首页> 美国卫生研究院文献>Regenerative Biomaterials >Distinctive effects of CD34- and CD133-specific antibody-coated stents on re-endothelialization and in-stent restenosis at the early phase of vascular injury
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Distinctive effects of CD34- and CD133-specific antibody-coated stents on re-endothelialization and in-stent restenosis at the early phase of vascular injury

机译:CD34和CD133特异性抗体涂层支架在血管损伤早期对重新内皮化和支架内再狭窄的独特作用

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摘要

It is not clear what effects of CD34- and CD133-specific antibody-coated stents have on re-endothelialization and in-stent restenosis (ISR) at the early phase of vascular injury. This study aims at determining the capabilities of different coatings on stents (e.g. gelatin, anti-CD133 and anti-CD34 antibodies) to promote adhesion and proliferation of endothelial progenitor cells (EPCs). The in vitro study revealed that the adhesion force enabled the EPCs coated on glass slides to withstand flow-induced shear stress, so that allowing for the growth of the cells on the slides for 48 h. The in vivo experiment using a rabbit model in which the coated stents with different substrates were implanted showed that anti-CD34 and anti-CD133 antibody-coated stents markedly reduced the intima area and restenosis than bare mental stents (BMS) and gelatin-coated stents. Compared with the anti-CD34 antibody-coated stents, the time of cells adhesion was longer and earlier present in the anti-CD133 antibody-coated stents and anti-CD133 antibody-coated stents have superiority in re-endothelialization and inhibition of ISR. In conclusion, this study demonstrated that anti-CD133 antibody as a stent coating for capturing EPCs is better than anti-CD34 antibody in promoting endothelialization and reducing ISR.
机译:尚不清楚CD34和CD133特异性抗体涂层支架在血管损伤早期对再内皮化和支架内再狭窄(ISR)有什么影响。这项研究旨在确定支架上不同涂层(例如明胶,抗CD133和抗CD34抗体)促进内皮祖细胞(EPC)粘附和增殖的能力。体外研究表明,粘附力使涂覆在载玻片上的EPC能够承受流动引起的剪切应力,从而使载玻片上的细胞能够生长48小时。使用兔子模型的体内实验(其中植入了具有不同基质的涂层支架)显示,与裸露的心理支架(BMS)和明胶涂层的支架相比,抗CD34和抗CD133抗体涂层的支架显着减少了内膜面积和再狭窄。 。与抗CD34抗体支架相比,抗CD133抗体支架的细胞粘附时间更长,而且存在时间更早,而抗CD133抗体支架在再内皮化和抑制ISR方面具有优势。总之,这项研究表明,抗CD133抗体作为捕获EPC的支架涂层,在促进内皮化和减少ISR方面优于抗CD34抗体。

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