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European Society of Biomechanics S.M. Perren Award 2012: The external mechanical environment can override the influence of local substrate in determining stem cell fate

机译:欧洲生物力学学会2012年佩伦奖(Perren Award 2012):外部机械环境在决定干细胞命运方面可以超越本地基质的影响

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The aim of this study was to explore how cell-matrix interactions and extrinsic mechanical signals interact to determine stem cell fate in response to transforming growth factor-Β3 (TGF-Β3). Bone marrow derived mesenchymal stem cells (MSCs) were seeded in agarose and fibrin hydrogels and subjected to dynamic compression in the presence of different concentrations of TGF-Β3. Markers of chondrogenic, myogenic and endochondral differentiation were assessed. MSCs embedded within agarose hydrogels adopted a spherical cell morphology, while cells directly adhered to the fibrin matrix and took on a spread morphology. Free-swelling agarose constructs stained positively for chondrogenic markers, with MSCs appearing to progress towards terminal differentiation as indicated by mineral staining. MSC seeded fibrin constructs progressed along an alternative myogenic pathway in long-term free-swelling culture. Dynamic compression suppressed differentiation towards any investigated lineage in both fibrin and agarose hydrogels in the short-term. Given that fibrin clots have been shown to support a chondrogenic phenotype in vivo within mechanically loaded joint defect environments, we next explored the influence of long term (42 days) dynamic compression on MSC differentiation. Mechanical signals generated by this extrinsic loading ultimately governed MSC fate, directing MSCs along a chondrogenic pathway as opposed to the default myogenic phenotype supported within unloaded fibrin clots. In conclusion, this study demonstrates that external cues such as the mechanical environment can override the influence specific substrates, scaffolds or hydrogels have on determining mesenchymal stem cell fate. The temporal data presented in this study highlights the importance of considering how MSCs respond to extrinsic mechanical signals in the long term.
机译:这项研究的目的是探讨细胞基质相互作用和外部机械信号如何相互作用,以确定干细胞的命运,以响应转化生长因子-Β3(TGF-Β3)。将骨髓来源的间充质干细胞(MSC)接种在琼脂糖和纤维蛋白水凝胶中,并在不同浓度的TGF-β3存在下进行动态压缩。评估了软骨形成,肌发生和软骨内分化的标记。嵌入琼脂糖水凝胶中的MSC呈球形细胞形态,而细胞直接粘附于血纤蛋白基质并呈扩散形态。自由膨胀的琼脂糖构建体对软骨生成标记物染色呈阳性,如矿物染色所示,MSC似乎朝着终末分化方向发展。 MSC播种的纤维蛋白构建体在长期自由溶胀培养中沿另一条成肌途径发展。动态压缩可在短期内抑制纤维蛋白和琼脂糖水凝胶向任何已研究谱系的分化。鉴于已经证明纤维蛋白凝块在机械负荷的关节缺损环境中可在体内支持软骨形成表型,我们接下来探讨了长期(42天)动态压缩对MSC分化的影响。由这种外在负载产生的机械信号最终决定了MSC的命运,使MSC沿着软骨生成途径而不是在未加载的纤维蛋白凝块中支持默认的肌源性表型。总之,这项研究表明,诸如机械环境之类的外部线索可以超越特定底物,支架或水凝胶对确定间充质干细胞命运的影响。这项研究中提供的时间数据突显了考虑MSC长期如何响应外部机械信号的重要性。

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