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首页> 外文期刊>Biomaterials Science >Spontaneous cardiomyocyte differentiation of mouse embryoid bodies regulated by hydrogel crosslink density
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Spontaneous cardiomyocyte differentiation of mouse embryoid bodies regulated by hydrogel crosslink density

机译:水凝胶交联密度调节小鼠胚状体的自发性心肌细胞分化

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摘要

Cellular therapies have great potential to provide alternative treatment options for those suffering from heart disease. In order to optimize cell delivery for therapeutic efficacy, a greater understanding of parameters that impact stem cell differentiation, survival, growth, and development are needed. In this study, we examine the role of hydrogel crosslink density on spontaneous cardiomyocyte (CM) differentiation of murine embryoid bodies (EBs). CM differentiation was accelerated in hydrogels of low crosslink density, where 100% of the hydrogels were positive for CM differentiation compared to only 53% in the high crosslink density group after 8 days of culture. DNA microarray data suggests that enhanced CM differentiation in the low crosslink density hydrogels was not tissue specific but rather a result of favoured EB development and cell proliferation. Additionally, enhanced EB growth and differentiation in low crosslink density hydrogels was independent of RGD ligand density and not a consequence of enhanced diffusion. We also demonstrate that matrix metalloproteinase activity is required for spontaneous CM differentiation in 3D hydrogels. Low hydrogel crosslink density regulates spontaneous EB differentiation by promoting EB growth and development. Elucidating the effects of microenvironmental cues on cell differentiation can aid in the optimization of stem cell-based therapies for tissue regeneration.
机译:细胞疗法具有巨大的潜力,可以为心脏病患者提供替代治疗选择。为了优化细胞递送以达到治疗功效,需要对影响干细胞分化,存活,生长和发育的参数有更深入的了解。在这项研究中,我们检查了水凝胶交联密度对鼠类胚体(EB)自发性心肌细胞(CM)分化的作用。低交联密度的水凝胶可促进CM分化,其中培养8天后100%的水凝胶对CM分化呈阳性,而高交联密度的水凝胶仅为53%。 DNA微阵列数据表明,低交联密度水凝胶中增强的CM分化不是组织特异性的,而是EB发育和细胞增殖受到促进的结果。另外,低交联密度水凝胶中增强的EB生长和分化与RGD配体密度无关,而不是扩散增强的结果。我们还证明3D水凝胶中自发CM分化需要基质金属蛋白酶活性。低水凝胶交联密度通过促进EB生长发育来调节自发EB分化。阐明微环境提示对细胞分化的影响可以帮助优化基于干细胞的组织再生疗法。

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