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重新审视双嘧达莫减少再狭窄的证据:系统评价和荟萃分析。

Revisiting the Evidence for Dipyridamole in Reducing Restenosis: A Systematic Review and Meta-analysis.

机构信息

Division of Cardiology, CAPITAL Research Group, University of Ottawa Heart Institute, Ottawa, Ontario, Canada.

Department of Cellular and Molecular Medicine, University of Ottawa, Ottawa, Ontario, Canada.

出版信息

J Cardiovasc Pharmacol. 2021 Apr 1;77(4):450-457. doi: 10.1097/FJC.0000000000000976.

DOI:10.1097/FJC.0000000000000976
PMID:33760800
Abstract

Atherosclerosis remains a leading cause of morbidity and mortality, with revascularization remaining a cornerstone of management. Conventional revascularization modalities remain challenged by target vessel reocclusion-an event driven by mechanical, thrombotic, and proliferative processes. Despite considerable advancements, restenosis remains the focus of ongoing research. Adjunctive agents, including dipyridamole, offer a multitude of effects that may improve vascular homeostasis. We sought to quantify the potential therapeutic impact of dipyridamole on vascular occlusion. We performed a literature search (EMBASE and MEDLINE) examining studies that encompassed 3 areas: (1) one of the designated medical therapies applied in (2) the setting of a vascular intervention with (3) an outcome including vascular occlusion rates and/or quantification of neointimal proliferation/restenosis. The primary outcome was vascular occlusion rates. The secondary outcome was the degree of restenosis by neointimal quantification. Both human and animal studies were included in this translational analysis. There were 6,839 articles screened, from which 73 studies were included, encompassing 16,146 vessels followed up for a mean of 327.3 days (range 7-3650 days). Preclinical studies demonstrate that dipyridamole results in reduced vascular occlusion rates {24.9% vs. 48.8%, risk ratio 0.53 [95% confidence interval (CI) 0.40-0.70], I2 = 39%, P < 0.00001}, owing to diminished neointimal proliferation [standardized mean differences -1.13 (95% CI -1.74 to -0.53), I2 = 91%, P = 0.0002]. Clinical studies similarly demonstrated reduced occlusion rates with dipyridamole therapy [23.5% vs. 31.0%, risk ratio 0.77 (95% CI 0.67-0.88), I2 = 84%, P < 0.0001]. Dipyridamole may improve post-intervention vascular patency and mitigate restenosis. Dedicated studies are warranted to delineate its role as an adjunctive agent after revascularization.

摘要

动脉粥样硬化仍然是发病率和死亡率的主要原因,血运重建仍然是其治疗的基石。传统的血运重建方式仍然受到靶血管再闭塞的挑战——这是由机械、血栓和增殖过程驱动的事件。尽管取得了相当大的进展,但再狭窄仍然是正在进行的研究的焦点。辅助药物,包括双嘧达莫,具有多种可能改善血管稳态的作用。我们试图量化双嘧达莫对血管闭塞的潜在治疗影响。我们进行了文献检索(EMBASE 和 MEDLINE),研究了涵盖以下 3 个方面的研究:(1)一种指定的医疗疗法之一在(2)血管介入治疗中应用,(3)血管闭塞率和/或新生内膜增殖/再狭窄的定量结果。主要结果是血管闭塞率。次要结果是通过新生内膜定量评估的再狭窄程度。这项转化分析纳入了人体和动物研究。经过筛选,共得到 6839 篇文章,其中纳入了 73 项研究,共纳入 16146 条血管,平均随访 327.3 天(范围 7-3650 天)。临床前研究表明,双嘧达莫可降低血管闭塞率[24.9%比 48.8%,风险比 0.53(95%置信区间 0.40-0.70),I2=39%,P<0.00001],归因于新生内膜增殖减少[标准化均数差-1.13(95%置信区间-1.74 至-0.53),I2=91%,P=0.0002]。临床研究也同样表明,双嘧达莫治疗可降低闭塞率[23.5%比 31.0%,风险比 0.77(95%置信区间 0.67-0.88),I2=84%,P<0.0001]。双嘧达莫可改善血管介入后的通畅性并减轻再狭窄。需要专门的研究来阐明其作为血运重建后的辅助药物的作用。

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