using microsomes from rats treated with phenobarbital or dexamethasone but not from untreated rats, showing that it binds to P450s induced by these agents. In contrast, erythromycin and/or a monoclonal antibody to P450 3A1/2 accelerated CO binding to microsomes from rats treated with phenobarbital but had no effect on microsomes from untreated or dexamethasone-treated rats. Based on the differential amounts and inducibilities of the P450 3A1 and 3A2 forms in these microsomal samples, these results indicate that erythromycin increased the rate for P450 3A2 but not P450 3A1. The divergent effects of erythromycin on these P450s, which exhibit 89% sequence similarity, were consistent with a model of the P450 substrate binding site in which erythromycin forms a more rigid complex with P450 3A1 than P450 3A2. These results demonstrate the sensitivity of P450 conformation/dynamics to substrate binding, and show that CO binding kinetics can distinguish among closely related P450s in a microsomal environment.

摘要

通过闪光光解技术测量一氧化碳与细胞色素P450结合的动力学,以此来探究红霉素与大鼠肝微粒体中细胞色素P450的相互作用。添加红霉素后,用苯巴比妥或地塞米松处理过的大鼠的微粒体产生了底物差异光谱,但未处理大鼠的微粒体则未产生,这表明红霉素与这些药物诱导产生的细胞色素P450结合。相反,红霉素和/或针对细胞色素P450 3A1/2的单克隆抗体加速了一氧化碳与用苯巴比妥处理过的大鼠的微粒体的结合,但对未处理或用地塞米松处理过的大鼠的微粒体没有影响。基于这些微粒体样品中细胞色素P450 3A1和3A2形式的不同含量和诱导性,这些结果表明红霉素提高了细胞色素P450 3A2而非细胞色素P450 3A1的反应速率。红霉素对这些具有89%序列相似性的细胞色素P450的不同影响,与细胞色素P450底物结合位点模型一致,即红霉素与细胞色素P450 3A1形成的复合物比与细胞色素P450 3A2形成的复合物更稳定。这些结果证明了细胞色素P450构象/动力学对底物结合的敏感性,并表明一氧化碳结合动力学可以在微粒体环境中区分密切相关的细胞色素P450。

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