ERα Dysfunction Caused by ESR1 Mutations and Therapeutic Pressure Promotes Lineage Plasticity in ER Breast Cancer

Overview

Journal Nat Cancer

Date 2025 Jan 13

PMID 39805955

Authors

Jackson Liang

Xiaosai Yao

Patrick Aouad

Bu-Er Wang

Lisa Crocker

Subhra Chaudhuri

Yuxin Liang

Spyros Darmanis

Jennifer Giltnane

Heather M Moore

Junko Aimi

Ching-Wei Chang

Mary R Gates

Jennifer Eng-Wong

Marc Hafner

Ciara Metcalfe

Affiliations

Soon will be listed here.

Abstract

Multiple next-generation molecules targeting estrogen receptor α (ERα) are being investigated in breast cancer clinical trials, encompassing thousands of women globally. Development of these molecules was partly motivated by the discovery of resistance-associated mutations in ESR1 (encodes ERα). Here, we studied the impact of ERα antagonist/degraders against Esr1 mutations expressed in mouse mammary glands. Inhibition of mutant ERα induced mixed-lineage cells, characterized by aberrant co-engagement of normally disparate master transcription factors. Lineage infidelity was also observed in Esr1-wild-type mice upon long-term estrogen deprivation. In ER breast cancer biopsy specimens, heavily pretreated tumors with no ESR1 mutation detected (NMD) frequently exhibited mixed-lineage features. ESR1-mutant tumors generally retained luminal features and higher ERα activity and exhibited an anti-proliferative response to the ERα antagonist giredestrant. ESR1-mutant tumors acquired mixed-lineage features following treatment. Lineage heterogeneity in advanced ER breast cancer may underpin the differential benefit of investigational ERα therapeutics observed in ESR1-mutant versus NMD contexts.

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