Evaluating the Cellular Targets of Anti-4-1BB Agonist Antibody during Immunotherapy of a Pre-Established Tumor in Mice

BACKGROUND: Manipulation of the immune system represents a promising avenue for cancer therapy. Rational advances in immunotherapy of cancer will require an understanding of the precise correlates of protection. Agonistic antibodies against the tumor necrosis factor receptor family member 4-1BB are...

Descripción completa

Detalles Bibliográficos
Autores principales: Lin, Gloria H. Y., Liu, Yuanqing, Ambagala, Thanuja, Kwon, Byoung S., Ohashi, Pamela S., Watts, Tania H.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2882368/
https://www.ncbi.nlm.nih.gov/pubmed/20543982
http://dx.doi.org/10.1371/journal.pone.0011003
_version_ 1782182181544656896
author Lin, Gloria H. Y.
Liu, Yuanqing
Ambagala, Thanuja
Kwon, Byoung S.
Ohashi, Pamela S.
Watts, Tania H.
author_facet Lin, Gloria H. Y.
Liu, Yuanqing
Ambagala, Thanuja
Kwon, Byoung S.
Ohashi, Pamela S.
Watts, Tania H.
author_sort Lin, Gloria H. Y.
collection PubMed
description BACKGROUND: Manipulation of the immune system represents a promising avenue for cancer therapy. Rational advances in immunotherapy of cancer will require an understanding of the precise correlates of protection. Agonistic antibodies against the tumor necrosis factor receptor family member 4-1BB are emerging as a promising tool in cancer therapy, with evidence that these antibodies expand both T cells as well as innate immune cells. Depletion studies have suggested that several cell types can play a role in these immunotherapeutic regimens, but do not reveal which cells must directly receive the 4-1BB signals for effective therapy. METHODOLOGY/PRINCIPAL FINDINGS: We show that re-activated memory T cells are superior to resting memory T cells in control of an 8-day pre-established E.G7 tumor in mice. We find that ex vivo activation of the memory T cells allows the activated effectors to continue to divide and enter the tumor, regardless of antigen-specificity; however, only antigen-specific reactivated memory T cells show any efficacy in tumor control. When agonistic anti-4-1BB antibody is combined with this optimized adoptive T cell therapy, 80% of mice survive and are fully protected from tumor rechallenge. Using 4-1BB-deficient mice and mixed bone marrow chimeras, we find that it is sufficient to have 4-1BB only on the endogenous host αβ T cells or only on the transferred T cells for the effects of anti-4-1BB to be realized. Conversely, although multiple immune cell types express 4-1BB and both T cells and APC expand during anti-4-1BB therapy, 4-1BB on cells other than αβ T cells is neither necessary nor sufficient for the effect of anti-4-1BB in this adoptive immunotherapy model. CONCLUSIONS/SIGNIFICANCE: This study establishes αβ T cells rather than innate immune cells as the critical target in anti-4-1BB therapy of a pre-established tumor. The study also demonstrates that ex vivo activation of memory T cells prior to infusion allows antigen-specific tumor control without the need for reactivation of the memory T cells in the tumor.
format Text
id pubmed-2882368
institution National Center for Biotechnology Information
language English
publishDate 2010
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-28823682010-06-11 Evaluating the Cellular Targets of Anti-4-1BB Agonist Antibody during Immunotherapy of a Pre-Established Tumor in Mice Lin, Gloria H. Y. Liu, Yuanqing Ambagala, Thanuja Kwon, Byoung S. Ohashi, Pamela S. Watts, Tania H. PLoS One Research Article BACKGROUND: Manipulation of the immune system represents a promising avenue for cancer therapy. Rational advances in immunotherapy of cancer will require an understanding of the precise correlates of protection. Agonistic antibodies against the tumor necrosis factor receptor family member 4-1BB are emerging as a promising tool in cancer therapy, with evidence that these antibodies expand both T cells as well as innate immune cells. Depletion studies have suggested that several cell types can play a role in these immunotherapeutic regimens, but do not reveal which cells must directly receive the 4-1BB signals for effective therapy. METHODOLOGY/PRINCIPAL FINDINGS: We show that re-activated memory T cells are superior to resting memory T cells in control of an 8-day pre-established E.G7 tumor in mice. We find that ex vivo activation of the memory T cells allows the activated effectors to continue to divide and enter the tumor, regardless of antigen-specificity; however, only antigen-specific reactivated memory T cells show any efficacy in tumor control. When agonistic anti-4-1BB antibody is combined with this optimized adoptive T cell therapy, 80% of mice survive and are fully protected from tumor rechallenge. Using 4-1BB-deficient mice and mixed bone marrow chimeras, we find that it is sufficient to have 4-1BB only on the endogenous host αβ T cells or only on the transferred T cells for the effects of anti-4-1BB to be realized. Conversely, although multiple immune cell types express 4-1BB and both T cells and APC expand during anti-4-1BB therapy, 4-1BB on cells other than αβ T cells is neither necessary nor sufficient for the effect of anti-4-1BB in this adoptive immunotherapy model. CONCLUSIONS/SIGNIFICANCE: This study establishes αβ T cells rather than innate immune cells as the critical target in anti-4-1BB therapy of a pre-established tumor. The study also demonstrates that ex vivo activation of memory T cells prior to infusion allows antigen-specific tumor control without the need for reactivation of the memory T cells in the tumor. Public Library of Science 2010-06-08 /pmc/articles/PMC2882368/ /pubmed/20543982 http://dx.doi.org/10.1371/journal.pone.0011003 Text en Lin et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Lin, Gloria H. Y.
Liu, Yuanqing
Ambagala, Thanuja
Kwon, Byoung S.
Ohashi, Pamela S.
Watts, Tania H.
Evaluating the Cellular Targets of Anti-4-1BB Agonist Antibody during Immunotherapy of a Pre-Established Tumor in Mice
title Evaluating the Cellular Targets of Anti-4-1BB Agonist Antibody during Immunotherapy of a Pre-Established Tumor in Mice
title_full Evaluating the Cellular Targets of Anti-4-1BB Agonist Antibody during Immunotherapy of a Pre-Established Tumor in Mice
title_fullStr Evaluating the Cellular Targets of Anti-4-1BB Agonist Antibody during Immunotherapy of a Pre-Established Tumor in Mice
title_full_unstemmed Evaluating the Cellular Targets of Anti-4-1BB Agonist Antibody during Immunotherapy of a Pre-Established Tumor in Mice
title_short Evaluating the Cellular Targets of Anti-4-1BB Agonist Antibody during Immunotherapy of a Pre-Established Tumor in Mice
title_sort evaluating the cellular targets of anti-4-1bb agonist antibody during immunotherapy of a pre-established tumor in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2882368/
https://www.ncbi.nlm.nih.gov/pubmed/20543982
http://dx.doi.org/10.1371/journal.pone.0011003
work_keys_str_mv AT lingloriahy evaluatingthecellulartargetsofanti41bbagonistantibodyduringimmunotherapyofapreestablishedtumorinmice
AT liuyuanqing evaluatingthecellulartargetsofanti41bbagonistantibodyduringimmunotherapyofapreestablishedtumorinmice
AT ambagalathanuja evaluatingthecellulartargetsofanti41bbagonistantibodyduringimmunotherapyofapreestablishedtumorinmice
AT kwonbyoungs evaluatingthecellulartargetsofanti41bbagonistantibodyduringimmunotherapyofapreestablishedtumorinmice
AT ohashipamelas evaluatingthecellulartargetsofanti41bbagonistantibodyduringimmunotherapyofapreestablishedtumorinmice
AT wattstaniah evaluatingthecellulartargetsofanti41bbagonistantibodyduringimmunotherapyofapreestablishedtumorinmice

Ejemplares similares