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Microgel Particles with Distinct Morphologies and Common Chemical Compositions: A Unified Description of the Responsivity to Temperature and Osmotic Stress

机译:微凝胶颗粒具有不同的形态和常用化学组合物:对温度和渗透胁迫的响应性的统一描述

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摘要

Poly(N-isopropylacrylamide) (PNIPAM) hydrogel microparticles with different core–shell morphologies have been designed, while maintaining an unvaried chemical composition: a morphology with (i) an un-crosslinked core with a crosslinked shell of PNIPAM chains and (ii) PNIPAM chains crosslinked to form the core with a shell consisting of tethered un-crosslinked PNIPAM chains to the core. Both morphologies with two different degrees of crosslinking have been assessed by confocal microscopy and tested with respect to their temperature responsivity and deformation by applying an osmotic stress. The thermal and mechanical behavior of these architectures have been framed within a Flory–Rehner modified model in order to describe the microgel volume shrinking occurring as response to a temperature increase or an osmotic perturbation. This study provides a background for assessing to what extent the mechanical features of the microgel particle surface affect the interactions occurring at the interface of a microgel particle with a cell, in addition to the already know ligand/receptor interaction. These results have direct implications in triggering a limited phagocytosis of microdevices designed as injectable drug delivery systems.
机译:设计了聚(N-异丙基丙烯酰胺)(泊铂)水凝胶微粒,具有不同的核壳形态,同时保持不变的化学成分:与(I)的形态与肺链的交联壳和(II)的交联壳PNIPAM链交联以形成核心,壳体由核心组成的壳体组成至核心。通过共聚焦显微镜评估具有两种不同程度的交联的形态,并通过施加渗透胁迫对其温度响应度和变形进行测试。这些架构的热量和力学行为已经在源 - 再料修改模型中伪造,以描述作为对温度升高或渗透扰动的响应发生的微凝胶体积缩小。该研究提供了用于评估微凝胶颗粒表面的机械特征在多大程度上影响在微凝胶颗粒与细胞的界面处发生的相互作用,除了已经知道的配体/受体相互作用之外。这些结果对触发设计为可注射药物递送系统的微生物有限的吞噬作用有直接影响。

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