INHIBITION OF CYTOCHROME-P-450 2E1 BY DIALLYL SULFIDE AND ITS METABOLITES

被引：249

作者：

BRADY, JF

ISHIZAKI, H

FUKUTO, JM

LIN, MC

FADEL, A

GAPAC, JM

YANG, CS

机构：

[1] RUTGERS STATE UNIV,COLL PHARM,DEPT CHEM BIOL & PHARMACOGNOSY,CANC RES LAB,PISCATAWAY,NJ 08855

[2] UNIV PACIFIC,SCH PHARM,STOCKTON,CA 95211

[3] UNIV CALIF LOS ANGELES,CTR HLTH SCI,DEPT PHARMACOL,LOS ANGELES,CA 90024

来源：

CHEMICAL RESEARCH IN TOXICOLOGY | 1991年 / 4卷 / 06期

关键词：

D O I：

10.1021/tx00024a008

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

Diallyl sulfide, a major flavor ingredient from garlic, was previously shown to inhibit chemically induced carcinogenesis and cytotoxicity in animal model systems. It modulated cytochrome P-450 compositions by inactivating P-450 2E1 and inducing P-450 2B1. The present studies examined the inhibition of P-450 2E1 mediated p-nitrophenol hydroxylase activity by diallyl sulfide and its putative metabolites diallyl sulfoxide and diallyl sulfone (DASO2). Each compound displayed competitive inhibition of p-nitrophenol hydroxylase activity in incubations using liver microsomes from acetone-pretreated male Sprague-Dawley rats. Preincubation of the microsomes with DASO2 inactivated p-nitrophenol hydroxylase activity in a process that was time- and NADPH-dependent and saturable, exhibited pseudo-first-order kinetics, was protected by alternate substrate, was accompanied by a loss of microsomal P-450-CO binding spectrum, and was unaffected by exogenous nucleophile. The K(i) value for DASO2 was 188-mu-M and the maximal rate of inactivation was 0.32 min-1. DASO2 was ineffective in the inactivation of ethoxyresorufin dealkylase, pentoxyresorufin dealkylase, or benzphetamine demethylase activity. Purified P-450 2E1 in a reconstituted system was inactivated in a time- and NADPH-dependent manner by DASO2. The metabolic conversion of diallyl sulfide to the sulfoxide and sulfone was observed in vivo and in vitro. The results suggest that diallyl sulfide inhibits the metabolism of P-450 2E1 substrates by competitive inhibition mechanisms and by inactivating P-450 2E1 via a suicide-inhibitory action of DASO2.

引用

页码：642 / 647

页数：6

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