Litcius/Paper detail

Androgen Receptor in Hormone Receptor-Positive Breast Cancer

Ashfia Fatima Khan, Samaneh Karami, Anthony S. Peidl, Kacie D. Waiters, Mariam Funmi Babajide, Tasneem Bawa‐Khalfe

2023International Journal of Molecular Sciences13 citationsDOIOpen Access PDF

Abstract

Breast cancer subtypes expressing hormone receptors (HR+ BCa) have a good prognosis and respond to first-line endocrine therapy (ET). However, the majority of HR+ BCa patients exhibit intrinsic or acquired ET resistance (ET-R) and rapid onset of incurable metastatic BCa. With the failure of conventional ET, limited targeted therapy exists for ET-R HR+ BCa patients. The androgen receptor (AR) in HR-negative BCa subtypes is emerging as an attractive alternative target for therapy. The AR drives Luminal AR (LAR) triple-negative breast cancer progression, and LAR patients consistently exhibit positive clinical benefits with AR antagonists in clinical trials. In contrast, the function of the AR in HR+ BCa is more conflicting. AR in HR+ BCa correlates with a favorable prognosis, and yet, the AR supports the development of ET-R BCa. While AR antagonists were ineffective, ongoing clinical trials with a selective AR modulator have shown promise for HR+ BCa patients. To understand the incongruent actions of ARs in HR+ BCa, the current review discusses how the structure and post-translational modification impact AR function. Additionally, completed and ongoing clinical trials with FDA-approved AR-targeting agents for BCa are presented. Finally, we identify promising investigational small molecules and chimera drugs for future HR+ BCa therapy.

Topics & Concepts

Androgen receptorMedicineClinical trialInternal medicineOncologyBreast cancerReceptorTriple-negative breast cancerCancerProstate cancerEstrogen and related hormone effectsAdvanced Breast Cancer TherapiesHER2/EGFR in Cancer Research