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Effective Tuning of Ligand Incorporation and Mechanical Properties in Visible Light Photopolymerized Poly(ethylene glycol) Diacrylate Hydrogels Dictates Cell Adhesion and Proliferation

机译:有效调整配体掺入和可见光光聚合聚(乙二醇)二丙烯酸酯水凝胶中的机械性能决定了细胞粘附和增殖

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摘要

Cell behavior is guided by the complex interplay of matrix mechanical properties as well as soluble and immobilized biochemical signals. The development of synthetic scaffolds that incorporate key functionalities of the native extracellular matrix (ECM) for support of cell proliferation and tissue regeneration requires that stiffness and immobilized concentrations of ECM signals within these biomaterials be tuned and optimized prior to in vitro and in vivo studies. A detailed experimental sensitivity analysis was conducted to identify the key polymerization conditions that result in significant changes in both elastic modulus and immobilized YRGDS within visible light photopolymerized poly(ethylene glycol) diacrylate (PEGDA) hydrogels. Among the polymerization conditions investigated, single as well as simultaneous variations in N-vinylpyrrolidinone (NVP) and precursor concentrations of Acryl-PEG3400-YRGDS resulted in a broad range of hydrogel elastic modulus (81 – 1178 kPa) and YRGDS surface concentration (0.04 – 1.72 pmol/cm2). Increasing the YRGDS surface concentration enhanced fibroblast cell adhesion and proliferation for a given stiffness, while increases in hydrogel elastic modulus caused decreases in cell adhesion and increases in proliferation. The identification of key polymerization conditions is critical for the tuning and optimization of biomaterial properties and the controlled study of cell-substrate interactions.
机译:细胞行为受基质机械性能以及可溶性和固定化生化信号复杂相互作用的指导。整合天然细胞外基质(ECM)关键功能以支持细胞增殖和组织再生的合成支架的开发要求在体外和体内研究之前对这些生物材料中的刚性和固定的ECM信号浓度进行调整和优化。进行了详细的实验灵敏度分析,以确定导致可见光光聚合的聚(乙二醇)二丙烯酸(PEGDA)水凝胶中弹性模量和固定YRGDS均发生重大变化的关键聚合条件。在研究的聚合条件中,N-乙烯基吡咯烷酮(NVP)和Acryl-PEG3400-YRGDS的前体浓度同时发生单一变化和同时变化,导致水凝胶弹性模量(81 – 1178 kPa)和YRGDS表面浓度(0.04 – 1.72 pmol / cm 2 )。在给定的硬度下,增加YRGDS表面浓度会增强成纤维细胞的粘附和增殖,而水凝胶弹性模量的增加会导致细胞粘附的减少和增殖的增加。关键聚合条件的确定对于调节和优化生物材料特性以及对细胞-底物相互作用的受控研究至关重要。

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