| Literature DB >> 32467605 |
Caroline La1,2, Bérengère de Toeuf2,3, Laure B Bindels4, Laurye Van Maele1,2, Assiya Assabban1,2, Maxime Melchior1,2, Justine Smout1,2, Arnaud Köhler1,2, Muriel Nguyen1,2, Séverine Thomas1,2, Romuald Soin2,3, Nadège Delacourt2,3, Hsüehlei Li2,3, Wenqian Hu5, Perry J Blackshear6, Véronique Kruys2,3, Cyril Gueydan2,3, Guillaume Oldenhove2,7, Stanislas Goriely8,9.
Abstract
AU-rich element (ARE)-mediated mRNA decay represents a key mechanism to avoid excessive production of inflammatory cytokines. Tristetraprolin (TTP, encoded by Zfp36) is a major ARE-binding protein, since Zfp36-/- mice develop a complex multiorgan inflammatory syndrome that shares many features with spondyloarthritis. The role of TTP in intestinal homeostasis is not known. Herein, we show that Zfp36-/- mice do not develop any histological signs of gut pathology. However, they display a clear increase in intestinal inflammatory markers and discrete alterations in microbiota composition. Importantly, oral antibiotic treatment reduced both local and systemic joint and skin inflammation. We further show that absence of overt intestinal pathology is associated with local expansion of regulatory T cells. We demonstrate that this is related to increased vitamin A metabolism by gut dendritic cells, and identify RALDH2 as a direct target of TTP. In conclusion, these data bring insights into the interplay between microbiota-dependent gut and systemic inflammation during immune-mediated disorders, such as spondyloarthritis.Entities:
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Year: 2020 PMID: 32467605 PMCID: PMC9386908 DOI: 10.1038/s41385-020-0302-x
Source DB: PubMed Journal: Mucosal Immunol ISSN: 1933-0219 Impact factor: 8.701