Non-cell-autonomous role for Cripto in axial midline formation during vertebrate embryogenesis

doi:10.1242/dev.02157

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Development ePress online publication date 16 Nov 2005
doi: 10.1242/dev.02157

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Research article

Non-cell-autonomous role for Cripto in axial midline formation during vertebrate embryogenesis

Jianhua Chu, Jixiang Ding, Katherine Jeays-Ward, Sandy M. Price, Marysia Placzek, and Michael M. Shen^*
^* Author for correspondence (e-mail: mshen{at}cabm.rutgers.edu)

Several membrane-associated proteins are known to modulatethe activity and range of potent morphogenetic signals duringdevelopment. In particular, members of the Egf-Cfc family encodeglycosyl-phosphatidylinositol (GPI)-linked proteins that areessential for activity of the transforming growth factor ${beta}$ (TGF ${beta}$ )ligand Nodal, a factor that plays a central role in establishingthe vertebrate body plan. Genetic and biochemical studies haveindicated that Egf-Cfc proteins function as cell-autonomousco-receptors for Nodal; by contrast, cell culture data havesuggested that the mammalian Egf-Cfc protein Cripto can actas a secreted signaling factor. Here we show that Cripto actsnon-cell-autonomously during axial mesendoderm formation inthe mouse embryo and may possess intercellular signaling activityin vivo. Phenotypic analysis of hypomorphic mutants demonstratesthat Cripto is essential for formation of the notochordal plate,prechordal mesoderm and foregut endoderm during gastrulation.Remarkably, Cripto null mutant cells readily contribute to thesetissues in chimeras, indicating non-cell-autonomy. Consistentwith these loss-of-function analyses, gain-of-function experimentsin chick embryos show that exposure of node/head process mesodermto soluble Cripto protein results in alterations in cell fatestoward anterior mesendoderm, in a manner that is dependent onNodal signaling. Taken together, our findings support a modelin which Cripto can function in trans as an intercellular mediatorof Nodal signaling activity.

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