McGann Christopher L, Akins Robert E, Kiick Kristi L
Nemours - Alfred I. duPont Hospital for Children, Department of Biomedical Research, Wilmington, Delaware 19803, United States.
Delaware Biotechnology Institute, 15 Innovation Way, Newark, Delaware 19711, United States.
Biomacromolecules. 2016 Jan 11;17(1):128-40. doi: 10.1021/acs.biomac.5b01255. Epub 2015 Dec 22.
Hydrogels derived from resilin-like polypeptides (RLPs) have shown outstanding mechanical resilience and cytocompatibility; expanding the versatility of RLP-based materials via conjugation with other polypeptides and polymers would offer great promise in the design of a range of materials. Here, we present an investigation of the biochemical and mechanical properties of hybrid hydrogels composed of a recombinant RLP and a multiarm PEG macromer. These hybrid hydrogels can be rapidly cross-linked through a Michael-type addition reaction between the thiols of cysteine residues on the RLP and vinyl sulfone groups on the multiarm PEG. Oscillatory rheology and tensile testing confirmed the formation of elastomeric hydrogels with mechanical resilience comparable to aortic elastin; hydrogel stiffness was easily modulated through the cross-linking ratio. Macromolecular phase separation of the RLP-PEG hydrogels offers the unique advantage of imparting a heterogeneous microstructure, which can be used to localize cells, through simple mixing and cross-linking. Assessment of degradation of the RLP by matrix metalloproteinases (MMPs) illustrated the specific proteolysis of the polypeptide in both its soluble form and when cross-linked into hydrogels. Finally, the successful encapsulation and viable three-dimensional culture of human mesenchymal stem cells (hMSCs) demonstrated the cytocompatibility of the RLP-PEG gels. Overall, the cytocompatibility, elastomeric mechanical properties, microheterogeneity, and degradability of the RLP-PEG hybrid hydrogels offer a suite of promising properties for the development of cell-instructive, structured tissue engineering scaffolds.
源自类弹性蛋白多肽(RLP)的水凝胶已展现出出色的机械弹性和细胞相容性;通过与其他多肽及聚合物共轭来拓展基于RLP材料的多功能性,有望为一系列材料的设计带来巨大前景。在此,我们对由重组RLP和多臂PEG大分子单体组成的混合水凝胶的生化和力学性能进行了研究。这些混合水凝胶可通过RLP上半胱氨酸残基的硫醇与多臂PEG上乙烯砜基团之间的迈克尔型加成反应快速交联。振荡流变学和拉伸测试证实形成了具有与主动脉弹性蛋白相当的机械弹性的弹性水凝胶;水凝胶的硬度可通过交联比轻松调节。RLP-PEG水凝胶的大分子相分离具有赋予异质微观结构的独特优势,通过简单混合和交联可用于定位细胞。基质金属蛋白酶(MMP)对RLP降解的评估表明,该多肽在其可溶形式以及交联入水凝胶时均会发生特异性蛋白水解。最后,人骨髓间充质干细胞(hMSCs)的成功包封和三维活细胞培养证明了RLP-PEG凝胶的细胞相容性。总体而言,RLP-PEG混合水凝胶的细胞相容性、弹性力学性能、微观异质性和可降解性为开发具有细胞指导作用的结构化组织工程支架提供了一系列有前景的特性。