Empirical identification and validation of tumor-targeting T cell receptors from circulation using autologous pancreatic tumor organoids

BACKGROUND: Tumor-specific cytotoxic T cells and T cell receptors are effective tools for cancer immunotherapy. Most efforts to identify them rely on known antigens or lymphocytes that have infiltrated into the tumor bed. Approaches to empirically identify tumor-targeting T cells and T cell receptor...

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Autores principales: Meng, Qingda, Xie, Shanshan, Gray, G Kenneth, Dezfulian, Mohammad H, Gandarilla, Omar, Li, Weilin, Huang, Ling, Akshinthala, Dipikaa, Ferrer, Elizabeth, Conahan, Catherine, Perea Del Pino, Sofia, Grossman, Joseph, Elledge, Stephen J, Hidalgo, Manuel, Muthuswamy, Senthil K
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BMJ Publishing Group 2021
Materias:
Clinical/Translational Cancer Immunotherapy
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8601084/
https://www.ncbi.nlm.nih.gov/pubmed/34789550
http://dx.doi.org/10.1136/jitc-2021-003213
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author Meng, Qingda
Xie, Shanshan
Gray, G Kenneth
Dezfulian, Mohammad H
Gandarilla, Omar
Li, Weilin
Huang, Ling
Akshinthala, Dipikaa
Ferrer, Elizabeth
Conahan, Catherine
Perea Del Pino, Sofia
Grossman, Joseph
Elledge, Stephen J
Hidalgo, Manuel
Muthuswamy, Senthil K
author_facet Meng, Qingda
Xie, Shanshan
Gray, G Kenneth
Dezfulian, Mohammad H
Gandarilla, Omar
Li, Weilin
Huang, Ling
Akshinthala, Dipikaa
Ferrer, Elizabeth
Conahan, Catherine
Perea Del Pino, Sofia
Grossman, Joseph
Elledge, Stephen J
Hidalgo, Manuel
Muthuswamy, Senthil K
author_sort Meng, Qingda
collection PubMed
description BACKGROUND: Tumor-specific cytotoxic T cells and T cell receptors are effective tools for cancer immunotherapy. Most efforts to identify them rely on known antigens or lymphocytes that have infiltrated into the tumor bed. Approaches to empirically identify tumor-targeting T cells and T cell receptors by exploiting all antigens expressed on tumor cell surfaces are not well developed for most carcinomas, including pancreatic cancer. METHODS: Autologous tumor organoids were stimulated with T cells from the patients’ peripheral blood for 2 weeks to generate the organoid-primed T (opT) cells. opT cell phenotype was analyzed by monitoring changes in the expression levels of 28 cell surface and checkpoint proteins. Expression of ligands of the immune checkpoints was investigated by immunohistochemistry staining. T cells were labeled with carboxyfluorescein succinimidyl ester (CFSE) and assayed by flow cytometry to monitor tumor-induced T cell proliferation changes. opT cell-mediated killing of three-dimensional organoids was measured using an M30 ELISA kit. T cell receptors (TCRs) were identified by deep sequencing of gDNA isolated from T cells, and the TCR specificity was confirmed by transferring TCRs to the T cell line SKW-3 or donor T cells. RESULTS: The co-culture was effective in the generation of CD8 + or CD4+opT cells. The opT cells killed autologous tumors in a granzyme B or Fas-Fas ligand-dependent manner and expressed markers of tissue-resident memory phenotype. Each patient-derived opT cell culture displayed a unique complement of checkpoint proteins. Interestingly, only NKG2A blockade showed a potent increase in the interferon-γ production compared with blocking programmed cell death protein 1 (PD-1) or programmed cell death ligand 1 (PD-L1) or TIM3 or TIGIT or LAG3. Importantly, TCR sequencing demonstrated a dramatic clonal expansion of T cells with a restricted subset of TCRs. Cloning and transferring the TCRs to heterologous T cells was sufficient to confer tumor cell recognition and cytotoxic properties in a patient-specific manner. CONCLUSION: We report a platform for expanding tumor-targeting T cells from the peripheral blood of patients with pancreatic cancer. We identify the NKG2A-HLA-E axis as a potentially important checkpoint for CD8 +T cells for pancreatic cancer. Lastly, we demonstrate empirical identification of tumor-targeting TCRs that can be used for TCR-therapeutics.
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spelling pubmed-86010842021-12-02 Empirical identification and validation of tumor-targeting T cell receptors from circulation using autologous pancreatic tumor organoids Meng, Qingda Xie, Shanshan Gray, G Kenneth Dezfulian, Mohammad H Gandarilla, Omar Li, Weilin Huang, Ling Akshinthala, Dipikaa Ferrer, Elizabeth Conahan, Catherine Perea Del Pino, Sofia Grossman, Joseph Elledge, Stephen J Hidalgo, Manuel Muthuswamy, Senthil K J Immunother Cancer Clinical/Translational Cancer Immunotherapy BACKGROUND: Tumor-specific cytotoxic T cells and T cell receptors are effective tools for cancer immunotherapy. Most efforts to identify them rely on known antigens or lymphocytes that have infiltrated into the tumor bed. Approaches to empirically identify tumor-targeting T cells and T cell receptors by exploiting all antigens expressed on tumor cell surfaces are not well developed for most carcinomas, including pancreatic cancer. METHODS: Autologous tumor organoids were stimulated with T cells from the patients’ peripheral blood for 2 weeks to generate the organoid-primed T (opT) cells. opT cell phenotype was analyzed by monitoring changes in the expression levels of 28 cell surface and checkpoint proteins. Expression of ligands of the immune checkpoints was investigated by immunohistochemistry staining. T cells were labeled with carboxyfluorescein succinimidyl ester (CFSE) and assayed by flow cytometry to monitor tumor-induced T cell proliferation changes. opT cell-mediated killing of three-dimensional organoids was measured using an M30 ELISA kit. T cell receptors (TCRs) were identified by deep sequencing of gDNA isolated from T cells, and the TCR specificity was confirmed by transferring TCRs to the T cell line SKW-3 or donor T cells. RESULTS: The co-culture was effective in the generation of CD8 + or CD4+opT cells. The opT cells killed autologous tumors in a granzyme B or Fas-Fas ligand-dependent manner and expressed markers of tissue-resident memory phenotype. Each patient-derived opT cell culture displayed a unique complement of checkpoint proteins. Interestingly, only NKG2A blockade showed a potent increase in the interferon-γ production compared with blocking programmed cell death protein 1 (PD-1) or programmed cell death ligand 1 (PD-L1) or TIM3 or TIGIT or LAG3. Importantly, TCR sequencing demonstrated a dramatic clonal expansion of T cells with a restricted subset of TCRs. Cloning and transferring the TCRs to heterologous T cells was sufficient to confer tumor cell recognition and cytotoxic properties in a patient-specific manner. CONCLUSION: We report a platform for expanding tumor-targeting T cells from the peripheral blood of patients with pancreatic cancer. We identify the NKG2A-HLA-E axis as a potentially important checkpoint for CD8 +T cells for pancreatic cancer. Lastly, we demonstrate empirical identification of tumor-targeting TCRs that can be used for TCR-therapeutics. BMJ Publishing Group 2021-11-16 /pmc/articles/PMC8601084/ /pubmed/34789550 http://dx.doi.org/10.1136/jitc-2021-003213 Text en © Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY. Published by BMJ. https://creativecommons.org/licenses/by/4.0/This is an open access article distributed in accordance with the Creative Commons Attribution 4.0 Unported (CC BY 4.0) license, which permits others to copy, redistribute, remix, transform and build upon this work for any purpose, provided the original work is properly cited, a link to the licence is given, and indication of whether changes were made. See https://creativecommons.org/licenses/by/4.0/.
spellingShingle Clinical/Translational Cancer Immunotherapy
Meng, Qingda
Xie, Shanshan
Gray, G Kenneth
Dezfulian, Mohammad H
Gandarilla, Omar
Li, Weilin
Huang, Ling
Akshinthala, Dipikaa
Ferrer, Elizabeth
Conahan, Catherine
Perea Del Pino, Sofia
Grossman, Joseph
Elledge, Stephen J
Hidalgo, Manuel
Muthuswamy, Senthil K
Empirical identification and validation of tumor-targeting T cell receptors from circulation using autologous pancreatic tumor organoids
title Empirical identification and validation of tumor-targeting T cell receptors from circulation using autologous pancreatic tumor organoids
title_full Empirical identification and validation of tumor-targeting T cell receptors from circulation using autologous pancreatic tumor organoids
title_fullStr Empirical identification and validation of tumor-targeting T cell receptors from circulation using autologous pancreatic tumor organoids
title_full_unstemmed Empirical identification and validation of tumor-targeting T cell receptors from circulation using autologous pancreatic tumor organoids
title_short Empirical identification and validation of tumor-targeting T cell receptors from circulation using autologous pancreatic tumor organoids
title_sort empirical identification and validation of tumor-targeting t cell receptors from circulation using autologous pancreatic tumor organoids
topic Clinical/Translational Cancer Immunotherapy
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8601084/
https://www.ncbi.nlm.nih.gov/pubmed/34789550
http://dx.doi.org/10.1136/jitc-2021-003213
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