TY - JOUR T1 - S 18126 ({2-[4-(2,3-dihydrobenzo[1,4]dioxin-6-yl)piperazin-1-yl methyl]indan-2-yl}), a Potent, Selective and Competitive Antagonist at Dopamine D<sub>4</sub> Receptors: An <em>In Vitro</em> and<em>In Vivo</em> Comparison with L 745,870 (3-(4-[4-chlorophenyl]piperazin-1-yl)methyl-1H-pyrrolo[2,3b]pyridine) and Raclopride JF - Journal of Pharmacology and Experimental Therapeutics JO - J Pharmacol Exp Ther SP - 167 LP - 186 VL - 287 IS - 1 AU - Mark J. Millan AU - Adrian Newman-Tancredi AU - Mauricette Brocco AU - Alain Gobert AU - Françoise Lejeune AU - Valérie Audinot AU - Jean-Michel Rivet AU - Rudy Schreiber AU - Anne Dekeyne AU - Michael Spedding AU - Jean-Paul Nicolas AU - Jean-Louis Peglion Y1 - 1998/10/01 UR - http://jpet.aspetjournals.org/content/287/1/167.abstract N2 - The novel benzoindane S 18126 possessed &gt; 100-fold higher affinity at cloned, human (h) D4 (Ki = 2.4 nM) vs. hD2 (738 nM), hD3(2840 nM), hD1 (&gt; 3000 nM) and hD5 (&gt; 3000 nM) receptors and about 50 other sites, except ς1receptors (1.6 nM). L 745,870 similarly showed selectivity for hD4 (2.5 nM) vs. hD2 (905 nM) and hD3 (&gt; 3000 nM) receptors. In contrast, raclopride displayed low affinity at hD4 (&gt; 3000 nM) vs.hD2 (1.1 nM) and hD3 receptors (1.4 nM). Stimulation of [35S]-GTPγS binding at hD4receptors by dopamine (DA) was blocked by S 18126 and L 745,870 withKb values of 2.2 and 1.0 nM, respectively, whereas raclopride (&gt; 1000 nM) was inactive. In contrast, raclopride inhibited stimulation of [35S]-GTPγS binding at hD2 sites by DA with a Kb of 1.4 nM, whereas S 18126 (&gt; 1000 nM) and L 745,870 (&gt; 1000 nM) were inactive. As concerns presynaptic dopaminergic receptors, raclopride (0.01–0.05 mg/kg s.c.) markedly enhanced DA synthesis in mesocortical, mesolimbic and nigrostriatal dopaminergic pathways. In contrast, even high doses (2.5–40.0 mg/kg s.c.) of S 18126 and L 745,870 were only weakly active. Similarly, raclopride (0.016 mg/kg i.v.) abolished inhibition of the firing rate of ventrotegmental dopaminergic neurons by apomorphine, whereas even high doses (0.5 mg/kg i.v.) of S 18126 and L 745,870 were only weakly active. As regards postsynaptic dopaminergic receptors, raclopride potently (0.01–0.3 mg/kg s.c.) reduced rotation elicited by quinpirole in rats with unilateral lesions of the substantia nigra, antagonized induction of hypothermia by PD 128,907, blocked amphetamine-induced hyperlocomotion and was effective in six further models of potential antipsychotic activity. In contrast, S 18126 and L 745,870 were only weakly active in these models (5.0–&gt; 40.0 mg/kg s.c.). In six models of extrapyramidal and motor symptoms, such as induction of catalepsy, raclopride was likewise potently active (0.01–2.0 mg/kg s.c.) whereas S 18126 and L 745,870 were only weakly active (10.0–80.0 mg/kg s.c.). In freely moving rats, raclopride (0.16 mg/kg s.c.) increased levels of DA by + 55% in dialysates of the frontal cortex. However, it also increased levels of DA in the accumbens and striatum by 70% and 75%, respectively. In contrast to raclopride, at a dose of 0.16 mg/kg s.c., neither S 18126 nor L 745,870 modified frontal cortex levels of DA. However, at a high dose (40.0 mg/kg s.c.), S 18126 increased dialysate levels of DA (+ 85%) and noradrenaline (+ 100%), but not serotonin (+ 10%), in frontal cortexwithout affecting DA levels in accumbens (+ 10%) and striatum (+ 10%). In conclusion, S 18126 and L 745,870 behave as potent and selective antagonists of cloned, hD4vs. other dopaminergic receptor types in vitro. However, their in vivo effects at high doses probably reflect residual antagonist actions at D2 (or D3) receptors. Selective blockade of D4receptors was thus associated neither with a modification of dopaminergic transmission nor with antipsychotic (antiproductive) or extrapyramidal properties. The functional effects of selective D4 receptor blockade remain to be established. The American Society for Pharmacology and Experimental Therapeutics ER -