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Pro-Resolving Lipid Mediators (SPMs) and Their Actions in Regulating miRNA in Novel Resolution Circuits in Inflammation

机译:亲分解脂质介体(SPMs)及其在炎症新分辨回路中调节miRNA的作用

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摘要

Unresolved inflammation is associated with several widely occurring diseases such as arthritis, periodontal diseases, cancer, and atherosclerosis. Endogenous mechanisms that curtail excessive inflammation and prompt its timely resolution are of considerable interest. In recent years, previously unrecognized chemical mediators derived from polyunsaturated fatty acids were identified that control the acute inflammatory response by activating local resolution programs. Among these are the so-called specialized pro-resolving lipid mediators (SPMs) that include lipoxins (LX), resolvins (Rv), protectins (PD), and maresins (MaR), because they are enzymatically biosynthesized during resolution of self-limited inflammation. They each possess distinct chemical structures and regulate cellular pathways by their ability to activate pro-resolving G-protein coupled receptors (GPCRs) in a stereospecific manner. For instance, RvD1 controls several miRNAs of interest in self-limited acute inflammation that counter-regulate the mediators and proteins that are involved in inflammation. Here, we overview some of the biosynthesis and mechanisms of SPM actions with focus on the recently reported miR involved in their pro-resolving responses that underscore their beneficial actions in the regulation of acute inflammation and its timely resolution. The elucidation of these mechanisms operating in vivo to keep acute inflammation within physiologic boundaries as well as stimulate resolution have opened resolution pharmacology and many new opportunities to target inflammation-related human pathologies via activating resolution mechanisms.
机译:未解决的炎症与多种广泛存在的疾病有关,例如关节炎,牙周疾病,癌症和动脉粥样硬化。减少过度炎症并及时解决炎症的内源性机制引起了人们的极大兴趣。近年来,人们发现了以前无法识别的衍生自多不饱和脂肪酸的化学介质,该介质通过激活局部分辨率程序来控制急性炎症反应。其中包括所谓的专门亲分解脂质介体(SPM),其中包括脂蛋白(LX),Resolvins(Rv),保护素(PD)和maresins(MaR),因为它们是在自我限制的分解过程中通过酶促生物合成的炎。它们各自具有独特的化学结构,并通过其以立体特异性方式激活促分解G蛋白偶联受体(GPCR)的能力来调节细胞途径。例如,RvD1控制自我限制的急性炎症中的几种感兴趣的miRNA,这些miRNA可反调节炎症中涉及的介质和蛋白质。在这里,我们概述了SPM动作的一些生物合成和机制,重点是最近报道的miR参与其促分辨反应,这些反应强调了其在急性炎症调节和及时解决中的有益作用。对这些在体内起作用以将急性炎症保持在生理范围内并刺激消退的机制的阐明,已经打开了消退药理学,并为通过激活消退机制靶向炎症相关的人类病理学提供了许多新机会。

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