Beatrice Flogerzi scite author profile

1 In the stomach, prostaglandins protect the gastric mucosa against injuries. One rate-limiting step in prostaglandin synthesis is mediated by prostaglandin endoperoxide synthase (PGHS), the target enzyme of non-steroidal anti-in¯ammatory drugs (NSAIDs). Two isoforms of PGHS exist: a constitutive (PGHS-1) and an inducible (PGHS-2) enzyme. PGHS-1 is the major source of gastric prostaglandins under physiological conditions. Inhibition of prostaglandin synthesis by traditional NSAIDs such as indomethacin and diclofenac which non-selectively inhibit both PGHS-1 and PGHS-2, causes gastric and intestinal ulceration and delays gastric ulcer healing in chronic models. It has been shown that selective PGHS-2 inhibitors such as L-745,337 (5-methanesulphonamide-6-(2,4-di¯uorothio-phenyl)-1-indanone) are not ulcerogenic and do not inhibit gastro-intestinal prostaglandin synthesis. However, minimal information is available on the long-term eects of PGHS-2 inhibitors on the healing of previously established gastric injuries. We assessed the cellular localization and expression of PGHS-1 and PGHS-2 during gastric ulcer healing and assessed the eects of L-745,337 on previously established cryoulcers in the rat gastric stomach. 2 PGHS-1 and PGHS-2 were located and quanti®ed by immunohistochemistry during experimental gastric ulcer healing. PGHS-2 immunoreactivity was only negligible in the normal gastric wall, but after gastric ulcerations, it was strongly detected in monocytes, macrophages, ®broblasts and endothelial cells below and between the regenerative glands. PGHS-1 immunoreactivity detected in normal gastric mucosa, disappeared after gastric ulceration in the mucosa adjacent to the ulcer crater. However, it reappeared in the regenerative glands from day 5 onwards. Thus, PGHS-1 and PGHS-2 were located at dierent sites and their maximal expression followed a dierent time-sequence. 3 We assessed the eects of L-745,337, indomethacin and diclofenac on gastric ulcer healing and histological healing parameters in rats. L-745,337, indomethacin and diclofenac dose-dependently decreased the healing of gastric ulcers. L-745,337, indomethacin and diclofenac decreased epithelial cell proliferation in the ulcer margin and microvessel density in the ulcer bed on day 8 and increased the thickness of the granulation tissue below the ulcer crater and the gap between both edges of the muscularis mucosae on day 15. Indomethacin and diclofenac, but not L-745,337, decreased synthesis of 6-keto-PGF 1a and PGE 2 in tissue fragments from the stomach and terminal ileum and decreased platelet thromboxane B 2 synthesis in clotting whole blood. 4 Dose-response curves for the inhibition of chronic gastric ulcer healing by L-745,337 (administered twice daily intragastrically) showed an ID 50 value of 1.7 mg (4.3 mmol) kg 71. Dose-response curves for the inhibition of PGE 2 synthesis in in¯ammatory exudates in the acute carrageenin sponge rat model, showed ID 50 values of 1.1 mg (3.1 mmol) kg 71 and 1.3 (3.3 mmol) mg kg 71 for indomethacin and L-745,33...

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Influence of acid and angiogenesis on kinetics of gastric ulcer healing in rats: interaction with indomethacin

Schmassmann

Tarnawski

Peskar

et al. 1995

American Journal of Physiology-Gastrointestinal and Liver Physi

106

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Indomethacin delays healing of experimental gastric ulcers. We investigated whether inhibition of gastric acid secretion by omeprazole or stimulation of angiogenesis by basic fibroblast growth factor (bFGF) may reverse this delay. Rats with gastric ulcers induced by cryoprobe were treated subcutaneously with either placebo, indomethacin (2 x 0.5 mg/kg), bFGF (2 x 100 micrograms/kg), omeprazole (1 x 40 mumol/kg), indomethacin plus omeprazole, or indomethacin plus bFGF given daily for 8, 10, 15, and 22 days. Ulcer size, epithelial cell proliferation, angiogenesis, and maturation of granulation tissue were sequentially quantified. Omeprazole significantly accelerated ulcer healing in an early phase (days 3-8). In contrast, bFGF accelerated healing in a late phase (days 10-15). Indomethacin significantly delayed ulcer healing in late phase and decreased prostaglandin generation, cell proliferation, angiogenesis, and maturation of granulation tissue. Despite stimulation of angiogenesis, bFGF did not reverse indomethacin-induced delay in ulcer healing. In contrast, omeprazole reversed indomethacin-induced effects on angiogenesis, cell proliferation, maturation of granulation tissue, and ulcer healing rate.

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Comparison of Interferon-Gamma Release AssayVersusTuberculin Skin Test for Tuberculosis Screening in Inflammatory Bowel Disease

Schoepfer

Flogerzi²,

Fallegger³

et al. 2008

107

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Roles of hepatocyte growth factor and its receptor Met during gastric ulcer healing in rats

Schmassmann¹,

Stettler²,

Poulsom³

et al. 1997

Gastroenterology

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