CAR T Cells Targeting Membrane-Bound Hsp70 on Tumor Cells Mimic Hsp70-Primed NK Cells

Strategies to boost anti-tumor immunity are urgently needed to treat therapy-resistant late-stage cancers, including colorectal cancers (CRCs). Cytokine stimulation and genetic modifications with chimeric antigen receptors (CAR) represent promising strategies to more specifically redirect anti-tumor...

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Autores principales: Bashiri Dezfouli, Ali, Yazdi, Mina, Benmebarek, Mohamed-Reda, Schwab, Melissa, Michaelides, Stefanos, Miccichè, Arianna, Geerts, Dirk, Stangl, Stefan, Klapproth, Sarah, Wagner, Ernst, Kobold, Sebastian, Multhoff, Gabriele
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/PMC9198541/
https://www.ncbi.nlm.nih.gov/pubmed/35720311
http://dx.doi.org/10.3389/fimmu.2022.883694
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author Bashiri Dezfouli, Ali
Yazdi, Mina
Benmebarek, Mohamed-Reda
Schwab, Melissa
Michaelides, Stefanos
Miccichè, Arianna
Geerts, Dirk
Stangl, Stefan
Klapproth, Sarah
Wagner, Ernst
Kobold, Sebastian
Multhoff, Gabriele
author_facet Bashiri Dezfouli, Ali
Yazdi, Mina
Benmebarek, Mohamed-Reda
Schwab, Melissa
Michaelides, Stefanos
Miccichè, Arianna
Geerts, Dirk
Stangl, Stefan
Klapproth, Sarah
Wagner, Ernst
Kobold, Sebastian
Multhoff, Gabriele
author_sort Bashiri Dezfouli, Ali
collection PubMed
description Strategies to boost anti-tumor immunity are urgently needed to treat therapy-resistant late-stage cancers, including colorectal cancers (CRCs). Cytokine stimulation and genetic modifications with chimeric antigen receptors (CAR) represent promising strategies to more specifically redirect anti-tumor activities of effector cells like natural killer (NK) and T cells. However, these approaches are critically dependent on tumor-specific antigens while circumventing the suppressive power of the solid tumor microenvironment and avoiding off-tumor toxicities. Previously, we have shown that the stress-inducible heat shock protein 70 (Hsp70) is frequently and specifically expressed on the cell surface of many different, highly aggressive tumors but not normal tissues. We could take advantage of tumors expressing Hsp70 on their membrane (‘mHsp70’) to attract and engage NK cells after in vitro stimulation with the 14-mer Hsp70 peptide TKDNNLLGRFELSG (TKD) plus low dose interleukin (IL)-2. However, a potential limitation of activated primary NK cells after adoptive transfer is their comparably short life span. T cells are typically long-lived but do not recognize mHsp70 on tumor cells, even after stimulation with TKD/IL-2. To combine the advantages of mHsp70-specificity with longevity, we constructed a CAR having specificity for mHsp70 and retrovirally transduced it into primary T cells. Co-culture of anti-Hsp70 CAR-transduced T cells with mHsp70-positive tumor cells stimulates their functional responsiveness. Herein, we demonstrated that human CRCs with a high mHsp70 expression similarly attract TKD/IL-2 stimulated NK cells and anti-Hsp70 CAR T cells, triggering the release of their lytic effector protein granzyme B (GrB) and the pro-inflammatory cytokine interferon (IFN)-γ, after 4 and 24 hours, respectively. In sum, stimulated NK cells and anti-Hsp70 CAR T cells demonstrated comparable anti-tumor effects, albeit with somewhat differing kinetics. These findings, together with the fact that mHsp70 is expressed on a large variety of different cancer entities, highlight the potential of TKD/IL-2 pre-stimulated NK, as well as anti-Hsp70 CAR T cells to provide a promising direction in the field of targeted, cell-based immunotherapies which can address significant unmet clinical needs in a wide range of cancer settings.
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spelling pubmed-91985412022-06-16 CAR T Cells Targeting Membrane-Bound Hsp70 on Tumor Cells Mimic Hsp70-Primed NK Cells Bashiri Dezfouli, Ali Yazdi, Mina Benmebarek, Mohamed-Reda Schwab, Melissa Michaelides, Stefanos Miccichè, Arianna Geerts, Dirk Stangl, Stefan Klapproth, Sarah Wagner, Ernst Kobold, Sebastian Multhoff, Gabriele Front Immunol Immunology Strategies to boost anti-tumor immunity are urgently needed to treat therapy-resistant late-stage cancers, including colorectal cancers (CRCs). Cytokine stimulation and genetic modifications with chimeric antigen receptors (CAR) represent promising strategies to more specifically redirect anti-tumor activities of effector cells like natural killer (NK) and T cells. However, these approaches are critically dependent on tumor-specific antigens while circumventing the suppressive power of the solid tumor microenvironment and avoiding off-tumor toxicities. Previously, we have shown that the stress-inducible heat shock protein 70 (Hsp70) is frequently and specifically expressed on the cell surface of many different, highly aggressive tumors but not normal tissues. We could take advantage of tumors expressing Hsp70 on their membrane (‘mHsp70’) to attract and engage NK cells after in vitro stimulation with the 14-mer Hsp70 peptide TKDNNLLGRFELSG (TKD) plus low dose interleukin (IL)-2. However, a potential limitation of activated primary NK cells after adoptive transfer is their comparably short life span. T cells are typically long-lived but do not recognize mHsp70 on tumor cells, even after stimulation with TKD/IL-2. To combine the advantages of mHsp70-specificity with longevity, we constructed a CAR having specificity for mHsp70 and retrovirally transduced it into primary T cells. Co-culture of anti-Hsp70 CAR-transduced T cells with mHsp70-positive tumor cells stimulates their functional responsiveness. Herein, we demonstrated that human CRCs with a high mHsp70 expression similarly attract TKD/IL-2 stimulated NK cells and anti-Hsp70 CAR T cells, triggering the release of their lytic effector protein granzyme B (GrB) and the pro-inflammatory cytokine interferon (IFN)-γ, after 4 and 24 hours, respectively. In sum, stimulated NK cells and anti-Hsp70 CAR T cells demonstrated comparable anti-tumor effects, albeit with somewhat differing kinetics. These findings, together with the fact that mHsp70 is expressed on a large variety of different cancer entities, highlight the potential of TKD/IL-2 pre-stimulated NK, as well as anti-Hsp70 CAR T cells to provide a promising direction in the field of targeted, cell-based immunotherapies which can address significant unmet clinical needs in a wide range of cancer settings. Frontiers Media S.A. 2022-06-01 /pmc/articles/PMC9198541/ /pubmed/35720311 http://dx.doi.org/10.3389/fimmu.2022.883694 Text en Copyright © 2022 Bashiri Dezfouli, Yazdi, Benmebarek, Schwab, Michaelides, Miccichè, Geerts, Stangl, Klapproth, Wagner, Kobold and Multhoff 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
Bashiri Dezfouli, Ali
Yazdi, Mina
Benmebarek, Mohamed-Reda
Schwab, Melissa
Michaelides, Stefanos
Miccichè, Arianna
Geerts, Dirk
Stangl, Stefan
Klapproth, Sarah
Wagner, Ernst
Kobold, Sebastian
Multhoff, Gabriele
CAR T Cells Targeting Membrane-Bound Hsp70 on Tumor Cells Mimic Hsp70-Primed NK Cells
title CAR T Cells Targeting Membrane-Bound Hsp70 on Tumor Cells Mimic Hsp70-Primed NK Cells
title_full CAR T Cells Targeting Membrane-Bound Hsp70 on Tumor Cells Mimic Hsp70-Primed NK Cells
title_fullStr CAR T Cells Targeting Membrane-Bound Hsp70 on Tumor Cells Mimic Hsp70-Primed NK Cells
title_full_unstemmed CAR T Cells Targeting Membrane-Bound Hsp70 on Tumor Cells Mimic Hsp70-Primed NK Cells
title_short CAR T Cells Targeting Membrane-Bound Hsp70 on Tumor Cells Mimic Hsp70-Primed NK Cells
title_sort car t cells targeting membrane-bound hsp70 on tumor cells mimic hsp70-primed nk cells
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9198541/
https://www.ncbi.nlm.nih.gov/pubmed/35720311
http://dx.doi.org/10.3389/fimmu.2022.883694
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