KDM6B-dependent chromatin remodelling underpins effective virus-specific CD8+ T cell differentiation

Author:

Li Jasmine,Hardy Kristine,Olshansky Moshe,Barugahare Adele,Gearing Linden J.,Prier Julia E.,Sng Xavier Y.X.,Thai Nguyen Michelle Ly,Piovesan Dana,Russ Brendan,La Gruta Nicole L.,Hertzog Paul J.,Rao Sudha,Turner Stephen J.ORCID

Abstract

SUMMARYNaive CD8+ T cell activation results in an autonomous program of cellular proliferation and differentiation. However, the mechanisms that underpin this process are unclear. Here we profiled genome-wide changes in chromatin accessibility, gene transcription and the deposition of a key chromatin modification (H3K27me3) early after naive CD8+ T cell activation. Rapid upregulation of the histone demethylase, KDM6B, prior to first cell division was required for initiating H3K27me3 removal at genes essential for subsequent T cell differentiation and proliferation. Inhibition of KDM6B-dependent H3K27me3 demethylation limited the magnitude of an effective primary virus-specific CD8+ T cell response and the formation of memory CD8+ T cell populations. Accordingly, we define the early spatio-temporal events underpinning early lineage-specific epigenetic reprogramming that is necessary for autonomous CD8+ T cell proliferation and differentiation.

Publisher

Cold Spring Harbor Laboratory

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