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CD25-targeted IL-2 signals promote improved outcomes of influenza infection and boost memory CD4 T cell formation

Authors :
Susan L. Swain
Fahmida Alam
Andrea M. Cooper
Valeria Flores-Malavet
Stewart Sell
Ayushi Singh
K. Kai McKinstry
Tara M. Strutt
Source :
J Immunol
Publication Year :
2020

Abstract

IL-2 is a pleotropic cytokine with potent pro- and anti-inflammatory effects. These divergent impacts can be directed in vivo by forming complexes of IL-2 and anti–IL-2 mAbs (IL-2C) to target IL-2 to distinct subsets of cells based on their expression of subunits of the IL-2R. In this study, we show that treatment of mice with a prototypical anti-inflammatory IL-2C, JES6-1–IL-2C, best known to induce CD25+ regulatory CD4 T cell expansion, surprisingly causes robust induction of a suite of inflammatory factors. However, treating mice infected with influenza A virus with this IL-2C reduces lung immunopathology. We compare the spectrum of inflammatory proteins upregulated by pro- and anti-inflammatory IL-2C treatment and uncover a pattern of expression that reveals potentially beneficial versus detrimental aspects of the influenza-associated cytokine storm. Moreover, we show that anti-inflammatory IL-2C can deliver survival signals to CD4 T cells responding to influenza A virus that improve their memory fitness, indicating a novel application of IL-2 to boost pathogen-specific T cell memory while simultaneously reducing immunopathology.

Details

Language :
English
Database :
OpenAIRE
Journal :
J Immunol
Accession number :
edsair.doi.dedup.....60b64aab4c695aad6e9cde0a9ec7766a