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Publication : Porcn-dependent Wnt signaling is not required prior to mouse gastrulation.

First Author  Biechele S Year  2013
Journal  Development Volume  140
Issue  14 Pages  2961-71
PubMed ID  23760955 Mgi Jnum  J:198636
Mgi Id  MGI:5498588 Doi  10.1242/dev.094458
Citation  Biechele S, et al. (2013) Porcn-dependent Wnt signaling is not required prior to mouse gastrulation. Development 140(14):2961-71
abstractText  In mice and humans the X-chromosomal porcupine homolog (Porcn) gene is required for the acylation and secretion of all 19 Wnt ligands and thus represents a bottleneck for all Wnt signaling. We have generated a mouse line carrying a floxed allele for Porcn and used zygotic, oocyte-specific and visceral endoderm-specific deletions to investigate embryonic and extra-embryonic requirements for Wnt ligand secretion. We show that there is no requirement for Porcn-dependent secretion of Wnt ligands during preimplantation development of the mouse embryo. Porcn-dependent Wnts are first required for the initiation of gastrulation, where Porcn function is required in the epiblast but not the visceral endoderm. Heterozygous female embryos, which are mutant in both trophoblast and visceral endoderm due to imprinted X chromosome inactivation, complete gastrulation but display chorio-allantoic fusion defects similar to Wnt7b mutants. Our studies highlight the importance of Wnt3 and Wnt7b for embryonic and placental development but suggest that endogenous Porcn-dependent Wnt secretion does not play an essential role in either implantation or blastocyst lineage specification.
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