The interaction of xKaiso with xTcf3: a revised model for integration of epigenetic and Wnt signalling pathways

doi:10.1242/dev.025577

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Development ePress online publication date 21 Jan 2009
doi: 10.1242/dev.025577

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The interaction of xKaiso with xTcf3: a revised model for integration of epigenetic and Wnt signalling pathways

Alexey Ruzov, Jamie A. Hackett, Anna Prokhortchouk, James P. Reddington, Monika J. Madej, Donncha S. Dunican, Egor Prokhortchouk, Sari Pennings, and Richard R. Meehan^*
^* Author for correspondence (e-mail: r.meehan{at}hgu.mrc.ac.uk)

We demonstrate that a direct interaction between the methyl-CpG-dependenttranscription repressor Kaiso and xTcf3, a transducer of theWnt signalling pathway, results in their mutual disengagementfrom their respective DNA-binding sites. Thus, the transcriptionfunctions of xTcf3 can be inhibited by overexpression of Kaisoin cell lines and Xenopus embryos. The interaction of Kaisowith xTcf3 is highly conserved and is dependent on its zinc-fingerdomains (ZF1-3) and the corresponding HMG DNA-binding domainof TCF3/4 factors. Our data rule out a model suggesting thatxKaiso is a direct repressor of Wnt signalling target genesin early Xenopus development via binding to promoter-proximalCTGCNA sequences as part of a xTcf3 repressor complex. Instead,we propose that mutual inhibition by Kaiso/TCF3 of their DNA-bindingfunctions may be important in developmental or cancer contextsand acts as a regulatory node that integrates epigenetic andWnt signalling pathways.

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