Pharmacological characterization of PD 152255, a novel dimeric benzimidazole dopamine D3 antagonist

被引：16

作者：

Corbin, AE

Pugsley, TA

Akunne, HC

Whetzel, SZ

Zoski, KT

Georgic, LM

Nelson, CB

Wright, JL

Wise, LD

Heffner, TG

机构：

[1] Warner Lambert Parke Davis, Parke Davis Pharmaceut Res, Psychiat Disorders Therapeut, Ann Arbor, MI 48105 USA

[2] Warner Lambert Parke Davis, Parke Davis Pharmaceut Res, Neurol & Neurodegenerat Dis Therapeut, Ann Arbor, MI 48105 USA

[3] Warner Lambert Parke Davis, Parke Davis Pharmaceut Res, Psychiat Disorders Chem, Ann Arbor, MI 48105 USA

来源：

PHARMACOLOGY BIOCHEMISTRY AND BEHAVIOR | 1998年 / 59卷 / 02期

关键词：

dopamine D-3 receptors; dopamine D-3 antagonist; locomotor activity; antipsychotic;

D O I：

10.1016/S0091-3057(97)00442-5

中图分类号：

B84 [心理学]; C [社会科学总论]; Q98 [人类学];

学科分类号：

03 ; 0303 ; 030303 ; 04 ; 0402 ;

摘要：

152255 (E-1,1'-(2-butene-1,4-diyl)bis [2-[4-[3-(1-piperidinyl)propoxy]-phenyl]-1H-benzimidazole]) exhibited high affinity (K-i = 12.7 nM) for human dopamine (DA) D-3 receptors expressed in CHO K1 cells but not for DA D-2L receptors (K-i = 565 nM), DA D-4.2 or DA D-1 receptors (K-i > 3 mu M) and a number of other neurotransmitter receptors. Affinity for human muscarinic receptors was seen in vitro but no functional muscarinic agonist and/or antagonist action was observed in vivo. Antagonist activity at DA D-3 receptors was demonstrated by blockade of quinpirole-stimulated [H-3]-thymidine uptake in D-3 transfected cells, an effect that was 28-fold more potent than in D-2-transfected cells. Unlike classical DA D-2 antagonists, PD 152255 did not increase rat brain DA synthesis and it increased locomotion in habituated rats. However, like antipsychotics, PD 152255 reduced locomotor activity in mice and reduced spontaneous and amphetamine-stimulated locomotion in nonhabituated rats. These results demonstrate that PD 152255 is a DA D-3 antagonist that may have antipsychotic activity. (C) 1998 Elsevier Science Inc.

引用

页码：487 / 493

页数：7

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