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Published March 15, 2005 | Published
Journal Article Open

To proliferate or to die: role of Id3 in cell cycle progression and survival of neural crest progenitors

Abstract

The neural crest is a unique population of mitotically active, multipotent progenitors that arise at the vertebrate neural plate border. Here, we show that the helix-loop-helix transcriptional regulator Id3 has a novel role in cell cycle progression and survival of neural crest progenitors in Xenopus. Id3 is localized at the neural plate border during gastrulation and neurulation, overlapping the domain of neural crest induction. Morpholino oligonucleotide-mediated depletion of Id3 results in the absence of neural crest precursors and a resultant loss of neural crest derivatives. This appears to be mediated by cell cycle inhibition followed by cell death of the neural crest progenitor pool, rather than a cell fate switch. Conversely, overexpression of Id3 increases cell proliferation and results in expansion of the neural crest domain. Our data suggest that Id3 functions by a novel mechanism, independent of cell fate determination, to mediate the decision of neural crest precursors to proliferate or die.

Additional Information

© 2005 Cold Spring Harbor Laboratory Press. Received September 1, 2004; revised version accepted January 19, 2005. We especially thank Drs. Scott Fraser, Laura Gammill, Tatjana Sauka-Spengler, Tanya Moreno, Daniel Meulemans, Peter Lwigale, and Byung Joon Hwang for critical comments on this manuscript; Samuel Ki for technical assistance; and members of our laboratories for technical advice and help. We are grateful to the people who provided plasmids, as mentioned in Materials and Methods. This work was supported by an American Heart Association Post-doctoral Fellowship to Y.K. and by NIH grant DE13223 to M.B.-F.

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