| Literature DB >> 23954131 |
Jorg van Loosdregt1, Veerle Fleskens, Machteld M Tiemessen, Michal Mokry, Ruben van Boxtel, Jenny Meerding, Cornelieke E G M Pals, Dorota Kurek, Miranda R M Baert, Eveline M Delemarre, Andrea Gröne, Marianne J A Groot Koerkamp, Alice J A M Sijts, Edward E S Nieuwenhuis, Madelon M Maurice, Johan H van Es, Derk Ten Berge, Frank C Holstege, Frank J T Staal, Dietmar M W Zaiss, Berent J Prakken, Paul J Coffer.
Abstract
Foxp3 is crucial for both the development and function of regulatory T (Treg) cells; however, the posttranslational mechanisms regulating Foxp3 transcriptional output remain poorly defined. Here, we demonstrate that T cell factor 1 (TCF1) and Foxp3 associates in Treg cells and that active Wnt signaling disrupts Foxp3 transcriptional activity. A global chromatin immunoprecipitation sequencing comparison in Treg cells revealed considerable overlap between Foxp3 and Wnt target genes. The activation of Wnt signaling reduced Treg-mediated suppression both in vitro and in vivo, whereas disruption of Wnt signaling in Treg cells enhanced their suppressive capacity. The activation of effector T cells increased Wnt3a production, and Wnt3a levels were found to be greatly increased in mononuclear cells isolated from synovial fluid versus peripheral blood of arthritis patients. We propose a model in which Wnt produced under inflammatory conditions represses Treg cell function, allowing a productive immune response, but, if uncontrolled, could lead to the development of autoimmunity.Entities:
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Year: 2013 PMID: 23954131 DOI: 10.1016/j.immuni.2013.07.019
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745