Wolfe S A, Kulsakdinun C, Battaglia G, Jaffe J H, De Souza E B
Neuroscience Branch, National Institute on Drug Abuse, Baltimore, Maryland.
J Pharmacol Exp Ther. 1988 Dec;247(3):1114-9.
Phencyclidine (PCP) has been reported to suppress a variety of immune functions in vitro. Because PCP binds with high affinity to both PCP and sigma receptors, the identity of the receptor(s) mediating the immunological effects of PCP is unknown. The aim of the present study was to identify and characterize the sites of PCP action (sigma and/or PCP receptors) in human peripheral blood leukocytes (PBL) using [3H]haloperidol or 1,3 di(2-([5-3H]tolyl)guanidine ([3H]DTG) to specifically label sigma receptors and 3,4-[3H]-(N)-[1-(2-thienyl)-cyclohexyl]-piperidine ([3H]TCP) to specifically label PCP receptors. [3H]Haloperidol binding was saturable and of high affinity with comparable KD values in human PBL (0.44 +/- 0.10 nM) and rat cerebellum (0.51 +/- 0.09 nM). Similarly, [3H]DTG binding was saturable with comparable KD values of 29.5 +/- 3.5 and 26.4 +/- 3.6 nM in rat cerebellum and human PBL, respectively. In contrast, there was a notable absence of [3H]TCP-labeled PCP receptors in human PBL and rat cerebellum. In competition studies, the pharmacologic profile of [3H]haloperidol-labeled sigma receptors in human PBL was virtually identical with that in rat cerebellum (slope, 0.87; correlation coefficient, 0.96); the rank order of potency of competing drugs was haloperidol greater than l-butaclamol = pentazocine greater than d-3-(hydroxyphenyl)-N-(1-propyl)-piperidine greater than DTG = d-butaclamol = d-SKF 10,047 greater than levallorphan greater than or equal to PCP greater than or equal to l-SKF 10,047 greater than TCP greater than MK-801.(ABSTRACT TRUNCATED AT 250 WORDS)
据报道,苯环利定(PCP)在体外可抑制多种免疫功能。由于PCP与PCP受体和σ受体均具有高亲和力结合,介导PCP免疫效应的受体身份尚不清楚。本研究的目的是使用[3H]氟哌啶醇或1,3-二(2-([5-3H]甲苯基)胍([3H]DTG)特异性标记σ受体,以及3,4-[3H]-(N)-[1-(2-噻吩基)-环己基]-哌啶([3H]TCP)特异性标记PCP受体,来鉴定和表征PCP在人外周血白细胞(PBL)中的作用位点(σ和/或PCP受体)。[3H]氟哌啶醇结合具有饱和性且亲和力高,在人PBL(0.44±0.10 nM)和大鼠小脑(0.51±0.09 nM)中的KD值相当。同样,[3H]DTG结合在大鼠小脑和人PBL中也具有饱和性,并分别具有29.5±3.5和26.4±3.6 nM的相当KD值。相比之下,在人PBL和大鼠小脑中明显不存在[3H]TCP标记的PCP受体。在竞争研究中,人PBL中[3H]氟哌啶醇标记的σ受体的药理学特征与大鼠小脑几乎相同(斜率为0.87;相关系数为0.96);竞争药物效力的顺序为氟哌啶醇大于l-布他拉莫=喷他佐辛大于d-3-(羟苯基)-N-(1-丙基)-哌啶大于DTG=d-布他拉莫=d-SKF 10,047大于左洛啡烷大于或等于PCP大于或等于l-SKF 10,047大于TCP大于MK-801。(摘要截短于250字)
