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RELA tunes innate-like interferon I/III responses in human T cells

Nadia Jeremiah, Hermine Ferran, Konstantina Antoniadou, Kevin de Azevedo, Jovan Nikolić, Mathieu Maurin, Philippe Benaroch, Nicolas Manel

2023The Journal of Experimental Medicine19 citationsDOIOpen Access PDF

Abstract

In innate immune cells, intracellular sensors such as cGAS-STING stimulate type I/III interferon (IFN) expression, which promotes antiviral defense and immune activation. However, how IFN-I/III expression is controlled in adaptive cells is poorly understood. Here, we identify a transcriptional rheostat orchestrated by RELA that confers human T cells with innate-like abilities to produce IFN-I/III. Despite intact cGAS-STING signaling, IFN-I/III responses are stunted in CD4+ T cells compared with dendritic cells or macrophages. We find that lysine residues in RELA tune the IFN-I/III response at baseline and in response to STING stimulation in CD4+ T cells. This response requires positive feedback driven by cGAS and IRF7 expression. By combining RELA with IRF3 and DNA demethylation, IFN-I/III production in CD4+ T cells reaches levels observed in dendritic cells. IFN-I/III production provides self-protection of CD4+ T cells against HIV infection and enhances the elimination of tumor cells by CAR T cells. Therefore, innate-like functions can be tuned and leveraged in human T cells.

Topics & Concepts

Innate immune systemBiologyInterferonIRF3IRF7Cell biologyTLR9StingInnate lymphoid cellImmune systemAcquired immune systemImmunologyGene expressionDNA methylationGeneEngineeringBiochemistryAerospace engineeringinterferon and immune responsesImmune Cell Function and Interaction
RELA tunes innate-like interferon I/III responses in human T cells | Litcius