BMC Cancer (Jun 2012)

Colon cancer molecular subtypes identified by expression profiling and associated to stroma, mucinous type and different clinical behavior

  • Perez Villamil Beatriz,
  • Romera Lopez Alejandro,
  • Hernandez Prieto Susana,
  • Lopez Campos Guillermo,
  • Calles Antonio,
  • Lopez Asenjo Jose Antonio,
  • Sanz Ortega Julian,
  • Fernandez Perez Cristina,
  • Sastre Javier,
  • Alfonso Rosario,
  • Caldes Trinidad,
  • Martin Sanchez Fernando,
  • Diaz Rubio Eduardo

DOI
https://doi.org/10.1186/1471-2407-12-260
Journal volume & issue
Vol. 12, no. 1
p. 260

Abstract

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Abstract Background Colon cancer patients with the same stage show diverse clinical behavior due to tumor heterogeneity. We aimed to discover distinct classes of tumors based on microarray expression patterns, to analyze whether the molecular classification correlated with the histopathological stages or other clinical parameters and to study differences in the survival. Methods Hierarchical clustering was performed for class discovery in 88 colon tumors (stages I to IV). Pathways analysis and correlations between clinical parameters and our classification were analyzed. Tumor subtypes were validated using an external set of 78 patients. A 167 gene signature associated to the main subtype was generated using the 3-Nearest-Neighbor method. Coincidences with other prognostic predictors were assesed. Results Hierarchical clustering identified four robust tumor subtypes with biologically and clinically distinct behavior. Stromal components (p BRAF mutations. Tumor subtypes were validated using an external set of 78 patients. A 167 gene signature associated to the Low-stroma-subtype distinguished low risk patients from high risk patients in the external cohort (Dukes B and C:HR = 8.56(2.53-29.01); Dukes B,C and D:HR = 1.87(1.07-3.25)). Eight different reported survival gene signatures segregated our tumors into two groups the Low-stroma-subtype and the other tumor subtypes. Conclusions We have identified novel molecular subtypes in colon cancer with distinct biological and clinical behavior that are established from the initiation of the tumor. Tumor microenvironment is important for the classification and for the malignant power of the tumor. Differential gene sets and biological pathways characterize each tumor subtype reflecting underlying mechanisms of carcinogenesis that may be used for the selection of targeted therapeutic procedures. This classification may contribute to an improvement in the management of the patients with CRC and to a more comprehensive prognosis.

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