Progesterone promotes immunomodulation and tumor development in the murine mammary gland

BACKGROUND: Clinical studies have linked usage of progestins (synthetic progesterone [P4]) to breast cancer risk. However, little is understood regarding the role of native P4, signaling through the progesterone receptor (PR), in breast tumor formation. Recently, we reported a link between PR and im...

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Autores principales: Werner, Lauryn R, Gibson, Katelin A, Goodman, Merit L, Helm, Dominika E, Walter, Katherine R, Holloran, Sean M, Trinca, Gloria M, Hastings, Richard C, Yang, Howard H, Hu, Ying, Wei, Junping, Lei, Gangjun, Yang, Xiao-Yi, Madan, Rashna, Molinolo, Alfredo A, Markiewicz, Mary A, Chalise, Prabhakar, Axelrod, Margaret L, Balko, Justin M, Hunter, Kent W, Hartman, Zachary C, Lange, Carol A, Hagan, Christy R
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BMJ Publishing Group 2021
Materias:
Basic Tumor Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8103939/
https://www.ncbi.nlm.nih.gov/pubmed/33958486
http://dx.doi.org/10.1136/jitc-2020-001710
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author Werner, Lauryn R
Gibson, Katelin A
Goodman, Merit L
Helm, Dominika E
Walter, Katherine R
Holloran, Sean M
Trinca, Gloria M
Hastings, Richard C
Yang, Howard H
Hu, Ying
Wei, Junping
Lei, Gangjun
Yang, Xiao-Yi
Madan, Rashna
Molinolo, Alfredo A
Markiewicz, Mary A
Chalise, Prabhakar
Axelrod, Margaret L
Balko, Justin M
Hunter, Kent W
Hartman, Zachary C
Lange, Carol A
Hagan, Christy R
author_facet Werner, Lauryn R
Gibson, Katelin A
Goodman, Merit L
Helm, Dominika E
Walter, Katherine R
Holloran, Sean M
Trinca, Gloria M
Hastings, Richard C
Yang, Howard H
Hu, Ying
Wei, Junping
Lei, Gangjun
Yang, Xiao-Yi
Madan, Rashna
Molinolo, Alfredo A
Markiewicz, Mary A
Chalise, Prabhakar
Axelrod, Margaret L
Balko, Justin M
Hunter, Kent W
Hartman, Zachary C
Lange, Carol A
Hagan, Christy R
author_sort Werner, Lauryn R
collection PubMed
description BACKGROUND: Clinical studies have linked usage of progestins (synthetic progesterone [P4]) to breast cancer risk. However, little is understood regarding the role of native P4, signaling through the progesterone receptor (PR), in breast tumor formation. Recently, we reported a link between PR and immune signaling pathways, showing that P4/PR can repress type I interferon signaling pathways. Given these findings, we sought to investigate whether P4/PR drive immunomodulation in the mammary gland and promote tumor formation. METHODS: To determine the effect of P4 on immune cell populations in the murine mammary gland, mice were treated with P4 or placebo pellets for 21 days. Immune cell populations in the mammary gland, spleen, and inguinal lymph nodes were subsequently analyzed by flow cytometry. To assess the effect of PR overexpression on mammary gland tumor development as well as immune cell populations in the mammary gland, a transgenic mouse model was used in which PR was overexpressed throughout the entire mouse. Immune cell populations were assessed in the mammary glands, spleens, and inguinal lymph nodes of 6-month-old transgenic and control mice by flow cytometry. Transgenic mice were also monitored for mammary gland tumor development over a 2-year time span. Following development of mammary gland tumors, immune cell populations in the tumors and spleens of transgenic and control mice were analyzed by flow cytometry. RESULTS: We found that mice treated with P4 exhibited changes in the mammary gland indicative of an inhibited immune response compared with placebo-treated mice. Furthermore, transgenic mice with PR overexpression demonstrated decreased numbers of immune cell populations in their mammary glands, lymph nodes, and spleens. On long-term monitoring, we determined that multiparous PR-overexpressing mice developed significantly more mammary gland tumors than control mice. Additionally, tumors from PR-overexpressing mice contained fewer infiltrating immune cells. Finally, RNA sequencing analysis of tumor samples revealed that immune-related gene signatures were lower in tumors from PR-overexpressing mice as compared with control mice. CONCLUSION: Together, these findings offer a novel mechanism of P4-driven mammary gland tumor development and provide rationale in investigating the usage of antiprogestin therapies to promote immune-mediated elimination of mammary gland tumors.
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spelling pubmed-81039392021-05-24 Progesterone promotes immunomodulation and tumor development in the murine mammary gland Werner, Lauryn R Gibson, Katelin A Goodman, Merit L Helm, Dominika E Walter, Katherine R Holloran, Sean M Trinca, Gloria M Hastings, Richard C Yang, Howard H Hu, Ying Wei, Junping Lei, Gangjun Yang, Xiao-Yi Madan, Rashna Molinolo, Alfredo A Markiewicz, Mary A Chalise, Prabhakar Axelrod, Margaret L Balko, Justin M Hunter, Kent W Hartman, Zachary C Lange, Carol A Hagan, Christy R J Immunother Cancer Basic Tumor Immunology BACKGROUND: Clinical studies have linked usage of progestins (synthetic progesterone [P4]) to breast cancer risk. However, little is understood regarding the role of native P4, signaling through the progesterone receptor (PR), in breast tumor formation. Recently, we reported a link between PR and immune signaling pathways, showing that P4/PR can repress type I interferon signaling pathways. Given these findings, we sought to investigate whether P4/PR drive immunomodulation in the mammary gland and promote tumor formation. METHODS: To determine the effect of P4 on immune cell populations in the murine mammary gland, mice were treated with P4 or placebo pellets for 21 days. Immune cell populations in the mammary gland, spleen, and inguinal lymph nodes were subsequently analyzed by flow cytometry. To assess the effect of PR overexpression on mammary gland tumor development as well as immune cell populations in the mammary gland, a transgenic mouse model was used in which PR was overexpressed throughout the entire mouse. Immune cell populations were assessed in the mammary glands, spleens, and inguinal lymph nodes of 6-month-old transgenic and control mice by flow cytometry. Transgenic mice were also monitored for mammary gland tumor development over a 2-year time span. Following development of mammary gland tumors, immune cell populations in the tumors and spleens of transgenic and control mice were analyzed by flow cytometry. RESULTS: We found that mice treated with P4 exhibited changes in the mammary gland indicative of an inhibited immune response compared with placebo-treated mice. Furthermore, transgenic mice with PR overexpression demonstrated decreased numbers of immune cell populations in their mammary glands, lymph nodes, and spleens. On long-term monitoring, we determined that multiparous PR-overexpressing mice developed significantly more mammary gland tumors than control mice. Additionally, tumors from PR-overexpressing mice contained fewer infiltrating immune cells. Finally, RNA sequencing analysis of tumor samples revealed that immune-related gene signatures were lower in tumors from PR-overexpressing mice as compared with control mice. CONCLUSION: Together, these findings offer a novel mechanism of P4-driven mammary gland tumor development and provide rationale in investigating the usage of antiprogestin therapies to promote immune-mediated elimination of mammary gland tumors. BMJ Publishing Group 2021-05-06 /pmc/articles/PMC8103939/ /pubmed/33958486 http://dx.doi.org/10.1136/jitc-2020-001710 Text en © Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ. https://creativecommons.org/licenses/by-nc/4.0/This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See http://creativecommons.org/licenses/by-nc/4.0/ (https://creativecommons.org/licenses/by-nc/4.0/) .
spellingShingle Basic Tumor Immunology
Werner, Lauryn R
Gibson, Katelin A
Goodman, Merit L
Helm, Dominika E
Walter, Katherine R
Holloran, Sean M
Trinca, Gloria M
Hastings, Richard C
Yang, Howard H
Hu, Ying
Wei, Junping
Lei, Gangjun
Yang, Xiao-Yi
Madan, Rashna
Molinolo, Alfredo A
Markiewicz, Mary A
Chalise, Prabhakar
Axelrod, Margaret L
Balko, Justin M
Hunter, Kent W
Hartman, Zachary C
Lange, Carol A
Hagan, Christy R
Progesterone promotes immunomodulation and tumor development in the murine mammary gland
title Progesterone promotes immunomodulation and tumor development in the murine mammary gland
title_full Progesterone promotes immunomodulation and tumor development in the murine mammary gland
title_fullStr Progesterone promotes immunomodulation and tumor development in the murine mammary gland
title_full_unstemmed Progesterone promotes immunomodulation and tumor development in the murine mammary gland
title_short Progesterone promotes immunomodulation and tumor development in the murine mammary gland
title_sort progesterone promotes immunomodulation and tumor development in the murine mammary gland
topic Basic Tumor Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8103939/
https://www.ncbi.nlm.nih.gov/pubmed/33958486
http://dx.doi.org/10.1136/jitc-2020-001710
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