自愈水凝胶
粘蛋白
蛋白酵素
材料科学
高分子
唾液酸
生物物理学
聚糖
生物化学
糖蛋白
生物
化学
酶
高分子化学
作者
Kun Jiang,Hongji Yan,Carolin A. Rickert,Matthias Marczynski,Kajsa Sixtensson,Francisco Vilaplana,Oliver Lieleg,Thomas Crouzier
标识
DOI:10.1002/adfm.202008428
摘要
Abstract Hydrogels made of crosslinked macromolecules used in regenerative medicine technologies can be designed to affect the fate of surrounding cells and tissues in defined ways. Their function typically depends on the type and number of bioactive moieties such as receptor ligands present in the hydrogel. However, the detail in how such moieties are presented to cells can also be instrumental. In this work, how the crosslinking architecture of a hydrogel can affect its bioactivity is explored. It is shown that bovine submaxillary mucins, a highly glycosylated and immune‐modulating protein, exhibit strikingly different bioactivities whether they are crosslinked through their glycans or their protein domains. Both the susceptibility to enzymatic degradation and macrophage response are affected, while rheological properties and barrier to diffusion are mostly unaffected. The results suggest that crosslinking architecture affects the accessibility of the substrate to proteases and the pattern of sialic acid residues exposed to the macrophages. Thus, modulating the accessibility of binding sites through the choice of the crosslinking strategy appears as a useful parameter to tune the bioactivity of hydrogel‐based systems.
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