首页> 外文期刊>Catheterization and cardiovascular interventions: Official journal of the Society for Cardiac Angiography & Interventions >Biological Effect on Drug Distribution and Vascular Healing Via Paclitaxel-Coated Balloon Technology in Drug Eluting Stent Restenosis Swine Model
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Biological Effect on Drug Distribution and Vascular Healing Via Paclitaxel-Coated Balloon Technology in Drug Eluting Stent Restenosis Swine Model

机译:紫杉醇涂层球囊技术在药物洗脱支架再狭窄猪模型中对药物分布和血管愈合的生物学效应

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Objectives: To evaluate the biological effect of a paclitaxel-coated balloon (PCB) technology on vascular drug distribution and healing in drug eluting stent restenosis (DES-ISR) swine model. Background: The mechanism of action and healing response via PCB technology in DES-ISR is not completely understood. Methods: A total of 27 bare metal stents were implanted in coronary arteries and 30 days later the in-stent restenosis was treated with PCB. Treated segments were harvested at 1 hr, 14 days and 30 days post treatment for the pharmacokinetic analysis. In addition, 24 DES were implanted in coronary arteries for 30 days, then all DES-ISRs were treated with either PCB (n = 12) or uncoated balloon (n = 12). At day 60, vessels were harvested for histology following angiography and optical coherence tomography (OCT). Results: The paclitaxel level in neointimal tissue was about 18 times higher (P = 0.0004) at 1 hr Cmax, and retained about five times higher (P = 0.008) at day 60 than that in vessel wall. A homogenous distribution of paclitaxel in ISR was demonstrated by using fluorescently labeled paclitaxel. Notably, in DES-ISR, both termination OCT and quantitative coronary angioplasty showed a significant neointimal reduction and less late lumen loss (P = 0.05 and P = 0.03, respectively) post PCB versus post uncoated balloon. The PES-ISR1PCB group displayed higher levels of peri-strut inflammation and fibrin scores compared to the -limus DES-ISR + PCB group. Conclusions: In ISR, paclitaxel is primarily deposited in neointimal tissue and effectively retained over time following PCB use. Despite the presence of metallic struts, a uniform distribution was characterized. PCB demonstrated an equivalent biological effect in DES-ISR without significantly increasing inflammation. (C) 2015 Wiley Periodicals, Inc.
机译:目的:评价紫杉醇涂层球囊(PCB)技术对药物洗脱支架再狭窄(DES-ISR)猪模型中血管药物分布和愈合的生物学影响。背景:DES-ISR中通过PCB技术产生的作用机理和治愈反应尚未完全了解。方法:将总共27个裸金属支架植入冠状动脉,并在30天后用PCB治疗支架内再狭窄。在治疗后1小时,14天和30天收获经治疗的片段以进行药代动力学分析。此外,将24 DES植入冠状动脉中30天,然后所有的DES-ISR均采用PCB(n = 12)或未包被的球囊(n = 12)进行治疗。在第60天,在血管造影和光学相干断层扫描(OCT)之后收集血管用于组织学。结果:在1小时Cmax时,新内膜组织中的紫杉醇水平约高18倍(P = 0.0004),在第60天时仍比血管壁高约5倍(P = 0.008)。通过使用荧光标记的紫杉醇证明了紫杉醇在ISR中的均匀分布。值得注意的是,在DES-ISR中,与未包被的球囊相比,终止OCT和定量冠状动脉成形术均显示出明显的新内膜减少和更少的晚期管腔丢失(分别为P = 0.05和P = 0.03)。与-limus DES-ISR + PCB组相比,PES-ISR1PCB组显示出更高的围栏周围炎症和纤维蛋白评分。结论:在ISR中,紫杉醇主要沉积在新内膜组织中,并在使用PCB后随时间有效保留。尽管存在金属支柱,但仍具有均匀分布的特征。 PCB在DES-ISR中表现出同等的生物学效应,而不会明显增加炎症。 (C)2015年Wiley Periodicals,Inc.

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