Monocytes Differentiate to Immune Suppressive Precursors of Metastasis-Associated Macrophages in Mouse Models of Metastatic Breast Cancer

Metastasis-associated macrophages (MAMs) play pivotal roles in breast cancer metastasis by promoting extravasation and survival of metastasizing cancer cells. In a metastatic breast cancer mouse model, we previously reported that circulating classical monocytes (C-MOs) preferentially migrated into t...

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Autores principales: Kitamura, Takanori, Doughty-Shenton, Dahlia, Cassetta, Luca, Fragkogianni, Stamatina, Brownlie, Demi, Kato, Yu, Carragher, Neil, Pollard, Jeffrey W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5776392/
https://www.ncbi.nlm.nih.gov/pubmed/29387063
http://dx.doi.org/10.3389/fimmu.2017.02004
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author Kitamura, Takanori
Doughty-Shenton, Dahlia
Cassetta, Luca
Fragkogianni, Stamatina
Brownlie, Demi
Kato, Yu
Carragher, Neil
Pollard, Jeffrey W.
author_facet Kitamura, Takanori
Doughty-Shenton, Dahlia
Cassetta, Luca
Fragkogianni, Stamatina
Brownlie, Demi
Kato, Yu
Carragher, Neil
Pollard, Jeffrey W.
author_sort Kitamura, Takanori
collection PubMed
description Metastasis-associated macrophages (MAMs) play pivotal roles in breast cancer metastasis by promoting extravasation and survival of metastasizing cancer cells. In a metastatic breast cancer mouse model, we previously reported that circulating classical monocytes (C-MOs) preferentially migrated into the tumor-challenged lung where they differentiated into MAMs. However, the fate and characteristics of C-MOs in the metastatic site has not been defined. In this study, we identified that adoptively transferred C-MOs (F4/80(low)CD11b(+)Ly6C(+)) differentiated into a distinct myeloid cell population that is characterized as F4/80(high)CD11b(high)Ly6C(high) and gives rise to MAMs (F4/80(low)CD11b(high)Ly6C(low)) within 18 h after migration into the metastatic lung. In mouse models of breast cancer, the CD11b(high)Ly6C(high) MAM precursor cells (MAMPCs) were commonly found in the metastatic lung, and their accumulation was increased during metastatic tumor growth. The morphology and gene expression profile of MAMPCs were distinct from C-MOs and had greater similarity to MAMs. For example MAMPCs expressed mature macrophage markers such as CD14, CD36, CD64, and CD206 at comparable levels with MAMs, suggesting that MAMPCs have committed to a macrophage lineage in the tumor microenvironment. MAMPCs also expressed higher levels of Arg1, Hmox1, and Stab1 than C-MOs to a comparable level to MAMs. Expression of these MAM-associated genes in MAMPCs was reduced by genetic deletion of colony-stimulating factor 1 receptor (CSF1R). On the other hand, transient CSF1R blockade did not reduce the number of MAMPCs in the metastatic site, suggesting that CSF1 signaling is active in MAMPCs but is not required for their accumulation. Functionally MAMPCs suppressed the cytotoxicity of activated CD8(+) T cells in vitro in part through superoxide production. Overall, our results indicate that immediately following migration into the metastatic tumors C-MOs differentiate into immunosuppressive cells that have characteristics of monocytic myeloid-derived suppressor cell phenotype and might be targeted to enhance efficacy of immunotherapy for metastatic breast cancer.
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spelling pubmed-57763922018-01-31 Monocytes Differentiate to Immune Suppressive Precursors of Metastasis-Associated Macrophages in Mouse Models of Metastatic Breast Cancer Kitamura, Takanori Doughty-Shenton, Dahlia Cassetta, Luca Fragkogianni, Stamatina Brownlie, Demi Kato, Yu Carragher, Neil Pollard, Jeffrey W. Front Immunol Immunology Metastasis-associated macrophages (MAMs) play pivotal roles in breast cancer metastasis by promoting extravasation and survival of metastasizing cancer cells. In a metastatic breast cancer mouse model, we previously reported that circulating classical monocytes (C-MOs) preferentially migrated into the tumor-challenged lung where they differentiated into MAMs. However, the fate and characteristics of C-MOs in the metastatic site has not been defined. In this study, we identified that adoptively transferred C-MOs (F4/80(low)CD11b(+)Ly6C(+)) differentiated into a distinct myeloid cell population that is characterized as F4/80(high)CD11b(high)Ly6C(high) and gives rise to MAMs (F4/80(low)CD11b(high)Ly6C(low)) within 18 h after migration into the metastatic lung. In mouse models of breast cancer, the CD11b(high)Ly6C(high) MAM precursor cells (MAMPCs) were commonly found in the metastatic lung, and their accumulation was increased during metastatic tumor growth. The morphology and gene expression profile of MAMPCs were distinct from C-MOs and had greater similarity to MAMs. For example MAMPCs expressed mature macrophage markers such as CD14, CD36, CD64, and CD206 at comparable levels with MAMs, suggesting that MAMPCs have committed to a macrophage lineage in the tumor microenvironment. MAMPCs also expressed higher levels of Arg1, Hmox1, and Stab1 than C-MOs to a comparable level to MAMs. Expression of these MAM-associated genes in MAMPCs was reduced by genetic deletion of colony-stimulating factor 1 receptor (CSF1R). On the other hand, transient CSF1R blockade did not reduce the number of MAMPCs in the metastatic site, suggesting that CSF1 signaling is active in MAMPCs but is not required for their accumulation. Functionally MAMPCs suppressed the cytotoxicity of activated CD8(+) T cells in vitro in part through superoxide production. Overall, our results indicate that immediately following migration into the metastatic tumors C-MOs differentiate into immunosuppressive cells that have characteristics of monocytic myeloid-derived suppressor cell phenotype and might be targeted to enhance efficacy of immunotherapy for metastatic breast cancer. Frontiers Media S.A. 2018-01-17 /pmc/articles/PMC5776392/ /pubmed/29387063 http://dx.doi.org/10.3389/fimmu.2017.02004 Text en Copyright © 2018 Kitamura, Doughty-Shenton, Cassetta, Fragkogianni, Brownlie, Kato, Carragher and Pollard. 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) or licensor 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
Kitamura, Takanori
Doughty-Shenton, Dahlia
Cassetta, Luca
Fragkogianni, Stamatina
Brownlie, Demi
Kato, Yu
Carragher, Neil
Pollard, Jeffrey W.
Monocytes Differentiate to Immune Suppressive Precursors of Metastasis-Associated Macrophages in Mouse Models of Metastatic Breast Cancer
title Monocytes Differentiate to Immune Suppressive Precursors of Metastasis-Associated Macrophages in Mouse Models of Metastatic Breast Cancer
title_full Monocytes Differentiate to Immune Suppressive Precursors of Metastasis-Associated Macrophages in Mouse Models of Metastatic Breast Cancer
title_fullStr Monocytes Differentiate to Immune Suppressive Precursors of Metastasis-Associated Macrophages in Mouse Models of Metastatic Breast Cancer
title_full_unstemmed Monocytes Differentiate to Immune Suppressive Precursors of Metastasis-Associated Macrophages in Mouse Models of Metastatic Breast Cancer
title_short Monocytes Differentiate to Immune Suppressive Precursors of Metastasis-Associated Macrophages in Mouse Models of Metastatic Breast Cancer
title_sort monocytes differentiate to immune suppressive precursors of metastasis-associated macrophages in mouse models of metastatic breast cancer
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5776392/
https://www.ncbi.nlm.nih.gov/pubmed/29387063
http://dx.doi.org/10.3389/fimmu.2017.02004
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