| Literature DB >> 33459589 |
Guillem Angulo1, Jelena Zeleznjak2,3, Pablo Martínez-Vicente1,4, Joan Puñet-Ortiz1,4, Hartmut Hengel5,6, Martin Messerle7, Annette Oxenius8, Stipan Jonjic2,3, Astrid Krmpotić3, Pablo Engel1,4, Ana Angulo1,4.
Abstract
Viral infections are controlled, and very often cleared, by activated T lymphocytes. The inducible co-stimulator (ICOS) mediates its functions by binding to its ligand ICOSL, enhancing T-cell activation and optimal germinal center (GC) formation. Here, we show that ICOSL is heavily downmodulated during infection of antigen-presenting cells by different herpesviruses. We found that, in murine cytomegalovirus (MCMV), the immunoevasin m138/fcr-1 physically interacts with ICOSL, impeding its maturation and promoting its lysosomal degradation. This viral protein counteracts T-cell responses, in an ICOS-dependent manner, and limits virus control during the acute MCMV infection. Additionally, we report that blockade of ICOSL in MCMV-infected mice critically regulates the production of MCMV-specific antibodies due to a reduction of T follicular helper and GC B cells. Altogether, these findings reveal a novel mechanism evolved by MCMV to counteract adaptive immune surveillance, and demonstrates a role of the ICOS:ICOSL axis in the host defense against herpesviruses.Entities:
Keywords: antigen presenting cells; cd275; cytomegalovirus; herpesvirus; icosl; immunology; inflammation; mouse; t-cell co-stimulation; viral immune evasion; virus
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Year: 2021 PMID: 33459589 PMCID: PMC7840182 DOI: 10.7554/eLife.59350
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140