Detailed phenotypic and functional characterization of CMV-associated adaptive NK cells in rhesus macaques

Previous research on adaptive NK cells in rhesus macaques suffered from the lack of specific antibodies to differentiate between inhibitory CD94/NKG2A and stimulatory CD94/NKG2C heterodimeric receptors. Recently we reported an expansion of NKG2C receptor-encoding genes in rhesus macaques, but their...

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Autores principales: Hasan, Mohammad Zahidul, Höltermann, Charlotte, Petersen, Beatrix, Schrod, Annette, Mätz-Rensing, Kerstin, Kaul, Artur, Salinas, Gabriela, Dressel, Ralf, Walter, Lutz
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9742600/
https://www.ncbi.nlm.nih.gov/pubmed/36518759
http://dx.doi.org/10.3389/fimmu.2022.1028788
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author Hasan, Mohammad Zahidul
Höltermann, Charlotte
Petersen, Beatrix
Schrod, Annette
Mätz-Rensing, Kerstin
Kaul, Artur
Salinas, Gabriela
Dressel, Ralf
Walter, Lutz
author_facet Hasan, Mohammad Zahidul
Höltermann, Charlotte
Petersen, Beatrix
Schrod, Annette
Mätz-Rensing, Kerstin
Kaul, Artur
Salinas, Gabriela
Dressel, Ralf
Walter, Lutz
author_sort Hasan, Mohammad Zahidul
collection PubMed
description Previous research on adaptive NK cells in rhesus macaques suffered from the lack of specific antibodies to differentiate between inhibitory CD94/NKG2A and stimulatory CD94/NKG2C heterodimeric receptors. Recently we reported an expansion of NKG2C receptor-encoding genes in rhesus macaques, but their expression and functional role on primary NK cells remained unknown due to this deficit. Thus, we established monoclonal antibodies 4A8 and 7B1 which show identical specificities and bind to both NKG2C-1 and NKG2C-2 but neither react with NKG2C-3 nor NKG2A on transfected cells. Using a combination of 4A8 and Z199 antibodies in multicolor flow cytometry we detected broad expression (4-73%) of NKG2C-1 and/or NKG2C-2 (NKG2C-1/2) on primary NK cells in rhesus macaques from our breeding colony. Stratifying our data to CMV-positive and CMV-negative animals, we noticed a higher proportion (23-73%) of primary NK cells expressing NKG2C-1/2 in CMV+ as compared to CMV- macaques (4-5%). These NKG2C-1/2-positive NK cells in CMV+ macaques are characterized by lower expression of IL12RB2, ZBTB16, SH2D1B, but not FCER1G, as well as high expression of IFNG, indicating that antibody 4A8 detects CMV-associated adaptive NK cells. Single cell RNA seq data of 4A8-positive NK cells from a rhCMV-positive macaque demonstrated that a high proportion of these adaptive NK cells transcribe in addition to NKG2C-1 and NKG2C-2 also NKG2C-3, but interestingly NKG2A as well. Remarkably, in comparison to NKG2A, NKG2C-1 and in particular NKG2C-2 bind Mamu-E with higher avidity. Primary NK cells exposed to Mamu-E-expressing target cells displayed strong degranulation as well as IFN-gamma expression of 4A8+ adaptive NK cells from rhCMV+ animals. Thus, despite co-expression of inhibitory and stimulatory CD94/NKG2 receptors the higher number of different stimulatory NKG2C receptors and their higher binding avidity to Mamu-E outreach inhibitory signaling via NKG2A. These data demonstrate the evolutionary conservation of the CMV-driven development of NKG2C-positive adaptive NK cells with particular molecular signatures in primates and with changes in gene copy numbers and ligand-binding strength of NKG2C isotypes. Thus, rhesus macaques represent a suitable and valuable nonhuman primate animal model to study the CMV-NKG2C liaison in vivo.
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spelling pubmed-97426002022-12-13 Detailed phenotypic and functional characterization of CMV-associated adaptive NK cells in rhesus macaques Hasan, Mohammad Zahidul Höltermann, Charlotte Petersen, Beatrix Schrod, Annette Mätz-Rensing, Kerstin Kaul, Artur Salinas, Gabriela Dressel, Ralf Walter, Lutz Front Immunol Immunology Previous research on adaptive NK cells in rhesus macaques suffered from the lack of specific antibodies to differentiate between inhibitory CD94/NKG2A and stimulatory CD94/NKG2C heterodimeric receptors. Recently we reported an expansion of NKG2C receptor-encoding genes in rhesus macaques, but their expression and functional role on primary NK cells remained unknown due to this deficit. Thus, we established monoclonal antibodies 4A8 and 7B1 which show identical specificities and bind to both NKG2C-1 and NKG2C-2 but neither react with NKG2C-3 nor NKG2A on transfected cells. Using a combination of 4A8 and Z199 antibodies in multicolor flow cytometry we detected broad expression (4-73%) of NKG2C-1 and/or NKG2C-2 (NKG2C-1/2) on primary NK cells in rhesus macaques from our breeding colony. Stratifying our data to CMV-positive and CMV-negative animals, we noticed a higher proportion (23-73%) of primary NK cells expressing NKG2C-1/2 in CMV+ as compared to CMV- macaques (4-5%). These NKG2C-1/2-positive NK cells in CMV+ macaques are characterized by lower expression of IL12RB2, ZBTB16, SH2D1B, but not FCER1G, as well as high expression of IFNG, indicating that antibody 4A8 detects CMV-associated adaptive NK cells. Single cell RNA seq data of 4A8-positive NK cells from a rhCMV-positive macaque demonstrated that a high proportion of these adaptive NK cells transcribe in addition to NKG2C-1 and NKG2C-2 also NKG2C-3, but interestingly NKG2A as well. Remarkably, in comparison to NKG2A, NKG2C-1 and in particular NKG2C-2 bind Mamu-E with higher avidity. Primary NK cells exposed to Mamu-E-expressing target cells displayed strong degranulation as well as IFN-gamma expression of 4A8+ adaptive NK cells from rhCMV+ animals. Thus, despite co-expression of inhibitory and stimulatory CD94/NKG2 receptors the higher number of different stimulatory NKG2C receptors and their higher binding avidity to Mamu-E outreach inhibitory signaling via NKG2A. These data demonstrate the evolutionary conservation of the CMV-driven development of NKG2C-positive adaptive NK cells with particular molecular signatures in primates and with changes in gene copy numbers and ligand-binding strength of NKG2C isotypes. Thus, rhesus macaques represent a suitable and valuable nonhuman primate animal model to study the CMV-NKG2C liaison in vivo. Frontiers Media S.A. 2022-11-25 /pmc/articles/PMC9742600/ /pubmed/36518759 http://dx.doi.org/10.3389/fimmu.2022.1028788 Text en Copyright © 2022 Hasan, Höltermann, Petersen, Schrod, Mätz-Rensing, Kaul, Salinas, Dressel and Walter https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Hasan, Mohammad Zahidul
Höltermann, Charlotte
Petersen, Beatrix
Schrod, Annette
Mätz-Rensing, Kerstin
Kaul, Artur
Salinas, Gabriela
Dressel, Ralf
Walter, Lutz
Detailed phenotypic and functional characterization of CMV-associated adaptive NK cells in rhesus macaques
title Detailed phenotypic and functional characterization of CMV-associated adaptive NK cells in rhesus macaques
title_full Detailed phenotypic and functional characterization of CMV-associated adaptive NK cells in rhesus macaques
title_fullStr Detailed phenotypic and functional characterization of CMV-associated adaptive NK cells in rhesus macaques
title_full_unstemmed Detailed phenotypic and functional characterization of CMV-associated adaptive NK cells in rhesus macaques
title_short Detailed phenotypic and functional characterization of CMV-associated adaptive NK cells in rhesus macaques
title_sort detailed phenotypic and functional characterization of cmv-associated adaptive nk cells in rhesus macaques
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9742600/
https://www.ncbi.nlm.nih.gov/pubmed/36518759
http://dx.doi.org/10.3389/fimmu.2022.1028788
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