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Medicine 2018-Dec

A novel mutation of SGSH and clinical features analysis of mucopolysaccharidosis type IIIA.

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Länken sparas på Urklipp
Xiaohua Li
Rui Xiao
Baiyu Chen
Guanglu Yang
Xiaomeng Zhang
Zhuo Fu
Junxian Fu
Mengli Zhuang
Yinglong Huang
ARTIKEL: 30593151
DOI: 10.1097/MD.0000000000013758
PMC: PMC6314651
BioSeek: 30593151

Nyckelord

trattbröst

atrofi

hepatomegali

contracture

esotropia

seizures

mucopolysaccharidosis iii

mucopolysaccharidoses

Abstrakt

The aim of this study was to analyze the clinical and imaging features of a pediatric patient with mucopolysaccharidosis type IIIA (MPS IIIA) and a novel mutation of the N-sulfoglucosamine sulfohydrolase (SGSH) in 1 pedigree.An 8-year-old female patient presented with developmental regression, seizures, cerebral atrophy, thickened calvarial diploe, apathy, esotropia, slender build, thick hair, prominent eyebrows, hepatomegaly, ankle clonus, muscle and joint contractures, and funnel chest.The patient was diagnosed as autosomal recessive (AR) MPS IIIA with a novel mutation in the SGSH gene.Genomic DNA was extracted from the peripheral blood and next-generation sequencing (NGS) technology was used to detect pathogenic genes, and the Sanger method was applied to perform pedigree verification for the detected suspicious pathogenic mutations.The NGS done for the girl and her family showed 2 variations that were both missense mutations in SGSH. The c.1298G > A (p.Arg433Gln) was a known mutation, and the c.630 G > T (p.Trp210Cys) was a novel variation.The common clinical manifestations of MPS IIIA were rapid developmental regression, seizures, cerebral atrophy, and thickened calvarial diploe. The results showed that the c.630 G > T was likely pathogenic according to bioinformatics analysis, which probably was a novel mutation. This study reports 1 case of MPS IIIA with some clinical features as determined via clinical and genetic analysis, and found a new mutation in the SGSH gene.

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