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Oral antiplatelet agents in ischemic heart disease: a review of the latest clinical evidence

机译:口服抗血小板药物治疗缺血性心脏病:最新临床证据回顾

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Platelet activation and aggregation play a central role in the pathophysiology of thrombogenesis in ischemic heart disease. Dual antiplatelet therapy with aspirin and clopidogrel is currently the golden standard in the prevention of cardiovascular complications after percutaneous coronary intervention. Newer antiplatelet drugs are continuously marketed to respond to the limitations of clopidogrel, namely a delayed onset of action, an irreversible inhibition of platelet aggregation as well as a substantial variability in antiplatelet effect, in part due to genetic polymorphism. The second-generation thienopyridine prasugrel is more potent than clopidogrel, but also manifests a greater bleeding risk. Ticagrelor, a third-generation thienopyridine, seems to have a better safety profile and has recently been approved as a first-choice antiplatelet treatment in acute coronary syndrome in Europe. This article will review the different oral antiplatelet drugs currently available, compare pharmacology and safety/efficacy profiles, and discuss their limitations.
机译:血小板活化和聚集在缺血性心脏病中血栓形成的病理生理中起着重要作用。阿司匹林和氯吡格雷双重抗血小板治疗目前是预防经皮冠状动脉介入治疗后心血管并发症的黄金标准。不断有新的抗血小板药物上市,以应对氯吡格雷的局限性,即起效延迟,对血小板凝集的不可逆抑制以及抗血小板作用的显着差异,部分原因是遗传多态性。第二代噻吩并吡啶普拉格雷比氯吡格雷更有效,但也显示出更大的出血风险。 Ticagrelor是第三代噻吩并吡啶,似乎具有更好的安全性,最近已被批准为欧洲急性冠脉综合征的首选抗血小板治疗药物。本文将回顾当前可用的各种口服抗血小板药物,比较药理学和安全性/功效概况,并讨论其局限性。

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