Liver X receptors induce antiproliferative effects in basal‐like breast cancer

Author:

Haugen Mads Haugland1,von der Lippe Gythfeldt Hedda1234ORCID,Egeland Eivind Valen1,Svartdal Normann Lisa15,Pandya Abhilash D.1,Vedin Lise‐Lotte6,Juell Siri1,Tenstad Ellen1,Øy Geir Frode1,Kristian Alexandr1,Marangoni Elisabetta7ORCID,Sørlie Therese24,Steffensen Knut6,Mælandsmo Gunhild Mari18,Engebraaten Olav134ORCID

Affiliation:

1. Department of Tumor Biology Oslo University Hospital Oslo Norway

2. Department of Cancer Genetics, Institute for Cancer Research Oslo University Hospital Norway

3. Department of Oncology Oslo University Hospital Norway

4. Insitute for Clinical Medicine University of Oslo Norway

5. Department of Research and Innovation Vestre Viken Hospital Trust Drammen Norway

6. Division of Clinical Chemistry, Department of Laboratory Medicine Karolinska Institutet Stockholm Sweden

7. Translational Research Department, Institut Curie PSL Research University Paris France

8. Department of Medical Biology, Faculty of Health Sciences The Arctic University of Norway‐University of Tromsø Norway

Abstract

Liver X receptors (LXRs) are nuclear transcription factors important in the regulation of cholesterol transport, and glucose and fatty acid metabolism. The antiproliferative role of LXRs has been studied in a variety of malignancies and may represent a therapeutic opportunity in cancers lacking targeted therapies, such as triple‐negative breast cancer. In this study, we investigated the impact of LXR agonists alone and in combination with carboplatin in preclinical models of breast cancer. In vitro experiments revealed a dose‐dependent decrease in tumor cell proliferation in estrogen receptor‐positive breast cancer cells, whereas LXR activation in vivo resulted in an increased growth inhibitory effect in a basal‐like breast cancer model (in combination with carboplatin). Functional proteomic analysis identified differences in protein expression between responding and nonresponding models related to Akt activity, cell‐cycle progression, and DNA repair. Furthermore, pathway analysis suggested that the LXR agonist in combination with carboplatin inhibits the activity of targets of E2F transcription factors and affects cholesterol homeostasis in basal‐like breast cancer.

Funder

Helse Sør-Øst RHF

National Institutes of Health

Publisher

Wiley

Subject

Cancer Research,Genetics,Molecular Medicine,General Medicine,Oncology

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