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An independent poor-prognosis subtype of breast cancer defined by a distinct tumor immune microenvironment

Author

Listed:
  • Xavier Tekpli

    (Institute for Cancer Research, Oslo University Hospital)

  • Tonje Lien

    (Institute for Cancer Research, Oslo University Hospital)

  • Andreas Hagen Røssevold

    (Institute for Cancer Research, Oslo University Hospital
    Oslo University Hospital)

  • Daniel Nebdal

    (Institute for Cancer Research, Oslo University Hospital)

  • Elin Borgen

    (Oslo University Hospital)

  • Hege Oma Ohnstad

    (Oslo University Hospital)

  • Jon Amund Kyte

    (Institute for Cancer Research, Oslo University Hospital
    Oslo University Hospital)

  • Johan Vallon-Christersson

    (Lund University)

  • Marie Fongaard

    (Institute for Cancer Research, Oslo University Hospital)

  • Eldri Undlien Due

    (Institute for Cancer Research, Oslo University Hospital)

  • Lisa Gregusson Svartdal

    (Oslo University Hospital)

  • My Anh Tu Sveli

    (Oslo University Hospital)

  • Øystein Garred

    (Oslo University Hospital)

  • Arnoldo Frigessi

    (Oslo Centre for Biostatistics and Epidemiology, University of Oslo and Research Support Services, Oslo University Hospital)

  • Kristine Kleivi Sahlberg

    (Institute for Cancer Research, Oslo University Hospital
    Vestre Viken Hospital Trust)

  • Therese Sørlie

    (Institute for Cancer Research, Oslo University Hospital
    Centre for Cancer Biomarkers CCBIO)

  • Hege G. Russnes

    (Institute for Cancer Research, Oslo University Hospital
    Oslo University Hospital)

  • Bjørn Naume

    (Oslo University Hospital
    University of Oslo)

  • Vessela N. Kristensen

    (Institute for Cancer Research, Oslo University Hospital
    Centre for Cancer Biomarkers CCBIO
    Akershus University Hospital)

Abstract

How mixtures of immune cells associate with cancer cell phenotype and affect pathogenesis is still unclear. In 15 breast cancer gene expression datasets, we invariably identify three clusters of patients with gradual levels of immune infiltration. The intermediate immune infiltration cluster (Cluster B) is associated with a worse prognosis independently of known clinicopathological features. Furthermore, immune clusters are associated with response to neoadjuvant chemotherapy. In silico dissection of the immune contexture of the clusters identified Cluster A as immune cold, Cluster C as immune hot while Cluster B has a pro-tumorigenic immune infiltration. Through phenotypical analysis, we find epithelial mesenchymal transition and proliferation associated with the immune clusters and mutually exclusive in breast cancers. Here, we describe immune clusters which improve the prognostic accuracy of immune contexture in breast cancer. Our discovery of a novel independent prognostic factor in breast cancer highlights a correlation between tumor phenotype and immune contexture.

Suggested Citation

  • Xavier Tekpli & Tonje Lien & Andreas Hagen Røssevold & Daniel Nebdal & Elin Borgen & Hege Oma Ohnstad & Jon Amund Kyte & Johan Vallon-Christersson & Marie Fongaard & Eldri Undlien Due & Lisa Gregusson, 2019. "An independent poor-prognosis subtype of breast cancer defined by a distinct tumor immune microenvironment," Nature Communications, Nature, vol. 10(1), pages 1-14, December.
  • Handle: RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-13329-5
    DOI: 10.1038/s41467-019-13329-5
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