Model of rapid gastrointestinal transit in dogs: effects of muscarinic antagonists and a nitric oxide synthase inhibitor

Our aims were to establish a canine model of rapid gastrointestinal transit, and to test the effects of muscarinic receptor antagonists (atropine, pirenzepine, AF‐DX116, and darifenacin), and an NOS inhibitor, l‐nitro‐N‐arginine (l‐NNA) in this model. For gastric emptying and small bowel transit,99m...

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Veröffentlicht in:Neurogastroenterology and motility 2002-10, Vol.14 (5), p.535-541
Hauptverfasser: Chiba, T., Bharucha, A. E., Thomforde, G. M., Kost, L. J., Phillips, S. F.
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Sprache:eng
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Zusammenfassung:Our aims were to establish a canine model of rapid gastrointestinal transit, and to test the effects of muscarinic receptor antagonists (atropine, pirenzepine, AF‐DX116, and darifenacin), and an NOS inhibitor, l‐nitro‐N‐arginine (l‐NNA) in this model. For gastric emptying and small bowel transit,99mTc‐labelled DTPA were added to a meal of skimmed milk (236 mL) that contained 2.4 g of magnesium hydroxide. Regional colonic transit was measured by111In‐labelled beads placed in a capsule that released isotope in the proximal colon. Scintiscans were taken at regular intervals and indices of transit were calculated. Drugs were administrated intravenously. Gastric emptying, small bowel and colonic transit were rapid. Atropine and darifenacin (a selective M3antagonist) delayed gastric emptying and colonic transit, the selective M1and M2muscarinic antagonists did not. The muscarinic blockers did not slow small bowel transit. l‐NNA delayed small bowel and colonic transit but did not slow gastric emptying. A model suitable for the preclinical study of antidiarrhoeals was established. M3receptors are important in the control of gastric emptying and colonic transit, and NOS inhibition slowed small bowel and colonic transit.
ISSN:1350-1925
1365-2982
DOI:10.1046/j.1365-2982.2002.00357.x