Functional equivalence of Brn3 POU-domain transcription factors in mouse retinal neurogenesis

doi:10.1242/dev.01646

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Development ePress online publication date 12 Jan 2005
doi: 10.1242/dev.01646

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Research article

Functional equivalence of Brn3 POU-domain transcription factors in mouse retinal neurogenesis

Ling Pan, Zhiyong Yang, Liang Feng, and Lin Gan^*
^* Author for correspondence (e-mail: lin gan{at}urmc.rochester.edu)

POU-domain transcription factors play essential roles in cellproliferation and differentiation. Previous studies have shownthat targeted deletion of each of the three POU-domain Brn3factors in mice leads to the developmental failure and apoptosisof a unique set of sensory neurons in retina, dorsal root ganglia,trigeminal ganglia and inner ear. The specific defects associatedwith the removal of each Brn3 gene closely reflect their characteristicspatiotemporal expression patterns. Nevertheless, it remainselusive whether Brn3 factors are functionally equivalent andact through a common molecular mechanism to regulate the developmentand survival of these sensory neurons. By knocking-in Brn3a(Brn3a^ki) into the Brn3b locus, we showed here that Brn3a^kiwas expressed in a spatiotemporal manner identical to that ofendogenous Brn3b. In addition, Brn3a^ki functionally restoredthe normal development and survival of retinal ganglion cells(RGCs) in the absence of Brn3b and fully reinstated the earlydevelopmental expression profiles of Brn3b downstream targetgenes in retina. These results indicate that Brn3 factors arefunctionally equal and that their unique roles in neurogenesisare determined by the distinctive Brn3 spatiotemporal expressionpatterns.

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