@article{2a9ece3d94c449109b5cf3e9bd5f4c7a,
title = "Phosphorylation of neurogenin2 specifies the migration properties and the dendritic morphology of pyramidal neurons in the neocortex",
abstract = "The molecular mechanisms specifying the dendritic morphology of different neuronal subtypes are poorly understood. Here we demonstrate that the bHLH transcription factor Neurogenin2 (Ngn2) is both necessary and sufficient for specifying the dendritic morphology of pyramidal neurons in vivo by specifying the polarity of its leading process during the initiation of radial migration. The ability of Ngn2 to promote a polarized leading process outgrowth requires the phosphorylation of a single tyrosine residue at position 241, an event that is neither involved in Ngn2 direct transactivation properties nor its proneural function. Interestingly, the migration defect observed in the Ngn2 knockout mouse and in progenitors expressing the Ngn2Y241F mutation can be rescued by inhibiting the activity of the small-GTPase RhoA in cortical progenitors. Our results demonstrate that Ngn2 coordinates the acquisition of the radial migration properties and the unipolar dendritic morphology characterizing pyramidal neurons through molecular mechanisms distinct from those mediating its proneural activity.",
author = "Randal Hand and Dante Bortone and Pierre Mattar and Laurent Nguyen and Heng, {Julian Ik Tsen} and Sabrice Guerrier and Elizabeth Boutt and Eldon Peters and Barnes, {Anthony P.} and Carlos Parras and Carol Schuurmans and Fran{\c c}ois Guillemot and Franck Polleux",
note = "Funding Information: We are grateful to K. Burridge, A. McMahon, M.J. Tsai, and A. Ghosh for providing constructs and to Dr. Nakafuku for providing the polyclonal anti-Ngn2 antibody. We would like to thank members of the K. Burridge, L. Graves, and M. Schaller{\textquoteright}s laboratories for helpful advices. The Nestin (Rat-401) monoclonal antibody developed by Dr. S. Hockfield was obtained through the Developmental Studies Hybridoma Bank (NICHD -University of Iowa, Dept. of Biol. Sciences). This project was partially funded by the NIH-National Institute of Neurological Disorders and Stroke (NS047701-01) (F.P.), by the Confocal and Multiphoton Imaging Facility of the NINDS Institutional Center Core Grant to Support Neuroscience Research (P30 NS45892-01), the Pew Charitable Trust (F.P.), and the March of Dimes Foundation for Birth Defects (F.P.). P.M. is a recipient of a CIHR Doctoral award, L.N. is supported by a EMBO long-term fellowship, J.I.-T.H. is supported by a Postdoctoral training fellowship from Australian NHMRC. F.G.{\textquoteright}s lab contribution was supported by MRC core funding and an European Commission RTD Program grant. ",
year = "2005",
month = oct,
day = "6",
doi = "10.1016/j.neuron.2005.08.032",
language = "English (US)",
volume = "48",
pages = "45--62",
journal = "Neuron",
issn = "0896-6273",
publisher = "Cell Press",
number = "1",
}