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细胞色素P-450 2D亚家族对大鼠肝微粒体中普萘洛尔代谢的区域选择性贡献。

Regioselective contribution of the cytochrome P-450 2D subfamily to propranolol metabolism in rat liver microsomes.

作者信息

Masubuchi Y, Kagimoto N, Narimatsu S, Fujita S, Suzuki T

机构信息

Laboratory of Biopharmaceutics, Faculty of Pharmaceutical Sciences, Chiba University, Japan.

出版信息

Drug Metab Dispos. 1993 Nov-Dec;21(6):1012-6.

PMID:7905378
Abstract

The metabolism of propranolol was examined by using microsomes from Dark Agouti rats known as a poor-metabolizer animal model for debrisoquine 4-hydroxylation and Wistar rats. Propranolol 4- and 5-hydroxylations followed biphasic Michaelis-Menten kinetics, and 7-hydroxylation and N-desisopropylation were monophasic in both strains. The kinetic studies showed that the Vmax for propranolol 7-hydroxylase activity and the Vmax of high-affinity phases for propranolol 4- and 5-hydroxylase activities were markedly low in Dark Agouti rats compared with those in Wistar rats. The antibody against a cytochrome P-450 isozyme, P-450BTL (Suzuki, T., et al., Drug Metab. Dispos. 20, 367-373, 1992), belonging to the CYP2D subfamily, inhibited by 90% propranolol 4-, 5-, and 7-hydroxylase activities in liver microsomes from male Wistar rats at a low propranolol concentration (5 microM). However, less inhibitory effects of the antibody on propranolol 4- and 5-hydroxylase activities were observed at a high propranolol concentration (1 mM), whereas a similar inhibitory effect of the antibody on propranolol 7-hydroxylase activity was shown. The antibody inhibited propranolol N-desisopropylase activity, but less extent of the inhibition on this activity than those on ring-hydroxylase activities was observed at the low and high propranolol concentrations. These results indicate that a polymorphic cytochrome P-450 isozyme(s) belonging to the CYP2D subfamily is involved predominantly in propranolol 4-, 5-, and 7-hydroxylations at low substrate concentrations in the rat.

摘要

使用深色刺豚鼠(已知为异喹胍4-羟基化代谢不良动物模型)和Wistar大鼠的微粒体研究了普萘洛尔的代谢。普萘洛尔4-和5-羟基化遵循双相米氏动力学,而7-羟基化和N-去异丙基化在两种品系中均为单相。动力学研究表明,与Wistar大鼠相比,深色刺豚鼠中普萘洛尔7-羟化酶活性的Vmax以及普萘洛尔4-和5-羟化酶活性高亲和力阶段的Vmax明显较低。针对属于CYP2D亚家族的细胞色素P-450同工酶P-450BTL(Suzuki, T., 等人,Drug Metab. Dispos. 20, 367 - 373, 1992)的抗体,在低普萘洛尔浓度(5 microM)下可抑制雄性Wistar大鼠肝微粒体中90%的普萘洛尔4-、5-和7-羟化酶活性。然而,在高普萘洛尔浓度(1 mM)下,观察到该抗体对普萘洛尔4-和5-羟化酶活性的抑制作用较小,而对普萘洛尔7-羟化酶活性的抑制作用相似。该抗体抑制普萘洛尔N-去异丙基酶活性,但在低和高普萘洛尔浓度下,对该活性的抑制程度低于对环羟化酶活性的抑制程度。这些结果表明,属于CYP2D亚家族的多态性细胞色素P-450同工酶在大鼠低底物浓度下主要参与普萘洛尔4-、5-和7-羟基化。

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