Abstract
Nonsteroidal anti-inflammatory drugs are among the most commonly used prescription and over-the-counter medications, but they often produce significant gastrointestinal ulceration and bleeding, particularly in elderly patients and patients with certain co-morbidities. Novel anti-inflammatory drugs are seldom tested in animal models that mimic the high risk human users, leading to an underestimate of the true toxicity of the drugs. In the present study we examined the effects of two novel NSAIDs and two commonly used NSAIDs in models in which mucosal defence was expected to be impaired. Naproxen, celecoxib, ATB-346 (a hydrogen sulfide- and naproxen-releasing compound) and NCX 429 (a nitric oxide- and naproxen-releasing compound) were evaluated in healthy, arthritic, obese, and hypertensive rats and in rats of advanced age (19 months) and rats co-administered low-dose aspirin and/or omeprazole. In all models except hypertension, greater gastric and/or intestinal damage was observed when naproxen was administered in these models than in healthy rats. Celecoxib-induced damage was significantly increased when co-administered with low-dose aspirin and/or omeprazole. In contrast, ATB-346 and NCX 429, when tested at doses that were as effective as naproxen and celecoxib in reducing inflammation and inhibiting cyclooxygenase activity, did not produce significant gastric or intestinal damage in any of the models. These results demonstrate that animal models of human co-morbidities display the same increased susceptibility to NSAID-induced gastrointestinal damage as observed in humans. Moreover, two novel NSAIDs that release mediators of mucosal defence (hydrogen sulfide and nitric oxide) do not induce significant gastrointestinal damage in these models of impaired mucosal defence.
Highlights
The ability of nonsteroidal anti-inflammatory drugs (NSAIDs) to cause significant ulceration and bleeding in the stomach and duodenum is well recognized [1]
In addition to examining the GI safety of these compounds when administered together with low-dose aspirin and/or a pump inhibitor (PPI), we evaluated them in models in which mucosal defence may be compromised
NSAID-induced gastroenteropathy is a significant limitation to the use of this class of drugs, which is a mainstream therapy for osteoarthritis and other chronic conditions characterized by inflammation and pain
Summary
The ability of nonsteroidal anti-inflammatory drugs (NSAIDs) to cause significant ulceration and bleeding in the stomach and duodenum is well recognized [1]. The most common approach used clinically to minimize gastroduodenal injury is to coadminister a proton pump inhibitor (PPI) with the NSAID. This has been shown to significantly reduce the incidence of gastro-duodenal damage [4], but recent animal studies suggest that suppression of acid secretion can lead to exacerbation of NSAID-induced small intestinal injury and bleeding [5]. There are several clinical studies that report high levels of intestinal damage in healthy volunteers taking NSAIDs plus a PPI [6,7,8,9], and one study showing significant elevation of a marker of intestinal inflammation (calprotectin) in patients taking PPIs [10]
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