Single Dose of a Small Molecule Leads to Complete Regressions of Large Breast Tumors in Mice

Overview

Journal ACS Cent Sci

Specialty Chemistry

Date 2025 Mar 3

PMID 40028352

Authors

Michael P Mulligan

Matthew W Boudreau

Brooke A Bouwens

Yoongyeong Lee

Hunter W Carrell

Junyao Zhu

Spyro Mousses

David J Shapiro

Erik R Nelson

Timothy M Fan

Paul J Hergenrother

Affiliations

Soon will be listed here.

Abstract

Patients with estrogen receptor α positive (ERα+) breast cancer typically undergo surgical resection, followed by 5-10 years of treatment with adjuvant endocrine therapy. This prolonged intervention is associated with a host of undesired side effects that reduce patient compliance, and ultimately therapeutic resistance and disease relapse/progression are common. An ideal anticancer therapy would be effective against recurrent and refractory disease with minimal dosing; however, there is little precedent for marked tumor regression with a single dose of a small molecule therapeutic. Herein we report as a small molecule that induces quantitative or near-quantitative regression of tumors in multiple mouse models of breast cancer with a single dose. Importantly, this effect is robust and independent of tumor size with eradication of even very large tumors (500-1500 mm) observed. Mechanistically, these tumor regressions are a consequence of rapid induction of necrotic cell death in the tumor and are immune cell independent. If successfully translated to human cancer patients, the benefits of such an anticancer drug that is effective with a single dose would be significant.

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