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The myofibroblast multiple origins for major roles in normal and pathological tissue repair

机译:肌成纤维细胞在正常和病理组织修复中起主要作用的多种起源

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摘要

Myofibroblasts differentiate, invade and repair injured tissues by secreting and organizing the extracellular matrix and by developing contractile forces. When tissues are damaged, tissue homeostasis must be re-established, and repair mechanisms have to rapidly provide harmonious mechanical tissue organization, a process essentially supported by (myo)fibroblasts. Under physiological conditions, the secretory and contractile activities of myofibroblasts are terminated when the repair is complete (scar formation) but the functionality of the tissue is only rarely perfectly restored. At the end of the normal repair process, myofibroblasts disappear by apoptosis but in pathological situations, myofibroblasts likely remain leading to excessive scarring. Myofibroblasts originate from different precursor cells, the major contribution being from local recruitment of connective tissue fibroblasts. However, local mesenchymal stem cells, bone marrow-derived mesenchymal stem cells and cells derived from an epithelial-mesenchymal transition process, may represent alternative sources of myofibroblasts when local fibroblasts are not able to satisfy the requirement for these cells during repair. These diverse cell types probably contribute to the appearance of myofibroblast subpopulations which show specific biological properties and which are important to understand in order to develop new therapeutic strategies for treatment of fibrotic and scarring diseases.
机译:肌成纤维细胞通过分泌和组织细胞外基质并发展收缩力来分化,侵袭和修复受损组织。当组织受损时,必须重新建立组织稳态,修复机制必须快速提供和谐的机械组织组织,这一过程主要由(肌)成纤维细胞支持。在生理条件下,修复完成(瘢痕形成)后,成纤维细胞的分泌和收缩活动就终止了,但组织的功能很少被完全恢复。在正常修复过程结束时,成纤维细胞会通过凋亡消失,但在病理情况下,成纤维细胞可能仍会导致过度瘢痕形成。肌成纤维细胞起源于不同的前体细胞,主要贡献来自结缔组织成纤维细胞的局部募集。但是,当局部成纤维细胞不能满足修复过程中对这些细胞的需求时,局部间充质干细胞,骨髓来源的间充质干细胞和衍生自上皮-间质转化过程的细胞可能代表了成纤维细胞的替代来源。这些不同的细胞类型可能有助于肌成纤维细胞亚群的出现,这些亚成纤维细胞亚群显示出特定的生物学特性,对于开发新的治疗纤维化和瘢痕性疾病的治疗策略而言,理解这些重要。

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