Δ-THC and related cannabinoids suppress substance P- induced neurokinin NK-receptor-mediated vomiting via activation of cannabinoid CB receptor.

Δ-THC suppresses cisplatin-induced vomiting through activation of cannabinoid CB receptors. Cisplatin-evoked emesis is predominantly due to release of serotonin and substance P (SP) in the gut and the brainstem which subsequently stimulate their corresponding 5-HT-and neurokinin NK-receptors to induce vomiting. Δ-THC can inhibit vomiting caused either by the serotonin precursor 5-HTP, or the 5-HT receptor selective agonist, 2-methyserotonin. In the current study, we explored whether Δ-THC and related CB/CB receptor agonists (WIN55,212-2 and CP55,940) inhibit vomiting evoked by SP (50 mg/kg, i.p.) or the NK receptor selective agonist GR73632 (5 mg/kg, i.p.). Behavioral methods were employed to determine the antiemetic efficacy of cannabinoids in least shrews. Our results showed that administration of varying doses of Δ-THC (i.p. or s.c.), WIN55,212-2 (i.p.), or CP55,940 (i.p.) caused significant suppression of SP-evoked vomiting in a dose-dependent manner. When tested against GR73632, Δ-THC also dose-dependently reduced the evoked emesis. The antiemetic effect of Δ-THC against SP-induced vomiting was prevented by low non-emetic doses of the CB receptor inverse-agonist/antagonist SR141716A (<10 mg/kg). We also found that the NK receptor antagonist netupitant can significantly suppress vomiting caused by a large emetic dose of SR141716A (20 mg/kg). In sum, Δ-THC and related cannabinoids suppress vomiting evoked by the nonselective (SP) and selective (GR73632) neurokinin NK receptor agonists via stimulation of cannabinoid CB receptors.