8-异前列腺素F2 α在人血小板中的形成。

Agents and actions. Supplements Pub Date : 1995-01-01
D Pratico, M Reilly, J Lawson, N Delanty, G A FitzGerald
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引用次数: 0

摘要

F2-异前列腺素是由花生四烯酸以不依赖酶的方式形成的自由基催化的前列腺素F2异构体(1)。其他类似的前列腺素异构体家族也被描述过。这些化合物在体内的检测被认为代表了一种定量评估人体自由基生成的方法(2)。此外,PGF2 α和PGE2的8-iso类似物已被证明可以诱导血管收缩,这一反应被血栓素受体的药物拮抗剂所阻止(3)。因此,可以想象这些特殊的异构体可能表现出一种自体功能。我们选择探索调节其中一种化合物8-iso-PGF2 α在体内和体外通过人类血小板生物合成的因素,以更清楚地了解这些化合物的发现如何被利用,以进一步了解自由基催化的体内过程。
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Formation of 8-iso-prostaglandin F2 alpha by human platelets.

F2-isoprostanes are free radical catalyzed prostaglandin F2 isomers formed from arachidonic acid in an enzyme independent manner (1). Analogous families of other prostaglandin isomers have also been described. Detection of these compounds in vivo has been postulated to represent an approach to the quantitative assessment of free radical generation in humans (2). Additionally, the 8-iso analogues of PGF2 alpha and PGE2 have been shown to induce vasoconstriction, a response which is prevented by pharmacological antagonists of the thromboxane receptor (3). Consequently, it is conceivable that these particular isomers might exhibit an autacoidal function. We chose to explore the factors which regulate the biosynthesis of one of these compounds, 8-iso-PGF2 alpha, in vivo and by human platelets in vitro, to understand more clearly how the discovery of these compounds might be exploited to further our understanding of free radical catalyzed processes in vivo.

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