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Cripto promotes A-P axis specification independently of its stimulatory effect on Nodal autoinduction

Academic Article
Publication Date:
2008
abstract:
The EGF-CFC gene cripto governs anterior-posterior (A-P) axis specification in the vertebrate embryo. Existing models suggest that Cripto facilitates binding of Nodal to an ActRII-activin-like kinase (ALK) 4 receptor complex. Cripto also has a crucial function in cellular transformation that is independent of Nodal and ALK4. However, how ALK4-independent Cripto pathways function in vivo has remained unclear. We have generated cripto mutants carrying the amino acid substitution F78A, which blocks the Nodal-ALK4-Smad2 signaling both in embryonic stem cells and cell-based assays. in cripto(F78A/F78A), mouse embryos, Nodal fails to expand its own expression domain and that of cripto, indicating that F78 is essential in vivo to stimulate Smad-dependent Nodal autoinduction. In sharp contrast to cripto-null mutants, cripto(F78A/F78A) embryos establish an A-P axis and initiate gastrulation movements. Our findings provide in vivo evidence that Cripto is required in the Nodal-Smad2 pathway to activate an autoinductive feedback loop, whereas it can promote A-P axis formation and initiate gastrulation movements independently of its stimulatory effect on the canonical Nodal-ALK4-Smad2 signaling pathway.
Iris type:
01.01 Articolo in rivista
Keywords:
MOUSE EMBRYO; GROWTH-FACTOR; SIGNALING PATHWAY; TGF-BETA; PRIMITIVE STREAK
List of contributors:
Minchiotti, Gabriella; Liguori, GIOVANNA LUCIA; Persico, Maria
Authors of the University:
LIGUORI GIOVANNA LUCIA
MINCHIOTTI GABRIELLA
Handle:
https://iris.cnr.it/handle/20.500.14243/26336
Published in:
THE JOURNAL OF CELL BIOLOGY
Journal
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URL

http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2234230/?tool=pubmed
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