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Volume 59, Issue 5, Pages (November 2013)

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1 Volume 59, Issue 5, Pages 1107-1117 (November 2013)
Wnt signaling and hepatocarcinogenesis: Molecular targets for the development of innovative anticancer drugs  Floriane Pez, Anaïs Lopez, Miran Kim, Jack R. Wands, Claude Caron de Fromentel, Philippe Merle  Journal of Hepatology  Volume 59, Issue 5, Pages (November 2013) DOI: /j.jhep Copyright © 2013 European Association for the Study of the Liver Terms and Conditions

2 Fig. 1 Canonical Wnt/FZD signaling pathway. (A) In the absence of Wnt signaling, soluble β-catenin is phosphorylated by a degradation complex consisting of the kinases GSK3β and CK1α and the scaffolding proteins APC and Axin1. Phosphorylated β-catenin is targeted for proteasomal degradation after ubiquitination by the SCF protein complex. In the nucleus and in the absence of β-catenin, TCF/LEF transcription factor activity is repressed by TLE-1; (B) activation of the canonical Wnt/FZD signaling leads to phosphorylation of Dvl/Dsh, which in turn recruits Axin1 and GSK3β adjacent to the plasma membrane, thus preventing the formation of the degradation complex. As a result, β-catenin accumulates in the cytoplasm and translocates into the nucleus, where it promotes the expression of target genes via interaction with TCF/LEF transcription factors and other proteins such as CBP, Bcl9, and Pygo. Journal of Hepatology  , DOI: ( /j.jhep ) Copyright © 2013 European Association for the Study of the Liver Terms and Conditions

3 Fig. 2 Non-canonical Wnt/FZD signaling pathways. Interaction of Wnt, FZD, and ROR2/RYK co-receptors leads to either (1) JNK activation, (2) PKCs activation, (3) NFAT transactivation, or (4) inhibition of β-catenin activity through binding of NLK to TCF/LEF. Journal of Hepatology  , DOI: ( /j.jhep ) Copyright © 2013 European Association for the Study of the Liver Terms and Conditions

4 Fig. 3 Potential Wnt-component targets for therapeutic intervention on tumor development and growth. Inactivation of Wnt signaling pathway could be achieved by: (1) targeting extracellular signaling molecules with monoclonal antibodies, soluble factors or small molecules; (2) preventing the FZD/Dvl interaction; (3) stabilizing the destruction complex or (4) increasing β-catenin proteasomal degradation and (5) preventing the interaction between β-catenin and its co-factors for transactivity in the nucleus. The relationship between therapeutic molecules and their protein targets is indicated by a color code. Molecules in bold have been tested in HCC model, those in italics in other models of tumor growth. Journal of Hepatology  , DOI: ( /j.jhep ) Copyright © 2013 European Association for the Study of the Liver Terms and Conditions

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