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炔诺酮环氧化物的不可逆蛋白质结合。

Irreversible protein binding of norethisterone (norethindrone) epoxide.

作者信息

Kappus H, Bolt H M

出版信息

Steroids. 1976 Jan;27(1):29-45. doi: 10.1016/0039-128x(76)90067-2.

Abstract

14,15-3H-Norethisterone-4 beta, 5 beta-epoxide, a metabolite of norethisterone, was incubated with several proteins and nucleic acids. After 30 min incubation 0.19 nmol of the epoxide were irreversibly bound per mg albumin which contains free sulfhydryl groups; proteins without SH-groups, such as concanavalin A, gamma-globulin, DNA and RNA, did not irreversibly bind norethisterone epoxide. A superoxide (O2) generating enzyme system comprised of xanthine oxidase and hypoxanthine was capable of catalyzing the irreversible binding of the parent compound, norethisterone, to albumin, indicating that an oxidation product was formed which reacted with the protein. When norethisterone epoxide was incubated for 60 min with hepatic microsomes of rats in absence of NADPH, about 2.0 nmol of the epoxide were irreversibly incorporated per mg microsomal protein. This binding was increased to 5.2 nmol by addition of a NADPH regenerating system. Addition of glutathione and cytosol decreased only the NADPH-dependent protein binding; phenobarbital pretreatment of rats induced this NADPH-dependent binding of norethisterone epoxide to microsomal protein by a factor of 2. In presence of NADPH, binding of the epoxide to microsomal protein depended on substrate concentration used. The results indicate that norethisterone epoxide is able to chemically react with proteins. In addition, hepatic microsomal enzymes convert the epoxide to another metabolite which also can react with proteins.

摘要

炔诺酮的代谢产物14,15 - 3H - 炔诺酮 - 4β,5β - 环氧化物与几种蛋白质和核酸一起孵育。孵育30分钟后,每毫克含有游离巯基的白蛋白不可逆地结合了0.19纳摩尔的环氧化物;不含SH基团的蛋白质,如伴刀豆球蛋白A、γ - 球蛋白、DNA和RNA,不会不可逆地结合炔诺酮环氧化物。由黄嘌呤氧化酶和次黄嘌呤组成的超氧化物(O₂)生成酶系统能够催化母体化合物炔诺酮与白蛋白的不可逆结合,表明形成了一种与蛋白质反应的氧化产物。当炔诺酮环氧化物在没有NADPH的情况下与大鼠肝微粒体孵育60分钟时,每毫克微粒体蛋白不可逆地掺入约2.0纳摩尔的环氧化物。通过添加NADPH再生系统,这种结合增加到5.2纳摩尔。添加谷胱甘肽和胞质溶胶仅降低了依赖NADPH的蛋白质结合;用苯巴比妥预处理大鼠可使炔诺酮环氧化物与微粒体蛋白的这种依赖NADPH的结合增加一倍。在NADPH存在下,环氧化物与微粒体蛋白的结合取决于所用底物的浓度。结果表明炔诺酮环氧化物能够与蛋白质发生化学反应。此外,肝微粒体酶将环氧化物转化为另一种也能与蛋白质反应的代谢产物。

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