Gene-expression molecular subtyping of triple-negative breast cancer tumours: importance of immune response

Pascal Jézéquel; Delphine Loussouarn; Catherine Guérin-Charbonnel; Loïc Campion; Antoine Vanier; Wilfried Gouraud; Hamza Lasla; Catherine Guette; Isabelle Valo; Véronique Verrièle; Mario Campone

doi:10.1186/s13058-015-0550-y

Gene-expression molecular subtyping of triple-negative breast cancer tumours: importance of immune response

Breast Cancer Res. 2015 Mar 20:17:43. doi: 10.1186/s13058-015-0550-y.

Authors

Pascal Jézéquel^{1

2

3

4}, Delphine Loussouarn^{5

6}, Catherine Guérin-Charbonnel^{7

8

9}, Loïc Campion^{10

11}, Antoine Vanier^{12

13}, Wilfried Gouraud^{14

15

16}, Hamza Lasla¹⁷, Catherine Guette¹⁸, Isabelle Valo¹⁹, Véronique Verrièle²⁰, Mario Campone^{21

22

23}

Affiliations

¹ Unité Mixte de Génomique du Cancer, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. Pascal.jezequel@ico.unicancer.fr.
² Unité de Bioinfomique, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. Pascal.jezequel@ico.unicancer.fr.
³ Département de Biopathologie, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. Pascal.jezequel@ico.unicancer.fr.
⁴ INSERM U892, IRT-UN, 8 quai Moncousu, 44007, Nantes Cedex, France. Pascal.jezequel@ico.unicancer.fr.
⁵ INSERM U892, IRT-UN, 8 quai Moncousu, 44007, Nantes Cedex, France. delphine.loussouarn@chu-nantes.fr.
⁶ Service d'Anatomie Pathologique B, Hôpital G&R Laënnec, Bd J. Monod, 44805, Saint Herblain, France. delphine.loussouarn@chu-nantes.fr.
⁷ Unité Mixte de Génomique du Cancer, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. catherine.guerin@ico.unicancer.fr.
⁸ Unité de Bioinfomique, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. catherine.guerin@ico.unicancer.fr.
⁹ INSERM U892, IRT-UN, 8 quai Moncousu, 44007, Nantes Cedex, France. catherine.guerin@ico.unicancer.fr.
¹⁰ INSERM U892, IRT-UN, 8 quai Moncousu, 44007, Nantes Cedex, France. loic.campion@ico.unicancer.fr.
¹¹ Unité de Biostatistique, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. loic.campion@ico.unicancer.fr.
¹² Sorbonne Universités, UPMC University, Département de Biostatistique, 4 place Jussieu, 75005, Paris, France. antoine.vanier@gmail.com.
¹³ AP-HP, University Hospitals Pitié-Salpêtrière Charles-Foix, Département de Biostatistique, Santé Publique et Informatique Médicale, 47-83 Bd de l'Hôpital, 75013, Paris, France. antoine.vanier@gmail.com.
¹⁴ Unité Mixte de Génomique du Cancer, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. wilfried.gouraud@ico.unicancer.fr.
¹⁵ Unité de Bioinfomique, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. wilfried.gouraud@ico.unicancer.fr.
¹⁶ INSERM U892, IRT-UN, 8 quai Moncousu, 44007, Nantes Cedex, France. wilfried.gouraud@ico.unicancer.fr.
¹⁷ Unité de Bioinfomique, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. hamza.lasla@ico.unicancer.fr.
¹⁸ Institut de Cancérologie de l'Ouest - site Paul Papin, 2 rue Moll, 49933, Angers Cedex 9, France. catherine.guette@ico.unicancer.fr.
¹⁹ Laboratoire d'Anatomie Pathologique, Institut de Cancérologie de l'Ouest - site Paul Papin, 2 rue Moll, 49933, Angers Cedex 9, France. isabelle.valo@ico.unicancer.fr.
²⁰ Laboratoire d'Anatomie Pathologique, Institut de Cancérologie de l'Ouest - site Paul Papin, 2 rue Moll, 49933, Angers Cedex 9, France. veronique.verriele@ico.unicancer.fr.
²¹ Unité de Bioinfomique, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. mario.campone@ico.unicancer.fr.
²² INSERM U892, IRT-UN, 8 quai Moncousu, 44007, Nantes Cedex, France. mario.campone@ico.unicancer.fr.
²³ Service d'Oncologie Médicale, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France. mario.campone@ico.unicancer.fr.

Abstract

Introduction: Triple-negative breast cancers need to be refined in order to identify therapeutic subgroups of patients.

Methods: We conducted an unsupervised analysis of microarray gene-expression profiles of 107 triple-negative breast cancer patients and undertook robust functional annotation of the molecular entities found by means of numerous approaches including immunohistochemistry and gene-expression signatures. A triple-negative external cohort (n=87) was used for validation.

Results: Fuzzy clustering separated triple-negative tumours into three clusters: C1 (22.4%), C2 (44.9%) and C3 (32.7%). C1 patients were older (mean=64.6 years) than C2 (mean=56.8 years; P=0.03) and C3 patients (mean=51.9 years; P=0.0004). Histological grade and Nottingham prognostic index were higher in C2 and C3 than in C1 (P<0.0001 for both comparisons). Significant event-free survival (P=0.03) was found according to cluster membership: patients belonging to C3 had a better outcome than patients in C1 (P=0.01) and C2 (P=0.02). Event-free survival analysis results were confirmed when our cohort was pooled with the external cohort (n=194; P=0.01). Functional annotation showed that 22% of triple-negative patients were not basal-like (C1). C1 was enriched in luminal subtypes and positive androgen receptor (luminal androgen receptor). C2 could be considered as an almost pure basal-like cluster. C3, enriched in basal-like subtypes but to a lesser extent, included 26% of claudin-low subtypes. Dissection of immune response showed that high immune response and low M2-like macrophages were a hallmark of C3, and that these patients had a better event-free survival than C2 patients, characterized by low immune response and high M2-like macrophages: P=0.02 for our cohort, and P=0.03 for pooled cohorts.

Conclusions: We identified three subtypes of triple-negative patients: luminal androgen receptor (22%), basal-like with low immune response and high M2-like macrophages (45%), and basal-enriched with high immune response and low M2-like macrophages (33%). We noted out that macrophages and other immune effectors offer a variety of therapeutic targets in breast cancer, and particularly in triple-negative basal-like tumours. Furthermore, we showed that CK5 antibody was better suited than CK5/6 antibody to subtype triple-negative patients.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Biomarkers, Tumor
Cluster Analysis
Computational Biology
Female
Gene Expression Profiling*
Gene Expression Regulation, Neoplastic*
Humans
Immunity, Innate
Immunohistochemistry
Kaplan-Meier Estimate
Middle Aged
Molecular Sequence Annotation
Neoplasm Staging
Prognosis
Reproducibility of Results
Retrospective Studies
Transcriptome
Triple Negative Breast Neoplasms / diagnosis
Triple Negative Breast Neoplasms / genetics*
Triple Negative Breast Neoplasms / immunology
Triple Negative Breast Neoplasms / mortality
Triple Negative Breast Neoplasms / therapy
Tumor Burden

Substances

Biomarkers, Tumor