Reprogramming of Tumor-reactive Tumor-infiltrating Lymphocytes to Human-induced Pluripotent Stem Cells

Tumor-infiltrating lymphocytes (TIL) that can recognize and kill tumor cells have curative potential in subsets of patients treated with adoptive cell transfer (ACT). However, lack of TIL therapeutic efficacy in many patients may be due in large part to a paucity of tumor-reactive T cells in TIL and...

Descripción completa

Detalles Bibliográficos
Autores principales: Islam, S.M. Rafiqul, Maeda, Takuya, Tamaoki, Naritaka, Good, Meghan L., Kishton, Rigel J., Paria, Biman C., Yu, Zhiya, Bosch-Marce, Marta, Bedanova, Nicole M., Liu, Chengyu, Kruhlak, Michael J., Restifo, Nicholas P., Vizcardo, Raul
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for Cancer Research 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10211394/
https://www.ncbi.nlm.nih.gov/pubmed/37377887
http://dx.doi.org/10.1158/2767-9764.CRC-22-0265
_version_ 1785047268283383808
author Islam, S.M. Rafiqul
Maeda, Takuya
Tamaoki, Naritaka
Good, Meghan L.
Kishton, Rigel J.
Paria, Biman C.
Yu, Zhiya
Bosch-Marce, Marta
Bedanova, Nicole M.
Liu, Chengyu
Kruhlak, Michael J.
Restifo, Nicholas P.
Vizcardo, Raul
author_facet Islam, S.M. Rafiqul
Maeda, Takuya
Tamaoki, Naritaka
Good, Meghan L.
Kishton, Rigel J.
Paria, Biman C.
Yu, Zhiya
Bosch-Marce, Marta
Bedanova, Nicole M.
Liu, Chengyu
Kruhlak, Michael J.
Restifo, Nicholas P.
Vizcardo, Raul
author_sort Islam, S.M. Rafiqul
collection PubMed
description Tumor-infiltrating lymphocytes (TIL) that can recognize and kill tumor cells have curative potential in subsets of patients treated with adoptive cell transfer (ACT). However, lack of TIL therapeutic efficacy in many patients may be due in large part to a paucity of tumor-reactive T cells in TIL and the exhausted and terminally differentiated status of those tumor-reactive T cells. We sought to reprogram exhausted TIL that possess T-cell receptors (TCR) specific for tumor antigens into induced pluripotent stem cells (iPSC) to rejuvenate them for more potent ACT. We first attempted to reprogram tumor neoantigen-specific TIL by αCD3 Ab prestimulation which resulted in failure of establishing tumor-reactive TIL-iPSCs, instead, T cell–derived iPSCs from bystander T cells were established. To selectively activate and enrich tumor-reactive T cells from the heterogenous TIL population, CD8(+) PD-1(+) 4-1BB(+) TIL population were isolated after coculture with autologous tumor cells, followed by direct reprogramming into iPSCs. TCR sequencing analysis of the resulting iPSC clones revealed that reprogrammed TIL-iPSCs encoded TCRs that were identical to the pre-identified tumor-reactive TCRs found in minimally cultured TIL. Moreover, reprogrammed TIL-iPSCs contained rare tumor antigen-specific TCRs, which were not detectable by TCR sequencing of the starting cell population. Thus, reprogramming of PD-1(+) 4-1BB(+) TIL after coculture with autologous tumor cells selectively generates tumor antigen-specific TIL-iPSCs, and is a distinctive method to enrich and identify tumor antigen-specific TCRs of low frequency from TIL. SIGNIFICANCE: Reprogramming of TIL into iPSC holds great promise for the future treatment of cancer due to their rejuvenated nature and the retention of tumor-specific TCRs. One limitation is the lack of selective and efficient methods for reprogramming tumor-specific T cells from polyclonal TIL. Here we addressed this limitation and present a method to efficiently reprogram TIL into iPSC colonies carrying diverse tumor antigen reactive TCR recombination.
format Online
Article
Text
id pubmed-10211394
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher American Association for Cancer Research
record_format MEDLINE/PubMed
spelling pubmed-102113942023-05-26 Reprogramming of Tumor-reactive Tumor-infiltrating Lymphocytes to Human-induced Pluripotent Stem Cells Islam, S.M. Rafiqul Maeda, Takuya Tamaoki, Naritaka Good, Meghan L. Kishton, Rigel J. Paria, Biman C. Yu, Zhiya Bosch-Marce, Marta Bedanova, Nicole M. Liu, Chengyu Kruhlak, Michael J. Restifo, Nicholas P. Vizcardo, Raul Cancer Res Commun Research Article Tumor-infiltrating lymphocytes (TIL) that can recognize and kill tumor cells have curative potential in subsets of patients treated with adoptive cell transfer (ACT). However, lack of TIL therapeutic efficacy in many patients may be due in large part to a paucity of tumor-reactive T cells in TIL and the exhausted and terminally differentiated status of those tumor-reactive T cells. We sought to reprogram exhausted TIL that possess T-cell receptors (TCR) specific for tumor antigens into induced pluripotent stem cells (iPSC) to rejuvenate them for more potent ACT. We first attempted to reprogram tumor neoantigen-specific TIL by αCD3 Ab prestimulation which resulted in failure of establishing tumor-reactive TIL-iPSCs, instead, T cell–derived iPSCs from bystander T cells were established. To selectively activate and enrich tumor-reactive T cells from the heterogenous TIL population, CD8(+) PD-1(+) 4-1BB(+) TIL population were isolated after coculture with autologous tumor cells, followed by direct reprogramming into iPSCs. TCR sequencing analysis of the resulting iPSC clones revealed that reprogrammed TIL-iPSCs encoded TCRs that were identical to the pre-identified tumor-reactive TCRs found in minimally cultured TIL. Moreover, reprogrammed TIL-iPSCs contained rare tumor antigen-specific TCRs, which were not detectable by TCR sequencing of the starting cell population. Thus, reprogramming of PD-1(+) 4-1BB(+) TIL after coculture with autologous tumor cells selectively generates tumor antigen-specific TIL-iPSCs, and is a distinctive method to enrich and identify tumor antigen-specific TCRs of low frequency from TIL. SIGNIFICANCE: Reprogramming of TIL into iPSC holds great promise for the future treatment of cancer due to their rejuvenated nature and the retention of tumor-specific TCRs. One limitation is the lack of selective and efficient methods for reprogramming tumor-specific T cells from polyclonal TIL. Here we addressed this limitation and present a method to efficiently reprogram TIL into iPSC colonies carrying diverse tumor antigen reactive TCR recombination. American Association for Cancer Research 2023-05-25 /pmc/articles/PMC10211394/ /pubmed/37377887 http://dx.doi.org/10.1158/2767-9764.CRC-22-0265 Text en © 2023 The Authors; Published by the American Association for Cancer Research https://creativecommons.org/licenses/by/4.0/This open access article is distributed under the Creative Commons Attribution 4.0 International (CC BY 4.0) license.
spellingShingle Research Article
Islam, S.M. Rafiqul
Maeda, Takuya
Tamaoki, Naritaka
Good, Meghan L.
Kishton, Rigel J.
Paria, Biman C.
Yu, Zhiya
Bosch-Marce, Marta
Bedanova, Nicole M.
Liu, Chengyu
Kruhlak, Michael J.
Restifo, Nicholas P.
Vizcardo, Raul
Reprogramming of Tumor-reactive Tumor-infiltrating Lymphocytes to Human-induced Pluripotent Stem Cells
title Reprogramming of Tumor-reactive Tumor-infiltrating Lymphocytes to Human-induced Pluripotent Stem Cells
title_full Reprogramming of Tumor-reactive Tumor-infiltrating Lymphocytes to Human-induced Pluripotent Stem Cells
title_fullStr Reprogramming of Tumor-reactive Tumor-infiltrating Lymphocytes to Human-induced Pluripotent Stem Cells
title_full_unstemmed Reprogramming of Tumor-reactive Tumor-infiltrating Lymphocytes to Human-induced Pluripotent Stem Cells
title_short Reprogramming of Tumor-reactive Tumor-infiltrating Lymphocytes to Human-induced Pluripotent Stem Cells
title_sort reprogramming of tumor-reactive tumor-infiltrating lymphocytes to human-induced pluripotent stem cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10211394/
https://www.ncbi.nlm.nih.gov/pubmed/37377887
http://dx.doi.org/10.1158/2767-9764.CRC-22-0265
work_keys_str_mv AT islamsmrafiqul reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT maedatakuya reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT tamaokinaritaka reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT goodmeghanl reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT kishtonrigelj reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT pariabimanc reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT yuzhiya reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT boschmarcemarta reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT bedanovanicolem reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT liuchengyu reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT kruhlakmichaelj reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT restifonicholasp reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells
AT vizcardoraul reprogrammingoftumorreactivetumorinfiltratinglymphocytestohumaninducedpluripotentstemcells

Ejemplares similares