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Globotriaosylsphingosine (lyso-Gb<sub>3</sub>) and analogues in plasma and urine of patients with Fabry disease and correlations with long-term treatment and genotypes in a nationwide female Danish cohort

Grigoris Effraimidis, Ulla Feldt‐Rasmussen, Åse Krogh Rasmussen, Paméla Lavoie, Mona Abaoui, Michel Boutin, Christiane Auray‐Blais

2020Journal of Medical Genetics19 citationsDOI

Abstract

Introduction Recent studies showed the usefulness of globotriaosylsphingosine (lyso-Gb 3 ) and related analogues, deacylated forms of globotriaosylceramide (Gb 3 ), for high-risk screening, treatment monitoring and follow-up for patients with Fabry disease. Methods We evaluated Gb 3 , lyso-Gb 3 and analogues using tandem mass spectrometry in 57 women with Fabry disease followed during a period of 15.4 years. Twenty-one women were never treated and 36 received treatment (agalsidase-beta, n=30; agalsidase-alfa, n=5; or migalastat, n=1). Lyso-Gb 3 and analogues at m/z (−28), (−2), (+16), (+34) and (+50) were analysed in plasma and urine. Total Gb 3 and lyso-Gb 3 analogues at m/z (−12) and (+14) were evaluated in urine while the analogue at m/z (+18) was evaluated in plasma. Results A strong correlation between plasma and urine lyso-Gb 3 and analogue levels was revealed. Plasma and urine lyso-Gb 3 and analogue levels were not statistically different between patients carrying missense (n=49), nonsense (n=6) or deletion mutations (n=2). Never treated patients had lower plasma lyso-Gb 3 and analogues at m/z (−28), (−2), (+16), (+34) and the seven urinary lyso-Gb 3 analogues compared with pretreatment levels of the treated patients. A significant reduction of plasma lyso-Gb 3 and five analogues, as well as urine Gb 3 and six lyso-Gb 3 analogues, but not lyso-Gb 3 and lyso-Gb 3 at m/z (+50), was observed post-treatment with agalsidase-beta. The same tendency was observed with agalsidase-alfa. Conclusion Women with Fabry disease who started treatment based on clinical manifestations had higher lyso-Gb 3 and analogue biomarker levels than never treated women. This indicates that a biomarker cut-off could potentially be a decision tool for treatment initiation in women with Fabry disease.

Topics & Concepts

Lyso-UrineGlobotriaosylceramideInternal medicineFabry diseaseGenotypeMedicineChemistryUrologyEndocrinologyPharmacologyDiseasePhysicsBiochemistryGeneDetectorScintillatorOpticsLysosomal Storage Disorders ResearchCarbohydrate Chemistry and SynthesisTrypanosoma species research and implications
Globotriaosylsphingosine (lyso-Gb<sub>3</sub>) and analogues in plasma and urine of patients with Fabry disease and correlations with long-term treatment and genotypes in a nationwide female Danish cohort | Litcius