京尼平
组织谷氨酰胺转胺酶
组织工程
材料科学
碳二亚胺
生物医学工程
成纤维细胞
因子XIIIa
基质(水族馆)
真皮成纤维细胞
纳米技术
生物物理学
高分子化学
生物化学
壳聚糖
体外
化学
酶
地质学
海洋学
生物
纤维蛋白原
医学
作者
Malavika Nair,Ramneek K. Johal,Samir W. Hamaia,Serena M. Best,Ruth E. Cameron
出处
期刊:Biomaterials
[Elsevier]
日期:2020-05-22
卷期号:254: 120109-120109
被引量:99
标识
DOI:10.1016/j.biomaterials.2020.120109
摘要
Due to its ubiquity and versatility in the human body, collagen is an ideal base material for tissue-engineering constructs. Chemical crosslinking treatments allow precise control of the biochemical and mechanical properties through macromolecular modifications to the structure of collagen. In this work, three key facets regarding the collagen crosslinking process are explored. Firstly, a comparison is drawn between the carbodiimide-succinimide (EDC-NHS) system and two emerging crosslinkers utilising alternate chemistries: genipin and tissue transglutaminase (TG2). By characterising the chemical changes upon treatment, the effect of EDC-NHS, genipin and TG2 crosslinking mechanisms on the chemical structure of collagen, and thus the mechanical properties conferred to the substrate is explored. Secondly, the relative importance of mechanical and biochemical cues on cellular phenomena are investigated, including cell viability, integrin-specific attachment, spreading and proliferation. Here, we observe that for human dermal fibroblasts, long-term, stable proliferation is preconditioned by the availability of suitable binding sites, irrespective of the substrate modulus post-crosslinking. Finally, as seen in the graphical abstract we show that by choosing the appropriate crosslinker chemistries, a materials selection map can be drawn for collagen films, encompassing both a range of tensile modulus and fibroblast proliferation which can be modified independently. Thus, in addition to a range of parameters that can be modified in collagen constructs, we demonstrate a route to obtaining tunable bioactivity and mechanics in collagen constructs is uncovered, that is exclusively driven by the crosslinking process.
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