Contractile and relaxant effects of dimaprit on guinea pig isolated intestinal cells

The effect of the histamine H₂ receptor agonist dimaprit on intestinal contractility was characterized on smooth muscle cells isolated from the longitudinal muscle of the guinea pig ileum. Dimaprit exerted two opposite effects on the contractility of isolated muscle cells: relaxation of cholecystokinin octapeptide (CCK-S)-induced contractions in the range of concentrations 10⁻¹⁷-10⁻¹³ M and contraction at concentrations higher than 10⁻¹³ M. The relaxant effect of dimaprit was totally prevented by the H₂ blocker famotidine (10⁻⁷ M), which, at the same time, enhanced the contractile effect of dimaprit, shifting to the left the concentration-response curve to the agonist. This contraction was not modified by the histamine H₁ receptor antagonists pyrilamine and temelastine, tested both at 10⁻⁷ M. By contrast, atropine 10⁻⁸ M abolished the contractile effect of dimaprit, while leaving unchanged the response to CCK-8. Our results clearly indicate that longitudinal muscle cells of the guinea pig ileum possess inhibitory H₂ receptors, which can be activated by very low concentrations of dimaprit; moreover, they revealed that dimaprit can have non-histaminergic effects, probably due to muscarinic receptor activation; however, concentrations about 10000 times higher than those necessary to activate H₂ receptors, are required.