Genetics, Treatment, and New Technologies of Hormone Receptor-Positive Breast Cancer

Author:

Sebastian William1,Forchette Lauren1,Donoughe Kelsey1,Lun Yibei1,Verma Anisha1,Liu Tuoen1ORCID

Affiliation:

1. West Virginia School of Osteopathic Medicine, Lewisburg, WV 24901, USA

Abstract

The current molecular classification divides breast cancer into four major subtypes, including luminal A, luminal B, HER2-positive, and basal-like, based on receptor gene expression profiling. Luminal A and luminal B are hormone receptor (HR, estrogen, and/or progesterone receptor)-positive and are the most common subtypes, accounting for around 50–60% and 15–20% of the total breast cancer cases, respectively. The drug treatment for HR-positive breast cancer includes endocrine therapy, HER2-targeted therapy (depending on the HER2 status), and chemotherapy (depending on the risk of recurrence). In this review, in addition to classification, we focused on discussing the important aspects of HR-positive breast cancer, including HR structure and signaling, genetics, including epigenetics and gene mutations, gene expression-based assays, the traditional and new drugs for treatment, and novel or new uses of technology in diagnosis and treatment. Particularly, we have summarized the commonly mutated genes and abnormally methylated genes in HR-positive breast cancer and compared four common gene expression-based assays that are used in breast cancer as prognostic and/or predictive tools in detail, including their clinical use, the factors being evaluated, patient demographics, and the scoring systems. All these topic discussions have not been fully described and summarized within other research or review articles.

Funder

West Virginia School of Osteopathic Medicine intramural grant

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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