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Protein Adsorption Mechanisms Determine the Efficiency of Thermally Controlled Cell Adhesion on Poly(/V-isopropyl acrylamide) Brushes

机译:蛋白质吸附机制决定了热控制细胞在聚(/ V-异丙基丙烯酰胺)刷上的粘附效率

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摘要

This study investigated the impact of the protein adsorption mechanism(s) on the efficiency of thermally controlled cell adhesion and release from poly(N-isopropyl acrylamide) brushes. Large format polymer gradients were used to screen for grafting densities and substrate chemistries that alter both cell adhesion at 37 °C and rapid cell release at 25 °C. In particular, die grafting conditions investigated allowed protein adsorption to the underlying substrate, penetration of the brush only, or adsorption to the outer edge of the film. At an average molecular weight of 30 kDa (degree of polymerization N ~ 270), the results show that robust protein adsorption to polymer brushes impairs rapid cell release below the lower critical solution temperature. Conversely, grafting conditions that permit protein penetration of the brush but block strong adsorption to the underlying substrate support cell adhesion above the transition temperature and ensure efficient cell recovery at lower temperature. These findings demonstrate the impact of protein adsorption mechanisms, surface chemistry, and polymer properties on thermally controlled cell capture and release.
机译:这项研究调查了蛋白质吸附机制对热控制细胞粘附和从聚(N-异丙基丙烯酰胺)刷子释放的效率的影响。大幅面聚合物梯度用于筛选接枝密度和底物化学性质,以改变37°C下的细胞粘附和25°C下的快速细胞释放。特别地,研究的芯片接枝条件允许蛋白质吸附到下面的基材上,仅渗透刷子,或吸附到薄膜的外边缘。结果表明,在平均分子量为30 kDa(聚合度N〜270)下,蛋白质在聚合物刷上的牢固吸附会削弱细胞在较低的临界溶液温度以下的快速释放。相反,嫁接条件允许蛋白质渗透刷,但阻止强烈吸附到下面的底物上,从而在过渡温度以上支持细胞粘附,并确保在较低温度下有效回收细胞。这些发现证明了蛋白质吸附机制,表面化学和聚合物性质对热控制细胞捕获和释放的影响。

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