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大鼠微粒体苯乙烯单加氧酶和苯乙烯环氧化物水解酶活性

Microsomal styrene mono-oxygenase and styrene epoxide hydrase activities in rats.

作者信息

Salmona M, Pachecka J, Cantoni L, Belvedere G, Mussini E, Garattini S

出版信息

Xenobiotica. 1976 Oct;6(10):585-91. doi: 10.3109/00498257609151671.

Abstract
  1. Styrene epoxide formation and styrene epoxide hydration have been studied in liver, lung, kidney, heart, spleen and brain of female and male rats. 2. Styrene epoxide formation is NADPH-dependent although it is enhanced when NADH is added together with NADP. This enzymic activity is inhibited by metyrapone and SKF 525-A but not by the effective inhibitors of epoxide hydrase, 1,2-epoxy-3,3,3-trichloropropene and cyclohexene oxide. 3. Known inducers of liver microsomal mono-oxygenases show a different activity on the two enzymes. Phenobarbital increases both formation and hydration of styrene epoxide; and carbamazepine increase the hydration but not the formation of styrene epoxide; a steroid contraceptive combination (lynestrenol+ mestranol) increases styrene epoxide formation while it inhibits epoxide hydrase; 3-methylcholanthrene does not affect either of the activities.
摘要
  1. 已在雌性和雄性大鼠的肝脏、肺、肾脏、心脏、脾脏和大脑中研究了苯乙烯环氧化物的形成及苯乙烯环氧化物的水化作用。2. 苯乙烯环氧化物的形成依赖于NADPH,不过当NADH与NADP一起添加时会增强。这种酶活性受到甲吡酮和SKF 525 - A的抑制,但不受环氧水解酶的有效抑制剂1,2 - 环氧 - 3,3,3 - 三氯丙烷和氧化环己烯的抑制。3. 已知的肝脏微粒体单加氧酶诱导剂对这两种酶表现出不同的活性。苯巴比妥会增加苯乙烯环氧化物的形成及水化作用;卡马西平会增加苯乙烯环氧化物的水化作用,但不会增加其形成;一种甾体避孕药组合(炔雌醇甲醚+炔雌醇)会增加苯乙烯环氧化物的形成,同时抑制环氧水解酶;3 - 甲基胆蒽对这两种活性均无影响。

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