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维生素K依赖性羧化酶:反应中氢过氧化物中间体的证据。

Vitamin K-dependent carboxylase: evidence for a hydroperoxide intermediate in the reaction.

作者信息

Larson A E, Suttie J W

出版信息

Proc Natl Acad Sci U S A. 1978 Nov;75(11):5413-6. doi: 10.1073/pnas.75.11.5413.

Abstract

Vitamin K is an essential cofactor for a microsomal carboxylase that converts glutamyl residues in endogenous precursor proteins to gamma-carboxyglutamyl residues in completed proteins. The same microsomal preparations convert vitamin K to its 2,3-epoxide, and it has been suggested that these two reactions (carboxylation and epoxidation) are coupled. Glutathione peroxidase, which reduces hydrogen peroxide and organic hydroperoxides, inhibits both of these reactions in a prepartion of microsomes solubilized by Triton X-100. Catalase has no effect. In the absence of vitamin K, and in the presence of NADPH, tert-butyl hydroperoxide acts as a weak vitamin K analog. At lower concentrations, tert-butyl hydroperoxide is an apparent competitive inhibitor of vitamin K for both the carboxylase and epoxidase reactions. These data are consistent with the hypothesis that both of these vitamin K-requiring reactions involve a common oxygenated intermediate, and that a hydroperoxide of the vitamin is the species involved.

摘要

维生素K是微粒体羧化酶的一种必需辅助因子,该羧化酶可将内源性前体蛋白中的谷氨酰残基转化为成熟蛋白中的γ-羧基谷氨酰残基。同样的微粒体制剂可将维生素K转化为其2,3-环氧化物,有人提出这两个反应(羧化和环氧化)是偶联的。还原过氧化氢和有机过氧化物的谷胱甘肽过氧化物酶在由 Triton X-100溶解的微粒体制剂中会抑制这两个反应。过氧化氢酶则无作用。在缺乏维生素K且存在NADPH的情况下,叔丁基过氧化氢可作为一种弱的维生素K类似物。在较低浓度下,叔丁基过氧化氢是维生素K对羧化酶和环氧化酶反应的一种明显竞争性抑制剂。这些数据与以下假设一致,即这两个需要维生素K的反应都涉及一种共同的氧化中间体,且维生素的一种过氧化物是所涉及的物质。

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