Carbon monoxide contributes to the constipating effects of granisetron in rat colon.

ABSTRACT

AIM: To investigate the mechanisms underlying the potential contribution of the heme oxygenase/carbon monoxide (HO/CO) pathway in the constipating effects of granisetron. METHODS: For in vivo studies, gastrointestinal motility was evaluated in male rats acutely treated with granisetron [25, 50, 75 µg/kg/subcutaneous (sc)], zinc protoporphyrin IX [ZnPPIX, 50 µg/kg/intraperitoneal (ip)] and hemin (50 µmol/L/kg/ip), alone or in combination. For in vitro studies, the contractile neurogenic response to electrical field stimulation (EFS, 3, 5, 10 Hz, 14 V, 1 ms, pulse trains lasting 10 s), as well as the contractile myogenic response to acetylcholine (ACh, 0.1-100 µmol/L) were evaluated on colon specimens incubated with granisetron (3 µmol/L, 15 min), ZnPPIX (10 µmol/L, 60 min) or CO-releasing molecule-3 (CORM-3, 100, 200, 400 µmol/L) alone or in combination. These experiments were performed under co-treatment with or without atropine (3 µmol/L, a muscarinic receptor antagonist) or NG-nitro-L-Arginine (L-NNA, 100 µmol/L, a nitric oxide synthase inhibitor). RESULTS: Administration of granisetron (50, 75 µg/kg) in vivo significantly increased the time to first defecation (P = 0.045 vs vehicle-treated rats), clearly suggesting a constipating effect of this drug. Although administration of ZnPPIX or hemin alone had no effect on this gastrointestinal motility parameter, ZnPPIX co-administered with granisetron abolished the granisetron-induced constipation. On the other hand, co-administration of hemin and granisetron did not modify the increased constipation observed under granisetron alone. When administered in vitro, granisetron alone (3 µmol/L) did not significantly modify the colon's contractile response to either EFS or ACh. Incubation with ZnPPIX alone (10 µmol/L) significantly reduced the colon's contractile response to EFS (P = 0.016) but had no effect on contractile response to ACh. Co-administration of ZnPPIX and atropine (3 µmol/L) abolished the ZnPPIX-mediated decrease in contractile response to EFS. Conversely, incubation with CORM-3 (400 µmol/L) alone increased both the contractile response to EFS at 10 Hz (10 Hz 71.02 ± 19.16 vs 116.25 ± 53.70, P = 0.01) and the contractile response to ACh (100 µmol/L) (P = 0.012). Co-administration of atropine abolished the CORM-3-mediated effects on the EFS-mediated response. When granisetron was co-incubated in vitro with ZnPPIX, the ZnPPIX-mediated decrease in colon contractile response to EFS was lost. On the other hand, co-incubation of granisetron and CORM-3 (400 µmol/L) further increased the colon's contractile response to EFS (at 5 Hz P = 0.007; at 10 Hz P = 0.001) and to ACh (ACh 10 µmol/L P = 0.001; ACh 100 µmol/L P = 0.001) elicited by CORM-3 alone. L-NNA co-administered with granisetron and CORM-3 abolished the potentiating effect of CORM-3 on granisetron on both the EFS-induced and ACh-induced contractile response. CONCLUSION: Taken together, findings from in vivo and in vitro studies suggest that the HO/CO pathway is involved in the constipating effects of granisetron.