Lysosphingolipid Quantitation in Plasma and Dried-Blood Spots Using Targeted High-Resolution Mass Spectrometry.

IF 2.6 4区 医学 Q2 MEDICAL LABORATORY TECHNOLOGY Journal of Clinical Laboratory Analysis Pub Date : 2025-01-01 Epub Date: 2024-12-27 DOI:10.1002/jcla.25131
Franklin Ducatez, Wladimir Mauhin, Jules Ottaviani, Thomas Plichet, Carine Pilon, Olivier Lidove, Fréderic Barbey, Régine Perrichot, Sabrina Vergnaud, Marc G Berger, Juliette Berger, Nadia Belmatoug, Yann Nadjar, Foudil Lamari, Esther Noel, Stéphane Marret, Soumeya Bekri, Abdellah Tebani
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Abstract

Background: Sphingolipidoses are rare inherited metabolic diseases belonging to lysosomal diseases. Early and accurate diagnosis is crucial for effective management and treatment. In this study, we aimed to develop a robust method to accelerate the diagnosis of these sphingolipidoses using dried blood spots and plasma.

Method: We employed high-resolution mass spectrometry coupled with liquid chromatography (LC-HRMS) to analyze 6 lysosphingolipids (GlcSph/Psychosine, LysoGb3, LysoSM, LysoSM509, LysoGM1, and LysoGM2) on dried blood spots and plasma samples. The method was used to measure the lysosphingolipid levels in a group of 30 control subjects and 204 samples from patients with sphingolipidoses (61 dB and 143 plasma) including Fabry, Gaucher, GM2 Gangliodosis, Niemann-Pick type A/B, and Niemann-Pick type C.

Results: The developed multiplex LC-HRMS method demonstrated linearity, precision, and quantification performances particularly for GlcSph/Psychosine and LysoGb3 on samples including controls and patients with sphingolipidoses. LysoSM showed recovery variability, wherease LysoGM1 and LysoGM2 showed higher matrix effect.

Conclusion: Our study presents a high-resolution mass spectrometry method along with the established cutoff values, providing a valuable tool for targeted screening, accurate diagnosis, and monitoring sphingolipidoses. Furthermore, DBS showed reliable results that lay the path to a broader adoption for screening these diseases.

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血浆和干血斑溶鞘脂定量的高分辨率质谱分析。
背景:鞘脂病是一种罕见的遗传性代谢疾病,属于溶酶体疾病。早期和准确的诊断对于有效的管理和治疗至关重要。在这项研究中,我们的目的是开发一种可靠的方法来加速这些鞘脂中毒的诊断,使用干燥的血斑和血浆。方法:采用高分辨率质谱联用液相色谱(LC-HRMS)对干血斑和血浆样品中的6种溶鞘磷脂(GlcSph/Psychosine、LysoGb3、LysoSM、LysoSM509、LysoGM1和LysoGM2)进行分析。该方法用于测量30名对照组和204例鞘脂症患者(61 dB和143血浆)(包括Fabry, Gaucher, GM2神经节病,Niemann-Pick a /B型和Niemann-Pick c型)的溶鞘脂水平。结果:建立的多重LC-HRMS方法对包括对照组和鞘脂症患者样品的GlcSph/Psychosine和LysoGb3具有良好的线性,精密度和定量性能。LysoSM具有恢复变异性,而LysoGM1和LysoGM2具有较高的基质效应。结论:我们的研究提出了一种高分辨率的质谱分析方法,并建立了截止值,为有针对性的筛查,准确诊断和监测鞘脂病提供了有价值的工具。此外,DBS显示了可靠的结果,为更广泛地采用筛查这些疾病奠定了道路。
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来源期刊
Journal of Clinical Laboratory Analysis
Journal of Clinical Laboratory Analysis 医学-医学实验技术
CiteScore
5.60
自引率
7.40%
发文量
584
审稿时长
6-12 weeks
期刊介绍: Journal of Clinical Laboratory Analysis publishes original articles on newly developing modes of technology and laboratory assays, with emphasis on their application in current and future clinical laboratory testing. This includes reports from the following fields: immunochemistry and toxicology, hematology and hematopathology, immunopathology, molecular diagnostics, microbiology, genetic testing, immunohematology, and clinical chemistry.
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