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FOXA1: A Pioneer of Nuclear Receptor Action in Breast Cancer

Darcie D. Seachrist, Lindsey J. Anstine, Ruth A. Keri

2021Cancers67 citationsDOIOpen Access PDF

Abstract

The pioneering function of FOXA1 establishes estrogen-responsive transcriptomes in luminal breast cancer. Dysregulated FOXA1 chromatin occupancy through focal amplification, mutation, or cofactor recruitment modulates estrogen receptor (ER) transcriptional programs and drives endocrine-resistant disease. However, ER is not the sole nuclear receptor (NR) expressed in breast cancers, nor is it the only NR for which FOXA1 serves as a licensing factor. Receptors for androgens, glucocorticoids, and progesterone are also found in the majority of breast cancers, and their functions are also impacted by FOXA1. These NRs interface with ER transcriptional programs and, depending on their activation level, can reprogram FOXA1-ER cistromes. Thus, NR interplay contributes to endocrine therapy response and resistance and may provide a vulnerability for future therapeutic benefit in patients. Herein, we review what is known regarding FOXA1 regulation of NR function in breast cancer in the context of cell identity, endocrine resistance, and NR crosstalk in breast cancer progression and treatment.

Topics & Concepts

FOXA1Breast cancerEstrogen receptorCancer researchNuclear receptorChromatinContext (archaeology)Endocrine systemMedicineBiologyInternal medicineTranscription factorBioinformaticsCancerHormoneGeneticsGenePaleontologyFOXO transcription factor regulationPI3K/AKT/mTOR signaling in cancerEstrogen and related hormone effects
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