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Biofunctionalization of Biomaterials for Accelerated in Situ Endothelialization: A Review

机译:促进原位内皮化的生物材料的生物功能化:审查。

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摘要

The higher patency rates of cardiovascular implants, including vascular bypass grafts, stents, and heart valves are related to their ability to inhibit thrombosis, intimal hyperplasia, and calcification. In native tissue, the endothelium plays a major role in inhibiting these processes. Various bioengineering research strategies thereby aspire to induce endothelialization of graft surfaces either prior to implantation or by accelerating in situ graft endothelialization. This article reviews potential bioresponsive molecular components that can be incorporated into (and/or released from) biomaterial surfaces to obtain accelerated in situ endothelialization of vascular grafts. These molecules could promote in situ endothelialization by the mobilization of endothelial progenitor cells (EPC) from the bone marrow, encouraging cell-specific adhesion (endothelial cells (EC) and/or EPC) to the graft and, once attached, by controlling the proliferation and differentiation of these cells. EC and EPC interactions with the extracellular matrix continue to be a principal source of inspiration for material biofunctionalization, and therefore, the latest developments in understanding these interactions will be discussed.
机译:心血管植入物(包括血管搭桥术,支架和心脏瓣膜)的通畅率较高,与它们抑制血栓形成,内膜增生和钙化的能力有关。在天然组织中,内皮在抑制这些过程中起主要作用。因此,各种生物工程研究策略都渴望在植入之前或通过加速原位移植物的内皮化来诱导移植物表面的内皮化。本文介绍了潜在的生物响应性分子成分,可以将其掺入生物材料表面(和/或从生物材料表面释放),以获得加速的血管移植物原位内皮化。这些分子可通过从骨髓中动员内皮祖细胞(EPC)来促进原位内皮化,从而促进细胞特异性粘附(内皮细胞(EC)和/或EPC)与移植物的结合,并在附着后通过控制增殖和这些细胞的分化。 EC和EPC与细胞外基质的相互作用仍然是材料生物功能化的主要灵感来源,因此,将讨论理解这些相互作用的最新进展。

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