Enhanced generation of influenza-specific tissue resident memory CD8 T cells in NK-depleted mice

Abstract Natural Killer (NK) cells are among the first effectors to directly contact influenza and influenza-infected cells and their activation affects not only their intrinsic functions, but also subsequent CD8+ T cell responses. We utilized a NK cell depletion model to interrogate the contributio...

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Main Authors: David L. Rose, Katie L. Reagin, Kimberly E. Oliva, S. Mark Tompkins, Kimberly D. Klonowski
Format: Article
Language:English
Published: Nature Publishing Group 2021-04-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-021-88268-7
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spelling doaj-4186236ee93440c690dfa446984e9c972021-05-02T11:31:27ZengNature Publishing GroupScientific Reports2045-23222021-04-0111111510.1038/s41598-021-88268-7Enhanced generation of influenza-specific tissue resident memory CD8 T cells in NK-depleted miceDavid L. Rose0Katie L. Reagin1Kimberly E. Oliva2S. Mark Tompkins3Kimberly D. Klonowski4Department of Shared Resources, Beckman Research Institute of the City of HopeDepartment of Biology, University of North Carolina at CharlotteDepartment of Cellular Biology, University of GeorgiaDepartment of Infectious Diseases, University of GeorgiaDepartment of Cellular Biology, University of GeorgiaAbstract Natural Killer (NK) cells are among the first effectors to directly contact influenza and influenza-infected cells and their activation affects not only their intrinsic functions, but also subsequent CD8+ T cell responses. We utilized a NK cell depletion model to interrogate the contribution of NK cells to the development of anti-influenza CD8+ T cell memory. NK cell ablation increased the number of influenza-specific memory CD8+ T cells in the respiratory tract and lung-draining lymph node. Interestingly, animals depleted of NK cells during primary influenza infection were protected as well as their NK-intact counterparts despite significantly fewer reactivated CD8+ T cells infiltrating the respiratory tract after lethal, heterosubtypic challenge. Instead, protection in NK-deficient animals seems to be conferred by rapid reactivation of an enlarged pool of lung tissue-resident (TRM) memory cells within two days post challenge. Further interrogation of how NK cell ablation enhances respiratory TRM indicated that TRM development is independent of global and NK cell derived IFN-γ. These data suggest that reduction in NK cell activation after vaccination with live, non-lethal influenza virus increases compartmentalized, broadly protective memory CD8+ T cell generation and decreases the risk of CD8+ T cell-mediated pathology following subsequent influenza infections.https://doi.org/10.1038/s41598-021-88268-7
collection DOAJ
language English
format Article
sources DOAJ
author David L. Rose
Katie L. Reagin
Kimberly E. Oliva
S. Mark Tompkins
Kimberly D. Klonowski
spellingShingle David L. Rose
Katie L. Reagin
Kimberly E. Oliva
S. Mark Tompkins
Kimberly D. Klonowski
Enhanced generation of influenza-specific tissue resident memory CD8 T cells in NK-depleted mice
Scientific Reports
author_facet David L. Rose
Katie L. Reagin
Kimberly E. Oliva
S. Mark Tompkins
Kimberly D. Klonowski
author_sort David L. Rose
title Enhanced generation of influenza-specific tissue resident memory CD8 T cells in NK-depleted mice
title_short Enhanced generation of influenza-specific tissue resident memory CD8 T cells in NK-depleted mice
title_full Enhanced generation of influenza-specific tissue resident memory CD8 T cells in NK-depleted mice
title_fullStr Enhanced generation of influenza-specific tissue resident memory CD8 T cells in NK-depleted mice
title_full_unstemmed Enhanced generation of influenza-specific tissue resident memory CD8 T cells in NK-depleted mice
title_sort enhanced generation of influenza-specific tissue resident memory cd8 t cells in nk-depleted mice
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2021-04-01
description Abstract Natural Killer (NK) cells are among the first effectors to directly contact influenza and influenza-infected cells and their activation affects not only their intrinsic functions, but also subsequent CD8+ T cell responses. We utilized a NK cell depletion model to interrogate the contribution of NK cells to the development of anti-influenza CD8+ T cell memory. NK cell ablation increased the number of influenza-specific memory CD8+ T cells in the respiratory tract and lung-draining lymph node. Interestingly, animals depleted of NK cells during primary influenza infection were protected as well as their NK-intact counterparts despite significantly fewer reactivated CD8+ T cells infiltrating the respiratory tract after lethal, heterosubtypic challenge. Instead, protection in NK-deficient animals seems to be conferred by rapid reactivation of an enlarged pool of lung tissue-resident (TRM) memory cells within two days post challenge. Further interrogation of how NK cell ablation enhances respiratory TRM indicated that TRM development is independent of global and NK cell derived IFN-γ. These data suggest that reduction in NK cell activation after vaccination with live, non-lethal influenza virus increases compartmentalized, broadly protective memory CD8+ T cell generation and decreases the risk of CD8+ T cell-mediated pathology following subsequent influenza infections.
url https://doi.org/10.1038/s41598-021-88268-7
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