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New highly active antiplatelet agents with dual specificity for platelet P2Y1 and P2Y12 adenosine diphosphate receptors

机译:新型高活性抗血小板药物,对血小板p2Y1和p2Y12二磷酸腺苷受体具有双重特异性

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摘要

Currently approved platelet adenosine diphosphate (ADP) receptor antagonists target only the platelet P2Y12 receptor. Moreover, especially in patients with acute coronary syndromes, there is a strong need for rapidly acting and reversible antiplatelet agents in order to minimize the risk of thrombotic events and bleeding complications. In this study, a series of new P(1),P(4)-di(adenosine-5\u27) tetraphosphate (Ap4A) derivatives with modifications in the base and in the tetraphosphate chain were synthesized and evaluated with respect to their effects on platelet aggregation and function of the platelet P2Y1, P2Y12, and P2X1 receptors. The resulting structure-activity relationships were used to design Ap4A analogs which inhibit human platelet aggregation by simultaneously antagonizing both P2Y1 and P2Y12 platelet receptors. Unlike Ap4A, the analogs do not activate platelet P2X1 receptors. Furthermore, the new compounds exhibit fast onset and offset of action and are significantly more stable than Ap4A to degradation in plasma, thus presenting a new promising class of antiplatelet agents.
机译:当前批准的血小板二磷酸腺苷(ADP)受体拮抗剂仅靶向血小板P2Y12受体。此外,特别是在患有急性冠状动脉综合征的患者中,强烈需要快速作用和可逆的抗血小板药,以使血栓形成事件和出血并发症的风险最小化。在这项研究中,合成了一系列新的在碱基和四磷酸链上有修饰的P(1),P(4)-di(adenosine-5 \ u27)四磷酸(Ap4A)衍生物,并对其效果进行了评估。血小板聚集和血小板P2Y1,P2Y12和P2X1受体的功能所得的结构-活性关系用于设计通过同时拮抗P2Y1和P2Y12血小板受体来抑制人血小板聚集的Ap4A类似物。与Ap4A不同,类似物不会激活血小板P2X1受体。此外,新化合物表现出快速的起效和抵消作用,并且在血浆中降解方面比Ap4A稳定得多,因此提供了一类新的有希望的抗血小板药。

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