Largent B L, Gundlach A L, Snyder S H
Proc Natl Acad Sci U S A. 1984 Aug;81(15):4983-7. doi: 10.1073/pnas.81.15.4983.
3-(3-Hydroxyphenyl)-N-(1-propyl)piperidine (3-PPP) has been proposed as a selective dopamine autoreceptor agonist in the central nervous system. This report describes the pharmacology and localization of specific high-affinity binding sites for (+)-[3H]3-PPP in brain. The drug specificity of (+)-[3H]3-PPP binding is identical to that of sigma receptors, which may mediate psychotomimetic effects of some opiates. Haloperidol and the opioid derivatives, pentazocine, cyclazocine, and SKF 10,047 are potent inhibitors of (+)-[3H]3-PPP binding. Stereoselectivity is exhibited for the (+) isomers of cyclazocine and SKF 10,047 at the sigma site, opposite to the stereoselectivity seen at mu, delta, and kappa opiate receptors. (+)-[3H]3-PPP does not label dopamine receptors, as potent dopamine agonists and antagonists are weak inhibitors of binding and the localization of specific (+)-[3H]3-PPP binding sites does not parallel that of dopamine neurons. Discrete localizations of (+)-[3H]3-PPP binding sites in many brain areas including limbic, midbrain, brainstem, and cerebellar regions may explain psychotomimetic actions of opiates and behavioral effects of 3-PPP.
3-(3-羟基苯基)-N-(1-丙基)哌啶(3-PPP)被认为是中枢神经系统中的一种选择性多巴胺自身受体激动剂。本报告描述了脑中(+)-[3H]3-PPP特异性高亲和力结合位点的药理学和定位。(+)-[3H]3-PPP结合的药物特异性与西格玛受体相同,西格玛受体可能介导某些阿片类药物的拟精神病效应。氟哌啶醇和阿片类衍生物喷他佐辛、环佐辛及SKF 10,047是(+)-[3H]3-PPP结合的强效抑制剂。环佐辛和SKF 10,047的(+)异构体在西格玛位点表现出立体选择性,这与在μ、δ和κ阿片受体上观察到的立体选择性相反。(+)-[3H]3-PPP不标记多巴胺受体,因为强效多巴胺激动剂和拮抗剂是结合的弱抑制剂,且特异性(+)-[3H]3-PPP结合位点的定位与多巴胺神经元的定位不一致。(+)-[3H]3-PPP结合位点在包括边缘系统、中脑、脑干和小脑区域在内的许多脑区中的离散定位,可能解释了阿片类药物的拟精神病作用和3-PPP的行为效应。
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