Precision therapeutics and emerging strategies for HR-positive metastatic breast cancer Review


Authors: Lloyd, M. R.; Jhaveri, K.; Kalinsky, K.; Bardia, A.; Wander, S. A.
Review Title: Precision therapeutics and emerging strategies for HR-positive metastatic breast cancer
Abstract: Anti-oestrogen-based therapies, often combined with a CDK4/6 inhibitor, are the current standard-of-care first-line therapy for patients with advanced-stage hormone receptor-positive (HR+) breast cancer. Resistance to anti-oestrogen agents inevitably occurs, mediated by oestrogen receptor (ER)-dependent or ER-independent mechanisms that drive tumour progression. Emerging endocrine therapies include, but are not limited to, next-generation oral ER degraders and proteolysis targeting chimeras, which might be particularly effective in patients with ESR1-mutant breast cancer. Furthermore, cancers harbouring driver alterations in oncogenic signalling pathways, including AKT and PI3K, might be susceptible to novel combination strategies involving targeted inhibitors. Next-generation CDK2/4 inhibitors are an area of active clinical investigation, and efforts are ongoing to evaluate the role of sequential CDK inhibition. Approved and emerging antibody–drug conjugates exploiting novel target antigens have also demonstrated promising clinical activity. These novel agents, as well as further identification and characterization of predictive biomarkers, will hopefully continue to improve clinical outcomes, reduce the incidence of toxicities, and limit the extent of overtreatment in this population. In this Review, we describe the evolving treatment paradigm for patients with metastatic HR+ breast cancer in light of the growing armamentarium of drugs and biomarkers that will help to shape the future therapeutic landscape. These strategies are expected to involve tumour molecular profiling to enable the delivery of precision medicine. © Springer Nature Limited 2024.
Keywords: signal transduction; genetics; review; biological marker; metabolism; metastasis; breast cancer; pathology; breast neoplasms; drug combination; breast tumor; neoplasm metastasis; receptors, estrogen; tumor growth; estrogen receptor; drug therapy; metastatic breast cancer; therapy; personalized medicine; molecularly targeted therapy; molecular targeted therapy; procedures; first-line treatment; humans; human; female; precision medicine; hormone receptor positive breast cancer; pharmacoeconomics; antibody drug conjugate; molecular fingerprinting; neoplastic cell transformation; proteolysis targeting chimera
Journal Title: Nature Reviews Clinical Oncology
Volume: 21
Issue: 10
ISSN: 1759-4774
Publisher: Nature Publishing Group  
Date Published: 2024-01-01
Start Page: 743
End Page: 761
Language: English
DOI: 10.1038/s41571-024-00935-6
PUBMED: 39179659
PROVIDER: scopus
DOI/URL:
Notes: Review -- Source: Scopus
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  1. Komal Lachhman Jhaveri
    201 Jhaveri