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Ripply suppresses Tbx6 to induce dynamic-to-static conversion in somite segmentation.

Taijiro YabeKoichiro UriuShinji Takada
Published in: Nature communications (2023)
The metameric pattern of somites is created based on oscillatory expression of clock genes in presomitic mesoderm. However, the mechanism for converting the dynamic oscillation to a static pattern of somites is still unclear. Here, we provide evidence that Ripply/Tbx6 machinery is a key regulator of this conversion. Ripply1/Ripply2-mediated removal of Tbx6 protein defines somite boundary and also leads to cessation of clock gene expression in zebrafish embryos. On the other hand, activation of ripply1/ripply2 mRNA and protein expression is periodically regulated by clock oscillation in conjunction with an Erk signaling gradient. Whereas Ripply protein decreases rapidly in embryos, Ripply-triggered Tbx6 suppression persists long enough to complete somite boundary formation. Mathematical modeling shows that a molecular network based on results of this study can reproduce dynamic-to-static conversion in somitogenesis. Furthermore, simulations with this model suggest that sustained suppression of Tbx6 caused by Ripply is crucial in this conversion.
Keyphrases
  • gene expression
  • high frequency
  • binding protein
  • signaling pathway
  • poor prognosis
  • protein protein
  • transcription factor
  • deep learning
  • molecular dynamics
  • machine learning
  • single molecule