Cytomegalovirus mediates expansion of IL-15–responsive innate-memory cells with SIV killing function
Gema Méndez-Lagares, … , Peter A. Barry, Dennis J. Hartigan-O’Connor
Gema Méndez-Lagares, … , Peter A. Barry, Dennis J. Hartigan-O’Connor
Published June 21, 2021
Citation Information: J Clin Invest. 2021;131(15):e148542. https://doi.org/10.1172/JCI148542.
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Research Article Immunology Infectious disease

Cytomegalovirus mediates expansion of IL-15–responsive innate-memory cells with SIV killing function

Abstract

Interindividual immune variability is driven predominantly by environmental factors, including exposure to chronic infectious agents such as cytomegalovirus (CMV). We investigated the effects of rhesus CMV (RhCMV) on composition and function of the immune system in young macaques. Within months of infection, RhCMV was associated with impressive changes in antigen presenting cells, T cells, and NK cells—and marked expansion of innate-memory CD8+ T cells. These cells express high levels of NKG2A/C and the IL-2 and IL-15 receptor beta chain, CD122. IL-15 was sufficient to drive differentiation of the cells in vitro and in vivo. Expanded NKG2A/C+CD122+CD8+ T cells in RhCMV-infected macaques, but not their NKG2-negative counterparts, were endowed with cytotoxicity against class I–deficient K562 targets and prompt IFN-γ production in response to stimulation with IL-12 and IL-18. Because RhCMV clone 68-1 forms the viral backbone of RhCMV-vectored SIV vaccines, we also investigated immune changes following administration of RhCMV 68-1–vectored SIV vaccines. These vaccines led to impressive expansion of NKG2A/C+CD8+ T cells with capacity to inhibit SIV replication ex vivo. Thus, CMV infection and CMV-vectored vaccination drive expansion of functional innate-like CD8 cells via host IL-15 production, suggesting that innate-memory expansion could be achieved by other vaccine platforms expressing IL-15.

Authors

Gema Méndez-Lagares, Ning Chin, W.L. William Chang, Jaewon Lee, Míriam Rosás-Umbert, Hung T. Kieu, David Merriam, Wenze Lu, Sungjin Kim, Lourdes Adamson, Christian Brander, Paul A. Luciw, Peter A. Barry, Dennis J. Hartigan-O’Connor

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Figure 7

NKG2A/C+CD8+ T cells have functional capacities similar to those of NK cells.

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NKG2A/C+CD8+ T cells have functional capacities similar to those of NK c...
(A) Cytolytic activity of sorted NKG2A/CCD8+ T cells, NKG2A/C+CD8+ T cells, or NK cells from 3 RhCMV+ rhesus macaques against Calcein AM-stained K562 at an E/T ratio of 5:1. (B) Resting PBMCs from 13 RhCMV+ rhesus macaques were incubated for 6 hours alone or with K562. IFN-γ and TNF-α expression were analyzed after gating on NKG2A/CCD8+ T cells, NKG2A/C+CD8+ T cells, or NK cells. Wilcoxon signed-rank tests were used to compare IFN-γ and TNF-α values. (C) Longitudinal representation of the percentage and absolute numbers of NKG2A/C+CD8+ T cells among lymphocytes before and after vaccination of 14 RhCMV rhesus macaques. Changes in numbers of NKG2A/C+CD8+ T cells with vaccination time were evaluated with Friedman tests. (D) Left: Representative FACS plots demonstrating viral outgrowth inhibition (assessed by intracellular Gag p27) observed when autologous, infected CD4+ T cells are cultured alone or in the presence of sorted NKG2A/CCD8+ T cells, NKG2A/C+CD8+ T cells, or NK cells at an E/T ratio of 1:1. Right: Percentage of viral inhibition. The assay was performed with spleen cells and PBMCs from necropsies, box plots show the median value, 25th and 75th quartiles, and the range of values, n = 3.