Oral Administration of Sepimostat Mesilate Prevents Acute Alcohol Pancreatic Injury in Rats

Author:

Yuasa Chie1,Irimura Kenji2,Oda Minoru3,Fukui Kiyoshi4,Oka Toshinori1

Affiliation:

1. Pharmacology Research Laboratory, Tokishima Research Center, Taiho Pharmaceutical Co. Ltd, 224-2 Ebisuno, Hiraishi, Kawauchi-cho, Tokushima 771-0194, Japan

2. Drug Safety Laboratory, R&D Headquarters, Tokishima Research Center, Taiho Pharmaceutical Co. Ltd, 224-2 Ebisuno, Hiraishi, Kawauchi-cho, Tokushima 771-0194, Japan

3. Research Project Planning Section, Research Laboratories, Torii Pharmaceutical Co. Ltd, 1–2-1 Ohnodai, Midori-ku, Chiba 267, Japan

4. Institute for Enzyme Research, The University of Tokushima, 3–18-15, Kuramoto, Tokushima 770–8503, Japan

Abstract

Abstract The preventive effect of a novel synthetic serine protease inhibitor, sepimostat mesilate (sepimostat), on acute alcohol pancreatic injury, induced by exocrine hyperstimulation and ethanol administration, was assessed and compared with that of a similar protease inhibitor, camostat mesilate (camostat). Conscious rats were infused with 1 μg mL−1 h−1 caerulein intravenously for 6 h and with 0.1g mL−1 h−1 ethanol for 9h, with the latter infusion beginning 3 h after the start of the caerulein infusion. Sepimostat or camostat was administered orally 1 h before the caerulein infusion. Rats infused with caerulein plus ethanol showed increased plasma amylase and lipase activities, and aggravated pancreatic interstitial oedema when compared with rats given caerulein alone. Sepimostat at 10 and 30mgkg−1 prevented the increase in plasma amylase and lipase activities caused by caerulein plus ethanol infusion. Sepimostat at 30mg kg−1 suppressed the histological change. Camostat did not show any preventive effects at the equivalent dose. When conscious rats were infused with 1 μg mL−1h−1 caerulein alone intravenously for 6 h, plasma amylase and lipase activities were increased compared with rats given saline. Neither drug prevented the increase in these activities at 30mg kg−1. Our results suggest that sepimostat has superior preventive effects on alcohol-induced acute pancreatic injury compared with camostat. Sepimostat may thus be a useful drug in the therapy of alcohol-induced pancreatitis.

Publisher

Oxford University Press (OUP)

Subject

Pharmaceutical Science,Pharmacology

Reference16 articles.

1. Exocrine hyperstimulation but not pancreatic duct obstruction increases the susceptibility to alcohol-related pancreatic injury;Foitzik;Arch. Surg.,1994

2. Effect of cessation of alcohol use on the course of pancreatic dysfunction in alcoholic pancreatitis;Gullo;Gastroenterology,1988

3. Individual susceptibility to alcoholic pancreatitis: still an enigma;Haber;J. Lab. Clin. Med.,1995

4. Suien ni taisuru FOY-305 no yakko hyoka;Ishii;Tashisetu nijyumokenho. Gendai Iryo,1980

5. Beneficial effects of preventive oral administration of camostate on cerulein-induced pancreatitis in rats;Kisfalvi;Dig. Dis. Sci.,1995

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