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The Dual-Pathway Strategy after Acute Coronary Syndrome: Rivaroxaban and Antiplatelet Agents in the ATLAS ACS 2-TIMI 51 Trial

机译:急性冠脉综合征后的双途径策略:ATLAS ACS 2-TIMI 51试验中的利伐沙班和抗血小板药

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摘要

Acute coronary syndrome (ACS) is a medical emergency often associated with an occlusive coronary event with consequent myocardial underperfusion. Patients require immediate antiplatelet therapy and long-term antithrombotic prophylaxis to reduce the risk of recurrence. Acetylsalicylic acid (ASA) alone or in combination with a platelet P2Y12 inhibitor (dual antiplatelet therapy [DAPT]) has become the clinically accepted antithrombotic prophylaxis for patients post-ACS. Historically, studies assessing the utility of adding oral anticoagulants (OACs) have not demonstrated a clinical benefit with regard to acceptable bleeding risk. Studies with vitamin K antagonists (VKAs) such as warfarin demonstrated a potential to reduce the risk of subsequent death by reinfarction but this benefit was offset by increases in bleeding. Results from studies of two targeted non-VKA OACs also proved disappointing, with little or no apparent reduction in the rate of ischemic events seen. However, the recent ATLAS studies assessing rivaroxaban (an oral factor Xa inhibitor) in patients with ACS demonstrated a reduction in the composite endpoint of deaths from cardiovascular causes, myocardial infarction (MI), or stroke, and a reduction in the rate of stent thrombosis. This review provides an overview of the pivotal studies in which the addition of OACs to antiplatelet therapy (the so-called “dual-pathway” approach) has been investigated for the management of patients post-ACS and considers the results of the ATLAS studies and their potential impact on the management of patients after an acute event.
机译:急性冠状动脉综合征(ACS)是一种医疗急症,通常与闭塞性冠状动脉事件相关,并伴有心肌灌注不足。患者需要立即进行抗血小板治疗和长期的抗血栓预防措施,以降低复发风险。乙酰水杨酸(ASA)单独或与血小板P2Y12抑制剂联合使用(双重抗血小板治疗[DAPT])已成为ACS后患者临床上公认的抗血栓预防方法。从历史上看,评估添加口服抗凝剂(OAC)的效用的研究尚未证明就可接受的出血风险而言具有临床益处。对维生素K拮抗剂(VKA)(如华法林)的研究表明,可以降低因再梗死而导致的后续死亡风险,但这种益处被出血增加所抵消。两种针对性的非VKA OAC的研究结果也令人失望,缺血事件发生率几乎没有或没有明显降低。但是,最近的ATLAS研究评估ACS患者中的利伐沙班(一种口服Xa抑制剂)表明,心血管原因,心肌梗塞(MI)或中风导致的死亡复合终点降低,支架血栓形成率降低。这篇综述概述了关键性研究,在该研究中,已经研究了在抗血小板治疗中添加OAC来治疗ACS后患者的方法(所谓的“双重途径”方法),并考虑了ATLAS研究的结果和它们对急性事件后患者管理的潜在影响。

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