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Notch Is a Critical Component of the Mouse Somitogenesis Oscillator and Is Essential for the Formation of the Somites

机译:缺刻是鼠标体发生振荡器的重要组成部分是形成体节必不可少的

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摘要

Segmentation of the vertebrate body axis is initiated through somitogenesis, whereby epithelial somites bud off in pairs periodically from the rostral end of the unsegmented presomitic mesoderm (PSM). The periodicity of somitogenesis is governed by a molecular oscillator that drives periodic waves of clock gene expression caudo-rostrally through the PSM with a periodicity that matches somite formation. To date the clock genes comprise components of the Notch, Wnt, and FGF pathways. The literature contains controversial reports as to the absolute role(s) of Notch signalling during the process of somite formation. Recent data in the zebrafish have suggested that the only role of Notch signalling is to synchronise clock gene oscillations across the PSM and that somite formation can continue in the absence of Notch activity. However, it is not clear in the mouse if an FGF/Wnt-based oscillator is sufficient to generate segmented structures, such as the somites, in the absence of all Notch activity. We have investigated the requirement for Notch signalling in the mouse somitogenesis clock by analysing embryos carrying a mutation in different components of the Notch pathway, such as Lunatic fringe (Lfng), Hes7, Rbpj, and presenilin1/presenilin2 (Psen1/Psen2), and by pharmacological blocking of the Notch pathway. In contrast to the fish studies, we show that mouse embryos lacking all Notch activity do not show oscillatory activity, as evidenced by the absence of waves of clock gene expression across the PSM, and they do not develop somites. We propose that, at least in the mouse embryo, Notch activity is absolutely essential for the formation of a segmented body axis.
机译:脊椎动物体轴的分段是通过体细胞发生而开始的,由此上皮体周期性地从未分段的早熟中胚层(PSM)的鼻端成对发芽。体发生的周期性由分子振荡器控制,该分子振荡器通过PSM周期性地驱动时钟基因表达的周期性波,其周期与体节形成匹配。迄今为止,时钟基因包含Notch,Wnt和FGF途径的组成部分。文献中有关于Notch信号在体节形成过程中的绝对作用的争议性报道。斑马鱼中的最新数据表明,Notch信号的唯一作用是使PSM上的时钟基因振荡同步,并且在没有Notch活性的情况下,so突的形成可以继续进行。但是,尚不清楚在没有所有Notch活性的情况下,基于FGF / Wnt的振荡器是否足以产生分段结构(如体节),在小鼠中尚不清楚。我们已经通过分析在Notch通路的不同组成部分(例如Lunatic条纹(Lfng),Hes7,Rbpj和presenilin1 / presenilin2(Psen1 / Psen2))中携带突变的胚胎,研究了小鼠体发生时钟中Notch信号的需求。通过Notch途径的药理学阻断。与鱼类研究相反,我们显示缺乏所有Notch活性的小鼠胚胎没有显示出振荡活性,这在整个PSM中都没有时钟基因表达的浪潮中得到了证明,并且它们不会发育出卵节。我们建议,至少在小鼠胚胎中,Notch活性对于分段的体轴形成绝对必要。

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