Origin and differentiation of human memory CD8 T cells after vaccination

Akondy, Rama; Fitch, Mark; Edupuganti, Srilatha; Yang, Shu; Kissick, Haydn; Li, Kelvin W.; Youngblood, Benjamin A.; Abdelsamed, Hossam; McGuire, Donald J.; Cohen, Kristen W.; Alexe, Gabriela; Nagar, Shashi; McCausland, Megan; Gupta, Satish Kumar; Tata, Pramila; Haining, W. Nicholas; McElrath, M. Juliana; Zhang, David; Hu, Bin; Greenleaf, William J.; Goronzy, Jörg J.; Mulligan, Mark J.; Hellerstein, Marc K.; Ahmed, Rafi

doi:10.1038/nature24633

Cited by 413 publications

(463 citation statements)

References 33 publications

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“…Further links between metabolism and epigenetic regulation of immune cells are beginning to emerge . Recent studies in mice and humans provide evidence that suggests memory T cells arise from effector T‐cell memory precursor pools and can retain an effector like epigenetic signature . This supports the concept that that memory T‐cell differentiation could be linked with epigenetic modifications at specific loci and that these cells are epigenetically poised to respond to secondary stimulation.…”

Section: Metabolic Signaling and Epigenetics In Memory T Cellsmentioning

confidence: 80%

The metabolic spectrum of memory T cells

O’Sullivan

2019

Immunol Cell Biol

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The development and persistence of memory T cells are integral to effective host defenses. Cell metabolism has a central role in the maintenance of these populations and engagement of specific metabolic pathways can influence T‐cell fate. Nuances in memory T‐cell metabolism are both context dependent, and exist, on a spectrum that complements and supports the activity of specific memory T‐cell subsets. This review explores how metabolic pathways and substrate choice can influence the phenotype and function of memory T cells.

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Section: Metabolic Signaling and Epigenetics In Memory T Cellsmentioning

confidence: 80%

The metabolic spectrum of memory T cells

O’Sullivan

2019

Immunol Cell Biol

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“…Since all these memory T cells share the same phenotypic markers, the lifespan of each of these types of memory cells remained unknown. Recently, Akondy et al reported on a long‐term deuterium‐labeling study to investigate the dynamics of cognate memory T cells in volunteers vaccinated against yellow fever (YF). The investigators were able to determine the deuterium enrichment in a relatively small CD8 + memory tetramer + T‐cell pool specific for this virus.…”

Section: Memory T‐cell Dynamics In Humans and Micementioning

confidence: 99%

“…A major new finding was that—despite the average lifespan of YV‐specific memory T cells of about 4 months—a large population of labeled memory cells persisted for years after vaccination, and that these persisting cells had a quiescent phenotype with features of stem‐cell‐like and effector‐like memory CD8 + T cells . The latter finding suggests that either CD8 + memory T cells slowly increase their longevity by becoming more quiescent over time, or that the population of antigen‐specific CD8 + memory T cells is kinetically heterogeneous, with the most quiescent subset becoming more predominant over time because they survive longer . Another major new finding was that YV‐specific memory cells had a very long intermitotic interval of 1/0.0015=666 days, that is, longer than their life expectancy.…”

Section: Memory T‐cell Dynamics In Humans and Micementioning

confidence: 99%

Current best estimates for the average lifespans of mouse and human leukocytes: reviewing two decades of deuterium‐labeling experiments

Borghans

Tesselaar

Boer³

2018

Immunological Reviews

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Deuterium is a non-toxic, stable isotope that can safely be administered to humans and mice to study their cellular turnover rates in vivo. It is incorporated into newly synthesized DNA strands during cell division, without interference with the kinetics of cells, and the accumulation and loss of deuterium in the DNA of sorted (sub-)populations of leukocytes can be used to estimate their cellular production rates and lifespans. In the past two decades, this powerful technology has been used to estimate the turnover rates of various types of leukocytes. Although it is the most reliable technique currently available to study leukocyte turnover, there are remarkable differences between the cellular turnover rates estimated by some of these studies. We have recently established that part of this variation is due to (a) difficulties in estimating deuterium availability in some deuterium-labeling studies, and (b) assumptions made by the mathematical models employed to fit the data. Being aware of these two problems, we here aim to approach a consensus on the life expectancies of different types of T cells, B cells, monocytes, and neutrophils in mice and men. We address remaining outstanding problems whenever appropriate and discuss for which immune subpopulations we currently have too little information to draw firm conclusions about their turnover.

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“…4 Although long-lasting debates have been focused on the identity of memory precursors and the differentiation path of memory T cells, 5 recent works have provided solid epigenetic evidence that virus-specific memory T cells transit through an effector stage, not directly derive from naïve cells in both mouse and human. 6,7 …”

Section: Introductionmentioning

confidence: 99%

Tissue-Specific Control of Tissue-Resident Memory T Cells

Liu

Zhang

2018

Crit Rev Immunol

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Tissue-resident memory T (TRM) cells have emerged to be a major component of T cell biology. Recent investigations have greatly advanced our understanding of TRMs. Common features have been discovered to distinguish memory T cells residing in various mucosal and non-mucosal tissues from their circulating counterparts. Given that most organs and tissues contain unique microenvironment, local signal-induced tissue-specific features are tightly associated with the differentiation, homeostasis and protective functions of TRMs. We will discuss the recent advances in TRM field with a special emphasis on the interaction between local signals and TRM cells in the context of individual tissue environment.

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Origin and differentiation of human memory CD8 T cells after vaccination

Cited by 413 publications

References 33 publications

The metabolic spectrum of memory T cells

The metabolic spectrum of memory T cells

Current best estimates for the average lifespans of mouse and human leukocytes: reviewing two decades of deuterium‐labeling experiments

Tissue-Specific Control of Tissue-Resident Memory T Cells

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