Allotransplantation Is Associated With Exacerbation of CD8 T-Cell Senescence: The Particular Place of the Innate CD8 T-Cell Component

Allotransplantation Is Associated With Exacerbation of CD8 T-Cell Senescence: The Particular Place of the Innate CD8 T-Cell Component

Immunosenescence is a physiological process that is associated with changes in the immune system, particularly among CD8 T-cells. Recent studies have hypothesized that senescent CD8 T-cells are produced with chronologic age by chronic stimulation, leading to the acquisition of hallmarks of innate-li...

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Main Authors: Lauren Daniel, Marion Tassery, Clara Lateur, Antoine Thierry, André Herbelin, Jean-Marc Gombert, Alice Barbarin
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-07-01
Series:Frontiers in Immunology
Subjects:
innate memory CD8(+) T-cells
NK-like T-cells
allotransplantation
senescence
immune memory
innateness gradient
Online Access:https://www.frontiersin.org/articles/10.3389/fimmu.2021.674016/full
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spelling doaj-dc98233988894258aa6db86be27698d52021-07-21T11:22:17ZengFrontiers Media S.A.Frontiers in Immunology1664-32242021-07-011210.3389/fimmu.2021.674016674016Allotransplantation Is Associated With Exacerbation of CD8 T-Cell Senescence: The Particular Place of the Innate CD8 T-Cell ComponentLauren Daniel0Lauren Daniel1Marion Tassery2Clara Lateur3Antoine Thierry4Antoine Thierry5Antoine Thierry6André Herbelin7André Herbelin8Jean-Marc Gombert9Jean-Marc Gombert10Jean-Marc Gombert11Alice Barbarin12Alice Barbarin13Inserm U1082, Poitiers, FranceUniversité de Poitiers, Poitiers, FranceService de Néphrologie, Hémodialyse et Transplantation, CHU de Poitiers, Poitiers, FranceService d’Immunologie et Inflammation, CHU de Poitiers, Poitiers, FranceInserm U1082, Poitiers, FranceUniversité de Poitiers, Poitiers, FranceService de Néphrologie, Hémodialyse et Transplantation, CHU de Poitiers, Poitiers, FranceInserm U1082, Poitiers, FranceUniversité de Poitiers, Poitiers, FranceInserm U1082, Poitiers, FranceUniversité de Poitiers, Poitiers, FranceService d’Immunologie et Inflammation, CHU de Poitiers, Poitiers, FranceInserm U1082, Poitiers, FranceCHU de Poitiers, Poitiers, FranceImmunosenescence is a physiological process that is associated with changes in the immune system, particularly among CD8 T-cells. Recent studies have hypothesized that senescent CD8 T-cells are produced with chronologic age by chronic stimulation, leading to the acquisition of hallmarks of innate-like T-cells. While conventional CD8 T-cells are quite well characterized, CD8 T-cells sharing features of NK cells and memory CD8 T-cells, are a newly described immune cell population. They can be distinguished from conventional CD8 T-cells by their combined expression of panKIR/NKG2A and Eomesodermin (E), a unique phenotype closely associated with IFN-γ production in response to innate stimulation. Here, we first provided new evidence in favor of the innate character of panKIR/NKG2A(+) E(+) CD8 T-cells in normal subjects, documenting their position at an intermediate level in the innateness gradient in terms of both innate IFN-γ production and diminished mitochondrial mass. We also revealed that CD8 E(+) panKIR/NKG2A(+) T-cells, hereafter referred to as Innate E(+) CD8 T-cells, exhibit increased senescent (CD27(-) CD28(-)) phenotype, compared to their conventional memory counterparts. Surprisingly, this phenomenon was not dependent on age. Given that inflammation related to chronic viral infection is known to induce NK-like marker expression and a senescence phenotype among CD8 T-cells, we hypothesized that innate E(+) CD8 T-cells will be preferentially associated with exacerbated cellular senescence in response to chronic alloantigen exposure or CMV infection. Accordingly, in a pilot cohort of stable kidney allotransplant recipients, we observed an increased frequency of the Innate E(+) CD8 T-cell subset, together with an exacerbated senescent phenotype. Importantly, this phenotype cannot be explained by age alone, in clear contrast to their conventional memory counterparts. The senescent phenotype in CD8 T-cells was further increased in cytomegalovirus (CMV) positive serology transplant recipients, suggesting that transplantation and CMV, rather than aging by itself, may promote an exacerbated senescent phenotype of innate CD8 T-cells. In conclusion, we proposed that kidney transplantation, via the setting of inflammatory stimuli of alloantigen exposure and CMV infection, may exogenously age the CD8 T-cell compartment, especially its innate component. The physiopathological consequences of this change in the immune system remain to be elucidated.https://www.frontiersin.org/articles/10.3389/fimmu.2021.674016/fullinnate memory CD8(+) T-cellsNK-like T-cellsallotransplantationsenescenceimmune memoryinnateness gradient
collection DOAJ
language English
format Article
sources DOAJ
author Lauren Daniel
Lauren Daniel
Marion Tassery
Clara Lateur
Antoine Thierry
Antoine Thierry
Antoine Thierry
André Herbelin
André Herbelin
Jean-Marc Gombert
Jean-Marc Gombert
Jean-Marc Gombert
Alice Barbarin
Alice Barbarin
spellingShingle Lauren Daniel
Lauren Daniel
Marion Tassery
Clara Lateur
Antoine Thierry
Antoine Thierry
Antoine Thierry
André Herbelin
André Herbelin
Jean-Marc Gombert
Jean-Marc Gombert
Jean-Marc Gombert
Alice Barbarin
Alice Barbarin
Allotransplantation Is Associated With Exacerbation of CD8 T-Cell Senescence: The Particular Place of the Innate CD8 T-Cell Component
Frontiers in Immunology
innate memory CD8(+) T-cells
NK-like T-cells
allotransplantation
senescence
immune memory
innateness gradient
author_facet Lauren Daniel
Lauren Daniel
Marion Tassery
Clara Lateur
Antoine Thierry
Antoine Thierry
Antoine Thierry
André Herbelin
André Herbelin
Jean-Marc Gombert
Jean-Marc Gombert
Jean-Marc Gombert
Alice Barbarin
Alice Barbarin
author_sort Lauren Daniel
title Allotransplantation Is Associated With Exacerbation of CD8 T-Cell Senescence: The Particular Place of the Innate CD8 T-Cell Component
title_short Allotransplantation Is Associated With Exacerbation of CD8 T-Cell Senescence: The Particular Place of the Innate CD8 T-Cell Component
title_full Allotransplantation Is Associated With Exacerbation of CD8 T-Cell Senescence: The Particular Place of the Innate CD8 T-Cell Component
title_fullStr Allotransplantation Is Associated With Exacerbation of CD8 T-Cell Senescence: The Particular Place of the Innate CD8 T-Cell Component
title_full_unstemmed Allotransplantation Is Associated With Exacerbation of CD8 T-Cell Senescence: The Particular Place of the Innate CD8 T-Cell Component
title_sort allotransplantation is associated with exacerbation of cd8 t-cell senescence: the particular place of the innate cd8 t-cell component
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2021-07-01
description Immunosenescence is a physiological process that is associated with changes in the immune system, particularly among CD8 T-cells. Recent studies have hypothesized that senescent CD8 T-cells are produced with chronologic age by chronic stimulation, leading to the acquisition of hallmarks of innate-like T-cells. While conventional CD8 T-cells are quite well characterized, CD8 T-cells sharing features of NK cells and memory CD8 T-cells, are a newly described immune cell population. They can be distinguished from conventional CD8 T-cells by their combined expression of panKIR/NKG2A and Eomesodermin (E), a unique phenotype closely associated with IFN-γ production in response to innate stimulation. Here, we first provided new evidence in favor of the innate character of panKIR/NKG2A(+) E(+) CD8 T-cells in normal subjects, documenting their position at an intermediate level in the innateness gradient in terms of both innate IFN-γ production and diminished mitochondrial mass. We also revealed that CD8 E(+) panKIR/NKG2A(+) T-cells, hereafter referred to as Innate E(+) CD8 T-cells, exhibit increased senescent (CD27(-) CD28(-)) phenotype, compared to their conventional memory counterparts. Surprisingly, this phenomenon was not dependent on age. Given that inflammation related to chronic viral infection is known to induce NK-like marker expression and a senescence phenotype among CD8 T-cells, we hypothesized that innate E(+) CD8 T-cells will be preferentially associated with exacerbated cellular senescence in response to chronic alloantigen exposure or CMV infection. Accordingly, in a pilot cohort of stable kidney allotransplant recipients, we observed an increased frequency of the Innate E(+) CD8 T-cell subset, together with an exacerbated senescent phenotype. Importantly, this phenotype cannot be explained by age alone, in clear contrast to their conventional memory counterparts. The senescent phenotype in CD8 T-cells was further increased in cytomegalovirus (CMV) positive serology transplant recipients, suggesting that transplantation and CMV, rather than aging by itself, may promote an exacerbated senescent phenotype of innate CD8 T-cells. In conclusion, we proposed that kidney transplantation, via the setting of inflammatory stimuli of alloantigen exposure and CMV infection, may exogenously age the CD8 T-cell compartment, especially its innate component. The physiopathological consequences of this change in the immune system remain to be elucidated.
topic innate memory CD8(+) T-cells
NK-like T-cells
allotransplantation
senescence
immune memory
innateness gradient
url https://www.frontiersin.org/articles/10.3389/fimmu.2021.674016/full
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