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Linking the foreign body response and protein adsorption to PEG-based hydrogels using proteomics

自愈水凝胶 PEG比率 乙二醇 蛋白质吸附 生物物理学 材料科学 吸附 体内 粘附 化学 高分子化学 有机化学 生物 财务 生物技术 经济
作者
Mark D. Swartzlander,Christopher A. Barnes,Anna K. Blakney,Joel L. Kaar,Themis R. Kyriakides,Stephanie J. Bryant
出处
期刊:Biomaterials [Elsevier BV]
卷期号:41: 26-36 被引量:148
标识
DOI:10.1016/j.biomaterials.2014.11.026
摘要

Poly(ethylene glycol) (PEG) hydrogels with their highly tunable properties are promising implantable materials, but as with all non-biological materials, they elicit a foreign body response (FBR). Recent studies, however, have shown that incorporating the oligopeptide RGD into PEG hydrogels reduces the FBR. To better understand the mechanisms involved and the role of RGD in mediating the FBR, PEG, PEG-RGD and PEG-RDG hydrogels were investigated. After a 28-day subcutaneous implantation in mice, a thinner and less dense fibrous capsule formed around PEG-RGD hydrogels, while PEG and PEG-RDG hydrogels exhibited stronger, but similar FBRs. Protein adsorption to the hydrogels, which is considered the first step in the FBR, was also characterized. In vitro experiments confirmed that serum proteins adsorbed to PEG-based hydrogels and were necessary to promote macrophage adhesion to PEG and PEG-RDG, but not PEG-RGD hydrogels. Proteins adsorbed to the hydrogels in vivo were identified using liquid chromatography-tandem mass spectrometry. The majority (245) of the total proteins (≥300) that were identified was present on all hydrogels with many proteins being associated with wounding and acute inflammation. These findings suggest that the FBR to PEG hydrogels may be mediated by the presence of inflammatory-related proteins adsorbed to the surface, but that macrophages appear to sense the underlying chemistry, which for RGD improves the FBR.
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