首页> 外文期刊>Journal of Neuroimmunology: Official Bulletin of the Research Committee on Neuroimmunology of the World Federation of Neurology >Muscle regeneration following injury can be modified in vivo by immune neutralization of basic fibroblast growth factor, transforming growth factor beta 1 or insulin-like growth factor I.
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Muscle regeneration following injury can be modified in vivo by immune neutralization of basic fibroblast growth factor, transforming growth factor beta 1 or insulin-like growth factor I.

机译:损伤后的肌肉再生可通过免疫中和碱性成纤维细胞生长因子,转化生长因子β1或胰岛素样生长因子I进行体内修饰。

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摘要

Previous in vitro studies pointed out the role played by several growth factors (basic fibroblast growth factor or bFGF, transforming growth factor beta-1 or TGF beta 1, insulin-like growth factor-I or IGF-I) on the proliferation, the differentiation and the fusion of myogenic precursor cells. We attempted to modify the muscle regeneration which follows the denervation-devascularization of extensor digitorum longus in mice, by acting on the growth factors which are possibly involved in this process. The injection of neutralizing antibodies against either bFGF or IGF-I into the muscle at the time of lesion reduced the number and diameter of regenerating myofibres, suggesting a delay in proliferation and/or fusion of activated satellite cells. The neutralization of TGF beta 1 led to an increased number of small regenerating myofibres, which would be due to the promoting effects of the remaining growth factors (i.e. bFGF and IGF-I) on myoblast proliferation. These contrasted results strongly suggest that the growth factors regulate in vivo muscle regeneration and would be accessible tools for future therapy of muscular disorders.
机译:先前的体外研究指出了几种生长因子(碱性成纤维细胞生长因子或bFGF,转化生长因子β-1或TGFβ1,胰岛素样生长因子-I或IGF-I)在增殖,分化中的作用。和成肌前体细胞的融合。我们试图通过作用于可能参与该过程的生长因子来改变小鼠长指伸肌神经支配-去血管化后的肌肉再生。在病变时向肌肉注射针对bFGF或IGF-1的中和抗体会减少再生的肌纤维的数量和直径,这提示活化的卫星细胞的增殖和/或融合会延迟。 TGFβ1的中和导致小的再生肌纤维的数目增加,这归因于其余生长因子(即bFGF和IGF-1)对成肌细胞增殖的促进作用。这些对比的结果强烈表明,生长因子调节体内肌肉的再生,将成为将来治疗肌肉疾病的工具。

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