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Breast cancer genome and transcriptome integration implicates specific mutational signatures with immune cell infiltration

Author

Listed:
  • Marcel Smid

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

  • F. Germán Rodríguez-González

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

  • Anieta M. Sieuwerts

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

  • Roberto Salgado

    (Breast Cancer Translational Research Laboratory, Université Libre de Bruxelles
    Department of Pathology/TCRU GZA)

  • Wendy J. C. Prager-Van der Smissen

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

  • Michelle van der Vlugt-Daane

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

  • Anne van Galen

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

  • Serena Nik-Zainal

    (Wellcome Trust Sanger Institute
    East Anglian Medical Genetics Service, Cambridge University Hospitals NHS Foundation Trust)

  • Johan Staaf

    (Lund University)

  • Arie B. Brinkman

    (Faculty of Science, Radboud Institute for Molecular Life Sciences, Radboud University Nijmegen)

  • Marc J. van de Vijver

    (Academic Medical Center)

  • Andrea L. Richardson

    (Brigham and Women's Hospital
    Dana-Farber Cancer Institute)

  • Aquila Fatima

    (Erasmus MC Cancer Institute, Erasmus University Medical Center)

  • Kim Berentsen

    (Faculty of Science, Radboud Institute for Molecular Life Sciences, Radboud University Nijmegen)

  • Adam Butler

    (Wellcome Trust Sanger Institute)

  • Sancha Martin

    (Wellcome Trust Sanger Institute)

  • Helen R. Davies

    (Wellcome Trust Sanger Institute)

  • Reno Debets

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

  • Marion E. Meijer-Van Gelder

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

  • Carolien H. M. van Deurzen

    (Erasmus MC Cancer Institute, Erasmus University Medical Center)

  • Gaëtan MacGrogan

    (Département de Biopathologie,)

  • Gert G. G. M. Van den Eynden

    (Department of Pathology/TCRU GZA
    Molecular Immunology Unit, Jules Bordet Institute)

  • Colin Purdie

    (Ninewells Hospital & Medical School)

  • Alastair M. Thompson

    (Ninewells Hospital & Medical School)

  • Carlos Caldas

    (Cancer Research UK Cambridge Institute, University of Cambridge)

  • Paul N. Span

    (Radboud University Medical Center
    Radboud University Medical Center)

  • Peter T. Simpson

    (The University of Queensland: UQ Centre for Clinical Research and School of Medicine)

  • Sunil R. Lakhani

    (The University of Queensland: UQ Centre for Clinical Research and School of Medicine
    Pathology Queensland, The Royal Brisbane and Women's Hospital)

  • Steven Van Laere

    (Center for Oncological Research, University of Antwerp & GZA Hospitals Sint-Augustinus)

  • Christine Desmedt

    (Breast Cancer Translational Research Laboratory, Université Libre de Bruxelles)

  • Markus Ringnér

    (Lund University)

  • Stefania Tommasi

    (IRCCS Istituto Tumori ‘Giovanni Paolo II’)

  • Jorunn Eyford

    (Cancer Research Laboratory, Faculty of Medicine, University of Iceland)

  • Annegien Broeks

    (The Netherlands Cancer Institute)

  • Anne Vincent-Salomon

    (Institut Curie)

  • P. Andrew Futreal

    (UT MD Anderson Cancer Center)

  • Stian Knappskog

    (University of Bergen
    Haukeland University Hospital)

  • Tari King

    (Memorial Sloan Kettering Cancer Center)

  • Gilles Thomas

    (Synergie Lyon Cancer,Centre Léon Bérard)

  • Alain Viari

    (Synergie Lyon Cancer,Centre Léon Bérard
    Equipe Erable, INRIA Grenoble-Rhône-Alpes)

  • Anita Langerød

    (Institute for Cancer Research, Oslo University Hospital The Norwegian Radiumhospital
    K.G. Jebsen Centre for Breast Cancer Research, Institute for Clinical Medicine, University of Oslo)

  • Anne-Lise Børresen-Dale

    (Institute for Cancer Research, Oslo University Hospital The Norwegian Radiumhospital
    K.G. Jebsen Centre for Breast Cancer Research, Institute for Clinical Medicine, University of Oslo)

  • Ewan Birney

    (European Molecular Biology Laboratory, European Bioinformatics Institute, Wellcome Trust Genome Campus)

  • Hendrik G. Stunnenberg

    (Faculty of Science, Radboud Institute for Molecular Life Sciences, Radboud University Nijmegen)

  • Mike Stratton

    (Wellcome Trust Sanger Institute)

  • John A. Foekens

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

  • John W. M. Martens

    (Erasmus MC Cancer Institute and Cancer Genomics Netherlands, Erasmus University Medical Center)

Abstract

A recent comprehensive whole genome analysis of a large breast cancer cohort was used to link known and novel drivers and substitution signatures to the transcriptome of 266 cases. Here, we validate that subtype-specific aberrations show concordant expression changes for, for example, TP53, PIK3CA, PTEN, CCND1 and CDH1. We find that CCND3 expression levels do not correlate with amplification, while increased GATA3 expression in mutant GATA3 cancers suggests GATA3 is an oncogene. In luminal cases the total number of substitutions, irrespective of type, associates with cell cycle gene expression and adverse outcome, whereas the number of mutations of signatures 3 and 13 associates with immune-response specific gene expression, increased numbers of tumour-infiltrating lymphocytes and better outcome. Thus, while earlier reports imply that the sheer number of somatic aberrations could trigger an immune-response, our data suggests that substitutions of a particular type are more effective in doing so than others.

Suggested Citation

  • Marcel Smid & F. Germán Rodríguez-González & Anieta M. Sieuwerts & Roberto Salgado & Wendy J. C. Prager-Van der Smissen & Michelle van der Vlugt-Daane & Anne van Galen & Serena Nik-Zainal & Johan Staa, 2016. "Breast cancer genome and transcriptome integration implicates specific mutational signatures with immune cell infiltration," Nature Communications, Nature, vol. 7(1), pages 1-9, December.
    • Handle: RePEc:nat:natcom:v:7:y:2016:i:1:d:10.1038_ncomms12910
    DOI: 10.1038/ncomms12910
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