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Degradation-mediated cellular traction directs stem cell fate in covalently crosslinked three-dimensional hydrogels

机译:降解介导的细胞牵引作用指导干细胞在共价交联的三维水凝胶中的命运

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摘要

Although cell-matrix adhesive interactions are known to regulate stem cell differentiation, the underlying mechanisms, in particular for direct three-dimensional (3D) encapsulation within hydrogels, are poorly understood. Here, we demonstrate that in covalently crosslinked hyaluronic acid (HA) hydrogels, the differentiation of human mesenchymal stem cells (hMSCs) is directed by the generation of degradation-mediated cellular-traction, independent of cell morphology or matrix mechanics. hMSCs within HA hydrogels of equivalent elastic moduli that either permit (restrict) cell-mediated degradation exhibited high (low) degrees of cell spreading and high (low) tractions, and favoured osteogenesis (adipogenesis). In addition, switching the permissive hydrogel to a restrictive state via delayed secondary crosslinking reduced further hydrogel degradation, suppressed traction, and caused a switch from osteogenesis to adipogenesis in the absence of changes to the extended cellular morphology. Also, inhibiting tension-mediated signalling in the permissive environment mirrored the effects of delayed secondary crosslinking, whereas upregulating tension induced osteogenesis even in the restrictive environment.
机译:尽管已知细胞-基质粘附相互作用调节干细胞的分化,但对潜在的机制,尤其是对水凝胶内直接三维(3D)封装的机制知之甚少。在这里,我们证明了在共价交联的透明质酸(HA)水凝胶中,人间充质干细胞(hMSCs)的分化是由降解介导的细胞牵引作用的产生,而与细胞形态或基质力学无关。具有相同弹性模量的HA水凝胶中的hMSC允许(限制)细胞介导的降解,表现出高(低)度的细胞扩散和高(低)牵引力,并有利于成骨(成脂)。此外,通过延迟的二次交联将允许的水凝胶转换为限制性状态可减少进一步的水凝胶降解,抑制牵引力,并在不改变扩展的细胞形态的情况下从成骨转变为成脂。同样,在允许的环境中抑制张力介导的信号转导反映了延迟的二次交联的效果,而即使在限制性环境中,上调张力也会诱导成骨作用。

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