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Memory CD8 T Cells Generated by Cytomegalovirus Vaccine Vector Expressing NKG2D Ligand Have Effector-Like Phenotype and Distinct Functional Features

Viral vectors have emerged as a promising alternative to classical vaccines due to their great potential for induction of a potent cellular and humoral immunity. Cytomegalovirus (CMV) is an attractive vaccine vector due to its large genome with many non-essential immunoregulatory genes that can be e...

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Autores principales: Šustić, Marko, Cokarić Brdovčak, Maja, Lisnić, Berislav, Materljan, Jelena, Juranić Lisnić, Vanda, Rožmanić, Carmen, Indenbirken, Daniela, Hiršl, Lea, Busch, Dirk H., Brizić, Ilija, Krmpotić, Astrid, Jonjić, Stipan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8218728/
https://www.ncbi.nlm.nih.gov/pubmed/34168650
http://dx.doi.org/10.3389/fimmu.2021.681380
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author Šustić, Marko
Cokarić Brdovčak, Maja
Lisnić, Berislav
Materljan, Jelena
Juranić Lisnić, Vanda
Rožmanić, Carmen
Indenbirken, Daniela
Hiršl, Lea
Busch, Dirk H.
Brizić, Ilija
Krmpotić, Astrid
Jonjić, Stipan
author_facet Šustić, Marko
Cokarić Brdovčak, Maja
Lisnić, Berislav
Materljan, Jelena
Juranić Lisnić, Vanda
Rožmanić, Carmen
Indenbirken, Daniela
Hiršl, Lea
Busch, Dirk H.
Brizić, Ilija
Krmpotić, Astrid
Jonjić, Stipan
author_sort Šustić, Marko
collection PubMed
description Viral vectors have emerged as a promising alternative to classical vaccines due to their great potential for induction of a potent cellular and humoral immunity. Cytomegalovirus (CMV) is an attractive vaccine vector due to its large genome with many non-essential immunoregulatory genes that can be easily manipulated to modify the immune response. CMV generates a strong antigen-specific CD8 T cell response with a gradual accumulation of these cells in the process called memory inflation. In our previous work, we have constructed a mouse CMV vector expressing NKG2D ligand RAE-1γ in place of its viral inhibitor m152 (RAE-1γMCMV), which proved to be highly attenuated in vivo. Despite attenuation, RAE-1γMCMV induced a substantially stronger CD8 T cell response to vectored antigen than the control vector and provided superior protection against bacterial and tumor challenge. In the present study, we confirmed the enhanced protective capacity of RAE-1γMCMV as a tumor vaccine vector and determined the phenotypical and functional characteristics of memory CD8 T cells induced by the RAE-1γ expressing MCMV. RNAseq data revealed higher transcription of numerous genes associated with effector-like CD8 T cell phenotype in RAE-1γMCMV immunized mice. CD8 T cells primed with RAE-1γMCMV were enriched in TCF1 negative population, with higher expression of KLRG1 and lower expression of CD127, CD27, and Eomes. These phenotypical differences were associated with distinct functional features as cells primed with RAE-1γMCMV showed inferior cytokine-producing abilities but comparable cytotoxic potential. After adoptive transfer into naive hosts, OT-1 cells induced with both RAE-1γMCMV and the control vector were equally efficient in rejecting established tumors, suggesting the context of latent infection and cell numbers as important determinants of enhanced anti-tumor response following RAE-1γMCMV vaccination. Overall, our results shed new light on the phenotypical and functional distinctness of memory CD8 T cells induced with CMV vector expressing cellular ligand for the NKG2D receptor.
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spelling pubmed-82187282021-06-23 Memory CD8 T Cells Generated by Cytomegalovirus Vaccine Vector Expressing NKG2D Ligand Have Effector-Like Phenotype and Distinct Functional Features Šustić, Marko Cokarić Brdovčak, Maja Lisnić, Berislav Materljan, Jelena Juranić Lisnić, Vanda Rožmanić, Carmen Indenbirken, Daniela Hiršl, Lea Busch, Dirk H. Brizić, Ilija Krmpotić, Astrid Jonjić, Stipan Front Immunol Immunology Viral vectors have emerged as a promising alternative to classical vaccines due to their great potential for induction of a potent cellular and humoral immunity. Cytomegalovirus (CMV) is an attractive vaccine vector due to its large genome with many non-essential immunoregulatory genes that can be easily manipulated to modify the immune response. CMV generates a strong antigen-specific CD8 T cell response with a gradual accumulation of these cells in the process called memory inflation. In our previous work, we have constructed a mouse CMV vector expressing NKG2D ligand RAE-1γ in place of its viral inhibitor m152 (RAE-1γMCMV), which proved to be highly attenuated in vivo. Despite attenuation, RAE-1γMCMV induced a substantially stronger CD8 T cell response to vectored antigen than the control vector and provided superior protection against bacterial and tumor challenge. In the present study, we confirmed the enhanced protective capacity of RAE-1γMCMV as a tumor vaccine vector and determined the phenotypical and functional characteristics of memory CD8 T cells induced by the RAE-1γ expressing MCMV. RNAseq data revealed higher transcription of numerous genes associated with effector-like CD8 T cell phenotype in RAE-1γMCMV immunized mice. CD8 T cells primed with RAE-1γMCMV were enriched in TCF1 negative population, with higher expression of KLRG1 and lower expression of CD127, CD27, and Eomes. These phenotypical differences were associated with distinct functional features as cells primed with RAE-1γMCMV showed inferior cytokine-producing abilities but comparable cytotoxic potential. After adoptive transfer into naive hosts, OT-1 cells induced with both RAE-1γMCMV and the control vector were equally efficient in rejecting established tumors, suggesting the context of latent infection and cell numbers as important determinants of enhanced anti-tumor response following RAE-1γMCMV vaccination. Overall, our results shed new light on the phenotypical and functional distinctness of memory CD8 T cells induced with CMV vector expressing cellular ligand for the NKG2D receptor. Frontiers Media S.A. 2021-06-03 /pmc/articles/PMC8218728/ /pubmed/34168650 http://dx.doi.org/10.3389/fimmu.2021.681380 Text en Copyright © 2021 Šustić, Cokarić Brdovčak, Lisnić, Materljan, Juranić Lisnić, Rožmanić, Indenbirken, Hiršl, Busch, Brizić, Krmpotić and Jonjić 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
Šustić, Marko
Cokarić Brdovčak, Maja
Lisnić, Berislav
Materljan, Jelena
Juranić Lisnić, Vanda
Rožmanić, Carmen
Indenbirken, Daniela
Hiršl, Lea
Busch, Dirk H.
Brizić, Ilija
Krmpotić, Astrid
Jonjić, Stipan
Memory CD8 T Cells Generated by Cytomegalovirus Vaccine Vector Expressing NKG2D Ligand Have Effector-Like Phenotype and Distinct Functional Features
title Memory CD8 T Cells Generated by Cytomegalovirus Vaccine Vector Expressing NKG2D Ligand Have Effector-Like Phenotype and Distinct Functional Features
title_full Memory CD8 T Cells Generated by Cytomegalovirus Vaccine Vector Expressing NKG2D Ligand Have Effector-Like Phenotype and Distinct Functional Features
title_fullStr Memory CD8 T Cells Generated by Cytomegalovirus Vaccine Vector Expressing NKG2D Ligand Have Effector-Like Phenotype and Distinct Functional Features
title_full_unstemmed Memory CD8 T Cells Generated by Cytomegalovirus Vaccine Vector Expressing NKG2D Ligand Have Effector-Like Phenotype and Distinct Functional Features
title_short Memory CD8 T Cells Generated by Cytomegalovirus Vaccine Vector Expressing NKG2D Ligand Have Effector-Like Phenotype and Distinct Functional Features
title_sort memory cd8 t cells generated by cytomegalovirus vaccine vector expressing nkg2d ligand have effector-like phenotype and distinct functional features
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8218728/
https://www.ncbi.nlm.nih.gov/pubmed/34168650
http://dx.doi.org/10.3389/fimmu.2021.681380
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