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Pharmacological characterization of RP 62203, a novel 5‐hydroxytryptamine 5‐HT 2 receptor antagonist
Author(s) -
Doble A.,
Girdlestone D.,
Piot O.,
Allam D.,
Betschart J.,
Boireau A.,
Dupuy A.,
Guérémy C.,
Ménager J.,
Zundel J.L.,
Blanchard J.C.
Publication year - 1992
Publication title -
british journal of pharmacology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.432
H-Index - 211
eISSN - 1476-5381
pISSN - 0007-1188
DOI - 10.1111/j.1476-5381.1992.tb14206.x
Subject(s) - receptor , 5 ht receptor , chemistry , serotonin , ritanserin , inositol phosphate , antagonist , receptor antagonist , endocrinology , medicine , pharmacology , inositol , biochemistry , biology
1 RP 62203 (2‐[3‐(4‐(4‐fluorophenyl)‐piperazinyl)propyl]naphto[1,8‐cd]isothiazole‐1,1‐dioxide) is a novel naphtosultam derivative which shows very high affinity for 5‐HT 2 receptors in the rat cerebral cortex ( K i = 50.0 p m ). 2 RP 62203 is relatively selective for this sub‐type of 5‐hydroxytryptamine (5‐HT) receptor, having lower affinity for the 5‐HT 1A receptor and very low affinity for the 5‐HT 3 receptor. RP 62203 displayed low to moderate affinity for α 1 ‐adrenoceptors, dopamine D 2 receptors and histamine H 1 receptors. 3 In vivo binding experiments demonstrated that oral administration of low doses of RP 62203 led to a long‐lasting (> 6 h) occupation of cortical 5‐HT 2 receptors (ID 50 = 0.39 mg kg −1 ). 4 In cortical slices from the neonatal rat, RP 62203 potently inhibited inositol phosphate formation evoked by 5‐HT, with an IC 50 of 7.76 n m . 5 The activity of neurones in the raphé and their responses to microiontophoretically applied 5‐HT were studied with extracellular recording electrodes in the anaesthetized rat. RP 62203 potently and dose‐dependently blocked excitations evoked by 5‐HT when administered at doses of 0.5–4.0 mg kg −1 , i.p. In contrast, neither 5‐HT‐evoked depressions nor glutamate‐evoked excitations of raphé neuronal firing were blocked by RP 62203 at doses as high as 8.0 mg kg −1 i.p. 6 Head twitches induced by 1‐(2,5‐dimethoxy‐4‐iodophenyl)‐2‐aminopropane (DOI) could be abolished by low doses of RP 62203 in mice (ED 50 = 0.44 mg kg −1 , p.o.) and in rats (ED 50 = 1.54 p.o.). Similar results were obtained with mescaline and 5‐hydroxytryptophan (5‐HTP). 7 The potency of RP 62203 was compared with that of three other 5‐HT 2 receptor antagonists, ritanserin, ICI 169,369 and ICI 170,809. In all models, RP 62203 showed similar activity to ritanserin, whilst either ICI 169,369 or ICI 170,809 was several fold less active. 8 It is concluded that RP 62203 is a potent and selective antagonist at 5‐HT 2 receptors in the rodent central nervous system.