Adding Help to an HLA-A*24:02 Tumor-Reactive γδTCR Increases Tumor Control

γδT cell receptors (γδTCRs) recognize a broad range of malignantly transformed cells in mainly a major histocompatibility complex (MHC)-independent manner, making them valuable additions to the engineered immune effector cell therapy that currently focuses primarily on αβTCRs and chimeric antigen re...

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Autores principales: Johanna, Inez, Hernández-López, Patricia, Heijhuurs, Sabine, Scheper, Wouter, Bongiovanni, Laura, de Bruin, Alain, Beringer, Dennis X., Oostvogels, Rimke, Straetemans, Trudy, Sebestyen, Zsolt, Kuball, Jürgen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8573335/
https://www.ncbi.nlm.nih.gov/pubmed/34759930
http://dx.doi.org/10.3389/fimmu.2021.752699
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author Johanna, Inez
Hernández-López, Patricia
Heijhuurs, Sabine
Scheper, Wouter
Bongiovanni, Laura
de Bruin, Alain
Beringer, Dennis X.
Oostvogels, Rimke
Straetemans, Trudy
Sebestyen, Zsolt
Kuball, Jürgen
author_facet Johanna, Inez
Hernández-López, Patricia
Heijhuurs, Sabine
Scheper, Wouter
Bongiovanni, Laura
de Bruin, Alain
Beringer, Dennis X.
Oostvogels, Rimke
Straetemans, Trudy
Sebestyen, Zsolt
Kuball, Jürgen
author_sort Johanna, Inez
collection PubMed
description γδT cell receptors (γδTCRs) recognize a broad range of malignantly transformed cells in mainly a major histocompatibility complex (MHC)-independent manner, making them valuable additions to the engineered immune effector cell therapy that currently focuses primarily on αβTCRs and chimeric antigen receptors (CARs). As an exception to the rule, we have previously identified a γδTCR, which exerts antitumor reactivity against HLA-A*24:02-expressing malignant cells, however without the need for defined HLA-restricted peptides, and without exhibiting any sign of off-target toxicity in humanized HLA-A*24:02 transgenic NSG (NSG-A24:02) mouse models. This particular tumor-HLA-A*24:02-specific Vγ5Vδ1TCR required CD8αα co-receptor for its tumor reactive capacity when introduced into αβT cells engineered to express a defined γδTCR (TEG), referred to as TEG011; thus, it was only active in CD8(+) TEG011. We subsequently explored the concept of additional redirection of CD4(+) T cells through co-expression of the human CD8α gene into CD4(+) and CD8(+) TEG011 cells, later referred as TEG011_CD8α. Adoptive transfer of TEG011_CD8α cells in humanized HLA-A*24:02 transgenic NSG (NSG-A24:02) mice injected with tumor HLA-A*24:02(+) cells showed superior tumor control in comparison to TEG011, and to mock control groups. The total percentage of mice with persisting TEG011_CD8α cells, as well as the total number of TEG011_CD8α cells per mice, was significantly improved over time, mainly due to a dominance of CD4(+)CD8(+) double-positive TEG011_CD8α, which resulted in higher total counts of functional T cells in spleen and bone marrow. We observed that tumor clearance in the bone marrow of TEG011_CD8α-treated mice associated with better human T cell infiltration, which was not observed in the TEG011-treated group. Overall, introduction of transgenic human CD8α receptor on TEG011 improves antitumor reactivity against HLA-A*24:02(+) tumor cells and further enhances in vivo tumor control.
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spelling pubmed-85733352021-11-09 Adding Help to an HLA-A*24:02 Tumor-Reactive γδTCR Increases Tumor Control Johanna, Inez Hernández-López, Patricia Heijhuurs, Sabine Scheper, Wouter Bongiovanni, Laura de Bruin, Alain Beringer, Dennis X. Oostvogels, Rimke Straetemans, Trudy Sebestyen, Zsolt Kuball, Jürgen Front Immunol Immunology γδT cell receptors (γδTCRs) recognize a broad range of malignantly transformed cells in mainly a major histocompatibility complex (MHC)-independent manner, making them valuable additions to the engineered immune effector cell therapy that currently focuses primarily on αβTCRs and chimeric antigen receptors (CARs). As an exception to the rule, we have previously identified a γδTCR, which exerts antitumor reactivity against HLA-A*24:02-expressing malignant cells, however without the need for defined HLA-restricted peptides, and without exhibiting any sign of off-target toxicity in humanized HLA-A*24:02 transgenic NSG (NSG-A24:02) mouse models. This particular tumor-HLA-A*24:02-specific Vγ5Vδ1TCR required CD8αα co-receptor for its tumor reactive capacity when introduced into αβT cells engineered to express a defined γδTCR (TEG), referred to as TEG011; thus, it was only active in CD8(+) TEG011. We subsequently explored the concept of additional redirection of CD4(+) T cells through co-expression of the human CD8α gene into CD4(+) and CD8(+) TEG011 cells, later referred as TEG011_CD8α. Adoptive transfer of TEG011_CD8α cells in humanized HLA-A*24:02 transgenic NSG (NSG-A24:02) mice injected with tumor HLA-A*24:02(+) cells showed superior tumor control in comparison to TEG011, and to mock control groups. The total percentage of mice with persisting TEG011_CD8α cells, as well as the total number of TEG011_CD8α cells per mice, was significantly improved over time, mainly due to a dominance of CD4(+)CD8(+) double-positive TEG011_CD8α, which resulted in higher total counts of functional T cells in spleen and bone marrow. We observed that tumor clearance in the bone marrow of TEG011_CD8α-treated mice associated with better human T cell infiltration, which was not observed in the TEG011-treated group. Overall, introduction of transgenic human CD8α receptor on TEG011 improves antitumor reactivity against HLA-A*24:02(+) tumor cells and further enhances in vivo tumor control. Frontiers Media S.A. 2021-10-25 /pmc/articles/PMC8573335/ /pubmed/34759930 http://dx.doi.org/10.3389/fimmu.2021.752699 Text en Copyright © 2021 Johanna, Hernández-López, Heijhuurs, Scheper, Bongiovanni, de Bruin, Beringer, Oostvogels, Straetemans, Sebestyen and Kuball 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
Johanna, Inez
Hernández-López, Patricia
Heijhuurs, Sabine
Scheper, Wouter
Bongiovanni, Laura
de Bruin, Alain
Beringer, Dennis X.
Oostvogels, Rimke
Straetemans, Trudy
Sebestyen, Zsolt
Kuball, Jürgen
Adding Help to an HLA-A*24:02 Tumor-Reactive γδTCR Increases Tumor Control
title Adding Help to an HLA-A*24:02 Tumor-Reactive γδTCR Increases Tumor Control
title_full Adding Help to an HLA-A*24:02 Tumor-Reactive γδTCR Increases Tumor Control
title_fullStr Adding Help to an HLA-A*24:02 Tumor-Reactive γδTCR Increases Tumor Control
title_full_unstemmed Adding Help to an HLA-A*24:02 Tumor-Reactive γδTCR Increases Tumor Control
title_short Adding Help to an HLA-A*24:02 Tumor-Reactive γδTCR Increases Tumor Control
title_sort adding help to an hla-a*24:02 tumor-reactive γδtcr increases tumor control
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8573335/
https://www.ncbi.nlm.nih.gov/pubmed/34759930
http://dx.doi.org/10.3389/fimmu.2021.752699
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