BMC Cancer (Sep 2012)

RON is not a prognostic marker for resectable pancreatic cancer

  • Tactacan Carole M,
  • Chang David K,
  • Cowley Mark J,
  • Humphrey Emily S,
  • Wu Jianmin,
  • Gill Anthony J,
  • Chou Angela,
  • Nones Katia,
  • Grimmond Sean M,
  • Sutherland Robert L,
  • Biankin Andrew V,
  • Daly Roger J

DOI
https://doi.org/10.1186/1471-2407-12-395
Journal volume & issue
Vol. 12, no. 1
p. 395

Abstract

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Abstract Background The receptor tyrosine kinase RON exhibits increased expression during pancreatic cancer progression and promotes migration, invasion and gemcitabine resistance of pancreatic cancer cells in experimental models. However, the prognostic significance of RON expression in pancreatic cancer is unknown. Methods RON expression was characterized in several large cohorts, including a prospective study, totaling 492 pancreatic cancer patients and relationships with patient outcome and clinico-pathologic variables were assessed. Results RON expression was associated with outcome in a training set, but this was not recapitulated in the validation set, nor was there any association with therapeutic responsiveness in the validation set or the prospective study. Conclusions Although RON is implicated in pancreatic cancer progression in experimental models, and may constitute a therapeutic target, RON expression is not associated with prognosis or therapeutic responsiveness in resected pancreatic cancer.

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