Memory impairment effect of Cannabidiol Oil and Prednisolone Treatment: Alteration of Neuro-oxidant markers and Acetylcholinesterase Activity in the Hippocampus of Cadmium-Induced Toxicity in Male Wistar Rats

S. K. Mobisson, Iheanyichukwu Wopara, P. C. Onyebuagu, James Boobondah Woha, Felicia N. Okwakpam, E. C. Madu, Fidelis Udochukwu Ibe, J. B. Monye, OtoAbasi Sunday Abaka, A. O. Obembe, Arthur Chuemere Nwafor
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Abstract

Background: There have been conflicting reports on the effect of Cannabis products on learning and memory. Hence this study  investigated CBD oil's and prednisolone treatment's cognitive impact on cadmium-induced toxicity in male Wistar rats. Methods: Forty  rats weighing between 150g to 200g were assigned into 8 groups (1-8) of five animals each. Group A control, Group B-H received 1mg/kg body weight prednisolone; 1.5mg/kg Cadmium; 1mg/kg pred+0.2mg/kg CBD-oil; 0.2mg/kg CBDoil+2mg/kg cadmium; 3mg/kg  pred+2mg/kg cadmium; 0.1mg/kg CBD-oil and 0.2mg/kg CBD-oil respectively. The administration was done using gavage for 14 days. A  T-maze test apparatus was used to determine the latency of object recognition before and after administration. Results: There was a  significant decrease in latency of object recognition in prednisolone, cadmium, and 0.2mg/kg CBD-oil treated groups than control after  administration. Calcium ion significantly (P<0.05) increased in the cadmium+ 0.1mg/kg CBD-oil treated group and decreased in the  pred+CBD-oil group compared to the control. Acetylcholinesterase significantly (P<0.05) increased in prednisolone, pred+cadmium, and  0.2mg/kg CBD-oil treated groups and decreased in cadmium, pred.+CBD-oil, cadmium+CBD-oil, and 0.1mg/kg CBD-oil treated groups  compared to control. Catalase significantly increased in pred+cadmium, 0.1mg/kg CBD-oil, and 0.2mg/kg CBD-oil treated groups  compared to control. SOD significantly decreased in the treatment groups than the control. Malondialdehyde significantly increased in  cadmium, pred+CBD-oil, cadmium+CBD-oil, 0.1mg/kg CBD-oil, and 0.2mg/kg CBD-oil than control. Glutathione peroxidase significantly  decreased in treated groups compared to control. Reduced glutathione significantly decreased across treated groups than the control.  Histology of the hippocampus revealed visible pathologic changes in pred+cadmium, 0.1mg/kg CBD-oil, and 0.2mg/kg CBD-oil treated  groups with cellular vacuolization, Perivascular leucocyte infiltration, and pycnotic nuclei, indicating slight inflammation and detrimental  effects of the treatment in the histoarchitecture of the hippocampus. Conclusions: CBD oil, prednisolone, and cadmium administration at  different doses induced biochemical alterations, and exacerbated cognitive and neurobehavioral decline by enhancing oxidative  stress, acetylcholinesterase activity, and alteration in the cytoarchitecture of the hippocampus 
大麻二酚油和泼尼松龙治疗对记忆损伤的影响镉诱导毒性雄性Wistar大鼠海马区神经氧化标记和乙酰胆碱酯酶活性的改变
背景:关于大麻产品对学习和记忆的影响,一直有相互矛盾的报道。因此,本研究调查了 CBD 油和泼尼松龙治疗对雄性 Wistar 大鼠镉诱导毒性的认知影响。研究方法将体重在 150 克至 200 克之间的 40 只大鼠分成 8 组(1-8 组),每组 5 只。A 组为对照组,B-H 组分别接受 1 毫克/千克体重的泼尼松龙;1.5 毫克/千克镉;1 毫克/千克镉+0.2 毫克/千克CBD-油;0.2 毫克/千克CBD-油+2 毫克/千克镉;3 毫克/千克镉+2 毫克/千克镉;0.1 毫克/千克CBD-油和 0.2 毫克/千克CBD-油。灌胃给药14天。用T迷宫测试仪测定给药前后的物体识别潜伏期。结果显示给药后,泼尼松龙、镉和 0.2 毫克/千克 CBD-oil 处理组的识物潜伏期比对照组明显缩短。与对照组相比,镉+0.1mg/kg CBD-油处理组的钙离子明显增加(P<0.05),而泼尼松龙+CBD-油处理组的钙离子明显减少(P<0.05)。与对照组相比,乙酰胆碱酯酶在泼尼松龙、pred+镉和0.2mg/kg CBD-油处理组中显著增加(P<0.05),在镉、pred.+CBD-油、镉+CBD-油和0.1mg/kg CBD-油处理组中显著减少。与对照组相比,过氧化氢酶在pred+镉、0.1mg/kg CBD-油和0.2mg/kg CBD-油处理组中明显增加。治疗组的 SOD 比对照组明显降低。与对照组相比,镉、pred+CBD-油、镉+CBD-油、0.1mg/kg CBD-油和 0.2mg/kg CBD-油处理组的丙二醛明显升高。与对照组相比,处理组的谷胱甘肽过氧化物酶明显降低。与对照组相比,治疗组的还原型谷胱甘肽明显减少。 海马组织学检查显示,镉前处理组、0.1 毫克/千克 CBD-oil 处理组和 0.2 毫克/千克 CBD-oil 处理组出现了明显的病理变化,细胞空泡化、血管周围白细胞浸润和细胞核黄染,表明治疗对海马的组织结构产生了轻微的炎症和不利影响。结论不同剂量的 CBD 油、泼尼松龙和镉会诱发生化改变,并通过增强氧化应激、乙酰胆碱酯酶活性和海马细胞结构的改变,加剧认知和神经行为的衰退。
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