Babadagli Hazal Ece, Ye Jian, Chen Jenny, Turgeon Ricky, Wang Erica Hz
Department of Pharmaceutical Sciences, Vancouver General Hospital, Vancouver, British Columbia, Canada
The University of British Columbia Faculty of Pharmaceutical Sciences, Vancouver, British Columbia, Canada.
Open Heart. 2025 Jan 30;12(1):e003158. doi: 10.1136/openhrt-2024-003158.
Mitral valve repair (MVr) is the gold standard treatment for degenerative mitral regurgitation, yet there is ongoing controversy regarding optimal anti-thrombotic therapy post-MVr. This scoping review aimed to summarise current evidence on the safety and efficacy of anti-thrombotic therapy after MVr, identify knowledge gaps and propose a future study design.
We searched MEDLINE, Embase, Cochrane Central Register of Controlled Trials, Clinicaltrials.gov, the WHO International Clinical Trials Registry Platform and bibliographies of included trials, guidelines and other reviews from inception to 17 September 2024. Randomised controlled trials (RCT) and cohort and case-control studies assessing any anti-thrombotic therapy with any outcomes after MVr were included. Using a predefined collection form, two authors independently extracted data on study characteristics and results were summarised narratively into themes based on the PICO elements.
Of 1296 screened references, we included 11 studies (10 cohort and one non-inferiority RCT). All studies compared vitamin K antagonist (VKA) to an anti-platelet, direct oral anti-coagulant or no anti-thrombotic therapy for median duration of 90 days. Thromboembolic and bleeding event incidences ranged from 0% to 14.3% and 0% to 9.1%, respectively. Seven studies reported no difference in thromboembolic events, and three reported reduced rates with VKA compared with control, while results for bleeding events varied widely. The RCT found edoxaban was non-inferior to warfarin for thromboembolic outcomes, but not for bleeding. Substantial methodological and clinical heterogeneity, high risk of bias and insufficient mitigation of confounders, such as concomitant atrial fibrillation, were prevalent across studies.
Based on this scoping review, existing literature on anti-thrombotic therapy after MVr is inconclusive due to design limitations. We proposed a study design for a pragmatic RCT that addresses prior study limitations and that could provide definitive evidence to guide anti-thrombotic management in MVr patients.
二尖瓣修复术(MVr)是退行性二尖瓣反流的金标准治疗方法,但MVr术后的最佳抗栓治疗仍存在争议。本综述旨在总结MVr术后抗栓治疗安全性和有效性的现有证据,识别知识空白,并提出未来的研究设计。
我们检索了MEDLINE、Embase、Cochrane对照试验中央注册库、Clinicaltrials.gov、世界卫生组织国际临床试验注册平台以及纳入试验的参考文献、指南和其他综述,检索时间从开始至2024年9月17日。纳入评估MVr术后任何抗栓治疗及任何结局的随机对照试验(RCT)、队列研究和病例对照研究。使用预定义的收集表,两名作者独立提取研究特征数据,并根据PICO要素将结果归纳为不同主题进行叙述性总结。
在1296篇筛选的参考文献中,我们纳入了11项研究(10项队列研究和1项非劣效性RCT)。所有研究均将维生素K拮抗剂(VKA)与抗血小板药物、直接口服抗凝剂或不进行抗栓治疗进行了比较,中位持续时间为90天。血栓栓塞和出血事件的发生率分别为0%至14.3%和0%至9.1%。七项研究报告血栓栓塞事件无差异,三项研究报告VKA组与对照组相比发生率降低,而出血事件的结果差异很大。该RCT发现,在血栓栓塞结局方面,依度沙班不劣于华法林,但在出血方面并非如此。研究中普遍存在大量的方法学和临床异质性、高偏倚风险以及对混杂因素(如合并心房颤动)的缓解不足。
基于本综述,由于设计局限性,MVr术后抗栓治疗的现有文献尚无定论。我们提出了一项实用RCT的研究设计,该设计解决了先前研究的局限性,并可为指导MVr患者的抗栓管理提供确凿证据。
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