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类花生酸在大脑中的作用。

The role of eicosanoids in the brain.

作者信息

Tassoni Daniella, Kaur Gunveen, Weisinger Richard S, Sinclair Andrew J

机构信息

Deakin University, School of Exercise & Nutrition Sciences, 221 Burwood Highway, Burwood, Victoria 3125, Australia.

出版信息

Asia Pac J Clin Nutr. 2008;17 Suppl 1:220-8.

Abstract

The brain contains two main polyunsaturated fatty acids (PUFA), arachidonic acid (AA) and docosahexaenoic acid (DHA). These PUFA are located almost exclusively in the sn2-position of phosphoglycerides which are found in the neural cell membranes. Liberation of these PUFA from the phosphoglycerides occurs via the action of specific phospholipases (PLA2). Free AA can be metabolised by cyclooxygenases to prostaglandins and thromboxane, while both AA and DHA can be metabolised by lipoxygenases to form hydroxy derivatives and leukotrienes. AA is also metabolised to lipoxins via the 5-lipoxygenase pathway. The eicosanoids formed play important roles in neural function including sleep induction (PGD2), long term potentiation, spatial learning and synaptic plasticity (PGE2), resolution of inflammation (lipoxins) and anti-inflammatory and neuroprotective bioactivity (dihydroxy-docosatriene, neuroprotectin D1, formed from DHA). COX-inhibitors have been shown to reduce oxidative stress and cognitive impairment. Additionally, drugs which are used to treat depression have been shown to reduce the turnover of AA to PGE2 in the brain. Diets deficient in omega 3 PUFA lead to reduced DHA in the brain and increased turnover of AA to eicosanoids, an effect which is overcome by restoring the omega 3 PUFA to the diet. In neural trauma and neurodegenerative diseases, there is a dramatic rise in the levels of AA-derived eicosanoids. In contrast, DHA-derived compounds can prevent neuroinflammation. Clearly, the eicosanoids are very important for the normal functioning of the brain, while the PUFA themselves are important in membrane structure and function.

摘要

大脑含有两种主要的多不饱和脂肪酸(PUFA),即花生四烯酸(AA)和二十二碳六烯酸(DHA)。这些PUFA几乎只存在于神经细胞膜中的磷酸甘油酯的sn2位上。这些PUFA从磷酸甘油酯中的释放是通过特定磷脂酶(PLA2)的作用实现的。游离的AA可被环氧化酶代谢为前列腺素和血栓素,而AA和DHA都可被脂氧合酶代谢形成羟基衍生物和白三烯。AA还可通过5-脂氧合酶途径代谢为脂oxin。所形成的类二十烷酸在神经功能中发挥重要作用,包括诱导睡眠(PGD2)、长期增强作用、空间学习和突触可塑性(PGE2)、炎症消退(脂oxin)以及抗炎和神经保护生物活性(由DHA形成的二羟基-二十二碳三烯、神经保护素D1)。已证明COX抑制剂可降低氧化应激和认知障碍。此外,用于治疗抑郁症的药物已显示可减少大脑中AA向PGE2的转化。缺乏ω-3 PUFA的饮食会导致大脑中DHA减少,并增加AA向类二十烷酸的转化,通过在饮食中恢复ω-3 PUFA可克服这种影响。在神经创伤和神经退行性疾病中,源自AA的类二十烷酸水平会急剧上升。相比之下,源自DHA的化合物可预防神经炎症。显然,类二十烷酸对大脑的正常功能非常重要,而PUFA本身在膜结构和功能中也很重要。

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