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Literature DB >> 27939672

Dynamic Changes in Chromatin Accessibility Occur in CD8⁺ T Cells Responding to Viral Infection.

James P Scott-Browne¹, Isaac F López-Moyado¹, Sara Trifari¹, Victor Wong¹, Lukas Chavez², Anjana Rao³, Renata M Pereira¹.

Abstract

In response to acute infection, naive CD8+ T cells expand, differentiate into effector cells, and then contract to a long-lived pool of memory cells after pathogen clearance. During chronic infections or in tumors, CD8+ T cells acquire an "exhausted" phenotype. Here we present genome-wide comparisons of chromatin accessibility and gene expression from endogenous CD8+ T cells responding to acute and chronic viral infection using ATAC-seq and RNA-seq techniques. Acquisition of effector, memory, or exhausted phenotypes was associated with stable changes in chromatin accessibility away from the naive T cell state. Regions differentially accessible between functional subsets in vivo were enriched for binding sites of transcription factors known to regulate these subsets, including E2A, BATF, IRF4, T-bet, and TCF1. Exhaustion-specific accessible regions were enriched for consensus binding sites for NFAT and Nr4a family members, indicating that chronic stimulation confers a unique accessibility profile on exhausted cells.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：
Chromatin

Year: 2016 PMID： 27939672 PMCID： PMC5214519 DOI： 10.1016/j.immuni.2016.10.028

Source DB: PubMed Journal: Immunity ISSN： 1074-7613 Impact factor: 31.745

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