Helsley S, Filipink R A, Bowen W D, Rabin R A, Winter J C
Department of Pharmacology and Toxicology, School of Medicine and Biomedical Sciences, State University of New York at Buffalo, 14214-3000, USA.
Pharmacol Biochem Behav. 1998 Feb;59(2):495-503. doi: 10.1016/s0091-3057(97)00454-1.
Although the mechanism of action of ibogaine, a hallucinogen that may be useful in the treatment of addiction, remains unknown, receptor binding studies suggest that ibogaine produces its effects via interactions with multiple receptor types. In addition to serotonergic receptors, which have been studied previously with respect to ibogaine, likely candidates include opiate, sigma (sigma), and phencyclidine (PCP) binding sites. In an attempt to determine which of these receptor interactions are involved in the in vivo effects of ibogaine, ligands for sigma, PCP, and opiate receptors were assessed for their ability to substitute for or to antagonize the ibogaine-induced discriminative stimulus (10 mg/kg I.P., 60 min presession) in Fischer-344 rats. Intermediate levels of generalization were observed with the subtype nonselective sigma ligands 3-(3-hydroxyphenyl)-N-(1-propyl)-piperidine [(+)-3-PPP] (69.0%) and 1,3-di(2-tolyl)guanidine (DTG) (73.5%) but not with the sigma1-selective agents (+)-N-allylnormetazocine [(+)-SKF 10,047] and (+)-pentazocine. These findings, along with observations that ibogaine has appreciable affinity for sigma2 receptors, suggest that these receptors may be involved in the ibogaine discriminative stimulus. With regard to opiate receptors, neither morphine, the prototypic mu agonist, nor kappa selective agonists (bremazocine,and U-50488) substituted for ibogaine. However, intermediate levels of generalization were observed with the mixed action opiates (-)-SKF 10,047 (78.9%), (+/-)-pentazocine (73.9%), nalorphine (70.4%), and diprenorphine (75.0%) indicating a potential role for opiate receptors in the ibogaine stimulus. Partial substitution was also observed with naltrexone (55.6%) but not with naloxone or the selective kappa antagonist nor-binaltorphimine (nor-BNI). These agents were largely ineffective as antagonists of the ibogaine cue, although naloxone produced a moderate but statistically significant antagonism (69.8%). In addition, naloxone produced complete antagonism of the ibogaine-appropriate responding elicited by both (-)-SKF 10,047 (19.7%) and nalorphine (25.8%), whereas the ibogaine-appropriate responding produced by diprenorphine was only partially antagonized (44.4%). The latter observations taken together with the finding that both nalorphine (>100 microM) and diprenorphine (30 microM) have extremely low affinity for sigma2 receptors, suggest that the ibogaine-appropriate responding produced by these agents is not mediated by sigma2 receptors. These findings imply that opiate effects may be involved in the ibogaine stimulus. In contrast to sigma2 and opiate receptors, ibogaine's reported interactions with NMDA receptors do not appear to be involved in its discriminative stimulus, as neither PCP nor MK-801 produced a significant level of ibogaine-appropriate responding. Thus, the present study offers evidence that unlike NMDA receptors, both sigma2 and opiate receptors may be involved in the ibogaine discriminative stimulus.
伊博格碱是一种可能对治疗成瘾有用的致幻剂,尽管其作用机制尚不清楚,但受体结合研究表明,伊博格碱通过与多种受体类型相互作用产生其效果。除了先前已针对伊博格碱进行研究的血清素能受体外,可能的候选受体包括阿片、西格玛(σ)和苯环己哌啶(PCP)结合位点。为了确定这些受体相互作用中哪些参与了伊博格碱的体内效应,评估了西格玛、PCP和阿片受体的配体替代或拮抗伊博格碱诱导的辨别刺激(腹腔注射10mg/kg,给药前60分钟)在Fischer-344大鼠中的能力。在非选择性亚型的西格玛配体3-(3-羟基苯基)-N-(1-丙基)-哌啶(+)-3-PPP和1,3-二(2-甲苯基)胍(DTG)(73.5%)中观察到中等程度的泛化,但在西格玛1选择性药物(+)-N-烯丙基去甲美沙酮[(+)-SKF 10,047]和(+)-喷他佐辛中未观察到。这些发现,连同伊博格碱对西格玛2受体具有明显亲和力的观察结果,表明这些受体可能参与了伊博格碱辨别刺激。关于阿片受体,原型μ激动剂吗啡和κ选择性激动剂(布瑞马唑辛和U-50488)均不能替代伊博格碱。然而,在混合作用的阿片类药物(-)-SKF 10,047(78.9%)、(+/-)-喷他佐辛(73.9%)、纳洛芬(70.4%)和二丙诺啡(75.0%)中观察到中等程度的泛化,表明阿片受体在伊博格碱刺激中可能发挥作用。纳曲酮(55.6%)也观察到部分替代,但纳洛酮或选择性κ拮抗剂去甲双丙吗啡(nor-BNI)则没有。这些药物作为伊博格碱线索的拮抗剂大多无效,尽管纳洛酮产生了中等程度但具有统计学意义的拮抗作用(69.8%)。此外,纳洛酮完全拮抗了由(-)-SKF 10,047(19.7%)和纳洛芬(25.8%)引起的与伊博格碱相符的反应,而二丙诺啡引起的与伊博格碱相符的反应仅被部分拮抗(44.4%)。后一观察结果与纳洛芬(>100μM)和二丙诺啡(30μM)对西格玛2受体具有极低亲和力的发现一起,表明这些药物引起的与伊博格碱相符的反应不是由西格玛2受体介导的。这些发现意味着阿片类效应可能参与了伊博格碱刺激。与西格玛2和阿片受体不同,伊博格碱与NMDA受体的报道相互作用似乎不参与其辨别刺激,因为PCP和MK-801均未产生显著水平的与伊博格碱相符反应。因此,本研究提供了证据表明,与NMDA受体不同,西格玛2和阿片受体都可能参与伊博格碱辨别刺激。
