Pathogenesis of NSAID-induced gastric damage: importance of cyclooxygenase inhibition and gastric hypermotility

Koji Takeuchi

doi:10.3748/wjg.v18.i18.2147

Pathogenesis of NSAID-induced gastric damage: importance of cyclooxygenase inhibition and gastric hypermotility

World J Gastroenterol. 2012 May 14;18(18):2147-60. doi: 10.3748/wjg.v18.i18.2147.

Author

Koji Takeuchi¹

Affiliation

¹ Department of Pharmacology and Experimental Therapeutics, Division of Pathological Sciences, Kyoto Pharmaceutical University, Kyoto 607-8414, Japan. takeuchi@mb.kyoto-phu.ac.jp

Abstract

This article reviews the pathogenic mechanism of non-steroidal anti-inflammatory drug (NSAID)-induced gastric damage, focusing on the relation between cyclooxygenase (COX) inhibition and various functional events. NSAIDs, such as indomethacin, at a dose that inhibits prostaglandin (PG) production, enhance gastric motility, resulting in an increase in mucosal permeability, neutrophil infiltration and oxyradical production, and eventually producing gastric lesions. These lesions are prevented by pretreatment with PGE₂ and antisecretory drugs, and also via an atropine-sensitive mechanism, not related to antisecretory action. Although neither rofecoxib (a selective COX-2 inhibitor) nor SC-560 (a selective COX-1 inhibitor) alone damages the stomach, the combined administration of these drugs provokes gastric lesions. SC-560, but not rofecoxib, decreases prostaglandin E₂ (PGE₂) production and causes gastric hypermotility and an increase in mucosal permeability. COX-2 mRNA is expressed in the stomach after administration of indomethacin and SC-560 but not rofecoxib. The up-regulation of indomethacin-induced COX-2 expression is prevented by atropine at a dose that inhibits gastric hypermotility. In addition, selective COX-2 inhibitors have deleterious influences on the stomach when COX-2 is overexpressed under various conditions, including adrenalectomy, arthritis, and Helicobacter pylori-infection. In summary, gastric hypermotility plays a primary role in the pathogenesis of NSAID-induced gastric damage, and the response, causally related with PG deficiency due to COX-1 inhibition, occurs prior to other pathogenic events such as increased mucosal permeability; and the ulcerogenic properties of NSAIDs require the inhibition of both COX-1 and COX-2, the inhibition of COX-1 upregulates COX-2 expression in association with gastric hypermotility, and PGs produced by COX-2 counteract the deleterious effect of COX-1 inhibition.

Keywords: Gastric damage; Gastric motility; Neutrophil; Non-steroidal anti-inflammatory drug; Pathogenesis.

Publication types

Review

MeSH terms

Animals
Anti-Inflammatory Agents, Non-Steroidal / adverse effects*
Anti-Ulcer Agents / therapeutic use
Cyclooxygenase 1 / metabolism*
Cyclooxygenase 2 / metabolism*
Cyclooxygenase Inhibitors / adverse effects*
Dinoprostone / metabolism
Gastric Mucosa / drug effects*
Gastric Mucosa / enzymology
Gastric Mucosa / pathology
Gastrointestinal Motility / drug effects*
Humans
Receptors, Prostaglandin E / metabolism
Risk Assessment
Risk Factors
Stomach Ulcer / chemically induced*
Stomach Ulcer / enzymology
Stomach Ulcer / pathology
Stomach Ulcer / physiopathology
Stomach Ulcer / prevention & control

Substances

Anti-Inflammatory Agents, Non-Steroidal
Anti-Ulcer Agents
Cyclooxygenase Inhibitors
Receptors, Prostaglandin E
Cyclooxygenase 1
Cyclooxygenase 2
Dinoprostone