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Publication : HeyL regulates the number of TrkC neurons in dorsal root ganglia.

First Author  Mukhopadhyay A Year  2009
Journal  Dev Biol Volume  334
Issue  1 Pages  142-51
PubMed ID  19631204 Mgi Jnum  J:153555
Mgi Id  MGI:4365702 Doi  10.1016/j.ydbio.2009.07.018
Citation  Mukhopadhyay A, et al. (2009) HeyL regulates the number of TrkC neurons in dorsal root ganglia. Dev Biol 334(1):142-51
abstractText  The basic-helix-loop-helix transcription factor HeyL is expressed at high levels by neural crest progenitor cells (NCPs) that give rise to neurons and glia in dorsal root ganglia (DRG). Since HeyL expression was observed in these NCPs during the period of neurogenesis, we generated HeyL null mutants to help examine the factor's role in ganglion neuronal specification. Homozygous null mutation of HeyL reduced the number of TrkC(+) neurons in DRG at birth including the subpopulation that expresses the ETS transcription factor ER81. Conversely, null mutation of the Hey paralog, Hey1, increased the number of TrkC(+) neurons. Null mutation of HeyL increased expression of the Hey paralogs Hey1 and Hey2, suggesting that HeyL normally inhibits their expression. Double null mutation of both Hey1 and HeyL rescued TrkC(+) neuron numbers to control levels. Thus, the balance between HeyL and Hey1 expression regulates the differentiation of a subpopulation of TrkC(+) neurons in the DRG.
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