Department of Cardiology-Cardiac Catheterization Laboratory, University of Modena and ReggioEmilia, Modena, Italy.
J Cardiovasc Med (Hagerstown). 2010 Jul;11(7):536-43. doi: 10.2459/JCM.0b013e32833499c4.
Drug-eluting stents (DES) have been designed to prevent restenosis, but long-term clinical outcome may be offset by an increased risk of stent thrombosis, which is associated with suboptimal stent implantation or delayed re-endothelialization. DES implantation has also been associated with local persistent endothelial dysfunction. Conversely, Trapidil is a potent anti-inflammatory, vasodilatator and antiproliferative drug and several studies have shown anti-restenotic effects, suggesting substantial clinical benefits through the use of Trapidil-eluting DES.
This is a longitudinal, single-blind, double-arm, randomized multicenter study. Forty patients with non-ST-elevation acute coronary syndromes who present at the index procedure with multivessel coronary disease in the major epicardial coronary arteries will be enrolled. Patients should present a culprit lesion with stenosis 70% or more associated with another stenosis 70% or more in another coronary artery. Patients will be randomized in a 1: 1 fashion to receive either an Intrepide trapidil-eluting stent or a Taxus paclitaxel-eluting stent on the culprit lesion. After 90 days, the nonculprit lesion will be treated with the stent of the opposite randomization arm and optical coherence tomography (OCT) analysis of the index stented segment will be performed. Follow-up angiography, combined with vasomotor analysis of endothelial function by rapid atrial pacing, will be done at 12 months after the index procedure on both stents. To further characterize the status of the endothelium, serum measurement of vascular endothelial growth factor gradient between the aorta and 15 mm distal to the implanted stent will be performed at 12 months. The primary endpoint of the study is to compare stent struts re-endothelialization at 90 days by OCT. The secondary endpoint is to compare angiographic outcome and coronary endothelial function 12 months after the index procedure and to compare clinical outcome at 1 and 2 years between trapidil-eluting DES versus paclitaxel-eluting DES.
We hypothesize that the utilization of trapidil-eluting DES in the setting of acute coronary syndromes will be characterized by a greater early re-endothelialization associated with an antiproliferative effect offering a similar efficacy with a better safety profile compared with first-generation DES.
药物洗脱支架(DES)的设计旨在预防再狭窄,但长期临床结果可能因支架血栓形成的风险增加而受到影响,这与支架植入不理想或延迟再内皮化有关。DES 的植入也与局部持续的内皮功能障碍有关。相反,Trapidil 是一种有效的抗炎、血管扩张和抗增殖药物,多项研究表明其具有抗再狭窄作用,表明通过使用 Trapidil 洗脱 DES 可以带来实质性的临床获益。
这是一项纵向、单盲、双臂、随机、多中心研究。将纳入 40 名非 ST 段抬高型急性冠状动脉综合征患者,这些患者在指数手术时存在主要心外膜冠状动脉多支血管疾病。患者应出现狭窄 70%以上的罪犯病变,并伴有另一支冠状动脉狭窄 70%以上的病变。患者将以 1:1 的比例随机接受 Intrepide Trapidil 洗脱支架或 Taxus 紫杉醇洗脱支架治疗罪犯病变。90 天后,将对非罪犯病变进行相反随机化手臂的支架治疗,并对指数支架段进行光学相干断层扫描(OCT)分析。在指数手术后 12 个月,对两个支架进行随访血管造影,并结合快速心房起搏的血管舒缩分析内皮功能。为了进一步描述内皮状态,将在指数支架植入后 12 个月测量主动脉和植入支架远端 15mm 之间血管内皮生长因子梯度的血清水平。该研究的主要终点是通过 OCT 在 90 天比较支架梁的再内皮化情况。次要终点是比较指数手术后 12 个月的血管造影结果和冠状动脉内皮功能,并比较 Trapidil 洗脱 DES 与紫杉醇洗脱 DES 之间 1 年和 2 年的临床结果。
我们假设在急性冠状动脉综合征中使用 Trapidil 洗脱 DES 将表现为更大的早期再内皮化,这与抗增殖作用有关,与第一代 DES 相比,提供类似的疗效和更好的安全性。
