Abstract 4308: BRD8 is a therapeutic vulnerability for overcoming resistance to dual ER/HER2 blockade therapy in HR+/HER2+ breast cancer

Ang Gao; Parth Khatri; Gui Ma; Peng Liu; Mark Burkard; Kari Wisinski; Charles Perou; Huy Dinh; Wei Xu

doi:10.1158/1538-7445.AM2025-4308

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Abstract 4308: BRD8 is a therapeutic vulnerability for overcoming resistance to dual ER/HER2 blockade therapy in HR+/HER2+ breast cancer

Ang Gao, Parth Khatri, Gui Ma, Peng Liu, Mark Burkard, Kari Wisinski, Charles Perou, Huy Dinh and Wei Xu

Cancer research (Chicago, Ill.), Vol.85(8_Supplement_1), pp.4308-4308

04/21/2025

DOI: 10.1158/1538-7445.AM2025-4308

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Abstract

Hormone receptor (HR)-positive, HER2-positive breast cancers often develop resistance to endocrine and anti-HER2 therapies due to the heterogeneous expression of estrogen receptor (ER) and HER2 and the crosstalk of these growth-promoting pathways. However, how anti-HER2 agents activate ER and other growth-promoting pathways remains unknown. Single-cell RNA sequencing of BT474 breast cancer cells identified Bromodomain Containing Protein 8 (BRD8), an acetyl-lysine reader protein in the histone acetylase EP400 complex, as a pivotal mediator to activate ER in response to neratinib treatment. BRD8 expression was rapidly induced by various anti-HER2 agents (neratinib, lapatinib, and trastuzumab), and its depletion disrupted the crosstalk between ER and HER2 signaling pathways and rendered HR+/HER2+ cells and PDxOs more sensitive to anti-HER2 agents. BRD8, ER, and ER target genes are co-induced by neratinib in single-nucleus RNA and ATAC sequencing of a patient-derived xenograft (PDX). SnATAC-seq also reveals that the activated genes share open chromatin regions enriched in ER, forkhead box (FOX), and ETS family transcription factors (TF) binding motifs. FOX family TFs are well-known for regulating estrogen signaling, and ETS proteins have been shown to promote tumorigenesis. Since EP400 enhances H2AZ deposition and acetylation on chromatin, we performed H2AZ and H2AZac ChIP-sequencing in the presence or absence of BRD8 and neratinib treatment. We found that, in response to neratinib treatment, BRD8 activates ER, FOX, and ETS target genes through modulating H2AZac deposition and chromatin decompaction. This finding coincides with RNA-sequencing where BRD8 promotes cell growth in an ER-dependent and -independent manner. In line with these findings, patients who responded poorly to the anti-HER2 therapies exhibited higher levels of BRD8 target gene signature as compared to the responders. Furthermore, BRD8 knockout ablates the ER and HER2 signaling crosstalk and re-sensitizes neratinib-resistant HR+/HER2+ cells to neratinib. In summary, this work not only explains why ER signaling is activated upon anti-HER2 therapies but also identifies BRD8 as a druggable vulnerability for treating HR+/HER2+ breast cancer.

Details

Title: Subtitle: Abstract 4308: BRD8 is a therapeutic vulnerability for overcoming resistance to dual ER/HER2 blockade therapy in HR+/HER2+ breast cancer
Creators: Ang Gao
Parth Khatri
Gui Ma
Peng Liu
Mark Burkard
Kari Wisinski
Charles Perou
Huy Dinh
Wei Xu
Resource Type: Abstract
Publication Details: Cancer research (Chicago, Ill.), Vol.85(8_Supplement_1), pp.4308-4308
Publisher: AMER ASSOC CANCER RESEARCH
DOI: 10.1158/1538-7445.AM2025-4308
ISSN: 0008-5472
eISSN: 1538-7445
Language: English
Date published: 04/21/2025
Academic Unit: Internal Medicine
Record Identifier: 9984813153502771

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