Functional proteomics outlines the complexity of breast cancer molecular subtypes

Angelo Gámez‐Pozo; Lucía Trilla‐Fuertes; Julia Berges‐Soria; Nathalie Selevsek; Rocío López‐Vacas; Mariana Díaz‐Almirón; Paolo Nanni; Jorge M. Arevalillo; Hilario Navarro; Jonas Grossmann; Francisco Gayá Moreno; Rubén Gómez Rioja; Guillermo Prado-Vázquez; Andrea Zapater‐Moros; Paloma Maı́n; Jaime Feliú; Purificación Martínez del Prado; Pilar Zamora; Eva Ciruelos; Enrique Espinosa; Juan Ángel Fresno Vara

doi:10.1038/s41598-017-10493-w

Functional proteomics outlines the complexity of breast cancer molecular subtypes

Angelo Gámez‐Pozo(Hospital Universitario La Paz), Lucía Trilla‐Fuertes, Julia Berges‐Soria(Hospital Universitario La Paz), Nathalie Selevsek(University of Zurich), Rocío López‐Vacas(Hospital Universitario La Paz), Mariana Díaz‐Almirón, Paolo Nanni(University of Zurich), Jorge M. Arevalillo(Universidad Nacional de Educación a Distancia), Hilario Navarro(Universidad Nacional de Educación a Distancia), Jonas Grossmann(University of Zurich), Francisco Gayá Moreno, Rubén Gómez Rioja(Hospital La Paz Institute for Health Research), Guillermo Prado-Vázquez(Hospital Universitario La Paz), Andrea Zapater‐Moros(Hospital Universitario La Paz), Paloma Maı́n(Universidad Complutense de Madrid), Jaime Feliú(Hospital Universitario La Paz), Purificación Martínez del Prado(Hospital de Basurto), Pilar Zamora(Hospital Universitario La Paz), Eva Ciruelos(Research Institute Hospital 12 de Octubre), Enrique Espinosa(Hospital Universitario La Paz), Juan Ángel Fresno Vara(Hospital Universitario La Paz)

Scientific Reports

August 24, 2017

10.1038/s41598-017-10493-w

Cited by 62Open Access

Full Text

Abstract

Breast cancer is a heterogeneous disease comprising a variety of entities with various genetic backgrounds. Estrogen receptor-positive, human epidermal growth factor receptor 2-negative tumors typically have a favorable outcome; however, some patients eventually relapse, which suggests some heterogeneity within this category. In the present study, we used proteomics and miRNA profiling techniques to characterize a set of 102 either estrogen receptor-positive (ER+)/progesterone receptor-positive (PR+) or triple-negative formalin-fixed, paraffin-embedded breast tumors. Protein expression-based probabilistic graphical models and flux balance analyses revealed that some ER+/PR+ samples had a protein expression profile similar to that of triple-negative samples and had a clinical outcome similar to those with triple-negative disease. This probabilistic graphical model-based classification had prognostic value in patients with luminal A breast cancer. This prognostic information was independent of that provided by standard genomic tests for breast cancer, such as MammaPrint, OncoType Dx and the 8-gene Score.

Related Papers

No related papers found

Powered by citation graph analysis