Litcius/Paper detail

Persistence of self-reactive CD8+ T cells in the CNS requires TOX-dependent chromatin remodeling

Nicolas Pagé, Sylvain Lemeille, Ilena Vincenti, Bogna Klimek, Alexandre Mariotte, Ingrid Wagner, Giovanni Di Liberto, Jonathan Kaye, Doron Merkler

2021Nature Communications36 citationsDOIOpen Access PDF

Abstract

Abstract Self-reactive CD8 + T cells are important mediators of progressive tissue damage in autoimmune diseases, but the molecular program underlying these cells’ functional adaptation is unclear. Here we characterize the transcriptional and epigenetic landscape of self-reactive CD8 + T cells in a mouse model of protracted central nervous system (CNS) autoimmunity and compare it to populations of CNS-resident memory CD8 + T cells emerging from acute viral infection. We find that autoimmune CD8 + T cells persisting at sites of self-antigen exhibit characteristic transcriptional regulation together with distinct epigenetic remodeling. This self-reactive CD8 + T cell fate depends on the transcriptional regulation by the DNA-binding HMG-box protein TOX which remodels more than 400 genomic regions including loci such as Tcf7 , which is central to stemness of CD8 + T cells. Continuous exposure to CNS self-antigen sustains TOX levels in self-reactive CD8 + T cells, whereas genetic ablation of TOX in CD8 + T cells results in shortened persistence of self-reactive CD8 + T cells in the inflamed CNS. Our study establishes and characterizes the genetic differentiation program enabling chronic T cell-driven immunopathology in CNS autoimmunity.

Topics & Concepts

Cytotoxic T cellBiologyCD8AutoimmunityEpigeneticsImmunologyCell biologyChromatinT cellAntigenImmune systemGeneticsGeneIn vitroT-cell and B-cell ImmunologyImmunotherapy and Immune ResponsesImmune Cell Function and Interaction