Contribution of tandem mass spectrometry to the diagnosis of lysosomal storage disorders

Piraud, Monique; Pettazzoni, Magali; Lavoie, Pamela; Ruet, Séverine; Pagan, Cécile; Cheillan, David; Latour, Philippe; Vianey‐Saban, Christine; Auray‐Blais, Christiane; Froissart, Roseline

doi:10.1007/s10545-017-0126-3

Cited by 27 publications

(19 citation statements)

References 205 publications

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“…We reported a sensitive multiplex method to measure various lysosphingolipids in the plasma for the diagnosis of Fabry, Gaucher, Krabbe, Niemann-Pick type A, B and C diseases and prosaposin deficiency [20,24]. Similar studies were performed by other groups [5,[21][22][23]. Despite the different analytical approaches in terms of sample preparation, internal standard and LC-MS/MS analysis, all these studies confirmed that a simultaneous LysoSL quantification could be a useful first-tier test to screen patients suspected for sphingolipidoses.…”

Section: Discussionmentioning

confidence: 80%

“…LysoGM1 and LysoGM2 have been proposed to be biomarkers of other two ultra-rare lysosomal diseases, the GM1 and GM2 gangliosidoses. The sensitivity of these markers in the plasma has been reported to be poor and critical for later onset forms [5,21]. We analyzed these markers in a limited number of patients (GM1 n = 1; GM2 n = 2).…”

Section: Discussionmentioning

confidence: 99%

“…The enzymatic activity in DBS was recently measured by tandem mass spectrometry (MS/MS) [3,4]. The versatility of MS/ MS has enabled this technique to be applied not only for enzymatic determination but also for biomarker detection [5]. In this context, lysosphingolipids (LysoSLs), the N-deacylated forms of sphingolipids, have been identified as potential biomarkers of several LSDs, specifically the sphingolipidoses, such as Gaucher disease (GD), Fabry disease (FD), Krabbe disease (KD) and Niemann-Pick type A/B (NPA/B) and type C (NPC) diseases, and the GM1 and GM2 gangliosidoses.…”

Section: Introductionmentioning

confidence: 99%

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Plasma and dried blood spot lysosphingolipids for the diagnosis of different sphingolipidoses: a comparative study

Polo¹,

Burlina

Ranieri

et al. 2019

Clinical Chemistry and Laboratory Medicine (CCLM)

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Background Lysosphingolipids, the N-deacylated forms of sphingolipids, have been identified as potential biomarkers of several sphingolipidoses, such as Gaucher, Fabry, Krabbe and Niemann-Pick diseases and in GM1 and GM2 gangliosidoses. To date, different methods have been developed to measure various lysosphingolipids (LysoSLs) in plasma. Here, we present a novel liquid chromatography tandem mass spectrometry (LC-MS/MS) assay for a simultaneous quantification of LysoSLs (HexSph, LysoGb3, LysoGM1, LysoGM2, LysoSM and LysoSM509) in dried blood spot (DBS). This LC-MS/MS method was used to compare the levels of LysoSLs in DBS and plasma in both affected patients and healthy controls. Methods Lysosphingolipids were extracted from a 3.2 mm diameter DBS with a mixture of methanol:acetonitrile:water (80:15:5, v/v) containing internal stable isotope standards. Chromatographic separation was performed using a C18 column with a gradient of water and acetonitrile both with 0.1% formic acid in a total run time of 4 min. The compounds were detected in the positive ion mode electrospray ionization (ESI)-MS/MS by multiple reaction monitoring (MRM). Results The method was validated on DBS to demonstrate specificity, linearity, lowest limit of quantification, accuracy and precision. The reference ranges were determined in pediatric and adult populations. The elevated levels of LysoSLs were identified in Gaucher disease (HexSph), Fabry disease (LysoGb3), prosaposin deficiency (HexSph and LysoGb3) and Niemann-Pick disease types A/B and C (LysoSM and LysoSM509). The correlation in the levels between DBS and plasma was excellent for LysoGb3 and HexSph but poor for LysoSM and LysoSM509. Conclusions Despite the fact that plasma LysoSLs determination remains the gold standard, our LC-MS/MS method allows a rapid and reliable quantification of lysosphingolipids in DBS. The method is a useful tool for the diagnosis of different sphingolipidoses except for Niemann-Pick type C.

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Section: Discussionmentioning

confidence: 80%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Plasma and dried blood spot lysosphingolipids for the diagnosis of different sphingolipidoses: a comparative study

Polo¹,

Burlina

Ranieri

et al. 2019

Clinical Chemistry and Laboratory Medicine (CCLM)

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“…Later, the unknown peak was reported to be useful for NPC diagnostic screening [95] and immediately cited in many guidelines [3,96,97]. Multiplex analyses of Lyso-SM-509 were useful for differentiation from other lysosomal diseases [98]. The differentiation between NPC and NP-A/B [99,100] and correlations between cholenoic acids and Lyso-SM-509 have also been reported [101].…”

Section: N-palmitoyl-o-phosphocholine-serine Previously Referred To mentioning

confidence: 98%

Identification and Evaluation of Biomarkers for Niemann-Pick Disease Type C Based on Chemical Analysis Techniques

Maekawa

Mano

2020

Chromatography

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Niemann-Pick disease type C (NPC) is an autosomal recessive disorder that features progressive neurodegeneration. Because NPC patients have mutations in NPC1 or NPC2 cholesterol transporting proteins, failures in cholesterol and other lipid trafficking occur. NPC patients represent a wide clinical spectrum in terms of age of onset and type of symptoms. Because conventional diagnostic methods are time-consuming and complicated, biomarker tests have attracted increased attention. In this review, recently reported biomarkers for NPC are discussed in detail. For example, oxysterols and some cholenoic acid conjugates, metabolized from excess cholesterol in NPC cells, can be detected in urine or plasma. In addition, two types of lysosphingolipids, sphingosylphosphorylcholine and glycosylsphingosine, are present at increased concentrations in NPC patients.A more recently discovered biomarker is N-palmitoyl-O-phosphorylcholine, previously called "lysosphingomyelin-509." These biomarkers are helpful for the early diagnosis of NPC and may contribute to a good prognosis for NPC patients.

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“…Measurements of plasma lysosphingomyelin levels also have been reported to be potentially useful in NPC disease (Welford et al, 2014). Lysosphingolipids, N-deacylated versions of their precursor sphingolipids, appear to be elevated in multiple disorders due to deficiencies of enzymes responsible for the breakdown of complex sphingolipids (Piraud et al, 2018). Moreover, lysosphingolipid measurements have attracted attention since compared to their acylated precursors, their accumulation is often up to an order of magnitude higher in these disease states, suggesting that they could be more reliable biomarkers than the other previously discussed sphingolipid metabolites (Welford et al, 2014).…”

Section: Sphingolipid Biomarkers Of Npcmentioning

confidence: 99%

Niemann-Pick type C disease: The atypical sphingolipidosis

Newton

Milstien

Spiegel

2018

Advances in Biological Regulation

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Niemann-Pick type C (NPC) disease is a lysosomal storage disorder resulting from mutations in either the NPC1 (95%) or NPC2 (5%) genes. NPC typically presents in childhood with visceral lipid accumulation and complex progressive neurodegeneration characterized by cerebellar ataxia, dysphagia, and dementia, resulting in a shortened lifespan. While cholesterol is widely acknowledged as the principal storage lipid in NPC, multiple species of sphingolipids accumulate as well. This accumulation of sphingolipids led to the initial assumption that NPC disease was caused by a deficiency in a sphingolipid catabolism enzyme, similar to sphingomyelinase deficiencies with which it shares a family name. It took about half a century to determine that NPC was in fact caused by a cholesterol trafficking defect, and still as we approach a century after the initial identification of the disease, the mechanisms by which sphingolipids accumulate remain poorly understood. Here we focus on the defects of sphingolipid catabolism in the endolysosomal compartment and how they contribute to the biology and pathology observed in NPC disease. This review highlights the need for further work on understanding and possibly developing treatments to correct the accumulation of sphingolipids in addition to cholesterol in this currently untreatable disease.

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Contribution of tandem mass spectrometry to the diagnosis of lysosomal storage disorders

Cited by 27 publications

References 205 publications

Plasma and dried blood spot lysosphingolipids for the diagnosis of different sphingolipidoses: a comparative study

Plasma and dried blood spot lysosphingolipids for the diagnosis of different sphingolipidoses: a comparative study

Identification and Evaluation of Biomarkers for Niemann-Pick Disease Type C Based on Chemical Analysis Techniques

Niemann-Pick type C disease: The atypical sphingolipidosis

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