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慢性青春期大麻素处理后成年大鼠的行为障碍与Fos蛋白表达改变

Behavioural disturbances and altered Fos protein expression in adult rats after chronic pubertal cannabinoid treatment.

作者信息

Wegener Nico, Koch Michael

机构信息

Brain Research Institute, Department of Neuropharmacology, University of Bremen, Bremen, Germany.

出版信息

Brain Res. 2009 Feb 9;1253:81-91. doi: 10.1016/j.brainres.2008.11.081. Epub 2008 Dec 3.

Abstract

Cannabis is one of the world's most popular recreational drugs. However, little is known about long-lasting cellular and neurobehavioural effects of chronic cannabinoid intake, especially during puberty where cannabis use among humans is commonly initiated. This study in rats investigates the long-term effect of pubertal cannabinoid treatment on prepulse inhibition (PPI), locomotor activity and on anxiety in the elevated-plus maze during adulthood. Furthermore, changes in adult basic neuronal activity, assessed by c-Fos immunoreactivity (Fos IR), and a potentially altered Fos expression after acute treatment with dopaminergic drugs was evaluated. Chronic treatment with the synthetic cannabinoid full agonist WIN 55,212-2 (WIN; 1.2 mg/kg) was carried out over 25 days of the rats' puberty and subsequent behavioural testing was conducted in adult animals. Finally, Fos IR was evaluated in several brain regions under basal conditions and after acute administration of haloperidol (0.1 mg/kg) and apomorphine (2 mg/kg). Chronic WIN treated animals exhibited a lasting disruption of PPI. These rats were also more active in the open field and less anxious in the elevated-plus maze than their vehicle treated controls. Additionally, when comparing Fos IR in selected brain regions, these animals displayed altered basal neuronal activity and responded differently to acute application of haloperidol or apomorphine. Taken together, these results indicate that chronic stimulation of the cannabinoid receptor CB(1) during the rats' puberty not only leads to persistent behavioural changes but also to cellular long-term adaptations within brain regions critical for drug of abuse or neuropsychiatric diseases.

摘要

大麻是全球最受欢迎的消遣性毒品之一。然而,对于长期摄入大麻素所产生的持久细胞和神经行为影响,我们知之甚少,尤其是在人类大麻使用通常始于青春期的这个阶段。本项针对大鼠的研究,探究了青春期给予大麻素对成年期前脉冲抑制(PPI)、运动活动以及高架十字迷宫中焦虑行为的长期影响。此外,通过c-Fos免疫反应性(Fos IR)评估成年期基础神经元活动的变化,并评估多巴胺能药物急性处理后Fos表达的潜在改变。在大鼠青春期的25天内,使用合成大麻素完全激动剂WIN 55,212-2(WIN;1.2毫克/千克)进行慢性处理,随后对成年动物进行行为测试。最后,在基础条件下以及急性给予氟哌啶醇(0.1毫克/千克)和阿扑吗啡(2毫克/千克)后,评估几个脑区的Fos IR。慢性WIN处理的动物表现出PPI的持续破坏。与给予赋形剂处理的对照相比,这些大鼠在旷场中也更活跃,在高架十字迷宫中焦虑程度更低。此外,在比较选定脑区的Fos IR时,这些动物显示出基础神经元活动改变,并且对氟哌啶醇或阿扑吗啡的急性应用反应不同。综上所述,这些结果表明,在大鼠青春期期间对大麻素受体CB(1)进行慢性刺激,不仅会导致持续的行为变化,还会导致对滥用药物或神经精神疾病至关重要的脑区内细胞的长期适应性改变。

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