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Simultaneous tissue profiling of eicosanoid and endocannabinoid lipid families in a rat model of osteoarthritis

机译:骨关节炎大鼠模型中类花生酸和内源性大麻素脂质家族的同时组织分析

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摘要

We describe a novel LC method for the simultaneous and quantitative profiling of 43 oxylipins including eicosanoids, endocannabinoids, and structurally related bioactive lipids with modified acyl groups. The LC-MS/MS method uses switching at a defined time between negative and positive electrospray ionization modes to achieve optimal detection sensitivity for all the lipids. The validated method is linear over a range of 0.01–5 nmol/g (0.1–50 nmol/g for 2-arachidonoyl glycerol) with intra- and interday precision and accuracy between 1.38 and 26.76% and 85.22 and 114.3%, respectively. The method successfully quantified bioactive lipids in different tissue types in the rat, including spinal cord, dorsal root ganglia (DRGs), knee joint, brain, and plasma. Distinct regional differences in the pattern of lipid measured between tissue types were observed using principle component analysis. The method was applied to analyze tissue samples from an established preclinical rat model of osteoarthritis (OA) pain and showed that levels of 12-hydroxyeicosatetraenoic acid were significantly increased in the OA rat knee joint compared with controls, and that 15-hydroxyeicosatetraenoic acid was significantly increased in the DRGs in the model of OA compared with controls. The developed LC-MS/MS method has the potential to provide detailed pathway profiling in tissues and biofluids where the disruption of bioactive oxylipins may be involved in disease states.
机译:我们描述了一种新的LC方法,用于同时定量定量分析43种脂蛋白,包括类花生酸,内源性大麻素和具有修饰酰基的结构相关生物活性脂质。 LC-MS / MS方法使用在规定的时间在负电喷雾电离模式和正电喷雾电离模式之间切换,以实现对所有脂质的最佳检测灵敏度。经过验证的方法在0.01–5 nmol / g(2-花生四烯酰基甘油为0.1–50 nmol / g)的范围内是线性的,日内和日间精度和准确度分别为1.38和26.76%和85.22和114.3%。该方法成功定量了大鼠不同组织类型中的生物活性脂质,包括脊髓,背根神经节(DRG),膝关节,大脑和血浆。使用主成分分析观察到了在组织类型之间测得的脂质模式的明显区域差异。该方法用于分析已建立的骨关节炎(OA)疼痛的临床前大鼠模型的组织样品,结果表明与对照组相比,OA大鼠膝关节中12-羟基二十碳四烯酸的水平显着增加,而15-羟基二十碳四烯酸的水平显着增加与对照组相比,OA模型中的DRG增加。发达的LC-MS / MS方法有可能在组织和生物流体中提供详细的途径概况分析,其中生物活性脂蛋白的破坏可能与疾病状态有关。

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