Publication

Acquired Transcriptional Programming in Functional and Exhausted Virus-specific CD8 T Cells

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Last modified
  • 02/20/2025
Type of Material
Authors
    Benjamin Alan Youngblood, Emory UniversityE. John Wherry, University of PennsylvaniaRafi Ahmed, Emory University
Language
  • English
Date
  • 2012-01
Publisher
  • Lippincott, Williams & Wilkins
Publication Version
Copyright Statement
  • © 2012, © 2012 Lippincott Williams
Final Published Version (URL)
Title of Journal or Parent Work
ISSN
  • 1746-630X
Volume
  • 7
Issue
  • 1
Start Page
  • 50
End Page
  • 57
Grant/Funding Information
  • E.J. Wherry is supported by the National Institutes of Health (AI071309, AI083022, AI095608, AI078897, AI082630, and HHSN266200500030C)
  • B. Youngblood is supported by the American Cancer Society (PF-09-134-01-MPC)
  • R. Ahmed is supported by the National Institutes of Health (P01 AI080192-01, R01 AI030048-20)
Abstract
  • Purpose of Review Failure to control viral infections such as HIV, results in TCR and inhibitory receptor driven exhaustion of antigen-specific T cells. Persistent signaling by these receptors during chronic viral infection sculpts the transcriptional regulatory programs of virus-specific T cells. The resulting gene expression profile is tailored to temper the potentially damaging effector functions of cytotoxic T cells and adapt them to an antigen and inflammation rich environment. Here we review recent studies investigating mechanisms of transcriptional regulation of effector, functional memory, and exhausted T cell functions during acute versus chronic infections. Recent Findings Patterns of gene expression in virus-specific CD8 T cells are a result of a combination of pro and inhibitory signals from antigen presentation (TCR-mediated) and co-inhibitory receptor ligation (PD-1, 2B4). Further, memory-specific transcriptional regulation of 2B4 expression and signaling impose a self-limiting secondary effector response to a prolonged viral infection. Additionally, differentiation of functional memory CD8 T cells is coupled to acquisition of a repressive epigenetic program for PD-1 expression. However, chronic infection provides a signal which blocks the acquisition of these epigenetic modifications reinforcing the suppression of CTL functions in exhausted cells. Summary Current findings suggest that the mechanism(s) that delineate functional memory versus exhaustion are coupled to acquisition of transcriptional programs at the effector stage of differentiation, reinforced by cessation or persistence of TCR signaling.
Author Notes
  • *Address correspondence and reprint requests to Dr. Ben Youngblood, Emory Vaccine Center 954 Gatewood Road, Atlanta, GA 30329. byoungb@emory.edu, Phone: (404) 727-4700
Keywords
Research Categories
  • Health Sciences, Immunology
  • Biology, Microbiology

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