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Replicative history marks transcriptional and functional disparity in the CD8 + T cell memory pool.

Authors :
Bresser, Kaspar
Kok, Lianne
Swain, Arpit C
King, Lisa A
Jacobs, Laura
Weber, Tom S
Perié, Leïla
Duffy, Ken R
de Boer, Rob J
Scheeren, Ferenc A
Schumacher, Ton N
Bresser, Kaspar
Kok, Lianne
Swain, Arpit C
King, Lisa A
Jacobs, Laura
Weber, Tom S
Perié, Leïla
Duffy, Ken R
de Boer, Rob J
Scheeren, Ferenc A
Schumacher, Ton N
Source :
Nature Immunology vol.23 (2022) nr.5 p.791-801 [ISSN 1529-2908]
Publication Year :
2022

Abstract

Clonal expansion is a core aspect of T cell immunity. However, little is known with respect to the relationship between replicative history and the formation of distinct CD8 + memory T cell subgroups. To address this issue, we developed a genetic-tracing approach, termed the DivisionRecorder, that reports the extent of past proliferation of cell pools in vivo. Using this system to genetically 'record' the replicative history of different CD8 + T cell populations throughout a pathogen-specific immune response, we demonstrate that the central memory T (T CM) cell pool is marked by a higher number of prior divisions than the effector memory T cell pool, owing to the combination of strong proliferative activity during the acute immune response and selective proliferative activity after pathogen clearance. Furthermore, by combining DivisionRecorder analysis with single-cell transcriptomics and functional experiments, we show that replicative history identifies distinct cell pools within the T CM compartment. Specifically, we demonstrate that lowly divided T CM cells display enriched expression of stem-cell-associated genes, exist in a relatively quiescent state, and are superior in eliciting a proliferative recall response upon activation. These data provide the first evidence that a stem-cell-like memory T cell pool that reconstitutes the CD8 + T cell effector pool upon reinfection is marked by prior quiescence.

Details

Database :
OAIster
Journal :
Nature Immunology vol.23 (2022) nr.5 p.791-801 [ISSN 1529-2908]
Notes :
DOI: 10.1038/s41590-022-01171-9, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1445826569
Document Type :
Electronic Resource