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XB-ART-2041
Cell 2005 Apr 08;1211:87-99. doi: 10.1016/j.cell.2005.01.033.
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Germ-layer specification and control of cell growth by Ectodermin, a Smad4 ubiquitin ligase.

Dupont S , Zacchigna L , Cordenonsi M , Soligo S , Adorno M , Rugge M , Piccolo S .


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TGF-beta signaling is essential for development and proliferative homeostasis. During embryogenesis, maternal determinants act in concert with TGF-beta signals to form mesoderm and endoderm. In contrast, ectoderm specification requires the TGF-beta response to be attenuated, although the mechanisms by which this is achieved remain unknown. In a functional screen for ectoderm determinants, we have identified Ectodermin (Ecto). In Xenopus embryos, Ecto is essential for the specification of the ectoderm and acts by restricting the mesoderm-inducing activity of TGF-beta signals to the mesoderm and favoring neural induction. Ecto is a RING-type ubiquitin ligase for Smad4, a TGF-beta signal transducer. Depletion of Ecto in human cells enforces TGF-beta-induced cytostasis and, moreover, plays a causal role in limiting the antimitogenic effects of Smad4 in tumor cells. We propose that Ectodermin is a key switch in the control of TGF-beta gene responses during early embryonic development and cell proliferation.

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Species referenced: Xenopus
Genes referenced: bmpr1a cer1 chrd ctnnb1 eomes fgfr1 isyna1 mix1 mixer myc myod1 ncam1 psmd6 smad1 smad10 smad2 smad4 sox2 tbxt tgfb1 tgfbr1 trim24 trim28 trim33 vegt ventx1.2 ventx2.2 wnt8a
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References :
Datto, Ubiquitin-mediated degradation a mechanism for fine-tuning TGF-beta signaling. 2005, Pubmed, Xenbase