Journal of Experimental & Clinical Cancer Research (Aug 2009)

CDX2 hox gene product in a rat model of esophageal cancer

  • Rizzetto Christian,
  • Polimeno Lorenzo,
  • Castoro Carlo,
  • Dazzo Emanuela,
  • Mescoli Claudia,
  • Fassan Matteo,
  • Segat Daniela,
  • Dall'Olmo Luigi,
  • Ingravallo Giuseppe,
  • Baroni Maurizio,
  • Zaninotto Giovanni,
  • Ancona Ermanno,
  • Rugge Massimo

DOI
https://doi.org/10.1186/1756-9966-28-108
Journal volume & issue
Vol. 28, no. 1
p. 108

Abstract

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Abstract Background Barrett's mucosa is the precursor of esophageal adenocarcinoma. The molecular mechanisms behind Barrett's carcinogenesis are largely unknown. Experimental models of longstanding esophageal reflux of duodenal-gastric contents may provide important information on the biological sequence of the Barrett's oncogenesis. Methods The expression of CDX2 hox-gene product was assessed in a rat model of Barrett's carcinogenesis. Seventy-four rats underwent esophago-jejunostomy with gastric preservation. Excluding perisurgical deaths, the animals were sacrificed at various times after the surgical treatment (Group A: 30 weeks). Results No Cdx2 expression was detected in either squamous epithelia of the proximal esophagus or squamous cell carcinomas. De novo Cdx2 expression was consistently documented in the proliferative zone of the squamous epithelium close to reflux ulcers (Group A: 68%; Group B: 64%; Group C: 80%), multilayered epithelium and intestinal metaplasia (Group A: 9%; Group B: 41%; Group C: 60%), and esophageal adenocarcinomas (Group B: 36%; Group C: 35%). A trend for increasing overall Cdx2 expression was documented during the course of the experiment (p = 0.001). Conclusion De novo expression of Cdx2 is an early event in the spectrum of the lesions induced by experimental gastro-esophageal reflux and should be considered as a key step in the morphogenesis of esophageal adenocarcinoma.