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Enzymatic Cross-Linking of Resilin-Based Proteins for Vascular Tissue Engineering Applications

机译:基于弹性蛋白的蛋白质的酶促交联在血管组织工程中的应用

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摘要

Protein-based biomaterials have received significant attention for tissue engineering applications. For example, resilin-based protein gels have been produced with different cross-linking chemistries for applications in cartilage, cardiovascular, and vocal fold engineering. In this study, we investigate an alternative cross-linking chemistry to form resilin-based protein hydrogels and demonstrate the versatility of the gels for investigating cell response to matrix stiffness. Specifically, transglutaminase was used to cross-link proteins and resulted in gel surfaces more suitable for long-term cell attachment compared to those formed by a Mannich-type condensation reaction. Since matrix stiffness is an important determinant in modulating cell response, we first tuned matrix stiffness by varying total protein concentration. Next, we observed that matrix stiffness modulated cell spreading and endothelial differentiation of human mesenchymal stem cells. In particular, our results show that cells differentiated on our matrices, which have a stiffness similar to subendothelial layers, had statistically equivalent endothelial function compared to cells differentiated on hard glass surfaces. Thus, our protein-based matrix system is a promising tool to provide substrates favorable for long-term cell attachment and better mimics the native subendothelial environment compared to conventional hard culture substrates.
机译:基于蛋白质的生物材料在组织工程应用中受到了极大的关注。例如,已经生产出具有不同交联化学的基于弹性蛋白的蛋白质凝胶,用于软骨,心血管和声带工程。在这项研究中,我们研究了形成交联蛋白的蛋白质水凝胶的另一种交联化学,并证明了该凝胶在研究细胞对基质刚度反应方面的多功能性。具体而言,与通过曼尼希型缩合反应形成的凝胶表面相比,转谷氨酰胺酶被用于使蛋白质交联,并导致凝胶表面更适合长期细胞附着。由于基质刚度是调节细胞反应的重要决定因素,因此我们首先通过改变总蛋白浓度来调节基质刚度。接下来,我们观察到基质刚度调节人间充质干细胞的细胞扩散和内皮分化。特别地,我们的结果表明,与在硬质玻璃表面上分化的细胞相比,在我们的基质上分化的细胞具有类似于内皮下层的硬度,具有统计学上等效的内皮功能。因此,与传统的硬质培养基质相比,我们基于蛋白质的基质系统是一种有前途的工具,可提供有利于长期细胞附着的基质,并更好地模拟天然的内皮下环境。

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