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Data from Hotspot ESR1 Mutations Are Multimodal and Contextual Modulators of Breast Cancer Metastasis

Posted on 2023-03-31 - 05:03
Abstract

Constitutively active estrogen receptor α (ER/ESR1) mutations have been identified in approximately one-third of ER+ metastatic breast cancers. Although these mutations are known as mediators of endocrine resistance, their potential role in promoting metastatic disease has not yet been mechanistically addressed. In this study, we show the presence of ESR1 mutations exclusively in distant but not local recurrences in five independent breast cancer cohorts. In concordance with transcriptomic profiling of ESR1-mutant tumors, genome-edited ESR1 Y537S and D538G-mutant cell models exhibited a reprogrammed cell adhesive gene network via alterations in desmosome/gap junction genes and the TIMP3/MMP axis, which functionally conferred enhanced cell–cell contacts while decreasing cell-extracellular matrix adhesion. In vivo studies showed ESR1-mutant cells were associated with larger multicellular circulating tumor cell (CTC) clusters with increased compactness compared with ESR1 wild-type CTCs. These preclinical findings translated to clinical observations, where CTC clusters were enriched in patients with ESR1-mutated metastatic breast cancer. Conversely, context-dependent migratory phenotypes revealed cotargeting of Wnt and ER as a vulnerability in a D538G cell model. Mechanistically, mutant ESR1 exhibited noncanonical regulation of several metastatic pathways, including secondary transcriptional regulation and de novo FOXA1-driven chromatin remodeling. Collectively, these data provide evidence for ESR1 mutation–modulated metastasis and suggest future therapeutic strategies for targeting ESR1-mutant breast cancer.

Significance:

Context- and allele-dependent transcriptome and cistrome reprogramming in mutant ESR1 cell models elicit diverse metastatic phenotypes related to cell adhesion and migration, which can be pharmacologically targeted in metastatic breast cancer.

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FUNDING

Susan G. Komen

NCI

Department of Defense

Department of Defense Breakthrough Fellowship

NIH Pathway to Independence

NIH

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Cancer Research

AUTHORS (39)

  • Zheqi Li
    Yang Wu
    Megan E. Yates
    Nilgun Tasdemir
    Amir Bahreini
    Jian Chen
    Kevin M. Levine
    Nolan M. Priedigkeit
    Azadeh Nasrazadani
    Simak Ali
    Laki Buluwela
    Spencer Arnesen
    Jason Gertz
    Jennifer K. Richer
    Benjamin Troness
    Dorraya El-Ashry
    Qiang Zhang
    Lorenzo Gerratana
    Youbin Zhang
    Massimo Cristofanilli

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