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Publication : Context-dependent effects of IL-2 rewire immunity into distinct cellular circuits.

First Author  Whyte CE Year  2022
Journal  J Exp Med Volume  219
Issue  7 PubMed ID  35699942
Mgi Jnum  J:354864 Mgi Id  MGI:7287371
Doi  10.1084/jem.20212391 Citation  Whyte CE, et al. (2022) Context-dependent effects of IL-2 rewire immunity into distinct cellular circuits. J Exp Med 219(7):e20212391
abstractText  Interleukin 2 (IL-2) is a key homeostatic cytokine, with therapeutic applications in both immunogenic and tolerogenic immune modulation. Clinical use has been hampered by pleiotropic functionality and widespread receptor expression, with unexpected adverse events. Here, we developed a novel mouse strain to divert IL-2 production, allowing identification of contextual outcomes. Network analysis identified priority access for Tregs and a competitive fitness cost of IL-2 production among both Tregs and conventional CD4 T cells. CD8 T and NK cells, by contrast, exhibited a preference for autocrine IL-2 production. IL-2 sourced from dendritic cells amplified Tregs, whereas IL-2 produced by B cells induced two context-dependent circuits: dramatic expansion of CD8+ Tregs and ILC2 cells, the latter driving a downstream, IL-5-mediated, eosinophilic circuit. The source-specific effects demonstrate the contextual influence of IL-2 function and potentially explain adverse effects observed during clinical trials. Targeted IL-2 production therefore has the potential to amplify or quench particular circuits in the IL-2 network, based on clinical desirability.
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