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Experimental and Computational Studies to Characterize and Evaluate the Therapeutic Effect of Albizia lebbeck (L.) Seeds in Alzheimer’s Disease

机译:表征和评估白花蛇舌草种子在阿尔茨海默氏病中的治疗效果的实验和计算研究

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摘要

Background and Objectives: Alzheimer’s disease (AD) is a neurodegenerative disorder that deteriorates daily life due to loss of memory and cognitive impairment. It is believed that oxidative stress and cholinergic deficit are the leading causes of AD. Disease-modifying therapies for the treatment of AD are a challenging task for this century. The search for natural and synthetic agents has attracted the attention of researchers. The objective of this study was a scientific approach to search for most suitable remedy for AD by exploiting the potential of Albizia lebbeck (L.) seeds. Materials and Methods: Hydromethanolic extract of Albizia lebbeck seeds (ALE) was prepared by maceration. The plant was characterized by physico-chemical, phyto-chemical, and high-performance liquid chromatography (HPLC). Thirty-six Wistar albino rats were used in this study and divided into six groups (n = 6). Group I: normal control; Group II: disease control (AlCl3; 100 mg/kg); Group III: standard control (galantamine; 0.5 mg/kg); Groups IV–VI were treated ALE at 100, 200 and 300 mg/kg dose levels, respectively. All the treatments were given orally for 21 consecutive days. Y-maze, T-maze, Morris water maze, hole board, and open field behavioral tests were performed to analyze the cognitive impairment. Biochemical, histological, and computational studies were performed to support the results of behavioral tests. Results: HPLC analysis indicated the presence of quercetin, gallic acid, m-coumaric acid, and sinapic acid. ALE significantly improved the memory and cognitive impairments. Endogenous antioxidant stress biomarker levels and histopathological outcomes supported the therapeutic potential of A. lebbeck in AD. Cholinergic deficits were also ameliorated by ALE co-administration, possibly by the inhibition of hyperactive acetylcholinesterase (AChE). Docking studies supported the potential of ALE against AD. Conclusions: The data suggested that ALE has neuroprotective potential that can be exploited for beneficial effects to treat AD.
机译:背景与目的:阿尔茨海默氏病(AD)是一种神经退行性疾病,由于记忆力减退和认知障碍而使日常生活恶化。据信氧化应激和胆碱能缺乏是AD的主要原因。在本世纪,用于AD的疾病改良疗法是一项艰巨的任务。寻找天然和合成药物引起了研究人员的注意。这项研究的目的是一种科学的方法,通过利用Albizia lebbeck(L.)种子的潜力来寻找最合适的AD药物。材料与方法:浸渍法制得白花种子(ALE)的氢甲醇提取物。该植物通过物理化学,植物化学和高效液相色谱(HPLC)进行表征。本研究使用了36只Wistar白化病大鼠,分为6组(n = 6)。第一组:正常对照;第二组:疾病控制(AlCl3; 100 mg / kg);第三组:标准对照(加兰他敏; 0.5 mg / kg); IV–VI组分别以100、200和300 mg / kg剂量水平治疗ALE。所有治疗均连续21天口服。进行了Y迷宫,T迷宫,莫里斯水迷宫,洞洞板和野外行为测试,以分析认知障碍。进行了生化,组织学和计算研究,以支持行为测试的结果。结果:HPLC分析表明存在槲皮素,没食子酸,间香豆酸和芥子酸。 ALE可显着改善记忆力和认知障碍。内源性抗氧化剂应激生物标志物水平和组织病理学结果支持了A. lebbeck在AD中的治疗潜力。 ALE共同给药还可以减轻胆碱能缺陷,可能是通过抑制过度活跃的乙酰胆碱酯酶(AChE)来实现的。对接研究支持ALE对抗AD的潜力。结论:数据表明ALE具有神经保护潜力,可被利用来治疗AD。

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