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Retinal patterning by Pax6‐dependent cell adhesion molecules
Authors:Elisabeth Rungger‐Brändle  Jürgen A. Ripperger  Kurt Steiner  Alain Conti  Ariane Stieger  Sahar Soltanieh  Duri Rungger
Affiliation:1. Cell Biology Laboratory, University Eye Clinic, HUG, 22, Rue Alcide Jentzer, Geneva CH‐1211, Switzerland;2. Department of Biochemistry, University of Fribourg, Rue Du Musée 5, Fribourg CH‐1700, Switzerland;3. Institute of Molecular Life Sciences IMLS, University of Zurich‐Irchel, Winterthurer Strasse 190, Zurich CH‐8057, Switzerland;4. Station de Zoologie Expérimentale, University of Geneva, 154, Rte de Malagnou, Chêne‐Bougeries CH‐1224, Switzerland
Abstract:Long‐standing evidence gained from Pax6 mutant embryos pointed to an involvement of Pax6‐dependent cell adhesion molecules in patterning the central nervous system and, in particular, the retina. However, direct evidence for such pathways remained elusive. We here present direct evidence that knockdown of Pax6 expression by morpholino antisense molecules in Xenopus embryos and knockdown of maternal N‐cadherin (mNcad), N‐cadherin (Ncad) and neural cell adhesion molecule (NCAM) produce similar phenotypes. Eye formation is reduced and retinal lamination is heavily disorganized. In Pax6 knockdown embryos, the levels of mRNAs coding for these cell adhesion molecules are markedly reduced. Overexpression of Pax6 efficiently rescues the phenotype of Pax6 knockdown embryos and restores expression of these putative target genes. Rescue of Pax6‐deficiency by the putative target gene mNcad moderately rescues eye formation. The promoters of the genes coding for cell adhesion molecules contain several putative Pax6 binding sites, as determined by computer analysis. Chromatin immunoprecipitation shows that, in embryonic heads, Pax6 binds to promoter regions containing such predicted binding sites. Thus, several cell adhesion molecules are direct target genes of Pax6 and cooperate in retinal patterning. © 2010 Wiley Periodicals, Inc. Develop Neurobiol 70: 764–780, 2010
Keywords:cadherins  NCAM  duplication  rosette  RPE
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