TGFβ-mediated MMP13 secretion drives myoepithelial cell dependent breast cancer progression

Author:

Gibson Shayin V.,Tomas Bort ElenaORCID,Rodríguez-Fernández Lucía,Allen Michael D.ORCID,Gomm Jennifer J.,Goulding Iain,auf dem Keller Ulrich,Agnoletto Andrea,Brisken CathrinORCID,Peck BarrieORCID,Cameron Angus J.,Marshall John F.,Jones J. LouiseORCID,Carter Edward P.ORCID,Grose Richard P.ORCID

Abstract

AbstractDuctal carcinoma in situ (DCIS) is a non-obligate precursor of invasive breast cancer. Virtually all women with DCIS are treated, despite evidence suggesting up to half would remain with stable, non-threatening, disease. Overtreatment thus presents a pressing issue in DCIS management. To understand the role of the normally tumour suppressive myoepithelial cell in disease progression we present a 3D in vitro model incorporating both luminal and myoepithelial cells in physiomimetic conditions. We demonstrate that DCIS-associated myoepithelial cells promote striking myoepithelial-led invasion of luminal cells, mediated by the collagenase MMP13 through a non-canonical TGFβ – EP300 pathway. In vivo, MMP13 expression is associated with stromal invasion in a murine model of DCIS progression and is elevated in myoepithelial cells of clinical high-grade DCIS cases. Our data identify a key role for myoepithelial-derived MMP13 in facilitating DCIS progression and point the way towards a robust marker for risk stratification in DCIS patients.

Funder

Cancer Research UK

Breast Cancer Now

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Radiology, Nuclear Medicine and imaging,Oncology

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