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基于质谱的蛋白质组学在研究聚乙二醇水凝胶上血清蛋白吸附/吸收及补体C3激活中的应用。

Application of MS-based proteomics to study serum protein adsorption/absorption and complement C3 activation on poly(ethylene glycol) hydrogels.

作者信息

Wang Xintong, Schmidt David R, Joyce Evan J, Kao W John

机构信息

a School of Pharmacy, University of Wisconsin-Madison, 777 Highland Avenue, Madison, WI 53705, USA.

出版信息

J Biomater Sci Polym Ed. 2011;22(10):1343-62. doi: 10.1163/092050610X508400.

Abstract

Although the interaction between cells and poly(ethylene glycol) (PEG) hydrogels is well documented, there lacks a thorough investigation into the adsorption of blood proteins on these surfaces which dictates the observed cellular and in vivo host response. Thus, a clear understanding of how surface-bound proteins mediate the unique biological property of PEG hydrogels is fundamentally important. The information obtained will also provide insights into future biomaterial design. In this study, several mass-spectrometrybased proteomic tools coupled with complementary immunoassays were employed to survey the complex surface-bound serum proteome. The adsorption of vitronectin, thrombin, fibrinogen and complement component C3 was significantly lower on PEG hydrogels than on tissue culture polystyrene (TCPS). Although PEG hydrogels mediated lower C3 adsorption than TCPS, the extent of C3 activation between the two surfaces was comparable. Adherent monocyte density was also significantly lower on PEG hydrogels as compared to TCPS. Taken together, these results support the critical role of the complement C3 in mediating monocyte adhesion on biomaterials. Thus we conclude that the biocompatibility of PEG hydrogels both in vitro and in vivo can be partly contributed to their limited C3 interaction and monocyte activity.

摘要

尽管细胞与聚乙二醇(PEG)水凝胶之间的相互作用已有充分记载,但对于这些表面上血液蛋白的吸附情况却缺乏深入研究,而血液蛋白的吸附决定了所观察到的细胞反应和体内宿主反应。因此,清楚了解表面结合蛋白如何介导PEG水凝胶的独特生物学特性至关重要。所获得的信息也将为未来生物材料的设计提供见解。在本研究中,使用了几种基于质谱的蛋白质组学工具并结合互补免疫测定法来检测复杂的表面结合血清蛋白质组。在PEG水凝胶上,玻连蛋白、凝血酶、纤维蛋白原和补体成分C3的吸附明显低于组织培养聚苯乙烯(TCPS)。尽管PEG水凝胶介导的C3吸附低于TCPS,但两个表面之间的C3活化程度相当。与TCPS相比,PEG水凝胶上贴壁单核细胞密度也明显更低。综上所述,这些结果支持补体C3在介导单核细胞黏附于生物材料上的关键作用。因此我们得出结论,PEG水凝胶在体外和体内的生物相容性部分可归因于其有限的C3相互作用和单核细胞活性。

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