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桉叶油通过靶向氧化应激、乙酰胆碱酯酶、促炎细胞因子、多巴胺和 GABA 缓解氯胺酮诱导的大鼠精神病。

Targeting oxidative stress, acetylcholinesterase, proinflammatory cytokine, dopamine and GABA by eucalyptus oil (Eucalyptus globulus) to alleviate ketamine-induced psychosis in rats.

机构信息

Faculty of Medical Sciences, Department of Pharmaceutical Sciences, Guru Jambheshwar University of Science and Technology, Hisar, 125001, India.

University Institute of Pharmaceutical Sciences, UGC Center of Advanced Study (UGC-CAS) in Pharmaceutical Sciences, Panjab University, Chandigarh, India.

出版信息

Inflammopharmacology. 2019 Apr;27(2):301-311. doi: 10.1007/s10787-018-0455-3. Epub 2018 Feb 20.

DOI:10.1007/s10787-018-0455-3
PMID:29464495
Abstract

Essential oil of eucalyptus species is among the most common traded essential oils in the world. There is an increasing interest in the application of eucalyptus oil as a natural additive in food and pharmaceutical industry. The present study was undertaken to identify the phytoconstituents present in the essential oil of Eucalyptus globulus leaves (EO) and ascertain their protective effect against ketamine-induced psychosis in rats. GC-MS technique was used for analysis of phytoconstituents present in EO. Ketamine (50 mg/kg, i.p.) was used to induce psychosis in rats. Photoactometer, forced swim test and pole climb avoidance test were used to evaluate the protective effects of the EO (500, 1000 and 2000 mg/kg, p.o.) on acute and chronic administration. Bar test was used to test the side effect of EO. Biochemical and neurochemical estimations were carried out to explore the possible mechanism of action. GC-MS analysis of EO showed the presence of a number of biologically active compounds. EO at the dose of 500, 1000 and 2000 mg/kg, p.o. on acute and chronic administration, decreased locomotor activity, immobility duration and latency to climb the pole. EO was effective to facilitate the release of GABA, increase GSH levels, inhibit dopamine neurotransmission and decrease TNF-α levels as well as diminish AChE activity in different regions of the brain. EO at the dose of 500, 1000 mg/kg did not produce cataleptic behavior in rats. EO at the dose of 500, 1000 mg/kg produced protective effects against ketamine-induced psychosis and can be further explored clinically against neuropsychiatric disorders.

摘要

桉树属植物精油是世界上最常见的交易精油之一。人们对将桉树油作为食品和制药工业中的天然添加剂的应用越来越感兴趣。本研究旨在鉴定蓝桉叶精油(EO)中的植物成分,并确定其对氯胺酮诱导的大鼠精神病的保护作用。GC-MS 技术用于分析 EO 中的植物成分。氯胺酮(50mg/kg,ip)用于诱导大鼠精神病。光测仪、强迫游泳试验和杆攀爬回避试验用于评估 EO(500、1000 和 2000mg/kg,po)对急性和慢性给药的保护作用。棒试验用于测试 EO 的副作用。进行生化和神经化学评估以探索可能的作用机制。EO 的 GC-MS 分析表明存在许多具有生物活性的化合物。EO 在急性和慢性给药时,剂量为 500、1000 和 2000mg/kg,po,可降低运动活动、不动时间和爬杆潜伏期。EO 有效促进 GABA 释放,增加 GSH 水平,抑制多巴胺神经传递,降低 TNF-α 水平,并减少大脑不同区域的 AChE 活性。EO 剂量为 500、1000mg/kg 时,不会在大鼠中产生僵住行为。EO 剂量为 500、1000mg/kg 时对氯胺酮诱导的精神病具有保护作用,可在临床上进一步探索用于治疗神经精神疾病。

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