SDZ PSD 958, a novel D1 receptor antagonist with potential limbic selectivity

Abstract

SDZ PSD 958, a novel benzo[g]quinoxaline derivative exhibits the properties of a potent orally active selective D₁ receptor antagonist. It has high affinity for D₁-like receptors (D₁, D₅; pKi=9.7–9.8) labelled by [³H]SCH23390 and is at least 400 fold less active at D₂-like receptors (i.e. D₂, D₄) labelled by [³H]spiperone. Effects in functional tests are consistent with d₁ receptor antagonist properties. SDZ PSD 958 inhibited apomorphine-induced rearing in mice and prevented prolongation of novelty-induced locomotion in rats elicited by the selective D₁ receptor agonist CY 208-243. By contrast, SDZ PSD 958 did not induce catalepsy and only weakly inhibited apomorphine-induced stereotyped gnawing in rats. This suggests that SDZ PSD 958 preferentially inhibits responses mediated by dopamine systems innervating the limbic system.