Interactions of new and conventional H3-antagonists with non-histaminergic receptors involved in neurogenic and myogenic contractile responses of guinea-pig ileum
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引用次数: 7
Abstract
1 Possible effects of new and conventional H3-receptor antagonists towards various non-histaminergic receptors (α2-adrenergic, 5-HT3-serotonin, μ-opiate, A1-adenosine, M1-and M3-muscarinic) involved in neurogenic and myogenic contractile responses of guinea-pig ileum are investigated.
2 When the isolated ileum was contracted by the 5-HT3 receptor agonist, 2-methyl-5-HT (5 × 10−−7–8 × 10−−6m), acetylcholine (1 × 10−−9–1 × 10−−7m), KCl (3 × 10−−2m) or electrical stimulation some of the drugs, included thioperamide and clobenpropit, reduced the contractile response when tested at micromolar concentrations (1–3 × 10−−5m) (only compound IV exhibited an M3 competitive antagonism with a pKB = 5.49 ± 0.18).
3 Ileal twitch responses to electrical stimulation were dose-dependently inhibited by the selective agonists clonidine (3 × 10−−10–1 × 10−−7m), dermorphin (1 × 10−−11–1 × 10−−8m), R-N6-(2-phenylisopropyl)-adenosine (1 × 10−−9–3 × 10−−8m) and McN-A-343 (1 × 10−−7–1 × 10−−5m) with different potencies and comparable efficacy (spike amplitude reduction > 85%). All the H3 antagonists under study (up to 1 × 10−−5m) showed no or minor interactions at the neuronal sites except the compound V which behaved as a weak competitive antagonist at α2-adrenoreceptors (pKB = 5.96 ± 0.06).
4 In conclusion, both new and conventional H3-blockers interacted at the enteric neuronal sites here studied with a 1000–30 000 fold lower antagonistic potency than that previously reported for the ileal H3 histamine receptors. Their spasmolytic activity precludes firm conclusions about the non-competitive interaction with 5-HT3 ileal receptor which requires further investigations.