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N-acyl-O-phosphocholineserines: structures of a novel class of lipids that are biomarkers for Niemann-Pick C1 disease

机译:N-酰基-O-磷化胆碱:一种新型脂质类脂质的结构其是Niemann-pick C1疾病的生物标志物

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摘要

Niemann-Pick disease type C1 (NPC1) is a fatal, neurodegenerative, cholesterol storage disorder. With new therapeutics in clinical trials, there is an urgency to improve diagnostics and monitor therapeutic efficacy with biomarkers. In this study, we sought to define the structure of an unknown lipid biomarker for NPC1 with [M + H]+ ion at m/z 509.3351, previously designated as lysoSM-509. The structure of N-palmitoyl-O-phosphocholineserine (PPCS) was proposed for the lipid biomarker based on the results from mass spectrometric analyses and chemical derivatizations. As no commercial standard is available, authentic PPCS was chemically synthesized, and the structure was confirmed by comparison of endogenous and synthetic compounds as well as their derivatives using liquid chromatography-tandem mass spectrometry (LC-MS/MS). PPCS is the most abundant species among N-acyl-O-phosphocholineserines (APCS), a class of lipids that have not been previously detected in biological samples. Further analysis demonstrated that all APCS species with acyl groups ranging from C14 to C24 were elevated in NPC1 plasma. PPCS is also elevated in both central and peripheral tissues of the NPC1 cat model. Identification of APCS structures provide an opportunity for broader exploration of the roles of these novel lipids in NPC1 disease pathology and diagnosis.
机译:Niemann-Pick疾病C1(NPC1)是致命的,神经变性的胆固醇储存障碍。在临床试验中具有新的治疗方法,迫切需要改善诊断和监测生物标志物的治疗疗效。在这项研究中,我们试图将NPC1的未知脂质生物标志物的结构定义为在M / Z 509.3351中用[M + H] +离子的NPC1,以前指定为Lysosm-509。基于质谱分析和化学衍生化的结果,提出了N-PalmItoyl-O-普啉甲酰胺(PPC)的结构。由于没有商业标准可用,所以通过使用液相色谱 - 串联质谱(LC-MS / MS)的内源和合成化合物以及它们的衍生物来证实正品PPC。 PPC是N-酰基-O-磷化胆碱(APC)中最丰富的物种,一类尚未在生物样品中检测到的脂质。进一步的分析证明,具有从C14至C24的酰基的所有APCS物种在NPC1血浆中升高。 PPC也升高了NPC1猫模型的中央和外周组织。 APCS结构的识别提供了更广泛探索这些新型脂质在NPC1疾病病理和诊断中的角色的机会。

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