首页> 外文OA文献 >Synthesis of 13(R)‐Hydroxy‐7Z,10Z,13R,14E,16Z,19Z Docosapentaenoic Acid (13R‐HDPA) and Its Biosynthetic Conversion to the 13-Series Resolvins
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Synthesis of 13(R)‐Hydroxy‐7Z,10Z,13R,14E,16Z,19Z Docosapentaenoic Acid (13R‐HDPA) and Its Biosynthetic Conversion to the 13-Series Resolvins

机译:13(R) - 羟基-7Z,10Z,13R,14E,16Z,19Z二十二碳五烯酸(13R-HDpa)的合成及其生物合成转化为13系列分解体

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摘要

Specialized pro-resolving lipid mediators are biosynthesized during the resolution phase of acute inflammation from n-3 polyunsaturated fatty acids. Recently, the isolation and identification of the four novel mediators denoted 13-series resolvins, namely, RvT1 (1), RvT2 (2), RvT3 (3) and RvT4 (4), were reported, which showed potent bioactions characteristic for specialized pro-resolving lipid mediators. Herein, based on results from LC/MS-MS metabololipidomics and the stereoselective synthesis of 13(R)-hydroxy-7Z,10Z,13R,14E,16Z,19Z docosapentaenoic acid (13R-HDPA, 5), we provide direct evidence that the four novel mediators 1−4 are all biosynthesized from the pivotal intermediate 5. The UV and LC/MS-MS results from synthetic 13R-HDPA (5) matched those from endogenously and biosynthetically produced material obtained from in vivo infectious exudates, endothelial cells, and human recombinant COX-2 enzyme. Stereochemically pure 5 was obtained with the use of a chiral pool starting material that installed the configuration at the C-13 atom as R. Two stereoselective Z-Wittig reactions and two Z-selective reductions of internal alkynes afforded the geometrically pure alkene moieties in 5. Incubation of 5 with isolated human neutrophils gave all four RvTs. The results presented herein provide new knowledge on the biosynthetic pathways and the enzymatic origin of RvTs 1−4.
机译:在急性炎症消退阶段,由n-3多不饱和脂肪酸生物合成专业的促分解脂质介体。最近,报道了分离和鉴定了四个新的介体,表示为13系列RESOLVIN,即RvT1(1),RvT2(2),RvT3(3)和RvT4(4),它们显示了专门的前体有力的生物作用特征。 -解析脂质介体。在此,基于LC / MS-MS代谢脂蛋白体学和13(R)-羟基-7Z,10Z,13R,14E,16Z,19Z二十碳五烯酸(13R-HDPA,5)的立体选择性合成结果,我们提供了直接证据四种新型介体1-4都是通过关键中间体5进行生物合成的。合成13R-HDPA的UV和LC / MS-MS结果(5)与从体内传染性分泌物,内皮细胞获得的内源性和生物合成材料相匹配和人重组COX-2酶。通过使用在C-13原子上作为R构型的手性池起始材料获得立体化学纯的5。两个立体选择性Z-Wittig反应和内部炔烃的两个Z选择性还原提供了5的几何纯烯烃部分用分离的人类嗜中性白细胞孵育5个,得到全部四个RvT。本文介绍的结果提供了有关RvTs1-4的生物合成途径和酶促起源的新知识。

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