CD4 T Help Promotes Influenza Virus-specific CD8 T Cell Memory by Limiting Metabolic Dysfunction

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2019 Feb 22

PMID 30787194

Citations 39

Authors

Jolie G Cullen

Hayley A McQuilten

Kylie M Quinn

Moshe Olshansky

Brendan E Russ

Alison Morey

Sanna Wei

Julia E Prier

Nicole L La Gruta

Peter C Doherty

Stephen J Turner

Affiliations

Soon will be listed here.

Abstract

There is continued interest in developing novel vaccine strategies that induce establish optimal CD8 cytotoxic T lymphocyte (CTL) memory for pathogens like the influenza A viruses (IAVs), where the recall of IAV-specific T cell immunity is able to protect against serologically distinct IAV infection. While it is well established that CD4 T cell help is required for optimal CTL responses and the establishment of memory, when and how CD4 T cell help contributes to determining the ideal memory phenotype remains unclear. We assessed the quality of IAV-specific CD8 T cell memory established in the presence or absence of a concurrent CD4 T cell response. We demonstrate that CD4 T cell help appears to be required at the initial priming phase of infection for the maintenance of IAV-specific CTL memory, with "unhelped" memory CTL exhibiting intrinsic dysfunction. High-throughput RNA-sequencing established that distinct transcriptional signatures characterize the helped vs. unhelped IAV-specific memory CTL phenotype, with the unhelped set showing a more "exhausted T cell" transcriptional profile. Moreover, we identify that unhelped memory CTLs exhibit defects in a variety of energetic pathways, leading to diminished spare respiratory capacity and diminished capacity to engage glycolysis upon reactivation. Hence, CD4 T help at the time of initial priming promotes molecular pathways that limit exhaustion by channeling metabolic processes essential for the rapid recall of memory CD8 T cells.

Citing Articles

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