Gastroesophageal reflux might cause esophagitis through a cytokine-mediated mechanism rather than caustic acid injury

RF Souza, X Huo, V Mittal, CM Schuler, SW Carmack… - Gastroenterology, 2009 - Elsevier
RF Souza, X Huo, V Mittal, CM Schuler, SW Carmack, HY Zhang, X Zhang, C Yu…
Gastroenterology, 2009Elsevier
BACKGROUND & AIMS: Reflux esophagitis is believed to be caused by the caustic effects of
refluxed gastric acid on esophageal epithelial cells. However, caustic chemical injuries
develop rapidly whereas esophagitis might not appear until weeks after the induction of
reflux in animal models. We studied early histologic events in the development of reflux
esophagitis in a rat model and performed in vitro experiments to determine whether
exposure to acidified bile salts causes esophageal epithelial cells to secrete chemokines …
BACKGROUND & AIMS
Reflux esophagitis is believed to be caused by the caustic effects of refluxed gastric acid on esophageal epithelial cells. However, caustic chemical injuries develop rapidly whereas esophagitis might not appear until weeks after the induction of reflux in animal models. We studied early histologic events in the development of reflux esophagitis in a rat model and performed in vitro experiments to determine whether exposure to acidified bile salts causes esophageal epithelial cells to secrete chemokines that might contribute to inflammation.
METHODS
At various time points after esophagoduodenostomy, the rat esophagus was removed and inflammatory changes were analyzed by histologic analyses. Human esophageal squamous cell lines were exposed to acidified bile salts to evaluate their effects on cytokine production and immune-cell migration.
RESULTS
Reflux esophagitis started at postoperative day 3 with lymphocytic infiltration of the submucosa that progressed to the epithelial surface—these findings contradicted those expected from a caustic chemical injury. Basal cell and papillary hyperplasia preceded the development of surface erosions. Exposure of squamous cells to acidified bile salts significantly increased the secretion of interleukin-8 and interleukin-1β; conditioned media from these cells caused significant increases in the migration rates of T cells and neutrophils.
CONCLUSIONS
These findings support, but do not prove, an alternative concept for the development of reflux esophagitis in which refluxed gastric juice does not directly damage the esophagus, but rather stimulates esophageal epithelial cells to secrete chemokines that mediate damage of esophageal tissue.
Elsevier