Luminal breast cancer identity is determined by loss of glucocorticoid receptor activity

Author:

Prekovic Stefan12ORCID,Chalkiadakis Theofilos2,Roest Merel1,Roden Daniel34,Lutz Catrin5,Schuurman Karianne1ORCID,Opdam Mark5ORCID,Hoekman Liesbeth6ORCID,Abbott Nina1,Tesselaar Tanja1,Wajahat Maliha7,Dwyer Amy R7,Mayayo‐Peralta Isabel1,Gomez Gabriela8ORCID,Altelaar Maarten69ORCID,Beijersbergen Roderick10,Győrffy Balázs1112ORCID,Young Leonie1314,Linn Sabine5,Jonkers Jos5ORCID,Tilley Wayne715ORCID,Hickey Theresa7ORCID,Vareslija Damir814ORCID,Swarbrick Alexander34ORCID,Zwart Wilbert116ORCID

Affiliation:

1. Division of Oncogenomics, Oncode Institute The Netherlands Cancer Institute Amsterdam The Netherlands

2. Center for Molecular Medicine UMC Utrecht Utrecht The Netherlands

3. Cancer Ecosystems Program Garvan Institute of Medical Research Darlinghurst NSW Australia

4. School of Clinical Medicine, Faculty of Medicine and Health UNSW Sydney Sydney NSW Australia

5. Division of Molecular Pathology, Oncode Institute The Netherlands Cancer Institute Amsterdam The Netherlands

6. Mass Spectrometry/Proteomics Facility The Netherlands Cancer Institute Amsterdam The Netherlands

7. Dame Roma Mitchell Cancer Research Laboratories, Adelaide Medical School University of Adelaide Adelaide SA Australia

8. School of Pharmacy and Biomolecular Sciences The Royal College of Surgeons University of Medicine and Health Sciences Dublin Ireland

9. Biomolecular Mass Spectrometry and Proteomics, Bijvoet Center for Biomolecular Research and Utrecht Institute for Pharmaceutical Sciences Utrecht University Utrecht The Netherlands

10. Division of Molecular Carcinogenesis and Robotics and Screening Centre Netherlands Cancer Institute Amsterdam The Netherlands

11. TTK Cancer Biomarker Research Group Institute of Enzymology Budapest Hungary

12. Department of Bioinformatics and 2nd Department of Pediatrics Semmelweis University Budapest Hungary

13. Endocrine Oncology Research Group, Department of Surgery The Royal College of Surgeons University of Medicine and Health Sciences Dublin Ireland

14. Beaumont RCSI Cancer Centre Beaumont Hospital Dublin Ireland

15. Freemasons Centre for Male Health and Wellbeing University of Adelaide Adelaide SA Australia

16. Laboratory of Chemical Biology and Institute for Complex Molecular Systems, Department of Biomedical Engineering Eindhoven University of Technology Eindhoven The Netherlands

Abstract

AbstractGlucocorticoid receptor (GR) is a transcription factor that plays a crucial role in cancer biology. In this study, we utilized an in silico‐designed GR activity signature to demonstrate that GR relates to the proliferative capacity of numerous primary cancer types. In breast cancer, the GR activity status determines luminal subtype identity and has implications for patient outcomes. We reveal that GR engages with estrogen receptor (ER), leading to redistribution of ER on the chromatin. Notably, GR activation leads to upregulation of the ZBTB16 gene, encoding for a transcriptional repressor, which controls growth in ER‐positive breast cancer and associates with prognosis in luminal A patients. In relation to ZBTB16's repressive nature, GR activation leads to epigenetic remodeling and loss of histone acetylation at sites proximal to cancer‐driving genes. Based on these findings, epigenetic inhibitors reduce viability of ER‐positive breast cancer cells that display absence of GR activity. Our findings provide insights into how GR controls ER‐positive breast cancer growth and may have implications for patients' prognostication and provide novel therapeutic candidates for breast cancer treatment.

Funder

KWF Kankerbestrijding

Nederlandse Organisatie voor Wetenschappelijk Onderzoek

Oncode Institute

Publisher

Springer Science and Business Media LLC

Subject

Molecular Medicine

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