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Mechanisms of smooth muscle cell proliferation and endothelial regeneration after vascular injury and stenting: approach to therapy.

机译:血管损伤和支架置入术后平滑肌细胞增殖和内皮再生的机制:治疗方法。

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摘要

Bare metal stents (BMS) successfully prevented abrupt artery closure and reduced the restenosis rate compared with balloon angioplasty. This review summarizes laboratory and recent clinical investigations concerning neointimal formation and endothelial regeneration after vascular injury. BMS efficacy was severely hampered by proliferating vascular smooth muscle cells (VSMCs), and the resultant neointimal hyperplasia, which is the only mechanism responsible for restenosis after metal stent placement. The advent of drug-eluting stents (DES) in 2002 have since then revolutionized interventional cardiology. By using the stent struts as a platform coated with polymers to elute drugs targeting VSMC proliferation, a substantial attenuation of in-stent restenosis is feasible. As with any medical innovation this technology still has restrictive factors, and novel approaches are promoted to improve the safety and efficacy of DES. Indeed, the antiproliferative properties of DES impair and/or delay endothelialization, hence leading to late stent thrombosis. Improvements in percutaneous coronary intervention procedures include the use of the so-called "second-generation DES", together with new coating technologies, bioabsorbable stents, and non-drug-based stent coatings. Particular emphasis will be placed on the concept that endothelial regeneration might be pursued as well as reduction of VSMC proliferation to allow stable successful revascularization after DES deployment.
机译:与气囊血管成形术相比,裸金属支架(BMS)成功地防止了动脉突然闭合并降低了再狭窄率。这篇综述总结了有关血管损伤后新内膜形成和内皮再生的实验室研究和近期临床研究。血管平滑肌细胞(VSMC)的增殖以及由此产生的新内膜增生严重阻碍了BMS的有效性,这是金属支架置入后引起再狭窄的唯一机制。自2002年以来,药物洗脱支架(DES)的问世彻底改变了介入心脏病学。通过使用支架支杆作为涂覆有聚合物的平台来洗脱靶向VSMC增殖的药物,可以切实缓解支架内再狭窄。像任何医疗创新一样,该技术仍然具有局限性,并且提出了新颖的方法来提高DES的安全性和有效性。实际上,DES的抗增殖特性损害和/或延迟内皮化,因此导致晚期支架血栓形成。经皮冠状动脉介入手术的改进包括使用所谓的“第二代DES”,以及新的涂层技术,可生物吸收的支架和基于非药物的支架涂层。将特别强调可能进行内皮再生以及减少VSMC增殖以允许在DES部署后稳定成功进行血运重建的概念。

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