Abstract
The effect of amphetamine on gastrointestinal (GI) transit and the plasma levels of cholecystokinin (CCK) were studied in male rats.
Gastric emptying was inhibited both acutely and chronically by the administration of amphetamine. GI transit was decreased by the acute administration of amphetamine but not affected by the chronic administration of amphetamine.
Plasma CCK levels were increased dose-dependently by amphetamine.
Proglumide, a CCK receptor antagonist, prevented amphetamine-induced inhibition of gastric emptying and the decrease in GI transit in male rats.
The selective CCKA receptor antagonist, lorglumide, dose-dependently attenuated the amphetamine-induced inhibition of gastric emptying in male rats. In contrast, the selective CCKB receptor antagonist, PD 135,158, did not reverse the effect of amphetamine on gastric emptying.
Both lorglumide and PD 135,158 reversed the inhibitory effect of amphetamine on GI transit in male rats.
These results suggest that amphetamine-induced inhibition of gastric emptying and intestinal transit is due in part to a mechanism associated with the hypersecretion of endogenous CCK.
Keywords: Amphetamine; cholecystokinin (CCK); gastric emptying; gastrointestinal (GI) transit; geometric centre; lorglumide; proglumide; PD 135,158
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