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ESR1 mutant breast cancers show elevated basal cytokeratins and immune activation

Author

Listed:
  • Zheqi Li

    (University of Pittsburgh
    UPMC Hillman Cancer Center
    Magee-Womens Research Institute)

  • Olivia McGinn

    (UPMC Hillman Cancer Center
    Magee-Womens Research Institute)

  • Yang Wu

    (UPMC Hillman Cancer Center
    Magee-Womens Research Institute
    Tsinghua University)

  • Amir Bahreini

    (UPMC Hillman Cancer Center
    Magee-Womens Research Institute
    University of Pittsburgh)

  • Nolan M. Priedigkeit

    (University of Pittsburgh
    UPMC Hillman Cancer Center
    Magee-Womens Research Institute)

  • Kai Ding

    (UPMC Hillman Cancer Center
    Magee-Womens Research Institute)

  • Sayali Onkar

    (UPMC Hillman Cancer Center
    Magee-Womens Research Institute
    University of Pittsburgh
    UPMC Hillman Cancer Center)

  • Caleb Lampenfeld

    (University of Pittsburgh
    UPMC Hillman Cancer Center
    UPMC Hillman Cancer Center)

  • Carol A. Sartorius

    (University of Colorado Anschutz Medical Campus)

  • Lori Miller

    (UPMC Hillman Cancer Center
    Magee-Womens Research Institute)

  • Margaret Rosenzweig

    (University of Pittsburgh)

  • Ofir Cohen

    (Dana-Farber Cancer Institute, Harvard Medical School
    Brigham and Women’s Hospital)

  • Nikhil Wagle

    (Dana-Farber Cancer Institute, Harvard Medical School
    Brigham and Women’s Hospital)

  • Jennifer K. Richer

    (University of Colorado Anschutz Medical Campus)

  • William J. Muller

    (McGill University)

  • Laki Buluwela

    (Hammersmith Hospital Campus)

  • Simak Ali

    (Hammersmith Hospital Campus)

  • Tullia C. Bruno

    (University of Pittsburgh
    UPMC Hillman Cancer Center
    UPMC Hillman Cancer Center)

  • Dario A. A. Vignali

    (University of Pittsburgh
    UPMC Hillman Cancer Center
    UPMC Hillman Cancer Center)

  • Yusi Fang

    (University of Pittsburgh)

  • Li Zhu

    (University of Pittsburgh)

  • George C. Tseng

    (University of Pittsburgh)

  • Jason Gertz

    (University of Utah)

  • Jennifer M. Atkinson

    (University of Pittsburgh
    UPMC Hillman Cancer Center
    Magee-Womens Research Institute)

  • Adrian V. Lee

    (University of Pittsburgh
    UPMC Hillman Cancer Center
    Magee-Womens Research Institute
    University of Pittsburgh)

  • Steffi Oesterreich

    (University of Pittsburgh
    UPMC Hillman Cancer Center
    Magee-Womens Research Institute
    University of Pittsburgh)

Abstract

Estrogen receptor alpha (ER/ESR1) is frequently mutated in endocrine resistant ER-positive (ER+) breast cancer and linked to ligand-independent growth and metastasis. Despite the distinct clinical features of ESR1 mutations, their role in intrinsic subtype switching remains largely unknown. Here we find that ESR1 mutant cells and clinical samples show a significant enrichment of basal subtype markers, and six basal cytokeratins (BCKs) are the most enriched genes. Induction of BCKs is independent of ER binding and instead associated with chromatin reprogramming centered around a progesterone receptor-orchestrated insulated neighborhood. BCK-high ER+ primary breast tumors exhibit a number of enriched immune pathways, shared with ESR1 mutant tumors. S100A8 and S100A9 are among the most induced immune mediators and involve in tumor-stroma paracrine crosstalk inferred by single-cell RNA-seq from metastatic tumors. Collectively, these observations demonstrate that ESR1 mutant tumors gain basal features associated with increased immune activation, encouraging additional studies of immune therapeutic vulnerabilities.

Suggested Citation

  • Zheqi Li & Olivia McGinn & Yang Wu & Amir Bahreini & Nolan M. Priedigkeit & Kai Ding & Sayali Onkar & Caleb Lampenfeld & Carol A. Sartorius & Lori Miller & Margaret Rosenzweig & Ofir Cohen & Nikhil Wa, 2022. "ESR1 mutant breast cancers show elevated basal cytokeratins and immune activation," Nature Communications, Nature, vol. 13(1), pages 1-18, December.
    • Handle: RePEc:nat:natcom:v:13:y:2022:i:1:d:10.1038_s41467-022-29498-9
    DOI: 10.1038/s41467-022-29498-9
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