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首页> 外文期刊>Journal of Bioactive and Compatible Polymers >Structural engineering to control density, conformation, and bioactivity of the poly(ethylene glycol)-grafted poly(urethane urea) scaffolds
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Structural engineering to control density, conformation, and bioactivity of the poly(ethylene glycol)-grafted poly(urethane urea) scaffolds

机译:控制聚(乙二醇) - 移植聚(氨基甲酸酯脲)支架的密度,构象和生物活性的结构工程

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摘要

Poly(urethane urea) scaffolds were fabricated through combined salt leaching and solvent casting methods. The scaffolds were then functionalized via aminolysis with poly(ethylene glycol) (PEG- g -PUU). To compare its bioactivity, gelatin was also grafted onto the aminolyzed poly(urethane urea) surface (Gel- g -PUU). Chemical changes at the surface were then monitored using quantitative/qualitative methods. Grafting with both gelatin and poly(ethylene glycol) remarkably enhanced the wettability of poly(urethane urea). Proliferation of human adipose–derived mesenchymal stem cells on poly(urethane urea) and the modified poly(urethane urea)s was evaluated by 3-[4,5-dimethylthiazol-2-yl]-2,5 diphenyl tetrazolium bromide assay. The cell experiment results showed that both the modified poly(urethane urea)s enhanced the attachment and proliferation of human adipose–derived mesenchymal stem cells compared to pure poly(urethane urea). Based on previous reports, while a supportive role is observed at adequate poly(ethylene glycol) graft densities, cell adhesion and proliferation are inhibited at very high grafting densities. To correlate the cell data to poly(ethylene glycol) conformations, the surface tension was measured. Data on human adipose–derived mesenchymal stem cells’ attachment/proliferation and contact angle/surface free energy together showed that the grafting density of poly(ethylene glycol) was regulated by optimizing aminolysis conditions, careful selection of poly(ethylene glycol)’s molecular weight, and bulk properties of the matrix poly(urethane urea). As a result, surface overcrowding and brush conformation of the poly(ethylene glycol) chains were avoided, and human adipose–derived mesenchymal stem cell attachment and proliferation occurred on the PEG- g -PUU scaffold at a comparable level to the Gel- g -PUU.
机译:通过组合盐浸出和溶剂铸造方法制造聚(氨基甲酸酯尿素)支架。然后通过用聚(乙二醇)(PEG-G-PUU)氨基溶液官能化支架。为了比较其生物活性,还将明胶接枝到氨基聚(氨基甲酸酯脲)表面(凝胶-G-PUU)上。然后使用定量/定性方法监测表面的化学变化。用明胶和聚(乙二醇)接枝显着提高了聚(氨基甲酸酯脲)的润湿性。通过3- [4,5-二甲基噻唑-2-基] -2,5二苯基四唑溴化物测定,评价人脂肪衍生的衍生间充质干细胞和改性聚(氨基甲酸酯脲)S的增殖。细胞实验结果表明,与纯聚(聚氨酯尿素)相比,改性聚(氨基甲酸酯脲)S增强了人脂肪衍生的间充质干细胞的附着和增殖。基于先前的报告,虽然在足够的聚(乙二醇)接枝的嫁接密度下观察到支持性作用,但在非常高的接枝密度下抑制细胞粘附和增殖。为了将细胞数据与聚(乙二醇)构象相关联,测量表面张力。人脂肪衍生的间充质干细胞的附着/增殖和接触角/表面自由能的数据表明,通过优化氨基溶质,仔细选择聚(乙二醇)的分子来调节聚(乙二醇)的移植密度基质聚(氨基甲酸酯尿素)的重量和块状性质。结果,避免了聚(乙二醇)链的表面过度拥挤和刷子构象,并且在PEG-G-PUU支架上以相当水平的凝胶 - G-P-G-g - puu。

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