Multidimensional profiling of human T cells reveals high CD38 expression, marking recent thymic emigrants and age-related naive T cell remodeling
Bohacova, Pavla; Terekhova, Marina; Tsurinov, Petr; Mullins, Riley; Husarcikova, Kamila; Shchukina, Irina; Antonova, Alina Ulezko; Echalar, Barbora; Kossl, Jan; Saidu, Adam; Francis, Thomas; Mannie, Chelsea; Arthur, Laura; Harridge, Stephen D R; Kreisel, Daniel; Mudd, Philip A; Taylor, Angela M; McNamara, Coleen A; Cella, Marina; Puram, Sidharth V; van den Broek, Theo; van Wijk, Femke; Eghtesady, Pirooz; Artyomov, Maxim N
(2024) Immunity, volume 57, issue 10, pp. 2362 - 2379.e10
(Article)
Abstract
Thymic involution is a key factor in human immune aging, leading to reduced thymic output and a decline in recent thymic emigrant (RTE) naive T cells in circulation. Currently, the precise definition of human RTEs and their corresponding cell surface markers lacks clarity. Analysis of single-cell RNA-seq/ATAC-seq data distinguished RTEs
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by the expression of SOX4, IKZF2, and TOX and CD38 protein, whereby surface CD38 hi expression universally identified CD8 + and CD4 + RTEs. We further determined the dynamics of RTEs and mature cells in a cohort of 158 individuals, including age-associated transcriptional reprogramming and shifts in cytokine production. Spectral cytometry profiling revealed two axes of aging common to naive CD8 + and CD4 + T cells: (1) a decrease in CD38 ++ cells (RTEs) and (2) an increase in CXCR3 hi cells. Identification of RTEs enables direct assessment of thymic health. Furthermore, resolving the dynamics of naive T cell remodeling yields insight into vaccination and infection responsiveness throughout aging.
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Keywords: PBMC, aging, human, naive T cells, recent thymic emigrants, Infectious Diseases, Immunology and Allergy, Immunology
ISSN: 1074-7613
Publisher: Cell Press
Note: Publisher Copyright: © 2024 The Author(s)
(Peer reviewed)