Acute Conditioning of Antigen-Expanded CD8(+) T Cells via the GSK3β-mTORC Axis Differentially Dictates Their Immediate and Distal Responses after Antigen Rechallenge

SIMPLE SUMMARY: Expanded, antigen-experienced CD8(+) T cells are utilized in immunotherapy to treat infections and cancers. Antigen rechallenge of these cells leads to their re-expansion. The effector functions of re-expanded CD8(+) T cells are critical for their therapeutic efficacy. We found that...

Descripción completa

Detalles Bibliográficos
Autores principales: Taborska, Pavla, Stakheev, Dmitry, Svobodova, Hana, Strizova, Zuzana, Bartunkova, Jirina, Smrz, Daniel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7765077/
https://www.ncbi.nlm.nih.gov/pubmed/33327544
http://dx.doi.org/10.3390/cancers12123766
_version_ 1783628407004725248
author Taborska, Pavla
Stakheev, Dmitry
Svobodova, Hana
Strizova, Zuzana
Bartunkova, Jirina
Smrz, Daniel
author_facet Taborska, Pavla
Stakheev, Dmitry
Svobodova, Hana
Strizova, Zuzana
Bartunkova, Jirina
Smrz, Daniel
author_sort Taborska, Pavla
collection PubMed
description SIMPLE SUMMARY: Expanded, antigen-experienced CD8(+) T cells are utilized in immunotherapy to treat infections and cancers. Antigen rechallenge of these cells leads to their re-expansion. The effector functions of re-expanded CD8(+) T cells are critical for their therapeutic efficacy. We found that acute conditioning of the cells, before antigen rechallenge, impacts their effector function after re-expansion. Our data showed that acute pharmacological modulation of the GSK3β-mTORC axis with TWS119 or rapamycin, but not Torin1, before antigen rechallenge promotes the effector functions of re-expanded CD8(+) T cells. These findings suggest that acute conditioning of the GSK3β-mTORC axis in expanded CD8(+) T cells, before antigen rechallenge, can promote the therapeutic performance of re-expanded CD8(+) T cells. ABSTRACT: CD8(+) T cells protect against tumors and intracellular pathogens. The inflammatory cytokines IL-2, IL-15, and IL-7 are necessary for their expansion. However, elevated serum levels of these cytokines are often associated with cancer, poorer prognosis of cancer patients, and exhaustion of antigen-expanded CD8(+) T cells. The impact of acute conditioning of antigen-expanded CD8(+) T cells with these cytokines is unknown. Here, we generated antigen-expanded CD8(+) T cells using dendritic cells and PC-3 cells. The cells were acutely (18–24 h) conditioned with IL-2 and either the GSK3β inhibitor TWS119, the mTORC1 inhibitor rapamycin, or the mTORC1/2 inhibitor Torin1, then their immediate and post-re-expansion (distal) cytokine responses after antigen rechallenge were evaluated. We found that acute IL-2 conditioning upregulated the immediate antigen-induced cytokine response of the tested cells. Following their re-expansion, however, the cells showed a decreased cytokine response. These IL-2 conditioning-mediated impacts were counteracted with TWS119 or rapamycin but not with Torin1. Our data revealed that the acute conditioning of antigen-expanded CD8(+) T cells with IL-2 modulates the GSK3β-mTORC signaling axis. This modulation differentially affected the immediate and distal cytokine responses of the cells. The acute targeting of this signaling axis could, therefore, represent a novel strategy for the modulation of antigen-expanded CD8(+) T cells.
format Online
Article
Text
id pubmed-7765077
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-77650772020-12-27 Acute Conditioning of Antigen-Expanded CD8(+) T Cells via the GSK3β-mTORC Axis Differentially Dictates Their Immediate and Distal Responses after Antigen Rechallenge Taborska, Pavla Stakheev, Dmitry Svobodova, Hana Strizova, Zuzana Bartunkova, Jirina Smrz, Daniel Cancers (Basel) Article SIMPLE SUMMARY: Expanded, antigen-experienced CD8(+) T cells are utilized in immunotherapy to treat infections and cancers. Antigen rechallenge of these cells leads to their re-expansion. The effector functions of re-expanded CD8(+) T cells are critical for their therapeutic efficacy. We found that acute conditioning of the cells, before antigen rechallenge, impacts their effector function after re-expansion. Our data showed that acute pharmacological modulation of the GSK3β-mTORC axis with TWS119 or rapamycin, but not Torin1, before antigen rechallenge promotes the effector functions of re-expanded CD8(+) T cells. These findings suggest that acute conditioning of the GSK3β-mTORC axis in expanded CD8(+) T cells, before antigen rechallenge, can promote the therapeutic performance of re-expanded CD8(+) T cells. ABSTRACT: CD8(+) T cells protect against tumors and intracellular pathogens. The inflammatory cytokines IL-2, IL-15, and IL-7 are necessary for their expansion. However, elevated serum levels of these cytokines are often associated with cancer, poorer prognosis of cancer patients, and exhaustion of antigen-expanded CD8(+) T cells. The impact of acute conditioning of antigen-expanded CD8(+) T cells with these cytokines is unknown. Here, we generated antigen-expanded CD8(+) T cells using dendritic cells and PC-3 cells. The cells were acutely (18–24 h) conditioned with IL-2 and either the GSK3β inhibitor TWS119, the mTORC1 inhibitor rapamycin, or the mTORC1/2 inhibitor Torin1, then their immediate and post-re-expansion (distal) cytokine responses after antigen rechallenge were evaluated. We found that acute IL-2 conditioning upregulated the immediate antigen-induced cytokine response of the tested cells. Following their re-expansion, however, the cells showed a decreased cytokine response. These IL-2 conditioning-mediated impacts were counteracted with TWS119 or rapamycin but not with Torin1. Our data revealed that the acute conditioning of antigen-expanded CD8(+) T cells with IL-2 modulates the GSK3β-mTORC signaling axis. This modulation differentially affected the immediate and distal cytokine responses of the cells. The acute targeting of this signaling axis could, therefore, represent a novel strategy for the modulation of antigen-expanded CD8(+) T cells. MDPI 2020-12-14 /pmc/articles/PMC7765077/ /pubmed/33327544 http://dx.doi.org/10.3390/cancers12123766 Text en © 2020 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
Taborska, Pavla
Stakheev, Dmitry
Svobodova, Hana
Strizova, Zuzana
Bartunkova, Jirina
Smrz, Daniel
Acute Conditioning of Antigen-Expanded CD8(+) T Cells via the GSK3β-mTORC Axis Differentially Dictates Their Immediate and Distal Responses after Antigen Rechallenge
title Acute Conditioning of Antigen-Expanded CD8(+) T Cells via the GSK3β-mTORC Axis Differentially Dictates Their Immediate and Distal Responses after Antigen Rechallenge
title_full Acute Conditioning of Antigen-Expanded CD8(+) T Cells via the GSK3β-mTORC Axis Differentially Dictates Their Immediate and Distal Responses after Antigen Rechallenge
title_fullStr Acute Conditioning of Antigen-Expanded CD8(+) T Cells via the GSK3β-mTORC Axis Differentially Dictates Their Immediate and Distal Responses after Antigen Rechallenge
title_full_unstemmed Acute Conditioning of Antigen-Expanded CD8(+) T Cells via the GSK3β-mTORC Axis Differentially Dictates Their Immediate and Distal Responses after Antigen Rechallenge
title_short Acute Conditioning of Antigen-Expanded CD8(+) T Cells via the GSK3β-mTORC Axis Differentially Dictates Their Immediate and Distal Responses after Antigen Rechallenge
title_sort acute conditioning of antigen-expanded cd8(+) t cells via the gsk3β-mtorc axis differentially dictates their immediate and distal responses after antigen rechallenge
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7765077/
https://www.ncbi.nlm.nih.gov/pubmed/33327544
http://dx.doi.org/10.3390/cancers12123766
work_keys_str_mv AT taborskapavla acuteconditioningofantigenexpandedcd8tcellsviathegsk3bmtorcaxisdifferentiallydictatestheirimmediateanddistalresponsesafterantigenrechallenge
AT stakheevdmitry acuteconditioningofantigenexpandedcd8tcellsviathegsk3bmtorcaxisdifferentiallydictatestheirimmediateanddistalresponsesafterantigenrechallenge
AT svobodovahana acuteconditioningofantigenexpandedcd8tcellsviathegsk3bmtorcaxisdifferentiallydictatestheirimmediateanddistalresponsesafterantigenrechallenge
AT strizovazuzana acuteconditioningofantigenexpandedcd8tcellsviathegsk3bmtorcaxisdifferentiallydictatestheirimmediateanddistalresponsesafterantigenrechallenge
AT bartunkovajirina acuteconditioningofantigenexpandedcd8tcellsviathegsk3bmtorcaxisdifferentiallydictatestheirimmediateanddistalresponsesafterantigenrechallenge
AT smrzdaniel acuteconditioningofantigenexpandedcd8tcellsviathegsk3bmtorcaxisdifferentiallydictatestheirimmediateanddistalresponsesafterantigenrechallenge

Ejemplares similares