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Comparative Study
Characterization of two models of drug-induced constipation in mice and evaluation of mustard oil in these models.
- Ryosuke Kojima, Hitoshi Doihara, Katsura Nozawa, Eri Kawabata-Shoda, Toshihide Yokoyama, and Hiroyuki Ito.
- Drug Discovery Research, Astellas Pharma Inc., Tsukuba, Ibaraki, Japan. ryosuke.kojima@jp.astellas.com
- Pharmacology. 2009 Jan 1; 84 (4): 227-33.
AbstractAlthough it is known that both clonidine and loperamide cause delayed colonic transit in mice, these models of drug-induced experimental constipation have not yet been fully characterized. Therefore, the aims of this study were to validate the clonidine- and loperamide-induced delays of colonic transit in mice as models of atonic and spastic constipation, respectively, and to evaluate the effect of mustard oil, a TRPA1 agonist, in both models. Colonic transit was evaluated in mice by determining the time needed to evacuate a bead inserted into the distal colon. Both loperamide and clonidine dose-dependently prolonged the evacuation time. Clonidine (10 microg/kg) and loperamide (0.3 mg/kg) tripled the evacuation time compared to controls. These delays were antagonized by the administration of yohimbine and naloxone, respectively. Tegaserod, a gastrointestinal motor-stimulating drug, reversed the delay in both models, but the effects were diminished at high doses. Atropine, an antispastic drug, improved the loperamide-induced delay, but did not affect the clonidine-induced delay. Mustard oil accelerated the colonic transit dose-dependently in both models of drug-induced constipations. These results indicate that clonidine- and loperamide-induced delays in colonic transit are models of atonic and spastic constipation, respectively, and that mustard oil may be effective on both types of constipation.
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