Neural transcription factors bias cleavage stage blastomeres to give rise to neural ectoderm

Shailly Gaur, Max Mandelbaum, Mona Herold, Himani Datta Majumdar, Karen M. Neilson, Thomas M. Maynard, Kathy Mood, Ira O. Daar, Sally A. Moody

Research output: Contribution to journalArticlepeer-review

18 Scopus citations

Abstract

The decision by embryonic ectoderm to give rise to epidermal versus neural derivatives is the result of signaling events during blastula and gastrula stages. However, there also is evidence in Xenopus that cleavage stage blastomeres contain maternally derived molecules that bias them toward a neural fate. We used a blastomere explant culture assay to test whether maternally deposited transcription factors bias 16-cell blastomere precursors of epidermal or neural ectoderm to express early zygotic neural genes in the absence of gastrulation interactions or exogenously supplied signaling factors. We found that Foxd4l1, Zic2, Gmnn, and Sox11 each induced explants made from ventral, epidermis-producing blastomeres to express early neural genes, and that at least some of the Foxd4l1 and Zic2 activities are required at cleavage stages. Similarly, providing extra Foxd4l1 or Zic2 to explants made from dorsal, neural plate-producing blastomeres significantly increased the expression of early neural genes, whereas knocking down either significantly reduced them. These results show that maternally delivered transcription factors bias cleavage stage blastomeres to a neural fate. We demonstrate that mouse and human homologs of Foxd4l1 have similar functional domains compared to the frog protein, as well as conserved transcriptional activities when expressed in Xenopus embryos and blastomere explants. genesis 54:334–349, 2016.

Original languageEnglish
Pages (from-to)334-349
Number of pages16
JournalGenesis
Volume54
Issue number6
DOIs
StatePublished - 1 Jun 2016
Externally publishedYes

Keywords

  • Foxd4
  • Foxd4l1
  • Foxd4l1.1
  • Foxd5
  • Sox11
  • Sox2
  • Zic1
  • Zic2
  • geminin
  • neural induction

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