| Literature DB >> 32338592 |
Clotilde Guyon1, Nada Jmari1, Francine Padonou1,2, Yen-Chin Li1, Olga Ucar3, Noriyuki Fujikado4, Fanny Coulpier5, Christophe Blanchet6, David E Root7, Matthieu Giraud1,2.
Abstract
The ability of the immune system to avoid autoimmune disease relies on tolerization of thymocytes to self-antigens whose expression and presentation by thymic medullary epithelial cells (mTECs) is controlled predominantly by Aire at the transcriptional level and possibly regulated at other unrecognized levels. Aire-sensitive gene expression is influenced by several molecular factors, some of which belong to the 3'end processing complex, suggesting they might impact transcript stability and levels through an effect on 3'UTR shortening. We discovered that Aire-sensitive genes display a pronounced preference for short-3'UTR transcript isoforms in mTECs, a feature preceding Aire's expression and correlated with the preferential selection of proximal polyA sites by the 3'end processing complex. Through an RNAi screen and generation of a lentigenic mouse, we found that one factor, Clp1, promotes 3'UTR shortening associated with higher transcript stability and expression of Aire-sensitive genes, revealing a post-transcriptional level of control of Aire-activated expression in mTECs.Entities:
Keywords: 3'UTR shortening; Aire; genetics; genomics; immunological tolerance; immunology; inflammation; mTEC; mouse; self-antigens; thymus
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Year: 2020 PMID: 32338592 PMCID: PMC7205469 DOI: 10.7554/eLife.52985
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140