首页> 外文期刊>Behavioural Brain Research: An International Journal >Effect of cannabidiol in a MK-801-rodent model of aspects of Schizophrenia.
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Effect of cannabidiol in a MK-801-rodent model of aspects of Schizophrenia.

机译:大麻酚在精神分裂症的MK-801-啮齿动物模型中的作用。

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Cannabidiol is a non-psychoactive phytocannabinoid which, based on several previous preclinical and clinical reports, is purported to have antipsychotic potential. The purpose of this investigation was to further investigate if these effects would be seen using an MK-801-induced rat model of aspects of schizophrenia. MK-801 is an NMDA receptor-antagonist known to produce hyperactivity, deficits in prepulse inhibition and social withdrawal, behaviours which correlate well with some of the positive, cognitive and negative symptoms of schizophrenia. Following a 4-day acclimatisation to the holding room, rats were acclimatised to startle chambers on day 5 and their prepulse inhibition (PPI) determined on day 6 following treatment with cannabidiol or vehicle and MK-801 or vehicle. On day 9, rats were acclimatised to the social interaction testing arena and on day 10, were tested for social interaction and locomotor activity following the same treatments. Cannabidiol treatment alone disrupted PPI and produced hyperactivity but had no effect on social behaviour. Cannabidiol had no effect on MK-801-induced disruption of PPI or hyperactivity but showed potential towards inhibiting MK-801-induced social withdrawal. As a comparator, we also tested the effect of the atypical antipsychotic clozapine which only partially reversed MK-801-induced disruption of PPI but was able to reverse MK-801-induced hyperactivity and social withdrawal. In conclusion, cannabidiol showed both propsychotic activity and partial antipsychotic activity in an MK-801-induced model of aspects of schizophrenia. Further behavioural studies would be required using a range of species, strains, animal models and testing paradigms to conclusively establish the antipsychotic potential of cannabidiol.
机译:卡纳比多醇是一种非精神活性植物大麻素,根据先前的一些临床前和临床报告,据称具有抗精神病药的潜力。这项研究的目的是进一步研究使用MK-801诱导的精神分裂症方面的大鼠模型是否会观察到这些影响。 MK-801是一种NMDA受体拮抗剂,已知会产生活动过度,前冲抑制不足和社交退缩,与精神分裂症的某些积极,认知和消极症状相关的行为。在适应贮藏室4天后,在第5天使大鼠适应惊吓室,并在用大麻素或媒介物和MK-801或媒介物治疗后第6天确定其预脉冲抑制(PPI)。在第9天,使大鼠适应社交互动测试领域,并在第10天,按照相同的治疗方法测试社交互动和运动能力。单用大麻二酚治疗会破坏PPI并产生过度活跃,但对社交行为没有影响。卡纳比多二醇对MK-801引起的PPI破坏或活动过度没有影响,但显示出抑制MK-801引起的社交退缩的潜力。作为比较者,我们还测试了非典型抗精神病药物氯氮平的作用,该作用仅部分逆转了MK-801引起的PPI破坏,但能够逆转MK-801引起的过度活跃和社交退缩。总之,在MK-801诱导的精神分裂症方面的模型中,大麻二酚同时显示了促精神病活性和部分抗精神病活性。需要使用一系列物种,品系,动物模型和测试范式进行进一步的行为研究,以最终确定大麻二酚的抗精神病潜力。

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