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Fibroblasts influence muscle progenitor differentiation and alignment in contact independent and dependent manners in organized co-culture devices

机译:成纤维细胞影响有组织的共培养装置的独立和依赖举止的肌肉祖细胞分化和对准

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摘要

Myoblasts are precursor muscle cells that lie nascent to mature skeletal muscle. Once muscle is damaged, these cells migrate, fuse, and regenerate the muscle tissue. It is known that skeletal muscle can partially regenerate in vivo after muscle tissue damage. However, this regeneration does not always occur, especially in more severe injuries. Cellular therapy using tissue-engineering approaches has been shown to improve organ repair and function. To exploit potential benefits of using cell therapy as an avenue for skeletal muscle repair, it is important to understand the cellular dynamics underlying skeletal myocyte formation and growth. Cardiac fibroblasts have been shown to have a major influence on cardiomyocyte function, repair, and overall spatial distribution. However, little is known regarding fibroblasts’ role on skeletal myocyte function. In this study, we utilized a reconfigurable co-culture device to understand the contact and paracrine effects of fibroblasts on skeletal myocyte alignment and differentiation using murine myoblast and fibroblast cell lines. We demonstrate that myotube alignment is increased by direct contact with fibroblasts, while myotube differentiation is reduced both in the gap and contact configurations with fibroblasts after 6 days of co-culture. Furthermore, neutralizing antibodies to FGF-2 can block these effects of fibroblasts on myotube differentiation and alignment. Finally, bi-directional signaling is critical to the observed myoblast-fibroblast interactions, since conditioned media could not reproduce the same effects observed in the gap configuration. These findings could have direct implications on cell therapies for repairing skeletal muscle, which have only utilized skeletal myoblasts or stem cell populations alone.
机译:成肌细胞是位于成熟骨骼肌新生的前体肌肉细胞。一旦肌肉受损,这些细胞就会迁移,融合并再生肌肉组织。已知骨骼肌在肌肉组织损伤后可以在体内部分再生。但是,这种再生并不总是发生,特别是在更严重的伤害中。使用组织工程方法的细胞疗法已显示可改善器官修复和功能。为了利用使用细胞疗法作为骨骼肌修复途径的潜在好处,了解骨骼肌细胞形成和生长的细胞动力学很重要。心脏成纤维细胞已显示出对心肌细胞功能,修复和整体空间分布有重大影响。然而,关于成纤维细胞对骨骼肌细胞功能的作用知之甚少。在这项研究中,我们利用可重构的共培养设备来了解成纤维细胞对骨骼肌细胞排列和分化的接触和旁分泌作用,并利用鼠成肌细胞和成纤维细胞系进行分化。我们证明,通过与成纤维细胞直接接触,肌管排列增加,而共培养6天后,与成纤维细胞的间隙和接触构型,肌管分化均减少。此外,针对FGF-2的中和抗体可以阻断成纤维细胞对肌管分化和排列的这些影响。最后,双向信号对于观察到的成肌细胞-成纤维细胞相互作用至关重要,因为条件培养基不能再现在间隙结构中观察到的相同作用。这些发现可能直接影响修复骨骼肌的细胞疗法,而骨骼肌仅利用骨骼肌成肌细胞或干细胞群体。

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