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甲吡酮和去甲哈尔满对微粒体单加氧酶和环氧水解酶活性的影响。

Effects of metyrapone and norharmane on microsomal mono-oxygenase and epoxide hydrolase activities.

作者信息

Bulleid N J, Craft J A

出版信息

Biochem Pharmacol. 1984 May 1;33(9):1451-7. doi: 10.1016/0006-2952(84)90412-x.

Abstract

This study was undertaken to examine the possibility that metyrapone and norharmane stimulate epoxide hydrolase and inhibit mono-oxygenase activities by binding to a cytochrome P-450 component of a stable complex containing the two enzymes. The concentration of metyrapone and norharmane which inhibited mono-oxygenase activities of hepatic microsomes from untreated and diethylnitrosamine treated rats was lower than that required to stimulate epoxide hydrolase of the same microsomes. The ability of metyrapone and norharmane to stimulate epoxide hydrolase in these microsomes was not inhibited by the addition of carbon monoxide and reductant. Epoxide hydrolase activity was inhibited by detergents but the enzyme was still stimulated by metyrapone and norharmane under conditions of total membrane disaggregation. When microsomes were solubilized, epoxide hydrolase could be quantitatively recovered by immunoprecipitation. The immunoprecipitate contained no detectable cytochrome P-450 but was stimulated by metyrapone and norharmane. A purified epoxide hydrolase was stimulated by metyrapone but not by norharmane. The response of the enzyme to norharmane was not restored by the inclusion of cytochrome P-448. These findings suggest that metyrapone and norharmane act at separate sites on both cytochrome P-450 and epoxide hydrolase.

摘要

本研究旨在探讨甲吡酮和去甲哈尔满通过与包含这两种酶的稳定复合物的细胞色素P - 450组分结合来刺激环氧水解酶并抑制单加氧酶活性的可能性。抑制未处理和经二乙基亚硝胺处理的大鼠肝脏微粒体单加氧酶活性的甲吡酮和去甲哈尔满浓度低于刺激相同微粒体环氧水解酶所需的浓度。添加一氧化碳和还原剂不会抑制甲吡酮和去甲哈尔满在这些微粒体中刺激环氧水解酶的能力。去污剂可抑制环氧水解酶活性,但在完全膜解体的条件下,该酶仍受甲吡酮和去甲哈尔满的刺激。当微粒体被溶解时,环氧水解酶可通过免疫沉淀进行定量回收。免疫沉淀物中未检测到细胞色素P - 450,但受甲吡酮和去甲哈尔满的刺激。纯化的环氧水解酶受甲吡酮刺激,但不受去甲哈尔满刺激。加入细胞色素P - 448不能恢复该酶对去甲哈尔满的反应。这些发现表明,甲吡酮和去甲哈尔满在细胞色素P - 450和环氧水解酶上的不同位点起作用。

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