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The alchemy of tendon repair: a primer for the (S)mad scientist

机译:肌腱修复的炼金术:(S)疯科学家的入门书

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摘要

During vertebrate development, mesenchymal progenitors capable of forming bone, cartilage, muscle, fat, or tendon arise from either neural crest or somitic mesoderm. Transcriptional programs that specify mesenchymal cell fates are initiated and modified by paracrine cues provided by TGF-β superfamily members and mediated in part via the regulated assembly of Smad-containing multiprotein transcription factor complexes. In this issue of the JCI, Hoffmann and colleagues have identified that Smad8 activation drives tendon formation from C3H10T1/2 cells, a murine cell line that recapitulates many features of normal multipotent mesenchymal cells (see the related article beginning on page 940). Cells programmed to the tenocyte cell fate in vitro formed tenogenic grafts in vivo. These results add to the accumulating evidence that proliferating, multipotent mesenchymal progenitor cells can be programmed to yield multiple cell types — e.g., osteoblasts, myocytes, chondrocytes, and tenocytes — that may be useful in cell-based therapeutic approaches to musculoskeletal diseases.
机译:在脊椎动物发育过程中,能够形成骨骼,软骨,肌肉,脂肪或肌腱的间充质祖细胞来自神经or或体细胞性中胚层。指定间充质细胞命运的转录程序是由TGF-β超家族成员提供的旁分泌线索启动和修饰的,并部分通过含Smad的多蛋白转录因子复合物的调控组装介导。在JCI的本期中,霍夫曼及其同事发现Smad8激活驱动了C3H10T1 / 2细胞的肌腱形成,C3H10T1 / 2细胞是一种鼠细胞系,可概括正常多能间充质细胞的许多功能(请参阅从第940页开始的相关文章)。体外编程为肌腱细胞命运的细胞在体内形成了肌腱移植物。这些结果增加了越来越多的证据,即可以对增殖的多能间充质祖细胞进行编程,以产生多种细胞类型,例如成骨细胞,肌细胞,软骨细胞和肌腱细胞,这可能在基于细胞的肌肉骨骼疾病的治疗方法中有用。

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