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Osteogenic differentiation of human amniotic fluid-derived stem cells induced by bone morphogenetic protein-7 and enhanced by nanofibrous scaffolds.

机译:骨形态发生蛋白7诱导并由纳米纤维支架增强的人羊水衍生干细胞的成骨分化。

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Amniotic fluid-derived stem cells (AFSCs) are becoming an important source of cells for regenerative medicine given their apparent advantages of accessibility, renewal capacity and multipotentiality. In the intermediate stage between the embryonic stem cells (ESCs) and adult stem cells, AFSCs may have a distinct mechanism to choose their fate. Unfortunately, until now, little is known about how bone morphogenetic proteins (BMPs) control the osteoblastic differentiation of AFSCs, especially on 3D scaffolds. Our research shows that human AFSCs (hAFSCs) can be induced for osteoblastic differentiation by rhBMP-7, and hAFSCs respond to rhBMP-7 more strongly than human mesenchymal stem cells (hMSCs). As synthetic ECM, scaffolds play a central role in tissue engineering. The hAFSCs, on the nanofibrous scaffolds (NF scaffolds) with morphology similar to that of natural collagen fibers, showed significantly enhanced alkaline phosphatase (ALP) activity, calcium content, von Kossa staining and the expression of osteogenic genes than those on the traditional scaffolds, i.e. solid walled scaffolds. The data on the bone formation in vivo presented further evidence that biomimetic NF scaffolds provided hAFSCs a more favorable synthetic ECM, and thus, facilitated the osteogenic differentiation of hAFSCs. The relative strong responsiveness to rhBMP-7 makes hAFSCs promising in bone regeneration. The synthetic NF scaffolds, which mimic the morphology of natural collagen fibers, enhanced the osteoblastic differentiation of hAFSCs in vitro and bone formation in vivo.
机译:羊水来源的干细胞(AFSCs)凭借其可及性,更新能力和多潜能的明显优势,正成为再生医学细胞的重要来源。在胚胎干细胞(ESC)和成年干细胞之间的中间阶段,AFSC可能具有选择其命运的独特机制。不幸的是,到目前为止,关于骨形态发生蛋白(BMP)如何控制AFSC的成骨细胞分化的了解甚少,尤其是在3D支架上。我们的研究表明,rhBMP-7可以诱导人AFSCs(hAFSCs)成骨细胞分化,并且hAFSCs对rhBMP-7的反应比人间充质干细胞(hMSCs)更强。作为合成的ECM,支架在组织工程中起着核心作用。形态类似于天然胶原纤维的纳米纤维支架(NF支架)上的hAFSCs与传统支架相比,其碱性磷酸酶(ALP)活性,钙含量,von Kossa染色和成骨基因表达明显增强,即坚固的壁式支架。关于体内骨形成的数据提供了进一步的证据,仿生NF支架为hAFSC提供了更有利的合成ECM,因此促进了hAFSC的成骨分化。对rhBMP-7的相对强响应性使hAFSC在骨再生中很有前景。合成的NF支架模仿天然胶原纤维的形态,在体外增强了hAFSC的成骨细胞分化能力,并在体内增强了骨形成。

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