POU domain factor Brn-3a controls the differentiation and survival of trigeminal neurons by regulating Trk receptor expression

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JOURNAL ARTICLES

POU domain factor Brn-3a controls the differentiation and survival of trigeminal neurons by regulating Trk receptor expression

EJ Huang, K Zang, A Schmidt, A Saulys, M Xiang and LF Reichardt
Program in Neuroscience, Department of Physiology, and Howard Hughes Medical Institute, University of California, San Francisco, CA 94143-0723. USA.

Mice lacking the POU domain-containing transcription factor Brn-3a have several neuronal deficits. In the present paper, we show that Brn-3a plays two distinct roles during development of the trigeminal ganglion. In this ganglion, neurons expressing the neurotrophin receptors, TrkB and TrkC, are born between E9.5 and E11.5. In the absence of Brn-3a, very few neurons ever express TrkC, but TrkB-expressing neurons are present at E12.5 in elevated numbers, suggesting that Brn-3a may be a constituent of a regulatory circuit determining which Trk receptor is expressed by these early-born neurons. Most neurons expressing the neurotrophin receptor TrkA are generated between E11.5 and E13.5 in this ganglion and their initial generation is not prevented by absence of Brn-3a. However, after E12. 5, absence of Brn-3a results in a progressive loss in neuronal TrkA and TrkB expression, which leads to a massive wave of apoptosis that peaks at E15.5. Despite complete absence of the Trk receptors at E17. 5 and P0, approximately 30% of the normal complement of neurons survive to birth in Brn-3a mutants. Approximately 70% of these express the GDNF receptor subunit, c-ret; many can be sustained by GDNF, but not by NGF in culture. Thus, the vast majority of surviving neurons are probably sustained in vivo by trophic factor(s) whose receptors are not regulated by Brn-3a. In conclusion, our data indicate the specific functions of Brn-3a in controlling the survival and differentiation of trigeminal neurons by regulating expression of each of the three Trk receptors.
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				S. R. Eng, J. Lanier, N. Fedtsova, and E. E. Turner Coordinated regulation of gene expression by Brn3a in developing sensory ganglia Development, August 15, 2004; 131(16): 3859 - 3870. [Abstract] [Full Text] [PDF]

				L. Ma, L. Lei, S. R. Eng, E. Turner, and L. F. Parada Brn3a regulation of TrkA/NGF receptor expression in developing sensory neurons Development, August 1, 2003; 130(15): 3525 - 3534. [Abstract] [Full Text] [PDF]

				S. W. Wang, X. Mu, W. J. Bowers, D.-S. Kim, D. J. Plas, M. C. Crair, H. J. Federoff, L. Gan, and W. H. Klein Brn3b/Brn3c double knockout mice reveal an unsuspected role for Brn3c in retinal ganglion cell axon outgrowth Development, March 3, 2003; 129(2): 467 - 477. [Abstract] [Full Text] [PDF]

				M. Trieu, A. Ma, S. R. Eng, N. Fedtsova, and E. E. Turner Direct autoregulation and gene dosage compensation by POU-domain transcription factor Brn3a Development, January 1, 2003; 130(1): 111 - 121. [Abstract] [Full Text] [PDF]

				E. J. Huang, W. Liu, B. Fritzsch, L. M. Bianchi, L. F. Reichardt, and M. Xiang Brn3a is a transcriptional regulator of soma size, target field innervation and axon pathfinding of inner ear sensory neurons Development, July 1, 2001; 128(13): 2421 - 2432. [Abstract] [Full Text] [PDF]

				S. R. Eng, K. Gratwick, J. M. Rhee, N. Fedtsova, L. Gan, and E. E. Turner Defects in Sensory Axon Growth Precede Neuronal Death in Brn3a-Deficient Mice J. Neurosci., January 15, 2001; 21(2): 541 - 549. [Abstract] [Full Text] [PDF]

				L Lei, L Ma, S Nef, T Thai, and L. Parada mKlf7, a potential transcriptional regulator of TrkA nerve growth factor receptor expression in sensory and sympathetic neurons Development, January 4, 2001; 128(7): 1147 - 1158. [Abstract] [PDF]

				V. A. BOTCHKAREV, N. V. BOTCHKAREVA, K. M. ALBERS, L.-H. CHEN, P. WELKER, and R. PAUS A role for p75 neurotrophin receptor in the control of apoptosis-driven hair follicle regression FASEB J, October 1, 2000; 14(13): 1931 - 1942. [Abstract] [Full Text]

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				E. Ensor, M. D. Smith, and D. S. Latchman The BRN-3A Transcription Factor Protects Sensory but Not Sympathetic Neurons from Programmed Cell Death/Apoptosis J. Biol. Chem., February 9, 2001; 276(7): 5204 - 5212. [Abstract] [Full Text] [PDF]