Synthesis and structure-activity relationship of the isoindolinyl benzisoxazolpiperidines as potent,selective, and orally active human dopamine D4 receptor antagonists |
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| Authors: | Hendrix James A Shimshock Stephen J Shutske Gregory M Tomer John D Kapples Kevin J Palermo Mark G Corbett Thomas J Roy Vargas Hugo M Kafka Sharon Brooks Karen M Laws-Ricker Lynn Lee David K H de Lannoy Inez Bordeleau Michel Rizkalla Geihan Owolabi Joshua Kamboj Rajender K |
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| Affiliation: | Aventis Pharmaceuticals Route, 202-206, PO Box 6800, Bridgewater, NJ 08807-0800, USA. james.hendrix@aventis.com |
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| Abstract: | A new class of potent dopamine D(4) antagonists was discovered with selectivity over dopamine D(2) and the alpha-1 adrenoceptor. The lead compound was discovered by screening our compound collection. The structure-activity relationships of substituted isoindoline rings and the chirality about the hydroxymethyl side chain were explored. The isoindoline analogues showed modest differences in potency and selectivity. The S enantiomer proved to be the more potent enantiomer at the D(4) receptor. Several analogues with greater than 100-fold selectivity for D(4) over D(2) and the alpha-1 adrenoreceptor were discovered. Several selective analogues were active in vivo upon oral or intraperitoneal administration. A chiral synthesis starting from either D- or L-O-benzylserine is also described. |
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