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Functional dissection of the paired domain of Pax6 revealsmolecular mechanisms of coordinating neurogenesis and proliferation.

Authors :
Walcher, Tessa
Qing Xie
Sun, Jian
Irmler, Martin
Beckers, Johannes
Öztürk, Timucin
Niessing, Dierk
Stoykova, Anastassia
Cvekl, Ales
Ninkovic, Jovica
Götz, Magdalena
Source :
Development (09501991). 3/1/2013, Vol. 140 Issue 5, p1123-1136. 14p.
Publication Year :
2013

Abstract

To achieve adequate organ development and size, cell proliferation and differentiation have to be tightly regulated and coordinated. The transcription factor Pax6 regulates patterning, neurogenesis and proliferation in forebrain development. The molecular basis of this regulation is not well understood. As the bipartite DNA-binding paired domain of Pax6 regulates forebrain development, we examined mice with point mutations in its individual DNA-binding subdomains PAI (Pax6Leca4, N50K) and RED (Pax6Leca2, R128C). This revealed distinct roles in regulating proliferation in the developing cerebral cortex, with the PAI and RED subdomain mutations reducing and increasing, respectively, the number of mitoses. Conversely, neurogenesis was affected only by the PAI subdomain mutation, phenocopying the neurogenic defects observed in full Pax6 mutants. Genome-wide expression profiling identified molecularly discrete signatures of Pax6Leca4 and Pax6Leca2 mutations. Comparison to Pax6 targets identified by chromatin immunoprecipitation led to the identification and functional characterization of distinct DNA motifs in the promoters of target genes dysregulated in the Pax6Leca2 or Pax6Leca4 mutants, further supporting the distinct regulatory functions of the DNA-binding subdomains. Thus, Pax6 achieves its key roles in the developing forebrain by utilizing particular subdomains to coordinate patterning, neurogenesis and proliferation simultaneously. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
09501991
Volume :
140
Issue :
5
Database :
Academic Search Index
Journal :
Development (09501991)
Publication Type :
Academic Journal
Accession number :
86725787
Full Text :
https://doi.org/10.1242/dev.082875