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对华法林耐药大鼠的维生素K环氧化物还原酶生成羟基维生素K的研究。

Formation of hydroxyvitamin K by vitamin K epoxide reductase of warfarin-resistant rats.

作者信息

Fasco M J, Preusch P C, Hildebrandt E, Suttie J W

出版信息

J Biol Chem. 1983 Apr 10;258(7):4372-80.

PMID:6833262
Abstract

A new metabolite of vitamin K, 2(3)-hydroxy-2,3-dihydro-2-methyl,3-phytyl-1,4-naphthoquinone (hydroxyvitamin K), has been identified as a product of vitamin K epoxide metabolism in hepatic microsomes from warfarin-resistant rats, but not in those derived from normal rats. The structure was determined by comparison of the high performance liquid chromatography retention times, UV, IR, CD, and mass spectra of the unknown with chemically synthesized standards. Alterations in the formation of hydroxyvitamin K occur in parallel with alterations in total vitamin K epoxide conversion with respect to reaction time, extent of reaction, detergent stimulation, and inhibition by warfarin. Thus, hydroxyvitamin K appears to be a product of the warfarin-resistant vitamin K epoxide reductase. It is neither a substrate nor an inhibitor of epoxide reduction. Hydroxyvitamin K is formed from both enantiomers of racemic vitamin K epoxide with little stereoselectivity for the configuration of either the oxirane ring or the phytyl side chain. The reaction is stereospecific; however, the biologically formed (+)-vitamin K epoxide yields exclusively (+)-3-hydroxyvitamin K. Observation of this product is discussed as a key to understanding the normal reaction mechanism of the enzyme.

摘要

维生素K的一种新代谢产物,即2(3)-羟基-2,3-二氢-2-甲基-3-植基-1,4-萘醌(羟基维生素K),已被鉴定为华法林抗性大鼠肝微粒体中维生素K环氧化物代谢的产物,而正常大鼠来源的肝微粒体中则未发现该产物。通过将未知物的高效液相色谱保留时间、紫外光谱、红外光谱、圆二色光谱和质谱与化学合成标准品进行比较来确定其结构。羟基维生素K形成的变化与总维生素K环氧化物转化在反应时间、反应程度、去污剂刺激和华法林抑制方面的变化平行。因此,羟基维生素K似乎是华法林抗性维生素K环氧化物还原酶的产物。它既不是环氧化物还原的底物也不是抑制剂。外消旋维生素K环氧化物的两种对映体均可形成羟基维生素K,对环氧乙烷环或植基侧链的构型几乎没有立体选择性。该反应具有立体特异性;然而,生物形成的(+)-维生素K环氧化物仅产生(+)-3-羟基维生素K。对该产物的观察被认为是理解该酶正常反应机制的关键。

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