Molecular mechanism of indomethacin-induced gastropathy

The probable cross talk among large numbers of inflammatory and angiogenic parameters in indomethacin (IND)-induced gastropathy and the associated signaling mechanism were studied in a mouse model. A single dose of IND (18 mg/kg, po) produced robust gastric ulceration in mice without any mortality, which peaked on the third day, but started healing from the fifth day onward. The ulceration was associated with increased myeloperoxidase activity and expression of proinflammatory (INF-alpha, adhesion molecules, COX-2) and antiangiogenic (endostatin) parameters. The levels of proangiogenic factors such as COX-1, prostaglandin E, VEGF, and von Willebrand factor VIII were downregulated by IND. Our results revealed that although the maximal and minimal levels of these parameters were attained sequentially at different time points, TNF-alpha upregulation was the primary event to initiate and induce gastric ulceration. IND also activated NF-kappa B and all the MAP kinases, but only the inhibitors of TNF-a, NF-kappa B, and JNK MAP kinase could abrogate the IND-induced damages. Further TNF-a inhibition also reduced the IND-mediated activation of NF-kappa B and JNK MAP kinase. All this evidence strongly suggests that mitigation of TNF-alpha may offer a potential solution to IND-mediated gastropathy. (C) 2012 Elsevier Inc. All rights reserved.