| Literature DB >> 29988089 |
Fiamma Salerno1, Sander Engels1, Maartje van den Biggelaar2, Floris P J van Alphen2, Aurelie Guislain1, Wanqi Zhao1, Deborah L Hodge3, Sarah E Bell4, Jan Paul Medema5, Marieke von Lindern1, Martin Turner4, Howard A Young3, Monika C Wolkers6.
Abstract
Memory T cells are critical for the immune response to recurring infections. Their instantaneous reactivity to pathogens is empowered by the persistent expression of cytokine-encoding mRNAs. How the translation of proteins from pre-formed cytokine-encoding mRNAs is prevented in the absence of infection has remained unclear. Here we found that protein production in memory T cells was blocked via a 3' untranslated region (3' UTR)-mediated process. Germline deletion of AU-rich elements (AREs) in the Ifng-3' UTR led to chronic cytokine production in memory T cells. This aberrant protein production did not result from increased expression and/or half-life of the mRNA. Instead, AREs blocked the recruitment of cytokine-encoding mRNA to ribosomes; this block depended on the ARE-binding protein ZFP36L2. Thus, AREs mediate repression of translation in mouse and human memory T cells by preventing undesirable protein production from pre-formed cytokine-encoding mRNAs in the absence of infection.Entities:
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Year: 2018 PMID: 29988089 PMCID: PMC6643272 DOI: 10.1038/s41590-018-0155-6
Source DB: PubMed Journal: Nat Immunol ISSN: 1529-2908 Impact factor: 25.606