开发凝血酶受体拮抗剂的挑战和前景。

Jing Yang, Ke Xu, Dietmar Seiffert
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引用次数: 8

摘要

尽管由阿司匹林和氯吡格雷组成的双重抗血小板治疗是可行的,但在治疗和预防动脉血栓性疾病方面仍有大量未满足的医疗需求。为了在不超过出血耐受性和安全性限制的情况下进一步减少心血管事件,新的抗血小板策略可能需要通过部分抑制重要的血小板激活途径或通过不同地靶向病理性和生理性血栓形成途径来交换抗血小板功效。凝血酶是凝血过程中的中心酶,也是体外试验中最有效的血小板激动剂,是驱动闭塞性血栓形成的关键因素之一。血小板凝血酶受体,即蛋白酶激活受体1 (PAR-1)和蛋白酶激活受体4 (PAR-4),协同作用引起血小板对凝血酶的强烈反应。PAR-1是一种高亲和力凝血酶受体,是一种新的抗血栓靶点。PAR-4是一种低亲和力凝血酶受体,其功能尚不清楚。本文综述了PAR-1靶点验证的遗传和药理学证据,重点介绍了口服PAR-1拮抗剂的开发进展和挑战,特别是默克/先灵葆雅公司的SCH 530348和卫材公司的E-5555,并介绍了赛诺菲-安万特公司和皮埃尔法伯公司最近专利披露的几种新的PAR-1拮抗剂化学系列。
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Challenges and promises of developing thrombin receptor antagonists.

Despite the availability of dual antiplatelet therapy comprised of aspirin and clopidogrel, there is still significant unmet medical need for treating and preventing arterial thrombotic diseases. To achieve further reduction of cardiovascular events without exceeding bleeding tolerability and safety limits, novel antiplatelet strategies might need to trade in antiplatelet efficacy by partial inhibition of an important platelet activation pathway or by differentially targeting pathological versus physiological thrombogenesis pathways. Thrombin, the central enzyme in coagulation and the most potent platelet agonist tested in vitro, is one of the key factors driving the formation of occlusive thrombi. Platelet thrombin receptors, namely protease-activated receptor 1 (PAR-1) and protease-activated receptor 4 (PAR-4), act in concert to elicit robust platelet responses to thrombin. PAR-1 is the high affinity thrombin receptor and represents a novel antithrombotic target. PAR-4 is a low affinity thrombin receptor with less understood function. This review discusses the genetic and pharmacological evidence for PAR-1 target validation and highlights the progresses and challenges in developing oral PAR-1 antagonists, especially SCH 530348 from Merck/Schering-Plough and E-5555 from Eisai Co. Recent patents disclosing several novel chemical series of PAR-1 antagonists from Sanofi-Aventis and Pierre Fabre are also presented.

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