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A whole-genome sequence and transcriptome perspective on HER2-positive breast cancers

Author

Listed:
  • Anthony Ferrari

    (Synergie Lyon Cancer, Plateforme de bioinformatique ‘Gilles Thomas’ Centre Léon Bérard)

  • Anne Vincent-Salomon

    (Institut Curie, PSL Research University)

  • Xavier Pivot

    (Centre Hospitalier Universitaire de Minjoz)

  • Anne-Sophie Sertier

    (Synergie Lyon Cancer, Plateforme de bioinformatique ‘Gilles Thomas’ Centre Léon Bérard)

  • Emilie Thomas

    (Synergie Lyon Cancer, Plateforme de bioinformatique ‘Gilles Thomas’ Centre Léon Bérard)

  • Laurie Tonon

    (Synergie Lyon Cancer, Plateforme de bioinformatique ‘Gilles Thomas’ Centre Léon Bérard)

  • Sandrine Boyault

    (Plateforme de génomique des cancers, Centre Léon Bérard)

  • Eskeatnaf Mulugeta

    (Institut Curie, UMR 3215 CNRS, Génétique et biologie du développement, Epigénèse et développement des mammifères)

  • Isabelle Treilleux

    (Centre Léon Bérard)

  • Gaëtan MacGrogan

    (Unité Inserm U916, Institut Bergonié)

  • Laurent Arnould

    (Centre Georges-François Leclerc et CRB Ferdinand Cabanne)

  • Janice Kielbassa

    (Synergie Lyon Cancer, Plateforme de bioinformatique ‘Gilles Thomas’ Centre Léon Bérard)

  • Vincent Le Texier

    (Synergie Lyon Cancer, Plateforme de bioinformatique ‘Gilles Thomas’ Centre Léon Bérard)

  • Hélène Blanché

    (Centre d'Etude du Polymorphisme Humain (CEPH), Fondation Jean Dausset)

  • Jean-François Deleuze

    (Centre d'Etude du Polymorphisme Humain (CEPH), Fondation Jean Dausset)

  • Jocelyne Jacquemier

    (Institut Paoli-Calmettes)

  • Marie-Christine Mathieu

    (Institut Gustave Roussy, Comité de Pathologie Mammaire)

  • Frédérique Penault-Llorca

    (Centre Jean Perrin, EA 4677 ERTICa, Université d'Auvergne)

  • Frédéric Bibeau

    (Institut Régional du Cancer de Montpellier (ICM))

  • Odette Mariani

    (Institut Curie, PSL Research University, Service de Pathologie, Centre de Ressources Biologiques)

  • Cécile Mannina

    (Institut Bergonié)

  • Jean-Yves Pierga

    (Institut Curie, PSL Research University, Université Paris Descartes)

  • Olivier Trédan

    (Centre Léon Bérard)

  • Thomas Bachelot

    (Centre Léon Bérard)

  • Hervé Bonnefoi

    (Institut Bergonié Unicancer, University of Bordeaux)

  • Gilles Romieu

    (Institut Régional du Cancer de Montpellier (ICM), Oncologie Sénologie)

  • Pierre Fumoleau

    (Centre Georges-François Leclerc et CRB Ferdinand Cabanne)

  • Suzette Delaloge

    (Institut Gustave Roussy, Comité de Pathologie Mammaire)

  • Maria Rios

    (Centre Alexis Vautrin)

  • Jean-Marc Ferrero

    (Centre Antoine Lacassagne)

  • Carole Tarpin

    (Institut Paoli-Calmettes)

  • Catherine Bouteille

    (Clinique Mutualiste de Bellevue, Chirurgie Gynécologique et Mammaire)

  • Fabien Calvo

    (Institut Gustave Roussy, Cancer Core Europe)

  • Ivo Glynne Gut

    (CNAG-CRG, Centre for Genomic Regulation (CRG)
    Universitat Pompeu Fabra)

  • Marta Gut

    (CNAG-CRG, Centre for Genomic Regulation (CRG)
    Universitat Pompeu Fabra)

  • Sancha Martin

    (Wellcome Trust Sanger Institute)

  • Serena Nik-Zainal

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

  • Michael R. Stratton

    (Wellcome Trust Sanger Institute)

  • Iris Pauporté

    (Institut National du Cancer)

  • Pierre Saintigny

    (INSERM U1052-CNRS 5286, Cancer Research Center of Lyon
    Université de Lyon
    Centre Léon Bérard)

  • Daniel Birnbaum

    (Institut Paoli-Calmettes, Centre de Recherche en Cancérologie de Marseille)

  • Alain Viari

    (Synergie Lyon Cancer, Plateforme de bioinformatique ‘Gilles Thomas’ Centre Léon Bérard
    Equipe Erable, INRIA Grenoble-Rhône-Alpes)

  • Gilles Thomas

    (Synergie Lyon Cancer, Plateforme de bioinformatique ‘Gilles Thomas’ Centre Léon Bérard)

Abstract

HER2-positive breast cancer has long proven to be a clinically distinct class of breast cancers for which several targeted therapies are now available. However, resistance to the treatment associated with specific gene expressions or mutations has been observed, revealing the underlying diversity of these cancers. Therefore, understanding the full extent of the HER2-positive disease heterogeneity still remains challenging. Here we carry out an in-depth genomic characterization of 64 HER2-positive breast tumour genomes that exhibit four subgroups, based on the expression data, with distinctive genomic features in terms of somatic mutations, copy-number changes or structural variations. The results suggest that, despite being clinically defined by a specific gene amplification, HER2-positive tumours melt into the whole luminal–basal breast cancer spectrum rather than standing apart. The results also lead to a refined ERBB2 amplicon of 106 kb and show that several cases of amplifications are compatible with a breakage–fusion–bridge mechanism.

Suggested Citation

  • Anthony Ferrari & Anne Vincent-Salomon & Xavier Pivot & Anne-Sophie Sertier & Emilie Thomas & Laurie Tonon & Sandrine Boyault & Eskeatnaf Mulugeta & Isabelle Treilleux & Gaëtan MacGrogan & Laurent Arn, 2016. "A whole-genome sequence and transcriptome perspective on HER2-positive breast cancers," Nature Communications, Nature, vol. 7(1), pages 1-9, November.
    • Handle: RePEc:nat:natcom:v:7:y:2016:i:1:d:10.1038_ncomms12222
    DOI: 10.1038/ncomms12222
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    Cited by:

    1. A. C. Katz-Summercorn & S. Jammula & A. Frangou & I. Peneva & M. O’Donovan & M. Tripathi & S. Malhotra & M. Pietro & S. Abbas & G. Devonshire & W. Januszewicz & A. Blasko & K. Nowicki-Osuch & S. MacRa, 2022. "Multi-omic cross-sectional cohort study of pre-malignant Barrett’s esophagus reveals early structural variation and retrotransposon activity," Nature Communications, Nature, vol. 13(1), pages 1-17, December.

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