Camostat, an Oral Trypsin Inhibitor, Reduces Pancreatic Fibrosis Induced by Repeated Administration of a Superoxide Dismutase Inhibitor in Rats

Overview

Journal J Gastroenterol Hepatol

Specialty Gastroenterology

Date 2005 Jun 11

PMID 15946137

Citations 11

Authors

Yasuyuki Emori

Takaaki Mizushima

Naoki Matsumura

Koji Ochi

Hiroaki Tanioka

Akinori Shirahige

Mitsuko Ichimura

Toshiyuki Shinji

Norio Koide

Mitsune Tanimoto

Affiliations

Soon will be listed here.

Abstract

Background And Aim: An oral trypsin inhibitor, camostat (CM), has a beneficial effect on chronic pancreatitis, but its mechanism is not yet fully understood. Recently, pancreatic stellate cells (PSC) have been reported to play an essential role in pancreatic fibrosis. An experimental model of pancreatic fibrosis induced by a superoxide dismutase (SOD) inhibitor (diethyldithiocarbamate [DDC]) was developed in rats. Thus, the effect of an oral trypsin inhibitor on pancreatic fibrosis and PSC was investigated.

Methods: Pancreatic fibrosis was induced in rats using DDC (DDC rats). DDC + CM rats were administered DDC, and subsequently were fed a diet containing CM. Immunohistochemistry of the pancreas was performed with monoclonal anti-alpha-smooth muscle actin (alpha-SMA) antibody and anti-desmin antibody.

Results: The DDC rats showed a significant increase in alpha-SMA-positive cells or desmin-positive cells compared with control rats. These significant increases in the fibrotic area improved after treatment with CM. The level of prolyl hydroxylase in the pancreas, which significantly increased as a result of DDC, decreased after treatment with CM.

Conclusion: Camostat has a beneficial effect on pancreatic fibrosis induced by the administration of a SOD inhibitor, which inhibits the proliferation and activation of PSC.

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