Pretreatment of Glioblastoma with Bortezomib Potentiates Natural Killer Cell Cytotoxicity through TRAIL/DR5 Mediated Apoptosis and Prolongs Animal Survival

Background: Natural killer (NK) cells are potential effectors in anti-cancer immunotherapy; however only a subset potently kills cancer cells. Here, we examined whether pretreatment of glioblastoma (GBM) with the proteasome inhibitor, bortezomib (BTZ), might sensitize tumour cells to NK cell lysis b...

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Autores principales: Gras Navarro, Andrea, Espedal, Heidi, Joseph, Justin Vareecal, Trachsel-Moncho, Laura, Bahador, Marzieh, Tore Gjertsen, Bjørn, Klæboe Kristoffersen, Einar, Simonsen, Anne, Miletic, Hrvoje, Øyvind Enger, Per, Rahman, Mohummad Aminur, Chekenya, Martha
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6678126/
https://www.ncbi.nlm.nih.gov/pubmed/31319548
http://dx.doi.org/10.3390/cancers11070996
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author Gras Navarro, Andrea
Espedal, Heidi
Joseph, Justin Vareecal
Trachsel-Moncho, Laura
Bahador, Marzieh
Tore Gjertsen, Bjørn
Klæboe Kristoffersen, Einar
Simonsen, Anne
Miletic, Hrvoje
Øyvind Enger, Per
Rahman, Mohummad Aminur
Chekenya, Martha
author_facet Gras Navarro, Andrea
Espedal, Heidi
Joseph, Justin Vareecal
Trachsel-Moncho, Laura
Bahador, Marzieh
Tore Gjertsen, Bjørn
Klæboe Kristoffersen, Einar
Simonsen, Anne
Miletic, Hrvoje
Øyvind Enger, Per
Rahman, Mohummad Aminur
Chekenya, Martha
author_sort Gras Navarro, Andrea
collection PubMed
description Background: Natural killer (NK) cells are potential effectors in anti-cancer immunotherapy; however only a subset potently kills cancer cells. Here, we examined whether pretreatment of glioblastoma (GBM) with the proteasome inhibitor, bortezomib (BTZ), might sensitize tumour cells to NK cell lysis by inducing stress antigens recognized by NK-activating receptors. Methods: Combination immunotherapy of NK cells with BTZ was studied in vitro against GBM cells and in a GBM-bearing mouse model. Tumour cells were derived from primary GBMs and NK cells from donors or patients. Flow cytometry was used for viability/cytotoxicity evaluation as well as in vitro and ex vivo phenotyping. We performed a Seahorse assay to assess oxygen consumption rates and mitochondrial function, Luminex ELISA to determine NK cell secretion, protein chemistry and LC–MS/MS to detect BTZ in brain tissue. MRI was used to monitor therapeutic efficacy in mice orthotopically implanted with GBM spheroids. Results: NK cells released IFNγ, perforin and granzyme A cytolytic granules upon recognition of stress-ligand expressing GBM cells, disrupted mitochondrial function and killed 24–46% of cells by apoptosis. Pretreatment with BTZ further increased stress-ligands, induced TRAIL-R2 expression and enhanced GBM lysis to 33–76% through augmented IFNγ release (p < 0.05). Blocking NKG2D, TRAIL and TRAIL-R2 rescued GBM cells treated with BTZ from NK cells, p = 0.01. Adoptively transferred autologous NK-cells persisted in vivo (p < 0.05), diminished tumour proliferation and prolonged survival alone (Log Rank(10.19), p = 0.0014, 95%CI 0.252–0.523) or when combined with BTZ (Log Rank(5.25), p = 0.0219, 95%CI 0.295–0.408), or either compared to vehicle controls (median 98 vs. 68 days and 80 vs. 68 days, respectively). BTZ crossed the blood–brain barrier, attenuated proteasomal activity in vivo (p < 0.0001; p < 0.01 compared to vehicle control or NK cells only, respectively) and diminished tumour angiogenesis to promote survival compared to vehicle-treated controls (Log Rank(6.57), p = 0.0104, 95%CI 0.284–0.424, median 83 vs. 68 days). However, NK ablation with anti-asialo-GM1 abrogated the therapeutic efficacy. Conclusions: NK cells alone or in combination with BTZ inhibit tumour growth, but the scheduling of BTZ in vivo requires further investigation to maximize its contribution to the efficacy of the combination regimen.
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spelling pubmed-66781262019-08-19 Pretreatment of Glioblastoma with Bortezomib Potentiates Natural Killer Cell Cytotoxicity through TRAIL/DR5 Mediated Apoptosis and Prolongs Animal Survival Gras Navarro, Andrea Espedal, Heidi Joseph, Justin Vareecal Trachsel-Moncho, Laura Bahador, Marzieh Tore Gjertsen, Bjørn Klæboe Kristoffersen, Einar Simonsen, Anne Miletic, Hrvoje Øyvind Enger, Per Rahman, Mohummad Aminur Chekenya, Martha Cancers (Basel) Article Background: Natural killer (NK) cells are potential effectors in anti-cancer immunotherapy; however only a subset potently kills cancer cells. Here, we examined whether pretreatment of glioblastoma (GBM) with the proteasome inhibitor, bortezomib (BTZ), might sensitize tumour cells to NK cell lysis by inducing stress antigens recognized by NK-activating receptors. Methods: Combination immunotherapy of NK cells with BTZ was studied in vitro against GBM cells and in a GBM-bearing mouse model. Tumour cells were derived from primary GBMs and NK cells from donors or patients. Flow cytometry was used for viability/cytotoxicity evaluation as well as in vitro and ex vivo phenotyping. We performed a Seahorse assay to assess oxygen consumption rates and mitochondrial function, Luminex ELISA to determine NK cell secretion, protein chemistry and LC–MS/MS to detect BTZ in brain tissue. MRI was used to monitor therapeutic efficacy in mice orthotopically implanted with GBM spheroids. Results: NK cells released IFNγ, perforin and granzyme A cytolytic granules upon recognition of stress-ligand expressing GBM cells, disrupted mitochondrial function and killed 24–46% of cells by apoptosis. Pretreatment with BTZ further increased stress-ligands, induced TRAIL-R2 expression and enhanced GBM lysis to 33–76% through augmented IFNγ release (p < 0.05). Blocking NKG2D, TRAIL and TRAIL-R2 rescued GBM cells treated with BTZ from NK cells, p = 0.01. Adoptively transferred autologous NK-cells persisted in vivo (p < 0.05), diminished tumour proliferation and prolonged survival alone (Log Rank(10.19), p = 0.0014, 95%CI 0.252–0.523) or when combined with BTZ (Log Rank(5.25), p = 0.0219, 95%CI 0.295–0.408), or either compared to vehicle controls (median 98 vs. 68 days and 80 vs. 68 days, respectively). BTZ crossed the blood–brain barrier, attenuated proteasomal activity in vivo (p < 0.0001; p < 0.01 compared to vehicle control or NK cells only, respectively) and diminished tumour angiogenesis to promote survival compared to vehicle-treated controls (Log Rank(6.57), p = 0.0104, 95%CI 0.284–0.424, median 83 vs. 68 days). However, NK ablation with anti-asialo-GM1 abrogated the therapeutic efficacy. Conclusions: NK cells alone or in combination with BTZ inhibit tumour growth, but the scheduling of BTZ in vivo requires further investigation to maximize its contribution to the efficacy of the combination regimen. MDPI 2019-07-17 /pmc/articles/PMC6678126/ /pubmed/31319548 http://dx.doi.org/10.3390/cancers11070996 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Gras Navarro, Andrea
Espedal, Heidi
Joseph, Justin Vareecal
Trachsel-Moncho, Laura
Bahador, Marzieh
Tore Gjertsen, Bjørn
Klæboe Kristoffersen, Einar
Simonsen, Anne
Miletic, Hrvoje
Øyvind Enger, Per
Rahman, Mohummad Aminur
Chekenya, Martha
Pretreatment of Glioblastoma with Bortezomib Potentiates Natural Killer Cell Cytotoxicity through TRAIL/DR5 Mediated Apoptosis and Prolongs Animal Survival
title Pretreatment of Glioblastoma with Bortezomib Potentiates Natural Killer Cell Cytotoxicity through TRAIL/DR5 Mediated Apoptosis and Prolongs Animal Survival
title_full Pretreatment of Glioblastoma with Bortezomib Potentiates Natural Killer Cell Cytotoxicity through TRAIL/DR5 Mediated Apoptosis and Prolongs Animal Survival
title_fullStr Pretreatment of Glioblastoma with Bortezomib Potentiates Natural Killer Cell Cytotoxicity through TRAIL/DR5 Mediated Apoptosis and Prolongs Animal Survival
title_full_unstemmed Pretreatment of Glioblastoma with Bortezomib Potentiates Natural Killer Cell Cytotoxicity through TRAIL/DR5 Mediated Apoptosis and Prolongs Animal Survival
title_short Pretreatment of Glioblastoma with Bortezomib Potentiates Natural Killer Cell Cytotoxicity through TRAIL/DR5 Mediated Apoptosis and Prolongs Animal Survival
title_sort pretreatment of glioblastoma with bortezomib potentiates natural killer cell cytotoxicity through trail/dr5 mediated apoptosis and prolongs animal survival
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6678126/
https://www.ncbi.nlm.nih.gov/pubmed/31319548
http://dx.doi.org/10.3390/cancers11070996
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