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正常和萘酚平处理的雄性DBA/2小鼠胞质和微粒体组分中环氧水解酶的器官分布

Organ distribution of epoxide hydrolases in cytosolic and microsomal fractions of normal and nafenopin-treated male DBA/2 mice.

作者信息

Waechter F, Bentley P, Bieri F, Muakkassah-Kelly S, Stäubli W, Villermain M

机构信息

Central Toxicology Unit, Ciba-Geigy Ltd, Basel, Switzerland.

出版信息

Biochem Pharmacol. 1988 Oct 15;37(20):3897-903. doi: 10.1016/0006-2952(88)90071-8.

Abstract

Using trans-stilbene oxide and styrene oxide as substrates, epoxide hydrolase activities were measured in cytosolic and microsomal fractions from liver, kidney, heart, lung and testis of male DBA/2 mice. The activities towards these two substrates are remarkably organ specific: trans-stilbene oxide was most effectively hydrolyzed in subcellular fractions from liver, kidney and heart, whereas styrene oxide was predominantly hydrolyzed in those from liver, lung and testis. Immunoblotting experiments were performed with two polyclonal antibodies isolated from goat antisera. Using an anti-mouse liver cytosolic epoxide hydrolase antibody, the corresponding antigen protein was predominantly detected in both cytosolic and microsomal fractions from liver, kidney and heart. An anti-rat liver microsomal epoxide hydrolase antibody proved to be cross-reactive with the mouse enzyme and stained SDS-gels run with microsomal fractions from liver, lung and testis. The anti-mouse liver cytosolic epoxide hydrolase antibody precipitated cytosolic epoxide hydrolase activities from liver, kidney and heart cytosolic fractions. Dietary exposure to the hypolipidemic agent nafenopin (2000 ppm/10 days) caused an induction of trans-stilbene oxide hydrolase and styrene oxide hydrolase activities in cytosolic and microsomal liver fractions whereas, in the other organs, the same activities were unaffected by this treatment. This finding was in accordance with the increased amounts of antigen protein as detected with the antibodies in liver fractions from treated animals. The anti-mouse liver cytosolic epoxide hydrolase antibody was found to precipitate the whole trans-stilbene oxide hydrolase activity also from liver cytosol of nafenopin-treated mice, which indicates the presence of a single cytosolic epoxide hydrolase following induction.

摘要

以反式氧化芪和氧化苯乙烯为底物,测定了雄性DBA/2小鼠肝脏、肾脏、心脏、肺和睾丸的胞质和微粒体部分的环氧水解酶活性。对这两种底物的活性具有显著的器官特异性:反式氧化芪在肝脏、肾脏和心脏的亚细胞部分水解最有效,而氧化苯乙烯主要在肝脏、肺和睾丸的亚细胞部分水解。用从山羊抗血清中分离出的两种多克隆抗体进行免疫印迹实验。使用抗小鼠肝脏胞质环氧水解酶抗体,在肝脏、肾脏和心脏的胞质和微粒体部分均主要检测到相应的抗原蛋白。抗大鼠肝脏微粒体环氧水解酶抗体被证明与小鼠酶有交叉反应,并能对用肝脏、肺和睾丸的微粒体部分进行SDS凝胶电泳染色。抗小鼠肝脏胞质环氧水解酶抗体沉淀了肝脏、肾脏和心脏胞质部分的胞质环氧水解酶活性。饮食中接触降血脂药物萘酚平(2000 ppm/10天)可诱导肝脏胞质和微粒体部分的反式氧化芪水解酶和氧化苯乙烯水解酶活性,而在其他器官中,相同的活性不受该处理的影响。这一发现与用抗体检测到的处理动物肝脏部分抗原蛋白量的增加一致。发现抗小鼠肝脏胞质环氧水解酶抗体也能从萘酚平处理小鼠的肝脏胞质中沉淀出全部反式氧化芪水解酶活性,这表明诱导后存在单一的胞质环氧水解酶。

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