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Neuroprotective action of omega-3 polyunsaturated fatty acids against neurodegenerative diseases: Evidence from animal studies.

机译:omega-3多不饱和脂肪酸对神经退行性疾病的神经保护作用:来自动物研究的证据。

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Studies in animals clearly show that oral intake of docosahexaenoic acid (DHA) can alter brain DHA concentrations and thereby modify brain functions. This provides us with an opportunity to use DHA as a nutraceutical or pharmaceutical tool in brain disorders such as Alzheimer disease (AD) and Parkinson disease (PD). Most of the published epidemiological studies are consistent with a positive association between high reported DHA consumption or high DHA blood levels and a lower risk of developing AD later in life. Such observations have prompted the investigation of DHA in three different transgenic models of AD. These analyses show that animal models of AD are more vulnerable to DHA depletion than controls and that DHA exerts a beneficial effect against pathological signs of AD, including Abeta accumulation, cognitive impairment, synaptic marker loss, and hyperphosphorylation of tau. Multiple mechanisms of action can be associated with the neuroprotective effects of DHA and include antioxidant properties and activation of distinct cell signaling pathways. Although the first randomized clinical assays have yet failed to demonstrate convincing beneficial effects of DHA for AD patients, the knowledge gathered in recent years holds out a hope for prevention and suggests that the elderly and people bearing a genetic risk for AD should at least avoid DHA deficiency.
机译:动物研究清楚地表明,口服二十二碳六烯酸(DHA)可以改变大脑DHA的浓度,从而改变大脑的功能。这为我们提供了将DHA用作脑部疾病(例如阿尔茨海默氏病(AD)和帕金森氏病(PD))的营养保健或药物工具的机会。大多数已发表的流行病学研究都与报告的高DHA摄入量或DHA血液水平高和以后生活中发生AD的风险较低之间呈正相关。这些观察结果促使人们在三种不同的AD转基因模型中研究DHA。这些分析表明,AD动物模型比对照组更容易遭受DHA耗竭,并且DHA对AD的病理征象具有有益作用,包括Abeta积累,认知障碍,突触标记物丢失和tau过度磷酸化。多种作用机制可能与DHA的神经保护作用有关,包括抗氧化特性和不同细胞信号通路的激活。尽管首批随机临床试验未能证明DHA对AD患者具有令人信服的有益作用,但近年来收集的知识为人们带来了预防的希望,并建议老年人和具有AD遗传风险的人至少应避免DHA不足。

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