Mucosal permeability is an intrinsic factor determining susceptibility to dextran sulfate sodium‐induced colitis in rats

Abstract

We investigated the differences in the pathogenesis of dextran sulfate sodium (DSS)‐induced colitis between two inbred rat strains, WKAH and DA rats, to determine an intrinsic factor responsible for the development of colitis. The body weight reduction, stool consistency, and rectal bleeding were daily evaluated during DSS treatment period. The clinical symptoms in DA rats were significantly severer than that in WKAH rats. In an early phase of DSS treatment period, we measured the expressions of cytokine mRNA and tight junction (TJ) proteins in the colonic mucosae. DSS treatment increased prominently the mRNA expression levels of TNF‐α, IL‐12 p35, and IL‐23 p19 in the DA rat. A colonic permeability was greater in the DA rats than in the WKAH rat. Higher expression of claudin‐4 and Junctional adhesion molecule (JAM)‐A proteins were observed in the DA rats than that in the WKAH rats without DSS conditions. The different expression pattern of TJ proteins probably determines the colonic permeability of rats. However, DSS treatment enhanced TNF‐α production in mesenteric leukocytes isolated from the WKAH rats rather than that from DA rats, suggesting that the response of immune cells to DSS in the DA rats was weaker than that of the WKAH rats. In conclusion, the intrinsic colonic permeability is one of critical factors responsible for the susceptibility to colitis.