Kshama D, Hrishikeshavan H J, Shanbhogue R, Munonyedi U S
Department of Pharmacology, Kasturba Medical College, Manipal, India.
Behav Neural Biol. 1990 Nov;54(3):234-53. doi: 10.1016/0163-1047(90)90617-f.
The present study adopts an ethoexperimental approach to examine the deportment subsequent to alteration in serotonin (5-HT) neurotransmission following treatment with site-specific neuropharmacological probes. The impact of perturbation in (5-HT) neurotransmission on baseline behavior was analyzed employing three animal models of anxiety, i.e., hole-board, elevated plus maze, and bright/dark arena. Inbred male rats (Wistar strain, weighing between 150 and 200 g) were used in this study. The vivarium and the behavioral laboratory were specially designed to permit operation of reversed light-dark cycle and all experiments were performed during the dark period. Pharmacological tools selected to influence 5-HT levels include (1) a combination of tranylcypromine and tryptophan (TCP + TRYPT) (0.75 mg/kg + 40 mg/kg) which augments 5-HT biosynthesis; (2) p-chlorophenylalanine (PCPA: 200 mg/kg), an inhibitor of 5-HT biosynthesis; and (3) 5-HT reuptake blockers, namely zimelidine (ZIM) (40 mg/kg) and fluoxetine (FLU) (10 mg/kg). Rats under the influence of PCPA exhibited anxiolytic response, whereas those under treatments to raise 5-HT levels, viz., TCP + TRYPT, ZIM and FLU, displayed anxiogenic-like reactions. Several other agents known to specifically interact with 5-HT receptor subtypes were also tested. 5-HT2 receptor stimulants, such as quipazine (5 mg/kg) and MK 212 (0.5 mg/kg), were found to be anxiogenic. Buspirone (2 mg/kg), a 5-HT1 agonist, surmounted normal behavioral inhibition. However, another 5-HT1 stimulant, 8-OH-DPAT (0.025 mg/kg), had anxiogenic action. Pretreatment with 5-HT3 antagonists [zacopride (2 mg/kg) and GR 38032F (0.1 mg/kg)] and putative 5-HT1 antagonist [propranolol (10 mg/kg)] resulted in borderline disinhibition of normal behavioral inhibition to novel environments. In contrast, cyproheptadine (0.5 mg/kg), a 5-HT2 antagonist, provoked anxiogenic-like behavior. Altogether, uniform results were obtained for each probe in all the three models, suggesting that the battery of anxiety tests chosen in this study is reliable and sensitive to detect unknown pharmacological responses. The results support the hypothesis that stimulation of serotonergic neurotransmission heightens normal anxiety, whereas its blockade releases normal behavioral inhibition. Furthermore, this work establishes the validity of using the three paradigms in evaluating the involvement of multiple neurotransmitter receptors in the control of behavior of rodents under natural circumstances and also detects any aberration following exposure to novelty and stress.
本研究采用行为实验方法,通过位点特异性神经药理学探针处理后,检测血清素(5-羟色胺,5-HT)神经传递改变后的行为表现。采用三种焦虑动物模型,即洞板实验、高架十字迷宫实验和明/暗箱实验,分析5-HT神经传递扰动对基线行为的影响。本研究使用近交系雄性大鼠(Wistar品系,体重150至200克)。专门设计了饲养室和行为实验室,以允许进行明暗颠倒的光周期操作,所有实验均在黑暗期进行。选择影响5-HT水平的药理学工具包括:(1)反苯环丙胺和色氨酸(TCP + TRYPT)(0.75毫克/千克 + 40毫克/千克)的组合,可增强5-HT生物合成;(2)对氯苯丙氨酸(PCPA:200毫克/千克),一种5-HT生物合成抑制剂;以及(3)5-HT再摄取阻滞剂,即齐美利定(ZIM)(40毫克/千克)和氟西汀(FLU)(10毫克/千克)。受PCPA影响的大鼠表现出抗焦虑反应,而接受提高5-HT水平处理的大鼠,即TCP + TRYPT、ZIM和FLU处理的大鼠,表现出焦虑样反应。还测试了其他几种已知与5-HT受体亚型特异性相互作用的药物。发现5-HT2受体激动剂,如喹哌嗪(5毫克/千克)和MK 212(0.5毫克/千克)具有致焦虑作用。丁螺环酮(2毫克/千克),一种5-HT1激动剂,克服了正常的行为抑制。然而,另一种5-HT1激动剂,8-羟基二丙胺基四氢萘(8-OH-DPAT)(0.025毫克/千克)具有致焦虑作用。用5-HT3拮抗剂[扎考必利(2毫克/千克)和GR 38032F(0.1毫克/千克)]和假定的5-HT1拮抗剂[普萘洛尔(10毫克/千克)]预处理导致对新环境的正常行为抑制出现临界去抑制。相比之下,赛庚啶(0.5毫克/千克),一种5-HT2拮抗剂,引发了焦虑样行为。总之,在所有三个模型中,每个探针都获得了一致的结果,这表明本研究中选择的一系列焦虑测试对于检测未知的药理学反应是可靠且敏感的。结果支持以下假设:血清素能神经传递的刺激会加剧正常焦虑,而其阻断会释放正常的行为抑制。此外,这项工作确立了使用这三种范式评估多种神经递质受体在自然情况下对啮齿动物行为控制中的作用的有效性,并且还检测了暴露于新奇和应激后是否存在任何异常。
