The actions of the cannabinoid receptor antagonist, SR 141716A, in the rat isolated mesenteric artery

Abstract

The actions of the cannabinoid receptor antagonist, SR 141716A, were examined in rat isolated mesenteric arteries. At concentrations greater than 3 μM, it caused concentration‐dependent, but endothelium‐independent, relaxations of both methoxamine‐ and 60 mM KCl‐precontracted vessels. SR 141716A (at 10 μM, but not at 1 μM) inhibited contractions to Ca²⁺ in methoxamine‐stimulated mesenteric arteries previously depleted of intracellular Ca²⁺ stores. Neither concentration affected the phasic contractions induced by methoxamine in the absence of extracellular Ca²⁺. SR 141716A (10 μM) caused a 130 fold rightward shift in the concentration‐response curve to levcromakalim, a K⁺ channel activator, but had no effect at 1 μM. SR 141716A (10 μM) attenuated relaxations to NS 1619 (which activates large conductance, Ca²⁺‐activated K⁺ channels; BK_Ca). The inhibitory effect of SR 141716A on NS 1619 was not significantly different from, and was not additive with, that caused by a selective BK_Ca inhibitor, iberiotoxin (100 nM). SR 141716A (1 μM) did not effect NS 1619 relaxation. SR 141716A (10 μM) had no effect on relaxations to the nitric oxide donor S‐nitroso‐N‐acetylpenicillamine, or relaxations to carbachol in the presence of 25 mM KCl. The results show that, at concentrations of 10 μM and above, SR 141716A causes endothelium‐independent vasorelaxation by inhibition of Ca²⁺ entry. It also inhibits relaxations mediated by K⁺ channel activation. This suggests that such concentrations of SR 141716A are not appropriate for investigation of cannabinoid receptor‐dependent processes. British Journal of Pharmacology (1998) 125, 689–696; doi:10.1038/sj.bjp.0702127