依非曲班钠:一种有效的TxA2/PGH2受体拮抗剂。

L. Rosenfeld, G. Grover, C. Stier
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引用次数: 26

摘要

本文综述了一种新型汤波烷A2/前列腺素H2受体拮抗剂——伊芙曲班钠的化学、药代动力学和药效学研究进展。血栓素A2是花生四烯酸的产物,由环加氧酶形成。与其他环加氧酶产物相比,血栓素A2已被证明参与血管收缩和血小板活化。总的来说,临床研究和动物实验结果表明,高血压与血小板的高聚集性和血液、尿液和组织中蒽醌A2水平升高有关。血栓素A2、前列腺素G2和前列腺素H2的前体也结合并激活相同的受体。因此,受体拮抗剂被认为是逆转血栓素A2/前列腺素H2作用的改进策略,而不是血栓素合成抑制剂。本文综述了伊芙曲班的合成和分析的新方法,它的组织分布,以及它在各种动物模型和疾病状态中的作用。我们描述了关于伊芙曲班如何放松实验性收缩的孤立血管组织的机制,以及对心肌缺血、高血压、中风、血栓形成的影响及其对血小板的影响的研究。这些实验是在几种动物模型上进行的,包括狗、雪貂和老鼠,以及人类。临床研究也被描述。这些研究表明,伊芙曲班钠可有效逆转血栓素A2和前列腺素h2介导的过程。
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Ifetroban sodium: an effective TxA2/PGH2 receptor antagonist.
This review presents a comprehensive discussion on the chemistry, pharmacokinetics, and pharmacodynamics of ifetroban sodium, a new thomboxane A2/prostaglandin H2 receptor antagonist. Thromboxane A2 is an arachidonic acid product, formed by the enzyme cyclooxygenase. In contrast to other cyclooxygenase products, thromboxane A2 has been shown to be involved in vascular contraction and has been implicated in platelet activation. In general, results of clinical studies and animal experiments indicate that hypertension is associated with hyperaggregability of platelets and increased thomboxane A2 levels in blood, urine, and tissues. The precursors to thromboxane A2, prostaglandin G2, and prostaglandin H2, also bind and activate the same receptors. Thus, a receptor antagonist was thought to be an improved strategy for reversing the actions of thromboxane A2/prostaglandin H2, rather than a thromboxane synthesis inhibitor. This review describes new methods for the synthesis and analysis of ifetroban, its tissue distribution, and its actions in a variety of animal models and disease states. We describe studies on the mechanisms of how ifetroban relaxes experimentally contracted isolated vascular tissue, and on the effects of ifetroban on myocardial ischemia, hypertension, stroke, thrombosis, and its effects on platelets. These experiments were conducted on several animal models, including dog, ferret, and rat, as well as on humans. Clinical studies are also described. These investigations show that ifetroban sodium is effective at reversing the effects of thromboxane A2- and prostaglandin H2-mediated processes.
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