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首页> 外文期刊>Current neuropharmacology >The Emerging Role of the Double-Edged Impact of Arachidonic Acid-Derived Eicosanoids in the Neuroinflammatory Background of Depression
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The Emerging Role of the Double-Edged Impact of Arachidonic Acid-Derived Eicosanoids in the Neuroinflammatory Background of Depression

机译:花生素酸衍生的籽糖蛋白在抑郁神经炎背景中的双刃抗冲击的新兴作用

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Eicosanoids are arachidonic acid (AA) derivatives belonging to a family of lipid signalling mediators that are engaged in both physiological and pathological processes in the brain. Recently, their implication in the prolonged inflammatory response has become a focus of particular interest because, in contrast to acute inflammation, chronic inflammatory processes within the central nervous system (CNS) are crucial for the development of brain pathologies including depression. The synthesis of eicosanoids is catalysed primarily by cyclooxygenases (COX), which are involved in the production of pro-inflammatory AA metabolites, including prostaglandins and thromboxanes. Moreover, eicosanoid synthesis is catalysed by lipoxygenases (LOXs), which generate both leukotrienes and anti-inflammatory derivatives such as lipoxins. Thus, AA metabolites have double-edged pro-inflammatory and anti-inflammatory, pro-resolving properties, and an imbalance between these metabolites has been proposed as a contributor or even the basis for chronic neuroinflammatory effects. This review focuses on important evidence regarding eicosanoid-related pathways (with special emphasis on prostaglandins and lipoxins) that has added a new layer of complexity to the idea of targeting the double-edged AA-derivative pathways for therapeutic benefits in depression. We also sought to explore future research directions that can support a pro-resolving response to control the balance between eicosanoids and thus to reduce the chronic neuroinflammation that underlies at least a portion of depressive disorders.
机译:异氰烷是属于一系列脂质信号调解器的花生素酸(AA)衍生物,其在大脑中接受生理和病理过程。最近,它们在延长的炎症反应中的含义已成为特别兴趣的焦点,因为与急性炎症相比,中枢神经系统(CNS)内的慢性炎症过程对于包括抑郁症包括抑郁症的脑病至关重要。二盐烷的合成主要通过环加氧基酶(COX)催化,其参与生产前炎症AA代谢物,包括前列腺素和血栓素。此外,七氧化合成由脂氧基酶(LOXS)催化,其产生白三烯和抗炎衍生物如脂氧氟丝。因此,AA代谢物具有双刃促炎和抗炎,促题性能,并且已经提出了这些代谢物之间的不平衡作为贡献者或甚至慢性神经炎作用的基础。本综述重点是有关卓越苷相关途径的重要证据(特别强调前列腺素和脂蛋白),这增加了一种对靶向抑郁症治疗益处的双刃AA衍生物途径的思想的新的复杂性。我们还寻求探索未来的研究方向,可以支持促进逐渐减少七穗素之间的平衡,从而减少慢性神经炎症,以减少至少一部分抑郁症的抑郁症。

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