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采用 LC-MS 和高能量碰撞解离碎裂进行血清脂质组学分析:重点检测和分析甘油三酯。

Serum lipidomics profiling using LC-MS and high-energy collisional dissociation fragmentation: focus on triglyceride detection and characterization.

机构信息

Department of Neurosurgery, Brigham and Women's Hospital, Harvard Medical School, 221 Longwood Avenue, LMRC-322, Boston, Massachusetts 02115, USA.

出版信息

Anal Chem. 2011 Sep 1;83(17):6648-57. doi: 10.1021/ac201195d. Epub 2011 Aug 5.

Abstract

There is a growing need both clinically and experimentally to improve the characterization of blood lipids. A liquid chromatography-mass spectrometry (LC-MS) method, developed for the qualitative and semiquantitative detection of lipids in biological samples and previously validated in mitochondrial samples, was now evaluated for the profiling of serum lipids. Data were acquired using high-resolution, full scan MS and high-energy, collisional dissociation (HCD), all ion fragmentation. The method was designed for efficient separation and detection in both positive and negative ionization mode and evaluated using standards spanning seven lipid classes. Platform performance, related to the identification and characterization of serum triglycerides (TGs), was assessed using extracted ion chromatograms with mass tolerance windows of 5 ppm or less from full scan exact mass measurements determined using SIEVE nondifferential LC-MS analysis software. The platform showed retention time coefficients of variation (CV) of <0.3%, mass accuracy values of <2 ppm error, and peak area CV of <13%, with the majority of that error coming from sample preparation and extraction rather than the LC-MS analysis, and linearity was shown to be over 4 orders of magnitude (r(2) = 0.999) for the standard TG (15:0)(3) spiked into serum. Instrument mass accuracy and precision were critical to the identification of unknown TG species, in part because these parameters enabled us to reduce false positives. In addition to detection and relative quantitation of TGs in serum, TG structures were characterized through the use of alternating HCD scans at different energies to produce diagnostic fragmentations on all ions in the analysis. The lipidomics method was applied to serum samples from 192 rats maintained on diets differing in macronutrient composition. The analysis identified 86 TG species with 81 unique masses that varied over 3.5 orders of magnitude and showed diet-dependency, consistent with TGs linking diet and disease risk.

摘要

临床和实验都越来越需要提高对血液脂质的特征描述。一种液相色谱-质谱(LC-MS)方法已经开发出来,用于定性和半定量检测生物样本中的脂质,并且已经在线粒体样本中得到验证,现在用于分析血清脂质。数据是使用高分辨率、全扫描 MS 和高能、碰撞诱导解离(HCD)、所有离子碎裂来获取的。该方法设计用于在正离子和负离子模式下高效分离和检测,并使用跨越七个脂质类别的标准品进行评估。使用具有质量公差窗口为 5 ppm 或更小的提取离子色谱图,从使用 SIEVE 非差分 LC-MS 分析软件确定的全扫描精确质量测量值中评估平台性能,与血清三酰甘油(TGs)的鉴定和特征描述有关。该平台显示出<0.3%的保留时间变异系数(CV)、<2 ppm 误差的质量准确度值和<13%的峰面积 CV,其中大部分误差来自样品制备和提取,而不是 LC-MS 分析,并且标准 TG(15:0)(3)被添加到血清中,线性度超过 4 个数量级(r(2) = 0.999)。仪器质量准确度和精度对于鉴定未知 TG 种类至关重要,部分原因是这些参数使我们能够减少假阳性。除了在血清中检测和相对定量 TG 之外,还通过使用不同能量的交替 HCD 扫描来对分析中的所有离子产生诊断碎裂来表征 TG 结构。脂质组学方法应用于 192 只在宏量营养素组成不同的饮食中饲养的大鼠的血清样本。该分析确定了 86 种 TG 种类,具有 81 个独特质量,变化超过 3.5 个数量级,并显示出饮食依赖性,与将饮食与疾病风险联系起来的 TG 一致。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22f4/3165109/df8a3152873a/nihms317345f1.jpg

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