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首页> 外文期刊>Acta biomaterialia >Compressive elasticity of three-dimensional nanofiber matrix directs mesenchymal stem cell differentiation to vascular cells with endothelial or smooth muscle cell markers
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Compressive elasticity of three-dimensional nanofiber matrix directs mesenchymal stem cell differentiation to vascular cells with endothelial or smooth muscle cell markers

机译:三维纳米纤维基质的压缩弹性将间充质干细胞分化导向具有内皮或平滑肌细胞标志物的血管细胞

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The importance of mesenchymal stem cells (MSC) in vascular regeneration is becoming increasingly recognized. However, few in vitro studies have been performed to identify the effects of environmental elasticity on the differentiation of MSC into vascular cell types. Electrospinning and photopolymerization techniques were used to fabricate a three-dimensional (3-D) polyethylene glycol dimethacrylate nanofiber hydrogel matrix with tunable elasticity for use as a cellular substrate. Compression testing demonstrated that the elastic modulus of the hydrated 3-D matrices ranged from 2 to 15 kPa, similar to the in vivo elasticity of the intima basement membrane and media layer. MSC seeded on rigid matrices (8-15 kPa) showed an increase in cell area compared with those seeded on soft matrices (2-5 kPa). Furthermore, the matrix elasticity guided the cells to express different vascular-specific phenotypes with high differentiation efficiency. Around 95% of MSC seeded on the 3-D matrices with an elasticity of 3 kPa showed Flk-1 endothelial markers within 24 h, while only 20% of MSC seeded on the matrices with elasticity >8 kPa demonstrated Flk-1 marker. In contrast, ~80% of MSC seeded on 3-D matrices with elasticity >8 kPa demonstrated smooth muscle α-actin marker within 24 h, while fewer than 10% of MSC seeded on 3-D matrices with elasticity <5 kPa showed α-actin markers. The ability to control MSC differentiation into either endothelial or smooth muscle-like cells based purely on the local elasticity of the substrate could be a powerful tool for vascular tissue regeneration.
机译:间充质干细胞(MSC)在血管再生中的重要性日益得到认可。但是,几乎没有进行体外研究来确定环境弹性对MSC分化为血管细胞类型的影响。使用静电纺丝和光聚合技术来制造具有可调弹性的三维(3-D)聚乙二醇二甲基丙烯酸酯纳米纤维水凝胶基质,用作细胞基质。压缩测试表明,水合3-D基质的弹性模量范围为2至15 kPa,类似于内膜基底膜和介质层的体内弹性。与接种在软基质(2-5 kPa)上的MSC相比,接种在刚性基质(8-15 kPa)上的MSC显示细胞面积增加。此外,基质弹性引导细胞以高分化效率表达不同的血管特异性表型。在弹性为3 kPa的3-D基质上播种的MSC中约有95%在24 h内显示Flk-1内皮标记,而在弹性大于8 kPa的基质上播种的MSC只有20%表现出Flk-1标记。相反,播种在弹性> 8 kPa的3-D基质上的〜80%的MSC在24 h内表现出平滑肌α-肌动蛋白标记,而播种在弹性<5 kPa的3-D基质上的MSC的不到10%显示α -肌动蛋白标记。仅基于基质的局部弹性来控制MSC分化为内皮细胞或平滑肌样细胞的能力可能是血管组织再生的强大工具。

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