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两种引起血小板聚集的前列腺素内过氧化物的分离与结构

Isolation and structure of two prostaglandin endoperoxides that cause platelet aggregation.

作者信息

Hamberg M, Svensson J, Wakabayashi T, Samuelsson B

出版信息

Proc Natl Acad Sci U S A. 1974 Feb;71(2):345-9. doi: 10.1073/pnas.71.2.345.

Abstract

Incubation for a short time of arachidonic acid with the microsomal fraction of a homogenate of the vesicular gland of sheep in the presence of 1 mM p-mercuribenzoate followed by extraction and silicic acid chromatography yielded two prostaglandin endoperoxides. The structures of these compounds, i.e., 15-hydroperoxy-9alpha,11alpha-peroxidoprosta-5,13-dienoic acid (prostaglandin G(2)) and 15-hydroxy-9alpha,11alpha-peroxidoprosta-5,13-dienoic acid (prostaglandin H(2)), were assigned mainly by a number of chemical transformations into previously known prostaglandins. The new prostaglandins were 50-200 times (prostaglandin G(2)) and 100-450 times (prostaglandin H(2)) more active than prostaglandin E(2) on the superfused aorta strip. The half-life of the prostaglandin endoperoxides in aqueous medium (about 5 min) was significantly longer than that of "rabbit aorta-contracting substance" released from guinea pig lung, indicating that none of the prostaglandin endoperoxides is identical with this factor. Addition of 10-300 ng/ml of the endoperoxides to suspensions of washed human platelets resulted in rapid aggregation. Furthermore, platelet aggregation induced by thrombin was accompanied by release of material reducible by stannous chloride into prostaglandin F(2alpha), thus indicating the involvement of endogenous prostaglandin endoperoxides in platelet aggregation.

摘要

在1 mM对氯汞苯甲酸存在的情况下,将花生四烯酸与绵羊精囊匀浆的微粒体部分短时间温育,随后进行提取和硅酸色谱分析,得到了两种前列腺素内过氧化物。这些化合物的结构,即15-氢过氧-9α,11α-过氧前列腺-5,13-二烯酸(前列腺素G(2))和15-羟基-9α,11α-过氧前列腺-5,13-二烯酸(前列腺素H(2)),主要是通过一系列化学转化为先前已知的前列腺素而确定的。新的前列腺素在离体主动脉条上的活性比前列腺素E(2)高50 - 200倍(前列腺素G(2))和100 - 450倍(前列腺素H(2))。前列腺素内过氧化物在水性介质中的半衰期(约5分钟)明显长于从豚鼠肺释放的“兔主动脉收缩物质”的半衰期,这表明没有一种前列腺素内过氧化物与该因子相同。向洗涤过的人血小板悬液中加入10 - 300 ng/ml的内过氧化物会导致快速聚集。此外,凝血酶诱导的血小板聚集伴随着可被氯化亚锡还原为前列腺素F(2α)的物质的释放,因此表明内源性前列腺素内过氧化物参与了血小板聚集。

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