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Arginine functionalization of hydrogels for heparin binding-a supramolecular approach to developing a pro-angiogenic biomaterial

机译:肝素结合水凝胶的精氨酸功能化-超分子方法开发促血管生成生物材料

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摘要

Our aim was to synthesize a biomaterial that stimulates angiogenesis for tissue engineering applications by exploiting the ability of heparin to bind and release vascular endothelial growth factor (VEGF). The approach adopted involved modification of a hydrogel with positively charged peptides (oligolysine or oligoarginine) to achieve heparin binding. Precursor hydrogels were produced from copolymerization of N-vinyl pyrolidone, diethylene glycol bis allyl carbonate and acrylic acid (PNDA) and functionalized after activation of the carboxylic acid groups with trilysine or triarginine peptides (PNDKKK and PNDRRR). Both hydrogels were shown to bind and release bioactive VEGF165 with arginine-modified hydrogel outperforming the lysine-modified hydrogel. Cytocompatibility of the hydrogels was confirmed in vitro with primary human dermal fibroblasts and human dermal microvascular endothelial cells (HUDMECs). Proliferation of HUDMECs was stimulated by triarginine-functionalized hydrogels, and to a lesser extent by lysine functionalized hydrogels once loaded with heparin and VEGF. The data suggests that heparin-binding hydrogels provide a promising approach to a pro-angiogenic biomaterial.
机译:我们的目标是通过利用肝素结合和释放血管内皮生长因子(VEGF)的能力,合成一种可刺激血管生成以用于组织工程应用的生物材料。所采用的方法涉及用带正电荷的肽(寡聚赖氨酸或寡聚精氨酸)修饰水凝胶以实现肝素结合。前体水凝胶由N-乙烯基吡咯烷酮,二甘醇双碳酸烯丙酯和丙烯酸(PNDA)的共聚反应制得,并在羧酸基团被三赖氨酸或三精氨酸肽(PNDKKK和PNDRRR)活化后被官能化。两种水凝胶均显示与精氨酸修饰的水凝胶结合并释放生物活性VEGF165,其性能优于赖氨酸修饰的水凝胶。在体外用原代人皮肤成纤维细胞和人皮肤微血管内皮细胞(HUDMEC)证实了水凝胶的细胞相容性。精氨酸功能化的水凝胶可刺激HUDMEC的增殖,而载有肝素和VEGF的赖氨酸功能化的水凝胶可在较小程度上促进HUDMEC的增殖。数据表明,结合肝素的水凝胶为促血管生成生物材料提供了一种有前途的方法。

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