Dev125740 1..14

نویسندگان

  • Berta Vidal
  • Anthony Santella
  • Esther Serrano-Saiz
  • Zhirong Bao
  • Chiou-Fen Chuang
چکیده

Neurogenesis involves deeply conserved patterning molecules, such as the proneural basic helix-loop-helix transcription factors. Sox proteins and specifically members of the SoxB and SoxC groups are anotherclassof conserved transcription factorswithan important role in neuronal fate commitment and differentiation in various species. In this study,we examine the expressionof all fiveSox genes of the nematode C. elegans and analyze the effect of null mutant alleles of all members of the SoxB and SoxC groups on nervous system development. Surprisingly, we find that, unlike in other systems, neither of the two C. elegans SoxB genes sox-2 (SoxB1) and sox-3 (SoxB2), nor the sole C. elegans SoxC gene sem-2, is broadly expressed throughout the embryonic or adult nervous system and that all three genes are mostly dispensable for embryonic neurogenesis. Instead, sox-2 is required to maintain the developmental potential of blast cells that are generated in the embryo but divide only postembryonically to give rise to differentiated neuronal cell types. Moreover, sox-2 and sox-3 have selective roles in the terminal differentiation of specific neuronal cell types. Our findings suggest that the common themes of SoxB gene function across phylogeny lie in specifying developmental potential and, later on, in selectively controlling terminal differentiation programs of specific neuron types, but not in broadly controlling neurogenesis.

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Dev125740 2464..2477

Neurogenesis involves deeply conserved patterning molecules, such as the proneural basic helix-loop-helix transcription factors. Sox proteins and specifically members of the SoxB and SoxC groups are anotherclassof conserved transcription factorswithan important role in neuronal fate commitment and differentiation in various species. In this study,we examine the expressionof all fiveSox genes of...

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تاریخ انتشار 2015