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Effect of RGD-functionalization and stiffness modulation of polyelectrolyte multilayer films on muscle cell differentiation

机译:RGD-官能化和刚度调节对肌细胞分化肌细胞的影响

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摘要

Skeletal muscle tissue engineering holds promise for the replacement of muscle due to an injury and for the treatment of muscle diseases. Although RGD substrates have been widely explored in tissue engineering, there is no study aimed at investigating the combined effects of RGD nanoscale presentation and matrix stiffness on myogenesis. In the present work, we use polyelectrolyte multilayer films made of poly(L-lysine) (PLL) and poly(L-glutamic) acid (PGA) as substrates of tunable stiffness that can be functionalized by a RGD adhesive peptide to investigate important events in myogenesis, including adhesion, migration, proliferation and differentiation. C2C12 myoblasts were used as cellular models. RGD presentation on soft films and increased film stiffness could both induce cell adhesion, but integrins involved in adhesion were different in case of soft and stiff films. Moreover, soft films with RGD peptide appeared to be the most appropriate substrate for myogenic differentiation while the stiff PLL/PGA films significantly induced cell migration, proliferation and inhibited myogenic differentiation. The ROCK kinase was found to be involved in myoblast response to the different films. Indeed, its inhibition was sufficient to rescue the differentiation on stiff films, but no significant changes were observed on stiff films with the RGD peptide. These results suggest that different signaling pathways may be activated depending on mechanical and biochemical properties of the multilayer films. This study emphasizes the superior advantage of the soft PLL/PGA films presenting the RGD peptide in terms of myogenic differentiation. This soft RGD-presenting film may be further used as coating of various polymeric scaffolds for muscle tissue engineering.
机译:骨骼肌组织工程有望因损伤而替换肌肉并治疗肌肉疾病。尽管RGD底物已在组织工程学中得到广泛研究,但尚无旨在研究RGD纳米级呈递和基质刚度对肌发生的综合影响的研究。在当前的工作中,我们使用由聚(L-赖氨酸)(PLL)和聚(L-谷氨酸)(PGA)制成的聚电解质多层膜作为可调刚度的底物,可以通过RGD粘合肽对其进行功能化以研究重要事件在肌发生中,包括粘附,迁移,增殖和分化。 C2C12成肌细胞用作细胞模型。 RGD在软膜上的呈现和增加的膜硬度都可以诱导细胞粘附,但是在软膜和硬膜的情况下,参与粘附的整联蛋白是不同的。此外,带有RGD肽的软膜似乎是最适合于成肌分化的底物,而坚硬的PLL / PGA膜则显着诱导细胞迁移,增殖并抑制了成肌分化。发现ROCK激酶参与了对不同膜的成肌细胞反应。实际上,其抑制作用足以挽救硬膜上的分化,但在带有RGD肽的硬膜上未观察到明显变化。这些结果表明,取决于多层膜的机械和生化特性,可以激活不同的信号通路。这项研究强调了呈现RGD肽的PLL / PGA软膜在成肌分化方面的优越性。该RGD呈递软膜可以进一步用作用于肌肉组织工程的各种聚合物支架的涂层。

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