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Clozapine attenuates disruptions in response inhibition and task efficiency induced by repeated phencyclidine administration in the intracranial self-stimulation procedure

机译:氯氮平减轻颅内自我刺激程序中反复苯环利定给药引起的反应抑制和任务效率的破坏

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摘要

Currently available antipsychotic medications lack satisfactory effectiveness against several symptom clusters of schizophrenia, including affective symptoms (e.g., anhedonia) and cognitive deficits (e.g., impulsivity). Translational animal models analogous to these symptoms are necessary to provide insights into the neurobiological events underlying these impairments and allow the development of improved schizophrenia treatments. We investigated the effects of repeated administration of the psychotomimetic phencyclidine (PCP), a noncompetitive N-methyl-D-aspartate receptor antagonist, on performance in the intracranial self-stimulation (ICSS) procedure, a test of reward function. We also explored how chronic treatment with clozapine, an atypical antipsychotic with limited effectiveness on affective and cognitive schizophrenia symptoms, would affect PCP-induced disruptions of ICSS performance. A single injection of 2 mg/kg PCP elevated ICSS thresholds, suggesting a reward deficit. Repeated PCP administration (2 mg/kg once daily for 2 consecutive days followed by a 2-week drug free period, and then 5 consecutive days of 2 mg/kg PCP daily, s.c., 30 min pretreatment) resulted in a small, but significant, lowering of ICSS reward thresholds, indicating increased reward function. Chronic clozapine did not alter the effects of repeated PCP on ICSS thresholds. Repeated PCP also increased the number of extra and timeout responses performed during the ICSS procedure, reflecting disinhibition of inappropriate responding and decreased task efficiency. Chronic clozapine attenuated the increase in extra responses induced by repeated PCP and tended to reduce the PCP-induced increase in timeout responses. These results suggest that repeated PCP administration does not produce an anhedonia-like state resembling that seen in schizophrenia. However, the increased impulsivity and reduced task efficiency seen with repeated PCP administration, and the sensitivity of these effects to attenuation with an atypical antipsychotic, suggest that repeated PCP administration may be a useful inducing condition for eliciting cognitive deficits with relevance to schizophrenia.
机译:当前可用的抗精神病药物对精神分裂症的几种症状簇缺乏令人满意的效果,包括情感症状(例如,快感不足)和认知缺陷(例如,冲动)。必须提供类似于这些症状的转化动物模型,以洞悉这些损伤背后的神经生物学事件,并开发出改进的精神分裂症治疗方法。我们研究了重复给药非竞争性N-甲基-D-天冬氨酸受体拮抗剂精神模拟物苯环利定(PCP)对颅内自我刺激(ICSS)程序(奖励功能测试)的表现的影响。我们还探讨了氯氮平(一种非典型的抗精神病药,对情感和认知型精神分裂症症状的疗效有限)的慢性治疗将如何影响PCP诱导的ICSS功能中断。单次注射2 mg / kg PCP可提高ICSS阈值,提示奖励不足。重复PCP给药(连续2天每天2 mg / kg一次,随后为期2周的无药期,然后连续5天每天2 mg / kg PCP进行皮下注射,治疗前30分钟)产生了少量但显着的结果,降低ICSS奖励阈值,表明奖励功能增强。慢性氯氮平并未改变反复PCP对ICSS阈值的影响。重复的PCP还增加了在ICSS程序中执行的额外响应和超时响应的数量,这反映了对不适当响应的抑制作用以及任务效率的降低。慢性氯氮平可减轻重复PCP引起的额外反应的增加,并倾向于减少PCP诱导的超时反应的增加。这些结果表明,反复给予PCP不会产生类似于精神分裂症的类似快感状态。但是,重复PCP给药会增加冲动性并降低任务效率,并且这些作用对非典型抗精神病药的缓解敏感,表明重复PCP给药可能是诱发与精神分裂症相关的认知缺陷的有用诱导条件。

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