L-Selectin Enhanced T Cells Improve the Efficacy of Cancer Immunotherapy

The homing molecule, L-selectin (CD62L), is commonly used as a T cell activation marker, since expression is downregulated following engagement of the T cell receptor. Studies in mice have shown that CD62L(+) central memory T cells are better at controlling tumor growth than CD62L(−) effector memory...

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Autores principales: Watson, H. Angharad, Durairaj, Ruban R. P., Ohme, Julia, Alatsatianos, Markella, Almutairi, Hanan, Mohammed, Rebar N., Vigar, Miriam, Reed, Sophie G., Paisey, Stephen J., Marshall, Christopher, Gallimore, Awen, Ager, Ann
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6582763/
https://www.ncbi.nlm.nih.gov/pubmed/31249570
http://dx.doi.org/10.3389/fimmu.2019.01321
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author Watson, H. Angharad
Durairaj, Ruban R. P.
Ohme, Julia
Alatsatianos, Markella
Almutairi, Hanan
Mohammed, Rebar N.
Vigar, Miriam
Reed, Sophie G.
Paisey, Stephen J.
Marshall, Christopher
Gallimore, Awen
Ager, Ann
author_facet Watson, H. Angharad
Durairaj, Ruban R. P.
Ohme, Julia
Alatsatianos, Markella
Almutairi, Hanan
Mohammed, Rebar N.
Vigar, Miriam
Reed, Sophie G.
Paisey, Stephen J.
Marshall, Christopher
Gallimore, Awen
Ager, Ann
author_sort Watson, H. Angharad
collection PubMed
description The homing molecule, L-selectin (CD62L), is commonly used as a T cell activation marker, since expression is downregulated following engagement of the T cell receptor. Studies in mice have shown that CD62L(+) central memory T cells are better at controlling tumor growth than CD62L(−) effector memory T cells, while L-selectin knockout T cells are poor at controlling tumor growth. Here, we test the hypothesis that T cells expressing genetically modified forms of L-selectin that are maintained following T cell activation (L-selectin enhanced T cells) are better at controlling tumor growth than wild type T cells. Using mouse models of adoptive cell therapy, we show that L-selectin enhancement improves the efficacy of CD8(+) T cells in controlling solid and disseminated tumor growth. L-selectin knockout T cells had no effect. Checkpoint blockade inhibitors synergized with wild type and L-selectin enhanced T cells but had no effect in the absence of T cell transfers. Reduced tumor growth by L-selectin enhanced T cells correlated with increased frequency of CD8(+) tumor infiltrating T cells 21 days after commencing therapy. Longitudinal tracking of Zirconium-89 ((89)Zr) labeled T cells using PET-CT showed that transferred T cells localize to tumors within 1 h and accumulate over the following 7 days. L-selectin did not promote T cell homing to tumors within 18 h of transfer, however the early activation marker CD69 was upregulated on L-selectin positive but not L-selectin knockout T cells. L-selectin positive and L-selectin knockout T cells homed equally well to tumor-draining lymph nodes and spleens. CD69 expression was upregulated on both L-selectin positive and L-selectin knockout T cells but was significantly higher on L-selectin expressing T cells, particularly in the spleen. Clonal expansion of isolated L-selectin enhanced T cells was slower, and L-selectin was linked to expression of proliferation marker Ki67. Together these findings demonstrate that maintaining L-selectin expression on tumor-specific T cells offers an advantage in mouse models of cancer immunotherapy. The beneficial role of L-selectin is unrelated to its' well-known role in T cell homing and, instead, linked to activation of therapeutic T cells inside tumors. These findings suggest that L-selectin may benefit clinical applications in T cell selection for cancer therapy and for modifying CAR-T cells to broaden their clinical scope.
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spelling pubmed-65827632019-06-27 L-Selectin Enhanced T Cells Improve the Efficacy of Cancer Immunotherapy Watson, H. Angharad Durairaj, Ruban R. P. Ohme, Julia Alatsatianos, Markella Almutairi, Hanan Mohammed, Rebar N. Vigar, Miriam Reed, Sophie G. Paisey, Stephen J. Marshall, Christopher Gallimore, Awen Ager, Ann Front Immunol Immunology The homing molecule, L-selectin (CD62L), is commonly used as a T cell activation marker, since expression is downregulated following engagement of the T cell receptor. Studies in mice have shown that CD62L(+) central memory T cells are better at controlling tumor growth than CD62L(−) effector memory T cells, while L-selectin knockout T cells are poor at controlling tumor growth. Here, we test the hypothesis that T cells expressing genetically modified forms of L-selectin that are maintained following T cell activation (L-selectin enhanced T cells) are better at controlling tumor growth than wild type T cells. Using mouse models of adoptive cell therapy, we show that L-selectin enhancement improves the efficacy of CD8(+) T cells in controlling solid and disseminated tumor growth. L-selectin knockout T cells had no effect. Checkpoint blockade inhibitors synergized with wild type and L-selectin enhanced T cells but had no effect in the absence of T cell transfers. Reduced tumor growth by L-selectin enhanced T cells correlated with increased frequency of CD8(+) tumor infiltrating T cells 21 days after commencing therapy. Longitudinal tracking of Zirconium-89 ((89)Zr) labeled T cells using PET-CT showed that transferred T cells localize to tumors within 1 h and accumulate over the following 7 days. L-selectin did not promote T cell homing to tumors within 18 h of transfer, however the early activation marker CD69 was upregulated on L-selectin positive but not L-selectin knockout T cells. L-selectin positive and L-selectin knockout T cells homed equally well to tumor-draining lymph nodes and spleens. CD69 expression was upregulated on both L-selectin positive and L-selectin knockout T cells but was significantly higher on L-selectin expressing T cells, particularly in the spleen. Clonal expansion of isolated L-selectin enhanced T cells was slower, and L-selectin was linked to expression of proliferation marker Ki67. Together these findings demonstrate that maintaining L-selectin expression on tumor-specific T cells offers an advantage in mouse models of cancer immunotherapy. The beneficial role of L-selectin is unrelated to its' well-known role in T cell homing and, instead, linked to activation of therapeutic T cells inside tumors. These findings suggest that L-selectin may benefit clinical applications in T cell selection for cancer therapy and for modifying CAR-T cells to broaden their clinical scope. Frontiers Media S.A. 2019-06-12 /pmc/articles/PMC6582763/ /pubmed/31249570 http://dx.doi.org/10.3389/fimmu.2019.01321 Text en Copyright © 2019 Watson, Durairaj, Ohme, Alatsatianos, Almutairi, Mohammed, Vigar, Reed, Paisey, Marshall, Gallimore and Ager. http://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
Watson, H. Angharad
Durairaj, Ruban R. P.
Ohme, Julia
Alatsatianos, Markella
Almutairi, Hanan
Mohammed, Rebar N.
Vigar, Miriam
Reed, Sophie G.
Paisey, Stephen J.
Marshall, Christopher
Gallimore, Awen
Ager, Ann
L-Selectin Enhanced T Cells Improve the Efficacy of Cancer Immunotherapy
title L-Selectin Enhanced T Cells Improve the Efficacy of Cancer Immunotherapy
title_full L-Selectin Enhanced T Cells Improve the Efficacy of Cancer Immunotherapy
title_fullStr L-Selectin Enhanced T Cells Improve the Efficacy of Cancer Immunotherapy
title_full_unstemmed L-Selectin Enhanced T Cells Improve the Efficacy of Cancer Immunotherapy
title_short L-Selectin Enhanced T Cells Improve the Efficacy of Cancer Immunotherapy
title_sort l-selectin enhanced t cells improve the efficacy of cancer immunotherapy
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6582763/
https://www.ncbi.nlm.nih.gov/pubmed/31249570
http://dx.doi.org/10.3389/fimmu.2019.01321
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