Fatty Acid Synthase Confers Tamoxifen Resistance to ER+/HER2+ Breast Cancer

Javier A Menendez; Adriana Papadimitropoulou; Travis Vander Steen; Elisabet Cuyàs; Bharvi P Oza-Gajera; Sara Verdura; Ingrid Espinoza; Luciano Vellon; Inderjit Mehmi; Ruth Lupu

doi:10.3390/cancers13051132

Fatty Acid Synthase Confers Tamoxifen Resistance to ER+/HER2+ Breast Cancer

Cancers (Basel). 2021 Mar 6;13(5):1132. doi: 10.3390/cancers13051132.

Authors

Javier A Menendez^{1

2}, Adriana Papadimitropoulou³, Travis Vander Steen⁴, Elisabet Cuyàs^{1

2}, Bharvi P Oza-Gajera⁵, Sara Verdura^{1

2}, Ingrid Espinoza^{6

7}, Luciano Vellon⁸, Inderjit Mehmi⁹, Ruth Lupu^{4

10

11}

Affiliations

¹ Metabolism and Cancer Group, Program Against Cancer Therapeutic Resistance (ProCURE), Catalan Institute of Oncology, 17007 Girona, Spain.
² Girona Biomedical Research Institute (IDIBGI), 17190 Girona, Spain.
³ Center of Basic Research, Biomedical Research Foundation of the Academy of Athens, 115 27 Athens, Greece.
⁴ Department of Laboratory Medicine and Pathology, Division of Experimental Pathology, Mayo Clinic, Rochester, MN 55905, USA.
⁵ Division of Nephrology, University of Cincinnati, Cincinnati, OH 45267, USA.
⁶ School of Population Health, University of Mississippi Medical Center, Jackson, MO 39216, USA.
⁷ Cancer Institute, School of Medicine, University of Mississippi Medical Center, Jackson, MO 39216, USA.
⁸ Stem Cells Laboratory, Institute of Biology and Experimental Medicine (IBYME-CONICET), Buenos Aires C1428ADN, Argentina.
⁹ The Angeles Clinic & Research Institute, Cedar Sinai affiliate, Los Angeles, CA 90025, USA.
¹⁰ Department of Biochemistry and Molecular Biology Laboratory, Mayo Clinic Minnesota, Rochester, MN 55905, USA.
¹¹ Mayo Clinic Cancer Center, Rochester, MN 55905, USA.

Abstract

The identification of clinically important molecular mechanisms driving endocrine resistance is a priority in estrogen receptor-positive (ER+) breast cancer. Although both genomic and non-genomic cross-talk between the ER and growth factor receptors such as human epidermal growth factor receptor 2 (HER2) has frequently been associated with both experimental and clinical endocrine therapy resistance, combined targeting of ER and HER2 has failed to improve overall survival in endocrine non-responsive disease. Herein, we questioned the role of fatty acid synthase (FASN), a lipogenic enzyme linked to HER2-driven breast cancer aggressiveness, in the development and maintenance of hormone-independent growth and resistance to anti-estrogens in ER/HER2-positive (ER+/HER2+) breast cancer. The stimulatory effects of estradiol on FASN gene promoter activity and protein expression were blunted by anti-estrogens in endocrine-responsive breast cancer cells. Conversely, an AKT/MAPK-related constitutive hyperactivation of FASN gene promoter activity was unaltered in response to estradiol in non-endocrine responsive ER+/HER2+ breast cancer cells, and could be further enhanced by tamoxifen. Pharmacological blockade with structurally and mechanistically unrelated FASN inhibitors fully impeded the strong stimulatory activity of tamoxifen on the soft-agar colony forming capacity-an in vitro metric of tumorigenicity-of ER+/HER2+ breast cancer cells. In vivo treatment with a FASN inhibitor completely prevented the agonistic tumor-promoting activity of tamoxifen and fully restored its estrogen antagonist properties against ER/HER2-positive xenograft tumors in mice. Functional cancer proteomic data from The Cancer Proteome Atlas (TCPA) revealed that the ER+/HER2+ subtype was the highest FASN protein expressor compared to basal-like, HER2-enriched, and ER+/HER2-negative breast cancer groups. FASN is a biological determinant of HER2-driven endocrine resistance in ER+ breast cancer. Next-generation, clinical-grade FASN inhibitors may be therapeutically relevant to countering resistance to tamoxifen in FASN-overexpressing ER+/HER2+ breast carcinomas.

Keywords: HER2; endocrine resistance; estrogen receptor; fatty acid synthase; tamoxifen.

Abstract

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