Licensing delineates helper and effector NK cell subsets during viral infection
Anthony E. Zamora, Ethan G. Aguilar, Can M. Sungur, Lam T. Khuat, Cordelia Dunai, G. Raymond Lochhead, Juan Du, Claire Pomeroy, Bruce R. Blazar, Dan L. Longo, Jeffrey M. Venstrom, Nicole Baumgarth, William J. Murphy
Anthony E. Zamora, Ethan G. Aguilar, Can M. Sungur, Lam T. Khuat, Cordelia Dunai, G. Raymond Lochhead, Juan Du, Claire Pomeroy, Bruce R. Blazar, Dan L. Longo, Jeffrey M. Venstrom, Nicole Baumgarth, William J. Murphy
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Research Article Immunology Inflammation

Licensing delineates helper and effector NK cell subsets during viral infection

Abstract

Natural killer (NK) cells can be divided into phenotypic subsets based on expression of receptors that bind self-MHC-I molecules, a concept termed licensing or education. Here we show NK cell subsets with different migratory, effector, and immunoregulatory functions in dendritic cell and antigen (ag)-specific CD8+ T cell responses during influenza and murine cytomegalovirus infections. Shortly after infection, unlicensed NK cells localized in draining lymph nodes and produced GM-CSF, which correlated with the expansion and activation of dendritic cells, and resulted in greater and sustained ag-specific T cell responses. In contrast, licensed NK cells preferentially migrated to infected tissues and produced IFN-γ. Importantly, human NK cell subsets exhibited similar phenotypic characteristics. Collectively, our studies demonstrate a critical demarcation between the functions of licensed and unlicensed NK cell subsets, with the former functioning as the classical effector subset and the latter as the stimulator of adaptive immunity helping to prime immune responses.

Authors

Anthony E. Zamora, Ethan G. Aguilar, Can M. Sungur, Lam T. Khuat, Cordelia Dunai, G. Raymond Lochhead, Juan Du, Claire Pomeroy, Bruce R. Blazar, Dan L. Longo, Jeffrey M. Venstrom, Nicole Baumgarth, William J. Murphy

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Figure 1

Differential distribution of unlicensed and licensed NK cells following viral infection.

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Differential distribution of unlicensed and licensed NK cells following ...
(A) Frequency or (B) absolute number of licensed (CD3NK1.1+Ly49C/I+G2+A+, Ly49C/I+G2+A, Ly49C/I+G2-A+, or Ly49C/I+G2A; shades of red) and unlicensed (CD3NK1.1+Ly49C/IG2+A+, Ly49C/IG2+A, Ly49C/IG2A+, or Ly49C/IG2A; shades of blue) NK cell subsets in the mediastinal lymph nodes (mLNs) of C57BL/6 (H2b) mice on day 5 after APR8 infection. (C) Frequency or (D) absolute number of licensed (shades of red) and unlicensed (shades of blue) NK cell subsets in the lung of C57BL/6 (H2b) mice on day 5 after APR8 infection. (E) Frequency or (F) absolute number of licensed (shades of red) and unlicensed (shades of blue) NK cell subsets in the draining lymph nodes (DLNs) of C57BL/6 (H2b) mice on day 5 after MCMV infection. (G) Frequency or (H) absolute number of licensed (shades of red) and unlicensed (shades of blue) NK cell subsets in the liver of C57BL/6 (H2b) mice on day 5 after MCMV infection. (I) Fold change of the absolute numbers of licensed or unlicensed NK cells subsets from MCMV-infected livers on day 5 over the absolute number of licensed or unlicensed NK cells subsets from uninfected livers. n = 3 mice per group, representative of 2 to 3 experiments. (B, D, F, and H) Two-way ANOVA with Tukey post-test used to compare groups. (I) Unpaired 2-tailed Student’s t test used to compare groups. *P < 0.05, **P < 0.01, ***P < 0.001.