Molecular typing of epithelial ovarian carcinomas using inflammatory markers

BACKGROUND: Ovarian epithelial carcinomas have recently been classified as slow growing type I tumors and rapidly growing highly aggressive type II tumors. The present study sought to molecularly characterize type I and II tumors using known molecular markers. METHODS: Specimens from 213 patients with ovarian carcinoma were categorized as type I or type II, and evaluated by immunohistochemistry for the inflammatory markers glucose transporter protein‐1 (Glut‐1), inducible nitric oxide synthase (iNOS), cyclooxygenase‐1 (COX‐1), cyclooxygenase‐2 (COX‐2), and nuclear factor kappa B. Statistical analysis was performed to investigate whether these molecular markers could distinguish between type I and type II tumors. Kaplan‐Meier survival curves and COX regression analysis were used to determine the prognostic effect of these markers on survival in the 2 types of tumors. RESULTS: Overexpression of COX‐1, COX‐2, iNOS, and Glut‐1 was significantly higher in type II tumors ( P < .05). Women with type II tumors had a poorer median survival (60 months) as compared with those with type I tumors (141 months) ( P = .0001). Multivariate analysis revealed type II tumors, late stage, and age >60 years as significant predictors of poor survival. For type II tumors, median survival of patients with tumors overexpressing COX‐2 was 44 compared with 85 months for those with tumors with low COX‐2 expression ( P = .029). Looking at both type I and II tumors, the number of markers simultaneously overexpressed in each tumor was a significant predictor of poor patient survival ( P = .005). CONCLUSIONS: The present study demonstrates that the new proposed histologic classification of ovarian epithelial carcinomas correlates with a distinct expression of inflammatory pathway proteins. High expression of these markers may explain the different biologic behavior of these 2 tumor types and provide targets for therapy. Cancer 2011. © 2010 American Cancer Society.