Vaccine-induced tumor regression requires a dynamic cooperation between T cells and myeloid cells at the tumor site

Most cancer immunotherapies under present investigation are based on the belief that cytotoxic T cells are the most important anti-tumoral immune cells, whereas intra-tumoral macrophages would rather play a pro-tumoral role. We have challenged this antagonistic point of view and searched for collabo...

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Autores principales: Thoreau, Maxime, Penny, HweiXian Leong, Tan, KarWai, Regnier, Fabienne, Weiss, Julia Miriam, Lee, Bernett, Johannes, Ludger, Dransart, Estelle, Le Bon, Agnès, Abastado, Jean-Pierre, Tartour, Eric, Trautmann, Alain, Bercovici, Nadège
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4695029/
https://www.ncbi.nlm.nih.gov/pubmed/26337837
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author Thoreau, Maxime
Penny, HweiXian Leong
Tan, KarWai
Regnier, Fabienne
Weiss, Julia Miriam
Lee, Bernett
Johannes, Ludger
Dransart, Estelle
Le Bon, Agnès
Abastado, Jean-Pierre
Tartour, Eric
Trautmann, Alain
Bercovici, Nadège
author_facet Thoreau, Maxime
Penny, HweiXian Leong
Tan, KarWai
Regnier, Fabienne
Weiss, Julia Miriam
Lee, Bernett
Johannes, Ludger
Dransart, Estelle
Le Bon, Agnès
Abastado, Jean-Pierre
Tartour, Eric
Trautmann, Alain
Bercovici, Nadège
author_sort Thoreau, Maxime
collection PubMed
description Most cancer immunotherapies under present investigation are based on the belief that cytotoxic T cells are the most important anti-tumoral immune cells, whereas intra-tumoral macrophages would rather play a pro-tumoral role. We have challenged this antagonistic point of view and searched for collaborative contributions by tumor-infiltrating T cells and macrophages, reminiscent of those observed in anti-infectious responses. We demonstrate that, in a model of therapeutic vaccination, cooperation between myeloid cells and T cells is indeed required for tumor rejection. Vaccination elicited an early rise of CD11b(+) myeloid cells that preceded and conditioned the intra-tumoral accumulation of CD8(+) T cells. Conversely, CD8(+) T cells and IFNγ production activated myeloid cells were required for tumor regression. A 4-fold reduction of CD8(+) T cell infiltrate in CXCR3KO mice did not prevent tumor regression, whereas a reduction of tumor-infiltrating myeloid cells significantly interfered with vaccine efficiency. We show that macrophages from regressing tumors can kill tumor cells in two ways: phagocytosis and TNFα release. Altogether, our data suggest new strategies to improve the efficiency of cancer immunotherapies, by promoting intra-tumoral cooperation between macrophages and T cells.
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spelling pubmed-46950292016-01-20 Vaccine-induced tumor regression requires a dynamic cooperation between T cells and myeloid cells at the tumor site Thoreau, Maxime Penny, HweiXian Leong Tan, KarWai Regnier, Fabienne Weiss, Julia Miriam Lee, Bernett Johannes, Ludger Dransart, Estelle Le Bon, Agnès Abastado, Jean-Pierre Tartour, Eric Trautmann, Alain Bercovici, Nadège Oncotarget Research Paper Most cancer immunotherapies under present investigation are based on the belief that cytotoxic T cells are the most important anti-tumoral immune cells, whereas intra-tumoral macrophages would rather play a pro-tumoral role. We have challenged this antagonistic point of view and searched for collaborative contributions by tumor-infiltrating T cells and macrophages, reminiscent of those observed in anti-infectious responses. We demonstrate that, in a model of therapeutic vaccination, cooperation between myeloid cells and T cells is indeed required for tumor rejection. Vaccination elicited an early rise of CD11b(+) myeloid cells that preceded and conditioned the intra-tumoral accumulation of CD8(+) T cells. Conversely, CD8(+) T cells and IFNγ production activated myeloid cells were required for tumor regression. A 4-fold reduction of CD8(+) T cell infiltrate in CXCR3KO mice did not prevent tumor regression, whereas a reduction of tumor-infiltrating myeloid cells significantly interfered with vaccine efficiency. We show that macrophages from regressing tumors can kill tumor cells in two ways: phagocytosis and TNFα release. Altogether, our data suggest new strategies to improve the efficiency of cancer immunotherapies, by promoting intra-tumoral cooperation between macrophages and T cells. Impact Journals LLC 2015-08-11 /pmc/articles/PMC4695029/ /pubmed/26337837 Text en Copyright: © 2015 Thoreau et al. http://creativecommons.org/licenses/by/2.5/ 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 credited.
spellingShingle Research Paper
Thoreau, Maxime
Penny, HweiXian Leong
Tan, KarWai
Regnier, Fabienne
Weiss, Julia Miriam
Lee, Bernett
Johannes, Ludger
Dransart, Estelle
Le Bon, Agnès
Abastado, Jean-Pierre
Tartour, Eric
Trautmann, Alain
Bercovici, Nadège
Vaccine-induced tumor regression requires a dynamic cooperation between T cells and myeloid cells at the tumor site
title Vaccine-induced tumor regression requires a dynamic cooperation between T cells and myeloid cells at the tumor site
title_full Vaccine-induced tumor regression requires a dynamic cooperation between T cells and myeloid cells at the tumor site
title_fullStr Vaccine-induced tumor regression requires a dynamic cooperation between T cells and myeloid cells at the tumor site
title_full_unstemmed Vaccine-induced tumor regression requires a dynamic cooperation between T cells and myeloid cells at the tumor site
title_short Vaccine-induced tumor regression requires a dynamic cooperation between T cells and myeloid cells at the tumor site
title_sort vaccine-induced tumor regression requires a dynamic cooperation between t cells and myeloid cells at the tumor site
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4695029/
https://www.ncbi.nlm.nih.gov/pubmed/26337837
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