Osteoblast-Derived Paracrine and Juxtacrine Signals Protect Disseminated Breast Cancer Cells from Stress

Osteoblast-Derived Paracrine and Juxtacrine Signals Protect Disseminated Breast Cancer Cells from Stress

Metastatic breast cancer in bone is incurable and there is an urgent need to develop new therapeutic approaches to improve survival. Key to this is understanding the mechanisms governing cancer cell survival and growth in bone, which involves interplay between malignant and accessory cell types. Her...

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Main Authors: Russell Hughes, Xinyue Chen, Natasha Cowley, Penelope D. Ottewell, Rhoda J. Hawkins, Keith D. Hunter, Jamie K. Hobbs, Nicola J. Brown, Ingunn Holen
Format: Article
Language:English
Published: MDPI AG 2021-03-01
Series:Cancers
Subjects:
skeletal
metastasis
dormancy
latency
breast cancer
Online Access:https://www.mdpi.com/2072-6694/13/6/1366
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spelling doaj-8c31729609b5434984e8fcbac523fc762021-03-19T00:00:29ZengMDPI AGCancers2072-66942021-03-01131366136610.3390/cancers13061366Osteoblast-Derived Paracrine and Juxtacrine Signals Protect Disseminated Breast Cancer Cells from StressRussell Hughes0Xinyue Chen1Natasha Cowley2Penelope D. Ottewell3Rhoda J. Hawkins4Keith D. Hunter5Jamie K. Hobbs6Nicola J. Brown7Ingunn Holen8Department of Oncology and Metabolism, University of Sheffield, and Experimental Cancer Medicine Centre, Sheffield S10 2RX, UKDepartment of Oncology and Metabolism, University of Sheffield, and Experimental Cancer Medicine Centre, Sheffield S10 2RX, UKDepartment of Physics and Astronomy, University of Sheffield, Sheffield S3 7RH, UKDepartment of Oncology and Metabolism, University of Sheffield, and Experimental Cancer Medicine Centre, Sheffield S10 2RX, UKDepartment of Physics and Astronomy, University of Sheffield, Sheffield S3 7RH, UKSchool of Clinical Dentistry, University of Sheffield, Sheffield S10 2TA, UKDepartment of Physics and Astronomy, University of Sheffield, Sheffield S3 7RH, UKDepartment of Oncology and Metabolism, University of Sheffield, and Experimental Cancer Medicine Centre, Sheffield S10 2RX, UKDepartment of Oncology and Metabolism, University of Sheffield, and Experimental Cancer Medicine Centre, Sheffield S10 2RX, UKMetastatic breast cancer in bone is incurable and there is an urgent need to develop new therapeutic approaches to improve survival. Key to this is understanding the mechanisms governing cancer cell survival and growth in bone, which involves interplay between malignant and accessory cell types. Here, we performed a cellular and molecular comparison of the bone microenvironment in mouse models representing either metastatic indolence or growth, to identify mechanisms regulating cancer cell survival and fate. In vivo, we show that regardless of their fate, breast cancer cells in bone occupy niches rich in osteoblastic cells. As the number of osteoblasts in bone declines, so does the ability to sustain large numbers of breast cancer cells and support metastatic outgrowth. In vitro, osteoblasts protected breast cancer cells from death induced by cell stress and signaling via gap junctions was found to provide important juxtacrine protective mechanisms between osteoblasts and both MDA-MB-231 (TNBC) and MCF7 (ER<sup>+</sup>) breast cancer cells. Combined with mathematical modelling, these findings indicate that the fate of DTCs is not controlled through the association with specific vessel subtypes. Instead, numbers of osteoblasts dictate availability of protective niches which breast cancer cells can colonize prior to stimulation of metastatic outgrowth.https://www.mdpi.com/2072-6694/13/6/1366skeletalmetastasisdormancylatencybreast cancer
collection DOAJ
language English
format Article
sources DOAJ
author Russell Hughes
Xinyue Chen
Natasha Cowley
Penelope D. Ottewell
Rhoda J. Hawkins
Keith D. Hunter
Jamie K. Hobbs
Nicola J. Brown
Ingunn Holen
spellingShingle Russell Hughes
Xinyue Chen
Natasha Cowley
Penelope D. Ottewell
Rhoda J. Hawkins
Keith D. Hunter
Jamie K. Hobbs
Nicola J. Brown
Ingunn Holen
Osteoblast-Derived Paracrine and Juxtacrine Signals Protect Disseminated Breast Cancer Cells from Stress
Cancers
skeletal
metastasis
dormancy
latency
breast cancer
author_facet Russell Hughes
Xinyue Chen
Natasha Cowley
Penelope D. Ottewell
Rhoda J. Hawkins
Keith D. Hunter
Jamie K. Hobbs
Nicola J. Brown
Ingunn Holen
author_sort Russell Hughes
title Osteoblast-Derived Paracrine and Juxtacrine Signals Protect Disseminated Breast Cancer Cells from Stress
title_short Osteoblast-Derived Paracrine and Juxtacrine Signals Protect Disseminated Breast Cancer Cells from Stress
title_full Osteoblast-Derived Paracrine and Juxtacrine Signals Protect Disseminated Breast Cancer Cells from Stress
title_fullStr Osteoblast-Derived Paracrine and Juxtacrine Signals Protect Disseminated Breast Cancer Cells from Stress
title_full_unstemmed Osteoblast-Derived Paracrine and Juxtacrine Signals Protect Disseminated Breast Cancer Cells from Stress
title_sort osteoblast-derived paracrine and juxtacrine signals protect disseminated breast cancer cells from stress
publisher MDPI AG
series Cancers
issn 2072-6694
publishDate 2021-03-01
description Metastatic breast cancer in bone is incurable and there is an urgent need to develop new therapeutic approaches to improve survival. Key to this is understanding the mechanisms governing cancer cell survival and growth in bone, which involves interplay between malignant and accessory cell types. Here, we performed a cellular and molecular comparison of the bone microenvironment in mouse models representing either metastatic indolence or growth, to identify mechanisms regulating cancer cell survival and fate. In vivo, we show that regardless of their fate, breast cancer cells in bone occupy niches rich in osteoblastic cells. As the number of osteoblasts in bone declines, so does the ability to sustain large numbers of breast cancer cells and support metastatic outgrowth. In vitro, osteoblasts protected breast cancer cells from death induced by cell stress and signaling via gap junctions was found to provide important juxtacrine protective mechanisms between osteoblasts and both MDA-MB-231 (TNBC) and MCF7 (ER<sup>+</sup>) breast cancer cells. Combined with mathematical modelling, these findings indicate that the fate of DTCs is not controlled through the association with specific vessel subtypes. Instead, numbers of osteoblasts dictate availability of protective niches which breast cancer cells can colonize prior to stimulation of metastatic outgrowth.
topic skeletal
metastasis
dormancy
latency
breast cancer
url https://www.mdpi.com/2072-6694/13/6/1366
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AT xinyuechen osteoblastderivedparacrineandjuxtacrinesignalsprotectdisseminatedbreastcancercellsfromstress
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