Ahmed H. El-Banna, Fatma I. Abo El-Ela, Ahmed Abdel-Wahab, Amr Gamal, Abdel-Razik H. Abdel-Razik, Hossny A. El-Banna, Salma.I. Elsamannoudy, Marwa A. Ibrahim, Asmaa K. Abdelghany
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Amygdaline has been shown to have antioxidant effects that mitigate oxidative damage, and free radicals scavenger activity, as well as amygdaline niosomes as a nanoparticle has been found to improve the drug’s efficiency and selectivity. The objectives of this investigation are to study the neuroprotective role of amygdaline, and amygdaline-loaded niosomes formulation in the diminishment of the incidence of AD in neurotoxin (aluminum chloride; AlCl<sub>3</sub>) AD animal model.</p><h3>Results</h3><p>Data revealed that AlCl<sub>3</sub> caused cognitive decline that was confirmed by cognitive behavioral tests (novel object and Y-maze); biochemical disturbances that include marked oxidative stress (elevated malondialdehyde and reduced total antioxidant capacity), reduced acetylcholinesterase, and brain monoamines levels (nor adrenalin; 4-dihydroxyphenylacetic acid; 5-hydroxytryptamine /serotonin; dopamine), and gene regulation upset (down-regulated transcript levels of acetylcholinesterase; monoamine oxidase; BCL-2 and up-regulated transcript levels of BAX), as well as neurodegenerative changes were observed in the hippocampus of AlCl<sub>3</sub>-treated rats. Treatment with amygdaline and amygdaline-loaded niosomes formulation improved working memory and recognition, alleviated oxidative stress, and restored the levels of brain monoamines and neurotransmitters. Moreover, gene expression data showed a significant down-regulation of <i>BAX</i>, while BCL-2, acetylcholinesterase, and monoamine oxidase were significantly up-regulated. 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引用次数: 0
摘要
背景阿尔茨海默病(AD)是一种特殊形式的神经变性,以记忆力和认知能力受损为特征。接触某些金属毒素,如铝(AL),与阿兹海默症的发病直接相关,因为铝通过多种接触途径进入人体,并能改变渗透性和穿过血脑屏障。由于杏仁蛋白的存在,杏核疗法治疗注意力缺失症被认为在大量研究中取得了成功。研究表明,杏仁蛋白具有减轻氧化损伤的抗氧化作用和清除自由基的活性,而且杏仁蛋白纳米粒还能提高药物的效率和选择性。本研究的目的是研究杏仁蛋白和杏仁蛋白载体在降低神经毒素(氯化铝;AlCl3)AD 动物模型中 AD 发病率方面的神经保护作用。结果数据显示,AlCl3 会导致认知能力下降,认知行为测试(新物体和 Y 型迷宫)证实了这一点;生化紊乱包括明显的氧化应激(丙二醛升高和总抗氧化能力降低)、乙酰胆碱酯酶和脑单胺类物质水平降低(肾上腺素、4-二羟基苯乙胺、4-二羟基苯乙胺和 4-二羟基苯乙胺);4-二羟基苯乙酸;5-羟色胺/羟色胺;多巴胺)和基因调节紊乱(乙酰胆碱酯酶、单胺氧化酶、BCL-2 的转录水平下调,BAX 的转录水平上调),以及在 AlCl3 处理的大鼠海马中观察到神经退行性变化。使用杏仁基质和杏仁基质负载的niosomes制剂可改善工作记忆和识别能力,缓解氧化应激,并恢复大脑单胺类和神经递质的水平。此外,基因表达数据显示 BAX 明显下调,而 BCL-2、乙酰胆碱酯酶和单胺氧化酶则明显上调。此外,组织病理学检查显示神经退行性病变有所减轻。结论总之,杏仁蛋白和杏仁蛋白载体新体制剂通过其强大的抗氧化潜能、神经递质和基因表达调控以及减少神经损伤的能力,显然具有保护神经和增强认知能力的作用。
Therapeutic efficacy of amygdaline and amygdaline-loaded niosomes in a rat model of Alzheimer’s disease via oxidative stress, brain neurotransmitters, and apoptotic pathway
Background
Alzheimer’s disease (AD) is a specific form of neurodegeneration that is marked by impairments in memory and cognition. Exposure to some metal toxins, such as aluminum (AL), was directly linked to the onset of AD as it was hosted in the body via several exposure routes and can change the permeability and cross the blood–brain barrier. Due to amygdaline’s existence, apricot kernel therapy for AD is believed to have been established to be successful in numerous investigations. Amygdaline has been shown to have antioxidant effects that mitigate oxidative damage, and free radicals scavenger activity, as well as amygdaline niosomes as a nanoparticle has been found to improve the drug’s efficiency and selectivity. The objectives of this investigation are to study the neuroprotective role of amygdaline, and amygdaline-loaded niosomes formulation in the diminishment of the incidence of AD in neurotoxin (aluminum chloride; AlCl3) AD animal model.
Results
Data revealed that AlCl3 caused cognitive decline that was confirmed by cognitive behavioral tests (novel object and Y-maze); biochemical disturbances that include marked oxidative stress (elevated malondialdehyde and reduced total antioxidant capacity), reduced acetylcholinesterase, and brain monoamines levels (nor adrenalin; 4-dihydroxyphenylacetic acid; 5-hydroxytryptamine /serotonin; dopamine), and gene regulation upset (down-regulated transcript levels of acetylcholinesterase; monoamine oxidase; BCL-2 and up-regulated transcript levels of BAX), as well as neurodegenerative changes were observed in the hippocampus of AlCl3-treated rats. Treatment with amygdaline and amygdaline-loaded niosomes formulation improved working memory and recognition, alleviated oxidative stress, and restored the levels of brain monoamines and neurotransmitters. Moreover, gene expression data showed a significant down-regulation of BAX, while BCL-2, acetylcholinesterase, and monoamine oxidase were significantly up-regulated. Additionally, the histopathological examination showed reduced neurodegeneration.
Conclusion
Conclusively, it was evident that amygdaline and amygdaline-loaded niosomes formulation possess a neuroprotective and cognitive enhancement role in AD via their potent antioxidant potential, neurotransmitters, and gene expression regulations, as well as neural damage reduction capability.
期刊介绍:
Beni-Suef University Journal of Basic and Applied Sciences (BJBAS) is a peer-reviewed, open-access journal. This journal welcomes submissions of original research, literature reviews, and editorials in its respected fields of fundamental science, applied science (with a particular focus on the fields of applied nanotechnology and biotechnology), medical sciences, pharmaceutical sciences, and engineering. The multidisciplinary aspects of the journal encourage global collaboration between researchers in multiple fields and provide cross-disciplinary dissemination of findings.
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