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急性冠状动脉综合征的个体化双联抗血小板治疗:在出血和血栓形成之间取得平衡。

Personalized Dual Antiplatelet Therapy in Acute Coronary Syndromes: Striking a Balance Between Bleeding and Thrombosis.

机构信息

School of Medicine, Royal College of Surgeons in Ireland, Dublin, Ireland.

Department of Cardiology, Connolly Hospital, Blanchardstown, Dublin, Ireland.

出版信息

Curr Cardiol Rep. 2023 Jul;25(7):693-710. doi: 10.1007/s11886-023-01892-9. Epub 2023 Jun 1.

Abstract

PURPOSE OF REVIEW

Dual antiplatelet therapy (DAPT)-aspirin in conjunction with a P2Y inhibitor-is the cornerstone of managing patients with acute coronary syndromes post-revascularization, but the clinical response is highly variable, with potentially devastating consequences. Herein, we review the mechanisms underpinning said variability and explore emerging approaches to normalizing therapeutic benefit.

RECENT FINDINGS

The potent P2Y inhibitors, prasugrel and ticagrelor, exhibit minimal inter-individual variability, replacing clopidogrel in DAPT and achieving greater rates of therapeutic response. However, these benefits decline in later phases when bleeding risk begins to supersede that of ischemia. Guided de-escalation of P2Y inhibition as well as shortening DAPT duration have emerged as strategies that retain antithrombotic efficacy while reducing bleeding risk. Aspirin is the other component of DAPT but is also used in isolation for secondary prevention of thrombotic disease. In contrast to the P2Y inhibitors, genetic influences on aspirin non-response appear to be outweighed by a triad of clinical factors: non-adherence, enteric aspirin use, and inappropriate dosing according to bodyweight and BMI. Multiple de-escalation strategies for DAPT have been shown to mitigate bleeding risk, but it remains unclear which approach is ideal, necessitating head-to-head investigations to determine which exhibits the most favorable cost-to-benefit ratio. However, there is likely a role for more than one approach in clinical practice, depending on patient risk profile. Our approach to aspirin use is also in need of reassessment: strategies to improve adherence, avoidance of enteric aspirin in cardiac patients, and dose adjustment according to bodyweight and/or BMI are all likely to improve rates of therapeutic response. Moreover, platelet function testing may have a role in identifying patients expected to benefit from primary prophylactic aspirin.

摘要

目的综述

双联抗血小板治疗(DAPT)——阿司匹林联合 P2Y 抑制剂——是经血管重建治疗后的急性冠脉综合征患者管理的基石,但临床反应高度可变,可能带来灾难性后果。在此,我们综述了导致这种变异性的潜在机制,并探讨了使治疗效益正常化的新方法。

最新发现

强效 P2Y 抑制剂普拉格雷和替格瑞洛的个体间变异性极小,取代了氯吡格雷在 DAPT 中的地位,提高了治疗反应率。然而,在出血风险开始超过缺血风险的后期阶段,这些益处会下降。P2Y 抑制作用的逐渐减弱以及 DAPT 持续时间的缩短已成为保留抗血栓疗效、降低出血风险的策略。阿司匹林是 DAPT 的另一个组成部分,但也单独用于血栓性疾病的二级预防。与 P2Y 抑制剂不同,遗传因素对阿司匹林无反应的影响似乎被三联临床因素所抵消:不遵医嘱、使用肠溶阿司匹林和根据体重和 BMI 进行不适当的剂量调整。多项 DAPT 降级策略已被证明能降低出血风险,但哪种方法最理想仍不清楚,需要进行头对头研究以确定哪种方法具有最有利的成本效益比。然而,根据患者的风险状况,可能需要不止一种方法,这在临床实践中可能有一定的作用。我们对阿司匹林的使用方法也需要重新评估:改善依从性的策略、避免在心脏患者中使用肠溶阿司匹林以及根据体重和/或 BMI 调整剂量,都可能提高治疗反应率。此外,血小板功能检测可能在识别预期从初级预防性阿司匹林中获益的患者方面具有一定作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6e0d/10307718/058a05808262/11886_2023_1892_Fig1_HTML.jpg

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