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Enhancing Cell Affinity of Nonadhesive Hydrogel Substrate: The Role of Silica Hybridization

机译:增强非粘性水凝胶基质的细胞亲和力:二氧化硅杂交的作用。

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摘要

The aim of this study is to elucidate the functional mechanism of nanosilica-induced cell affinity for the normally attachment-fouling hydrogel substrates. Investigations were conducted in the following three major aspects: (1) environmental protein adsorption before cell contacts, which determines the presence of adhesive ligands; (2) integrin expression profile, which reflects the cell responses via surface receptor turning-over; and (3) vinculin activation and F-actin assembly, which sketches the induced cytoskeletal organization posing for focal adhesion. The results indicate that the hybridized nanosilica additives are capable of arresting adhesive proteins from the environment. As binding ligands, such immobilized proteins activate α5β1-specific pathway for cell focal adhesion, but fail in invoking β3-participated signaling cascade. This partial activation enables modest amount of high-quality cell adhesion on the modified substrate, by which a conservative cell affinity is established on hydrogel matrices.
机译:这项研究的目的是阐明正常附着污损水凝胶基质的纳米二氧化硅诱导的细胞亲和力的功能机制。从以下三个主要方面进行了研究:(1)细胞接触之前环境蛋白的吸附,这决定了粘附配体的存在; (2)整合素表达谱,其通过表面受体翻转反应细胞反应; (3)纽蛋白活化和F-肌动蛋白组装,勾画出诱导的细胞骨架组织构成的粘着斑。结果表明,杂交的纳米二氧化硅添加剂能够阻止环境中的粘附蛋白。作为结合配体,这种固定化的蛋白质激活了α5β1特异性途径来粘附细胞,但无法激活参与β3的信号传导级联。这种部分活化使得在修饰的基质上适量的高质量细胞粘附成为可能,从而在水凝胶基质上建立了保守的细胞亲和力。

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