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Nanotopographical cues of electrospun PLLA efficiently modulate non-coding RNA network to osteogenic differentiation of mesenchymal stem cells during BMP signaling pathway

机译:ElectromeCul PLLA的纳米音响线索有效地调节非编码RNA网络在BMP信号通路期间间充质干细胞的骨质发生分化

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Application of stem cells in combination with nanoflbrous substrates is an interesting biomimetic approach for enhanced regeneration of damaged tissues such as bone and cartilage. The investigation of the complex interplay between nanotopographical cues of niche and noncoding RNAs in stem cells fate is an effective tool to find a new strategy for enhancing the induction of osteogenesis. In this study, we investigated the effects of aligned and random orientations of nanofibers as a natural ECM-mimicking environment on the network of noncoding RNA in mesenchymal stem cells. Aligned and randomly oriented Ploy (L-lactide) PLLA scaffolds were fabricated via electrospinning. Human Adipose Tissue-Derived Mesenchymal Stem Cells (hASCs) were isolated from adipose tissue and were cultured on surfaces of these scaffolds. Their capacity to support hMSCs proliferation was also investigated by MTT assay and the expression of c-Myc gene. Then, after 7, 14 and 21 days, the osteogenic commitment of hMSCs and the miRNA regulatory network in BMP signaling pathway were evaluated by measuring alkaline phosphatase (ALP) activity, extracellular calcium deposition, and bone-related gene activation by Real-Time PCR. Furthermore, osteogenic differentiation was evaluated with regard to their noncoding RNA network. Our results for the first time showed an interaction between nanotopographical cues and miRNA activity in hMSCs. We found that the nanotopographical cues could be used to influence the osteogenic differentiation process of hMSCs through the modulation of lncRNAs and miR-125b as negative regulators of osteogenesis as well as the H19 modulator BMP signaling pathway that acts as a miRNA sponge. Moreover, we also demonstrated for the first time that MEG3 as a long noncoding RNA is controlled by miR-125b and microRNA-triggered lncRNA decay mechanism. This strategy seems to be an important tool for controlling stem cell fate in engineered tissues and provide new insights into most biocom
机译:干细胞与纳米粘性底物组合的应用是一种有趣的仿生方法,用于增强受损组织如骨和软骨的再生。在干细胞命运中纳米内和非编码RNA的纳米检测性提示复杂相互作用是一种有效的工具,用于寻找增强骨肉诱导的新策略。在这项研究中,我们研究了纳米纤维的对齐和随机取向作为间充质干细胞非编码RNA网络的天然ECM模拟环境的影响。通过电刺刀制造对准和随机取向的犁(L-丙交酯)PLLA支架。人脂肪组织衍生的间充质干细胞(HASC)与脂肪组织分离,并在这些支架的表面上培养。通过MTT测定和C-MYC基因的表达,还研究了它们支持HMSCs增殖的能力。然后,在7,14和21天后,通过使用实时PCR测量碱性磷酸酶(ALP)活性,细胞外钙沉积和骨相关基因激活来评估HMSCs和MiRNA调节网络的骨质发生承诺。通过实时PCR来评价BMP信号通路中的BMP信号传导途径。此外,关于其非编码RNA网络评估了骨质发生分化。我们第一次首次出现了纳米检测性提示与HMSCs中的miRNA活性之间的相互作用。我们发现纳米检测性提示可用于通过调节LNCRNA和miR-125b作为成骨的负调节剂以及用作miRNA海绵的H19调节剂BMP信号通路来影响HMSCs的成骨分化过程。此外,我们还在MIR-125B和MicroRNA-触发的LNCRNA衰减机制中首次证明了MEG3作为长的非编码RNA。该策略似乎是控制工程组织中的干细胞命运的重要工具,并为大多数生物传染提供新的见解

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