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Myostatin imposes reversible quiescence on embryonic muscle precursors.

机译:肌生长抑制素使胚胎肌肉前体具有可逆的静止性。

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We have previously shown that Myostatin, a member of the transforming growth factor beta (TFG-beta) family of signalling molecules, is expressed in developing muscle, and that treatment with recombinant Myostatin inhibited the expression of key myogenic transcription factors during chick embryogenesis. In this study, we followed the fate of muscle precursors after exposure to Myostatin. We report that in contrast to the down-regulation in expression of Pax-3, Myf-5, MyoD, and Myogenin, expression of Pax-7 was maintained. However, Myostatin completely inhibited cell division in the Pax-7-expressing cells. The inhibitory effect of Myostatin was reversible, as upon withdrawal myogenic cells re-initiated cell proliferation as well as expression of Pax-3 and MyoD. These results led us to investigate the temporal and spatial distribution of quiescent muscle precursors during development. To this end, we analysed distribution and mitotic behaviour of Pax-7-expressing cells during muscle development. Our studies revealed two populations of Pax-7-expressing cells, one that proliferated and incorporated BrdU, whilst the other did not. At early developmental stages, a high proportion of Pax-7-expressing cells proliferated, but there was a significant number of non-dividing Pax-7-expressing cells intermingled with differentiated muscle. Proliferating precursors became less frequent as development proceeded and at late fetal stages all Pax-7-expressing cells were mitotically quiescent. We suggest that Myostatin is an important signalling molecule responsible for imposing quiescence upon myogenic precursors during embryonic and foetal development.
机译:我们以前已经表明,肌生长抑制素是信号转导分子的转化生长因子β(TFG-beta)家族的成员,在发育中的肌肉中表达,而重组肌生长抑制素的处理抑制了鸡胚发生过程中关键肌发生转录因子的表达。在这项研究中,我们跟踪了肌生长抑制素后肌肉前体的命运。我们报告,与下调Pax-3,Myf-5,MyoD和Myogenin的表达相反,维持了Pax-7的表达。但是,Myostatin完全抑制了Pax-7表达细胞的细胞分裂。 Myostatin的抑制作用是可逆的,因为停药后成肌细胞会重新启动细胞增殖以及Pax-3和MyoD的表达。这些结果使我们研究了发育过程中静态肌肉前体的时间和空间分布。为此,我们分析了Pax-7表达细胞在肌肉发育过程中的分布和有丝分裂行为。我们的研究显示了两个Pax-7表达细胞群,一个增殖并掺入BrdU,而另一个则不。在发育的早期阶段,高比例的Pax-7表达细胞增殖,但是有大量未分裂的Pax-7表达细胞与分化的肌肉混合在一起。随着发育的进行,增殖前体的频率降低,并且在胎儿晚期,所有表达Pax-7的细胞都处于有丝分裂静止状态。我们建议肌生长抑制素是重要的信号分子,负责在胚胎和胎儿发育过程中对肌原性前体施加静止。

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