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Satellite cells, connective tissue fibroblasts and their interactions are crucial for muscle regeneration.

机译:卫星细胞,结缔组织成纤维细胞及其相互作用对肌肉再生至关重要。

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Muscle regeneration requires the coordinated interaction of multiple cell types. Satellite cells have been implicated as the primary stem cell responsible for regenerating muscle, yet the necessity of these cells for regeneration has not been tested. Connective tissue fibroblasts also are likely to play a role in regeneration, as connective tissue fibrosis is a hallmark of regenerating muscle. However, the lack of molecular markers for these fibroblasts has precluded an investigation of their role. Using Tcf4, a newly identified fibroblast marker, and Pax7, a satellite cell marker, we found that after injury satellite cells and fibroblasts rapidly proliferate in close proximity to one another. To test the role of satellite cells and fibroblasts in muscle regeneration in vivo, we created Pax7(CreERT2) and Tcf4(CreERT2) mice and crossed these to R26R(DTA) mice to genetically ablate satellite cells and fibroblasts. Ablation of satellite cells resulted in a complete loss of regenerated muscle, as well as misregulation of fibroblasts and a dramatic increase in connective tissue. Ablation of fibroblasts altered the dynamics of satellite cells, leading to premature satellite cell differentiation, depletion of the early pool of satellite cells, and smaller regenerated myofibers. Thus, we provide direct, genetic evidence that satellite cells are required for muscle regeneration and also identify resident fibroblasts as a novel and vital component of the niche regulating satellite cell expansion during regeneration. Furthermore, we demonstrate that reciprocal interactions between fibroblasts and satellite cells contribute significantly to efficient, effective muscle regeneration.
机译:肌肉再生需要多种细胞类型的协调相互作用。卫星细胞被认为是负责肌肉再生的主要干细胞,但尚未测试这些细胞再生的必要性。结缔组织成纤维细胞也可能在再生中发挥作用,因为结缔组织纤维化是肌肉再生的标志。但是,由于缺乏针对这些成纤维细胞的分子标记,因此无法对其作用进行研究。使用新鉴定的成纤维细胞标记物Tcf4和卫星细胞标记物Pax7,我们发现受伤后卫星细胞和成纤维细胞彼此之间迅速增殖。为了测试卫星细胞和成纤维细胞在体内肌肉再生中的作用,我们创建了Pax7(CreERT2)和Tcf4(CreERT2)小鼠,并将它们与R26R(DTA)小鼠杂交,以遗传方式消融卫星细胞和成纤维细胞。卫星细胞的消融导致再生肌肉完全丧失,成纤维细胞调节异常,结缔组织急剧增加。成纤维细胞的消融改变了卫星细胞的动力学,导致卫星细胞过早分化,卫星细胞早期池耗竭以及再生的肌纤维较小。因此,我们提供了直接的遗传证据,证明卫星细胞是肌肉再生所必需的,并且还将驻留的成纤维细胞确定为在再生过程中调节卫星细胞扩增的利基的新的重要组成部分。此外,我们证明,成纤维细胞和卫星细胞之间的相互影响显着促进了有效,有效的肌肉再生。

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