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Virus activated artificial ECM induces the osteoblastic differentiation of mesenchymal stem cells without osteogenic supplements

机译:病毒激活的人工ECM诱导间充质干细胞的成骨细胞分化而无需添加成骨剂

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摘要

Biochemical and topographical features of an artificial extracellular matrix (aECM) can direct stem cell fate. However, it is difficult to vary only the biochemical cues without changing nanotopography to study their unique role. We took advantage of two unique features of M13 phage, a non-toxic nanofiber-like virus, to generate a virus-activated aECM with constant ordered ridge/groove nanotopography but displaying different fibronectin-derived peptides (RGD, its synergy site PHSRN, and a combination of RGD and PHSRN). One feature is the self-assembly of phage into a ridge/groove structure, another is the ease of genetically surface-displaying a peptide. We found that the unique ridge/groove nanotopography and the display of RGD and PHSRN could induce the osteoblastic differentiation of mesenchymal stem cells (MSCs) without any osteogenic supplements. The aECM formed through self-assembly and genetic engineering of phage can be used to understand the role of peptide cues in directing stem cell behavior while keeping nanotopography constant.
机译:人工细胞外基质(aECM)的生化和地形特征可以指导干细胞的命运。但是,仅改变生化线索而不改变纳米形貌来研究其独特作用是困难的。我们利用M13噬菌体(一种无毒的纳米纤维样病毒)的两个独特功能来生成具有恒定有序脊/槽纳米形貌但显示不同纤连蛋白衍生肽(RGD,其协同位点PHSRN和RGD和PHSRN的组合)。一个特征是将噬菌体自组装成脊/槽结构,另一个特征是从基因上展示肽的容易性。我们发现独特的脊/槽纳米形貌和RGD和PHSRN的显示可以诱导间充质干细胞(MSCs)的成骨细胞分化,而无需任何成骨补充剂。通过噬菌体的自组装和基因工程形成的aECM可用于了解肽提示在指导干细胞行为的同时保持纳米形貌不变。

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