| Literature DB >> 34644150 |
Vandana Kalia1,2, Yevgeniy Yuzefpolskiy2, Adithya Vegaraju2, Hanxi Xiao2, Florian Baumann3, Shashank Jatav4, Candice Church5, Martin Prlic6,7,8, Abhishek Jha4, Paul Nghiem5,9, Stanley Riddell9,10, Surojit Sarkar1,2,7.
Abstract
Inhibitory signaling in dysfunctional CD8 T cells through the programmed cell death 1 (PD-1) axis is well established in chronic viral infections and cancers. PD-1 is also transiently induced to high concentrations during priming of acute infections and immunizations, yet its impact on the development of long-lived antigen-independent T cell memory remains unclear. In addition to its expected role in restraining clonal effector expansion, here, we show that PD-1 expression on antigen-specific CD8 T cells is required for the development of a durable CD8 T cell memory pool after antigen clearance. Loss of T cell–specific PD-1 signaling led to increased contraction and a defect in antigen-independent renewal of memory CD8 T cells in response to homeostatic cytokine signals, thus resulting in attrition of the memory pool over time. Whereas exhausted CD8 T cells regain function after PD-1 checkpoint blockade during chronic viral infection, the preexisting pool of resting functional bystander memory CD8 T cells established in response to a previously administered immunogen decreased. Metabolically, PD-1 signals were necessary for regulating the critical balance of mTOR-dependent anabolic glycolysis and fatty acid oxidation programs to meet the bioenergetic needs of quiescent CD8 T cell memory. These results define PD-1 as a key metabolic regulator of protective T cell immunity. Furthermore, these results have potential clinical implications for preexisting CD8 T cell memory during PD-1 checkpoint blockade therapy.Entities:
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Year: 2021 PMID: 34644150 PMCID: PMC8896520 DOI: 10.1126/scitranslmed.aba6006
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956