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E 系列消退素的手性脂质组学:阿司匹林与新型介质的生物合成

Chiral lipidomics of E-series resolvins: aspirin and the biosynthesis of novel mediators.

作者信息

Oh Sungwhan F, Vickery Thad W, Serhan Charles N

机构信息

Department of Anesthesiology, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.

出版信息

Biochim Biophys Acta. 2011 Nov;1811(11):737-47. doi: 10.1016/j.bbalip.2011.06.007. Epub 2011 Jun 16.

Abstract

Control of the inflammatory response is of wide interest given its important role in many diseases. In recent years we identified novel mechanisms and lipid mediators that play an active role in stimulating the resolution of self-limited acute inflammation. These novel pro-resolving mediators include the essential fatty acid-derived lipoxins, resolvins, protectins and maresins. Members of each possess a unique pro-resolving mechanism of action; each limits neutrophilic infiltration, regulates local mediators (chemokines, cytokines) as well as stimulates macrophage-enhanced clearance of apoptotic PMN, cellular debris and microbes. Given this unique mechanism of action, resolvins have already been shown to play pivotal roles in regulating key events in a wide range of experimental inflammatory diseases. These pro-resolving mediators also provide a molecular link between omega-3 essential fatty acids (e.g. EPA, DHA) and the resolution process of inflammation and tissue homeostasis. Here, we review recent evidence obtained using chiral LC-MS-MS-based lipidomics to identify a novel 18S-series of resolvins derived from EPA. Resolvin E1 possesses potent actions in vivo and in vitro demonstrated now in many laboratories, and herein we review comparisons in E-series resolvin biosynthesis and action of 18S-resolvin E1 and 18S-resolvin E2. The biosynthesis and formation of both 18S and 18R-series are enhanced with aspirin treatment and involve the utilization of dietary EPA as well as recombinant human 5-lipoxygenase and LTA(4) hydrolase in their stereospecific biosynthesis. Herein we also demonstrate the utility of LC-MS-MS-based lipidomics in identifying resolvins, protectins and related products in marine organisms such as Engraulis (Peruvian anchovy). These new findings emphasize the utility of chiral LC-MS-MS lipidomics and the potential for identifying new resolution circuits with chiral LC-MS-MS-based lipidomics and metabolomics.

摘要

鉴于炎症反应在许多疾病中发挥的重要作用,对其控制受到广泛关注。近年来,我们发现了在刺激自限性急性炎症消退中发挥积极作用的新机制和脂质介质。这些新型促消退介质包括必需脂肪酸衍生的脂氧素、消退素、保护素和maresin。每一类的成员都具有独特的促消退作用机制;每一种都能限制中性粒细胞浸润,调节局部介质(趋化因子、细胞因子),并刺激巨噬细胞增强对凋亡性多形核白细胞、细胞碎片和微生物的清除。鉴于这种独特的作用机制,消退素已被证明在多种实验性炎症疾病的关键事件调节中发挥关键作用。这些促消退介质还在ω-3必需脂肪酸(如二十碳五烯酸、二十二碳六烯酸)与炎症消退过程和组织稳态之间提供了分子联系。在此,我们综述了利用基于手性液相色谱-质谱联用的脂质组学获得的最新证据,以鉴定源自二十碳五烯酸的新型18S系列消退素。消退素E1在体内和体外均具有强大作用,目前许多实验室都已证明,在此我们综述了E系列消退素生物合成以及18S-消退素E1和18S-消退素E2作用的比较。18S和18R系列的生物合成和形成在阿司匹林处理后均会增强,并且在其立体特异性生物合成中涉及膳食二十碳五烯酸以及重组人5-脂氧合酶和白三烯A4水解酶的利用。在此我们还展示了基于液相色谱-质谱联用的脂质组学在鉴定海洋生物(如秘鲁鳀鱼)中的消退素、保护素及相关产物方面的实用性。这些新发现强调了手性液相色谱-质谱联用脂质组学的实用性以及利用基于手性液相色谱-质谱联用的脂质组学和代谢组学鉴定新的消退途径的潜力。

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