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Effective Liquid Chromatography-Trapped Ion Mobility Spectrometry-Mass Spectrometry Separation of Isomeric Lipid Species

机译:有效的液相色谱捕获的离子迁移光谱 - 质谱分离异构脂质物种

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Lipids are a major class of molecules that play key roles in different biological processes. Understanding their biological roles and mechanisms remains analytically challenging due to their high isomeric content (e.g., varying acyl chain positions and/or double bond locations/geometries) in eukaryotic cells. In the present work, a combination of liquid chromatography (LC) followed by high resolution trapped ion mobility spectrometry mass spectrometry (TIMS-MS) was used to investigate common isomeric glycerophosphocholine (PC) and diacylglycerol (DG) lipid species from human plasma. The LC dimension was effective for the separation of isomeric lipid species presenting distinct double bond locations or geometries but was not able to differentiate lipid isomers with distinct acyl chain positions. High resolution TIMS-MS resulted in the identification of lipid isomers that differ in the double bond locations/geometries as well as in the position of the acyl chain with resolving power (R) up to similar to 410 (R similar to 320 needed on average). Extremely small structural differences exhibiting collision cross sections (CCS) of less than 1% (down to 0.2%) are sufficient for the discrimination of the isomeric lipid species using TIMS-MS. The same level of performance was maintained in the complex biological mixture for the biologically relevant PC 16:0/18:1 lipid isomers. These results suggest several advantages of using complementary LC-TIMS-MS separations for regular lipidomic analysis, with the main emphasis in the elucidation of isomer-specific lipid biological activities.
机译:脂质是在不同生物过程中起关键作用的主要分子。理解他们的生物学作用和机制仍然是由于其高异构含量(例如,改变酰基链位置和/或双键位置/几何)在真核细胞中的分析挑战。在本作研究中,使用液相色谱(LC)的组合,然后是高分辨率捕获的离子迁移光谱质谱(TIMS-MS)来研究来自人血浆的常见异构甘油磷胆碱(PC)和二酰基甘油(DG)脂质物种。 LC尺寸对于呈现不同的双键位置或几何形状的异构脂质物种是有效的,但不能与不同的酰基链位置区分脂质异构体。高分辨率TIMS-MS导致鉴定在双键位置/几何形状中不同的脂质异构体以及酰基链的位置,其中缩回功率(R)至类似于410(类似于320的R) )。表现出小于1%(下降至0.2%)的碰撞横截面(CCS)的极小结构差是使用TIMS-MS对异构脂质物种的判断。在基础上相关的PC 16:0/18:1脂质异构体的复杂生物混合物中保持相同水平的性能。这些结果表明使用互补LC-TIMS-MS用于常规脂质体分析的若干优点,主要重点是阐明异构体特异性脂质生物活性。

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