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血栓素B2的生物合成:人血小板中酶系统的测定、分离及特性

Biosynthesis of thromboxane B2: assay, isolation, and properties of the enzyme system in human platelets.

作者信息

Ho P P, Walters C P, Sullivan H R

出版信息

Prostaglandins. 1976 Dec;12(6):951-70. doi: 10.1016/0090-6980(76)90129-5.

Abstract

The microsomal fraction of human platelets catalyzed the conversion of arachidonic acid to an unstable platelet-aggregating factor and a hydrolyzed product on the thin-layer chromatography (TLC). This product was isolated on TLC, purified by silica gel column chromatography and identified by combined gas chromatography-mass spectrometry as the hemiacetal derivative of 8-(1-hydroxy-3-oxopropyl)-9, 12L-dihydroxy-5, 10-heptadecatrienoic acid (thromboxane B2). The enzymatic activity was dependent upon methemoglobin and tryptophan as cofactors. Reduced glutathione had no effect either alone or in combination with other cofactors. Methemoglobin could be replaced by hematin or hemin; and tryptophan by 3-indolacetic acid or catecholamines. The apparent requirement for methemoglobin is due to the reductive activity of ferriprotoporphyrin IX. The reaction, however, catalyzed by the ferriprotoporphyrin IX in the thromboxane synthesizing system is different from that described for the decomposition of lipid peroxides. Certain transition metals and hydrogen donors, such as hydroquinone and ascorbate, which have been shown to stimulate the catalytic activity of ferriproroporphyrin IX in the decomposition of 15-hydroperoxy-prostaglandin E1 are inhibitors of thromboxane B2 formation. This enzyme preparation also transformed eicosa-8. 11, 14-trienoic acid to an unknown product on TLC. The enzyme system was rapidly inactivated upon incubation in the reaction mixture.

摘要

人血小板微粒体部分在薄层色谱法(TLC)上催化花生四烯酸转化为一种不稳定的血小板聚集因子和一种水解产物。该产物在TLC上分离,通过硅胶柱色谱法纯化,并通过气相色谱 - 质谱联用鉴定为8-(1-羟基-3-氧代丙基)-9,12L-二羟基-5,10-十七碳三烯酸(血栓素B2)的半缩醛衍生物。酶活性依赖于高铁血红蛋白和色氨酸作为辅助因子。还原型谷胱甘肽单独或与其他辅助因子联合使用均无作用。高铁血红蛋白可用血红素或氯高铁血红素替代;色氨酸可用3-吲哚乙酸或儿茶酚胺替代。对高铁血红蛋白的明显需求是由于铁原卟啉IX的还原活性。然而,血栓素合成系统中铁原卟啉IX催化的反应与脂质过氧化物分解所描述的反应不同。某些过渡金属和氢供体,如对苯二酚和抗坏血酸,已被证明可刺激铁原卟啉IX在15-氢过氧前列腺素E1分解中的催化活性,但它们是血栓素B2形成的抑制剂。这种酶制剂还在TLC上将二十碳-8,11,14-三烯酸转化为一种未知产物。该酶系统在反应混合物中孵育后迅速失活。

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