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Biomaterial Surface Hydrophobicity-Mediated Serum Protein Adsorption and Immune Responses

机译:生物材料表面疏水性介导的血清蛋白质吸附和免疫应答

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The nature of the protein corona forming on biomaterial surfaces can affect the performance of implanted devices. This study investigated the role of surface chemistry and wettability on human serum-derived protein corona formation on biomaterial surfaces and the subsequent effects on the cellular innate immune response. Plasma polymerization, a substrate-independent technique, was employed to create nanothin coatings with four specific chemical functionalities and a spectrum of surface charges and wettability. The amount and type of protein adsorbed was strongly influenced by surface chemistry and wettability but did not show any dependence on surface charge. An enhanced adsorption of the dysopsonin albumin was observed on hydrophilic carboxyl surfaces while high opsonin IgG2 adsorption was seen on hydrophobic hydrocarbon surfaces. This in turn led to a distinct immune response from macrophages; hydrophilic surfaces drove greater expression of anti-inflammatory cytokines by macrophages, whilst surface hydrophobicity caused increased production of proinflammatory signaling molecules. These findings map out a unique relationship between surface chemistry, hydrophobicity, protein corona formation, and subsequent cellular innate immune responses; the potential outcomes of these studies may be employed to tailor biomaterial surface modifications, to modulate serum protein adsorption and to achieve the desirable innate immune response to implanted biomaterials and devices.
机译:在生物材料表面上形成的蛋白质电晕的性质可以影响植入装置的性能。本研究调查了表面化学和润湿性对人血清衍生蛋白电晕形成的生物材料表面和随后对细胞先天性免疫应答的影响。采用基材无关的技术等离子体聚合,以产生具有四种特定化学功能的纳米型涂层和表面电荷和润湿性。吸附的蛋白质的量和类型受到表面化学和润湿性的强烈影响,但没有显示出对表面电荷的任何依赖性。在亲水性羧基表面上观察到脱染蛋白白蛋白的增强的吸附,而在疏水性烃表面上观察到高opsonin IgG2吸附。这反过来导致巨噬细胞的不同免疫反应;亲水性表面通过巨噬细胞驱动更大的抗炎细胞因子的表达,而表面疏水性导致促炎信号分子的产生增加。这些发现将表面化学,疏水性,蛋白质电晕形成和随后的细胞先天免疫反应之间的独特关系。这些研究的潜在结果可以用于定制生物材料表面修饰,以调节血清蛋白质吸附,并达到植入生物材料和装置的理想的先天免疫应答。

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