Age-associated microenvironmental changes highlight the role of PDGF-C in ER+ breast cancer metastatic relapse

Author:

Turrell Frances K.,Orha Rebecca,Guppy Naomi J.,Gillespie Andrea,Guelbert Matthew,Starling Chris,Haider SyedORCID,Isacke Clare M.ORCID

Abstract

AbstractPatients with estrogen receptor (ER)-positive breast cancer are at risk of metastatic relapse for decades after primary tumor resection and treatment, a consequence of dormant disseminated tumor cells (DTCs) reawakening at secondary sites. Here we use syngeneic ER+ mouse models in which DTCs display a dormant phenotype in young mice but accelerated metastatic outgrowth in an aged or fibrotic microenvironment. In young mice, low-level Pdgfc expression by ER+ DTCs is required for their maintenance in secondary sites but is insufficient to support development of macrometastases. By contrast, the platelet-derived growth factor (PDGF)-Chi environment of aging or fibrotic lungs promotes DTC proliferation and upregulates tumor cell Pdgfc expression stimulating further stromal activation, events that can be blocked by pharmacological inhibition of PDGFRα or with a PDGF-C-blocking antibody. These results highlight the role of the changing microenvironment in regulating DTC outgrowth and the opportunity to target PDGF-C signaling to limit metastatic relapse in ER+ breast cancer.

Funder

Breast Cancer Now

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Oncology

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