ADP受体:抗血小板治疗的抑制策略。

Marco Cattaneo
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引用次数: 0

摘要

腺苷-5′-二磷酸(ADP)与其血小板受体(P2Y1和P2Y12)的相互作用在血栓形成中起着非常重要的作用。噻氯匹定噻苯吡啶是第一个在预防动脉血栓事件的随机临床试验中检测血小板P2Y12 ADP受体的特异性拮抗剂。虽然噻氯匹定降低了高危患者血管事件的发生率,但不幸的是,它也有一些显著的缺点:毒性作用的发生率相对较高,在某些情况下可能是致命的;行动延迟;个体之间的反应差异很大。第二种噻吩吡啶,氯吡格雷,已经取代了噻氯匹定,因为它也是一种有效的抗血栓药物,而且毒性比噻氯匹定小。然而,氯吡格雷并非完全没有缺陷:严重的毒性作用,尽管发生的频率远低于噻氯匹定,但仍可能使患者的给药复杂化;使用大负荷剂量可以加速药理作用的开始,但可能仍然不是最佳的;患者间反应的高度差异仍然是一个重要问题。这些担忧证明了继续寻找能够通过更高的疗效和/或安全性进一步改善动脉粥样硬化患者临床结果的药物是合理的。与氯吡格雷相比,一种新的噻吩吡啶基化合物普拉格雷具有更高的效力和更快的起效,目前正在进行临床评估。两种直接可逆的P2Y12拮抗剂,angrelor和AZD6140,具有非常快速的起效和逆转血小板抑制的特点,这使它们成为噻吩吡啶的有吸引力的替代品,特别是当需要快速抑制血小板聚集或快速逆转血小板聚集时。与新的P2Y12拮抗剂一起,ADP的其他血小板受体抑制剂P2Y1拮抗剂正在开发中,并可能被证明是有效的抗血栓药物。
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ADP receptors: inhibitory strategies for antiplatelet therapy.

The interaction of adenosine-5'-diphosphate (ADP) with its platelet receptors (P2Y1 and P2Y12) plays a very important role in thrombogenesis. The thienopyridine ticlopidine was the first specific antagonist of the platelet P2Y12 ADP receptor to be tested in randomized clinical trials for the prevention of arterial thrombotic events. Although ticlopidine reduces the incidence of vascular events in patients at risk, it also unfortunately has some significant drawbacks: a relatively high incidence of toxic effects, which may be fatal in some cases; delayed onset of action; and a high interindividual variability in response. A second thienopyridine, clopidogrel, has superseded ticlopidine, because it is also an efficacious antithrombotic drug and is less toxic than ticlopidine. However, clopidogrel is not completely free from faults: severe toxic effects, albeit occurring much less frequently than with ticlopidine, may still complicate its administration to patients; the onset of pharmacologic action can be accelerated by the use of large loading doses, but may still not be optimal; the high interpatient variability in response remains an important issue. These concerns justify the continued search for agents that can further improve the clinical outcome of patients with atherosclerosis through greater efficacy and/or safety. A new thienopyridyl compound, prasugrel, which is characterized by higher potency and faster onset of action compared with clopidogrel, is currently under clinical evaluation. Two direct and reversible P2Y12 antagonists, cangrelor and AZD6140, feature very rapid onset and reversal of platelet inhibition, which make them attractive alternatives to thienopyridines, especially when rapid inhibition of platelet aggregation or its quick reversal are required. Along with new the P2Y12 antagonists, inhibitors of the other platelet receptor for ADP, the antagonists P2Y1, are under development and may prove to be effective antithrombotic agents.

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