Amsterdam UMC location University of Amsterdam, Departments of Laboratory Medicine and Pediatrics, Laboratory Genetic Metabolic Diseases, Emma Children's Hospital, Meibergdreef 9, Amsterdam, the Netherlands; Amsterdam Gastroenterology Endocrinology Metabolism, Inborn errors of metabolism, Amsterdam, the Netherlands; Core Facility Metabolomics, Amsterdam UMC location University of Amsterdam, Amsterdam, the Netherlands; United for Metabolic Diseases, the Netherlands.
Department of Pediatric Neurology, Radboud University Medical Center, Amalia Children's Hospital, Donders Institute for Brain Cognition and Behaviour, Nijmegen, the Netherlands.
Biochim Biophys Acta Mol Cell Biol Lipids. 2024 Mar;1869(2):159447. doi: 10.1016/j.bbalip.2023.159447. Epub 2024 Jan 3.
Sjögren-Larsson syndrome (SLS) is a rare neurometabolic disorder that mainly affects brain, eye and skin and is caused by deficiency of fatty aldehyde dehydrogenase. Our recent finding of a profoundly disturbed brain tissue lipidome in SLS prompted us to search for similar biomarkers in plasma as no functional test in blood is available for SLS.
We performed plasma lipidomics and used a newly developed bioinformatics tool to mine the untargeted part of the SLS plasma and brain lipidome to search for SLS biomarkers. Plasma lipidomics showed disturbed ether lipid metabolism in known lipid classes. Untargeted lipidomics of both plasma and brain (white and grey matter) uncovered two new endogenous lipid classes highly elevated in SLS. The first biomarker group were alkylphosphocholines/ethanolamines containing different lengths of alkyl-chains where some alkylphosphocholines were > 600-fold elevated in SLS plasma. The second group of biomarkers were a set of 5 features of unknown structure. Fragmentation studies suggested that they contain ubiquinol and phosphocholine and one feature was also found as a glucuronide conjugate in plasma. The plasma features were highly distinctive for SLS with levels >100-1000-fold the level in controls, if present at all. We speculate on the origin of the alkylphosphocholines/ethanolamines and the nature of the ubiquinol-containing metabolites.
The metabolites identified in this study represent novel endogenous lipid classes thus far unknown in humans. They represent the first plasma metabolite SLS-biomarkers and may also yield more insight into SLS pathophysiology.
干燥综合征-莱尔综合征(SLS)是一种罕见的神经代谢疾病,主要影响大脑、眼睛和皮肤,是由于脂肪醛脱氢酶缺乏引起的。我们最近发现 SLS 患者脑组织脂质组存在严重紊乱,促使我们在血液中寻找类似的生物标志物,因为目前尚无针对 SLS 的功能检测。
我们进行了血浆脂质组学研究,并使用新开发的生物信息学工具对 SLS 患者的血浆和脑组织脂质组进行非靶向分析,以寻找 SLS 的生物标志物。血浆脂质组学显示已知脂质类别的醚脂质代谢紊乱。对血浆和大脑(白质和灰质)进行非靶向脂质组学分析,揭示了两种新的内源性脂质类物质在 SLS 中高度升高。第一个生物标志物组是含有不同长度烷基链的烷基磷酸胆碱/乙醇胺,其中一些 SLS 血浆中的烷基磷酸胆碱升高了 600 多倍。第二个标志物组是一组 5 种未知结构的特征。片段研究表明,它们含有泛醇和磷酸胆碱,其中一种特征也被发现为血浆中的葡萄糖醛酸缀合物。如果存在,这些血浆特征对 SLS 具有高度特异性,水平比对照高 100-1000 倍。我们推测烷基磷酸胆碱/乙醇胺的来源和含泛醇代谢物的性质。
本研究中鉴定的代谢物代表了迄今为止在人类中未知的新型内源性脂质类物质。它们代表了第一个 SLS 血浆代谢物生物标志物,也可能为 SLS 病理生理学提供更多的见解。
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