The chromatin remodelling factor Brg-1 interacts with β-catenin to promote target gene activation

Nick Barker, Adam Hurlstone, Hannah Musisi, Antony Miles, Mariann Bienz, Hans Clevers

    Research output: Contribution to journalArticlepeer-review

    Abstract

    Wnt-induced formation of nuclear Tcf-β-catenin complexes promotes transcriptional activation of target genes involved in cell fate decisions. Inappropriate expression of Tcf target genes resulting from mutational activation of this pathway is also implicated in tumorigenesis. The C-terminus of β-catenin is indispensable for the transactivation function, which probably reflects the presence of binding sites for essential transcriptional coactivators such as p300/CBP. However, the precise mechanism of transactivation remains unclear. Here we demonstrate an interaction between β-catenin and Brg-1, a component of mammalian SWI/SNF and Rsc chromatin-remodelling complexes. A functional consequence of reintroduction of Brg-1 into Brg-1-deficient cells is enhanced activity of a Tcf-responsive reporter gene. Consistent with this, stable expression of inactive forms of Brg-1 in colon carcinoma cell lines specifically inhibits expression of endogenous Tcf target genes. In addition, we observe genetic interactions between the Brg-1 and β-catenin homologues in flies. We conclude that β-catenin recruits Brg-1 to Tcf target gene promoters, facilitating chromatin remodelling as a prerequisite for transcriptional activation.
    Original languageEnglish
    Pages (from-to)4935-4943
    Number of pages8
    JournalEMBO Journal
    Volume20
    Issue number17
    DOIs
    Publication statusPublished - 3 Sept 2001

    Keywords

    • β-catenin
    • Brg-1
    • Chromatin remodelling
    • SNF
    • SWI
    • Tcf

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