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西洛他唑预防再狭窄(CREST)随机多中心试验的原理与设计

Rationale and design of the randomized, multicenter, cilostazol for RESTenosis (CREST) trial.

作者信息

Douglas John S, Weintraub William S, Holmes David

机构信息

Division of Cardiology, Emory Center for Outcomes Research, Emory University School of Medicine, Atlanta, Georgia, USA.

出版信息

Clin Cardiol. 2003 Oct;26(10):451-4. doi: 10.1002/clc.4960261004.

Abstract

Restenosis of a segment of diseased coronary artery following metallic stenting is a common clinical problem and a major limitation of the procedure. Systemic pharmacologic interventions to deal with this problem have met with little success. Several small studies suggest that cilostazol, a phosphodiesterase III inhibitor whose pharmacologic properties include antiplatelet, antithrombotic, and vasodilatory effects; a beneficial effect on serum lipids; and in vitro inhibition of smooth muscle cell proliferation, may help prevent platelet aggregation and impede the accumulation of new intimal tissue in the stented artery. The Cilostazol for RESTenosis (CREST) trial will aim to evaluate more definitively the ability of cilostazol to prevent restenosis following uncomplicated stent implantation for de novo coronary artery stenosis. In this randomized, double-blind, multicenter study, 700 patients will receive clopidogrel, aspirin, and either cilostazol or placebo after successful intracoronary stent implantation. The primary endpoint is minimal luminal diameter (MLD) of the first lesion stented after 6 months; secondary endpoints include MLD in all lesions, mean percent diameter stenosis, target lesion revascularization, and major angiographic endpoints. Safety endpoints are abnormal complete blood count and liver function tests at 1, 3, and 6 months. The trial has been initiated, and enrollment is anticipated to be concluded in 2003. Cilostazol has properties that may reduce or avert in-stent coronary restenosis. The CREST trial is a large, rigorously conducted trial that may corroborate the favorable effects of cilostazol on coronary stent restenosis suggested by earlier studies.

摘要

金属支架置入术后,病变冠状动脉节段的再狭窄是一个常见的临床问题,也是该手术的主要局限性。针对这一问题的全身药物干预收效甚微。几项小型研究表明,西洛他唑是一种磷酸二酯酶III抑制剂,其药理特性包括抗血小板、抗血栓形成和血管舒张作用;对血脂有有益影响;并在体外抑制平滑肌细胞增殖,可能有助于预防血小板聚集,并阻止新内膜组织在支架置入动脉中的积聚。西洛他唑预防再狭窄(CREST)试验旨在更明确地评估西洛他唑预防初发冠状动脉狭窄单纯支架植入术后再狭窄的能力。在这项随机、双盲、多中心研究中,700例患者在冠状动脉内支架植入成功后将接受氯吡格雷、阿司匹林以及西洛他唑或安慰剂治疗。主要终点是6个月后首次置入支架病变的最小管腔直径(MLD);次要终点包括所有病变的MLD、平均直径狭窄百分比、靶病变血管重建以及主要血管造影终点。安全性终点是1、3和6个月时的血常规和肝功能检查异常。该试验已启动,预计2003年完成入组。西洛他唑具有可能减少或避免支架内冠状动脉再狭窄的特性。CREST试验是一项大规模、严格实施的试验,可能会证实早期研究提示的西洛他唑对冠状动脉支架再狭窄的有利作用。

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