NF-κB subunits RelA and c-Rel selectively control CD4+ T cell function in multiple sclerosis and cancer

Author:

Lalle Guilhem1ORCID,Lautraite Raphaëlle1ORCID,Bouherrou Khaled1ORCID,Plaschka Maud1ORCID,Pignata Aurora2ORCID,Voisin Allison1ORCID,Twardowski Julie1ORCID,Perrin-Niquet Marlène1ORCID,Stéphan Pierre1ORCID,Durget Sarah1ORCID,Tonon Laurie3ORCID,Ardin Maude3ORCID,Degletagne Cyril1ORCID,Viari Alain3ORCID,Belgarbi Dutron Laurence4ORCID,Davoust Nathalie5ORCID,Postler Thomas S.6ORCID,Zhao Jingyao6ORCID,Caux Christophe1ORCID,Caramel Julie1ORCID,Dalle Stéphane1ORCID,Cassier Philippe A.1ORCID,Klein Ulf7ORCID,Schmidt-Supprian Marc8910ORCID,Liblau Roland2ORCID,Ghosh Sankar6ORCID,Grinberg-Bleyer Yenkel1ORCID

Affiliation:

1. Cancer Research Center of Lyon, Labex DEV2CAN, Institut Convergence Plascan, Centre Léon Bérard, UMR INSERM 1052, CNRS 5286, Université Claude Bernard Lyon 1 1 , Lyon, France

2. Toulouse Institute for Infectious and Inflammatory Diseases (Infinity), UMR INSERM 1291, CNRS 5051, Université Toulouse III 2 , Toulouse, France

3. Cancer Research Center of Lyon, Labex DEV2CAN, Institut Convergence Plascan, Centre Léon Bérard, Gilles Thomas Bioinformatics Platform, UMR INSERM 1052, CNRS 5286, Université Claude Bernard Lyon 1 3 , Lyon, France

4. Ecole Normale Supérieure of Lyon 4 Biology Department, , Lyon, France

5. Laboratory of Biology and Modelling of the Cell, Ecole Normale Supérieure of Lyon, CNRS UMR 5239, INSERM U1293 5 , Lyon, France

6. College of Physicians and Surgeons, Columbia University 6 Department of Microbiology and Immunology, , New York, NY, USA

7. Leeds Institute of Medical Research at St. James’s, University of Leeds 7 Division of Haematology and Immunology, , Leeds, UK

8. Institute of Experimental Hematology, School of Medicine, Technical University of Munich 8 , Munich, Germany

9. Center for Translational Cancer Research, School of Medicine, Technical University of Munich 9 , Munich, Germany

10. German Cancer Consortium and German Cancer Research Center 10 , Heidelberg, Germany

Abstract

The outcome of cancer and autoimmunity is often dictated by the effector functions of CD4+ conventional T cells (Tconv). Although activation of the NF-κB signaling pathway has long been implicated in Tconv biology, the cell-autonomous roles of the separate NF-κB transcription-factor subunits are unknown. Here, we dissected the contributions of the canonical NF-κB subunits RelA and c-Rel to Tconv function. RelA, rather than c-Rel, regulated Tconv activation and cytokine production at steady-state and was required for polarization toward the TH17 lineage in vitro. Accordingly, RelA-deficient mice were fully protected against neuroinflammation in a model of multiple sclerosis due to defective transition to a pathogenic TH17 gene-expression program. Conversely, Tconv-restricted ablation of c-Rel impaired their function in the microenvironment of transplanted tumors, resulting in enhanced cancer burden. Moreover, Tconv required c-Rel for the response to PD-1-blockade therapy. Our data reveal distinct roles for canonical NF-κB subunits in different disease contexts, paving the way for subunit-targeted immunotherapies.

Funder

Centre National de la Recherche Scientifique

Institut National de la Santé et de la Recherche Médicale

Labex DEVweCAN

ARSEP Foundation

ARC Foundation

Fondation pour la Recherche Médicale

Publisher

Rockefeller University Press

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