| Literature DB >> 33826894 |
Giulio Cavalli1, Isak W Tengesdal2, Mark Gresnigt3, Travis Nemkov4, Rob J W Arts5, Jorge Domínguez-Andrés5, Raffaella Molteni6, Davide Stefanoni7, Eleonora Cantoni7, Laura Cassina6, Silvia Giugliano8, Kiki Schraa5, Taylor S Mills9, Eric M Pietras9, Elan Z Eisenmensser4, Lorenzo Dagna10, Alessandra Boletta6, Angelo D'Alessandro4, Leo A B Joosten5, Mihai G Netea11, Charles A Dinarello12.
Abstract
Trained immunity (TI) is a de facto innate immune memory program induced in monocytes/macrophages by exposure to pathogens or vaccines, which evolved as protection against infections. TI is characterized by immunometabolic changes and histone post-translational modifications, which enhance production of pro-inflammatory cytokines. As aberrant activation of TI is implicated in inflammatory diseases, tight regulation is critical; however, the mechanisms responsible for this modulation remain elusive. Interleukin-37 (IL-37) is an anti-inflammatory cytokine that curbs inflammation and modulates metabolic pathways. In this study, we show that administration of recombinant IL-37 abrogates the protective effects of TI in vivo, as revealed by reduced host pro-inflammatory responses and survival to disseminated candidiasis. Mechanistically, IL-37 reverses the immunometabolic changes and histone post-translational modifications characteristic of TI in monocytes, thus suppressing cytokine production in response to infection. IL-37 thereby emerges as an inhibitor of TI and as a potential therapeutic target in immune-mediated pathologies.Entities:
Keywords: IL-1 family; cell energy metabolism; cytokines; epigenetics; immunometabolism; infection; inflammation; innate immunity; neutrophils; regulatory cytokine; trained immunity
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Year: 2021 PMID: 33826894 DOI: 10.1016/j.celrep.2021.108955
Source DB: PubMed Journal: Cell Rep Impact factor: 9.995