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Novel subtype of mucopolysaccharidosis caused by arylsulfatase K (ARSK) deficiency

硫酸皮肤素 粘多糖病 糖胺聚糖 芳基磺酸酶A 分子生物学 异染性白质营养不良 生物 表型 生物化学 硫酸乙酰肝素 化学 基因
作者
Sarah Verheyen,Jasmin Blatterer,Michael R. Speicher,Gandham SriLakshmi Bhavani,Geert‐Jan Boons,Mai-Britt Ilse,Dominik Andrae,Jens Sproß,Frédéric M. Vaz,Susanne Gerit Kircher,Laura Posch-Pertl,Daniela Baumgartner,Torben Lübke,Hitesh Shah,Ali Al Kaissi,Katta M. Girisha,Barbara Plecko
出处
期刊:Journal of Medical Genetics [BMJ]
卷期号:59 (10): 957-964 被引量:35
标识
DOI:10.1136/jmedgenet-2021-108061
摘要

Mucopolysaccharidoses (MPS) are monogenic metabolic disorders that significantly affect the skeleton. Eleven enzyme defects in the lysosomal degradation of glycosaminoglycans (GAGs) have been assigned to the known MPS subtypes (I-IX). Arylsulfatase K (ARSK) is a recently characterised lysosomal hydrolase involved in GAG degradation that removes the 2-O-sulfate group from 2-sulfoglucuronate. Knockout of Arsk in mice was consistent with mild storage pathology, but no human phenotype has yet been described.In this study, we report four affected individuals of two unrelated consanguineous families with homozygous variants c.250C>T, p.(Arg84Cys) and c.560T>A, p.(Leu187Ter) in ARSK, respectively. Functional consequences of the two ARSK variants were assessed by mutation-specific ARSK constructs derived by site-directed mutagenesis, which were ectopically expressed in HT1080 cells. Urinary GAG excretion was analysed by dimethylene blue and electrophoresis, as well as liquid chromatography/mass spectrometry (LC-MS)/MS analysis.The phenotypes of the affected individuals include MPS features, such as short stature, coarse facial features and dysostosis multiplex. Reverse phenotyping in two of the four individuals revealed additional cardiac and ophthalmological abnormalities. Mild elevation of dermatan sulfate was detected in the two subjects investigated by LC-MS/MS. Human HT1080 cells expressing the ARSK-Leu187Ter construct exhibited absent protein levels by western blot, and cells with the ARSK-Arg84Cys construct showed markedly reduced enzyme activity in an ARSK-specific enzymatic assay against 2-O-sulfoglucuronate-containing disaccharides as analysed by C18-reversed-phase chromatography followed by MS.Our work provides a detailed clinical and molecular characterisation of a novel subtype of mucopolysaccharidosis, which we suggest to designate subtype X.

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