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Electrospun biomimetic scaffold of hydroxyapatite/chitosan supports enhanced osteogenic differentiation of mMSCs

机译:羟基磷灰石/壳聚糖的静电纺丝仿生支架支持mMSCs的成骨分化

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Engaging functional biomaterial scaffolds to regulate stem cell differentiation has drawn a great deal of attention in the tissue engineering and regenerative medicine community. In this study, biomimetic composite nanofibrous scaffolds of hydroxyapatite/chitosan (HAp/CTS) were prepared to investigate their capacity for inducing murine mesenchymal stem cells (mMSCs) to differentiate into the osteogenic lineage, in the absence and presence of an osteogenic supplementation (i.e., ascorbic acid, β-glycerol phosphate, and dexamethasone), respectively. Using electrospun chitosan (CTS) nanofibrous scaffolds as the control, cell morphology, growth, specific osteogenic genes expression, and quantified proteins secretion on the HAp/CTS scaffolds were sequentially examined and assessed. It appeared that the HAp/CTS scaffolds supported better attachment and proliferation of the mMSCs. Most noteworthy was that in the absence of the osteogenic supplementation, expression of osteogenic genes including collagen I (Col I), runt-related transcription factor 2 (Runx2), alkaline phosphatase (ALP), and osteocalcin (OCN) were significantly upregulated in mMSCs cultured on the HAp/CTS nanofibrous scaffolds. Also increased secretion of the osteogenesis protein markers of alkaline phosphatase and collagen confirmed that the HAp/CTS nanofibrous scaffold markedly promoted the osteogenic commitment in the mMSCs. Moreover, the presence of osteogenic supplementation proved an enhanced efficacy of mMSC osteogenesis on the HAp/CTS nanofibrous scaffolds. Collectively, this study demonstrated that the biomimetic nanofibrous HAp/CTS scaffolds could support and enhance the adhesion, proliferation, and particularly osteogenic differentiation of the mMSCs. It also substantiated the potential of using biomimetic nanofibrous scaffolds of HAp/CTS for functional bone repair and regeneration applications.
机译:参与功能性生物材料支架来调节干细胞分化已引起组织工程和再生医学界的极大关注。在这项研究中,制备了羟基磷灰石/壳聚糖的仿生复合纳米纤维支架(HAp / CTS),以研究它们在不存在和存在成骨作用的情况下诱导鼠间充质干细胞(mMSCs)分化为成骨细胞的能力。 ,抗坏血酸,β-甘油磷酸酯和地塞米松)。使用静电纺丝壳聚糖(CTS)纳米纤维支架作为对照,依次检查和评估细胞形态,生长,特定成骨基因表达以及HAp / CTS支架上定量的蛋白质分泌。似乎HAp / CTS支架支持mMSC更好的附着和增殖。最值得注意的是,在不进行成骨性补充的情况下,mMSCs中包括胶原蛋白I(Col I),矮子相关转录因子2(Runx2),碱性磷酸酶(ALP)和骨钙素(OCN)的成骨基因的表达明显上调。在HAp / CTS纳米纤维支架上培养。碱性磷酸酶和胶原的成骨蛋白标记物的分泌也增加,证实了HAp / CTS纳米纤维支架显着促进了mMSC中的成骨作用。此外,成骨补充剂的存在证明了mMSC对HAp / CTS纳米纤维支架的成骨作用增强。总体而言,这项研究表明,仿生纳米纤维HAp / CTS支架可以支持和增强mMSC的粘附,增殖,尤其是成骨分化。它还证实了将仿生纳米纤维HAp / CTS支架用于功能性骨修复和再生应用的潜力。

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