2023
DOI: 10.1002/ajmg.a.63342
|View full text |Cite
|
Sign up to set email alerts
|

Clinical, biochemical, and molecular characterization of mucopolysaccharidosis type III in 34 Egyptian patients

Abstract: Mucopolysaccharidosis type III (MPS III) is a rare autosomal recessive lysosomal storage disorder characterized by progressive neurocognitive deterioration. There are four MPS III subtypes (A, B, C, and D) that are clinically indistinguishable with variable rates of progression. A retrospective analysis was carried out on 34 patients with MPS III types at Cairo University Children's Hospital. We described the clinical, biochemical, and molecular spectrum of MPS III patients. Of 34 patients, 22 patients had MPS… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
1

Citation Types

0
1
0

Year Published

2024
2024
2024
2024

Publication Types

Select...
1

Relationship

0
1

Authors

Journals

citations
Cited by 1 publication
(1 citation statement)
references
References 40 publications
0
1
0
Order By: Relevance
“…The p.L146P is a missense mutation previously described only in one Italian patient, drastically changing the protein structure, and leading to a severe phenotype [ 33 ]. Neurodegeneration in mucopolysaccharidosis III has been demonstrated independently of the specific genetic mutation [ 34 36 ], being the result of axonal dystrophy with an accumulation of ubiquitin-positive lesions containing phosphorylated-tau, wildtype α-synuclein, APP and β-amyloid, as shown by clinical and preclinical evidence [ 37 39 ]. However, mice carrying heterozygous p.D31N mutation in SGSH did not show an increased presence of brain pathology or neurodegeneration compared to controls, nor a significant accumulation of heparan sulfate despite a 50% reduction in SGSH levels.…”
Section: Discussionmentioning
confidence: 99%
“…The p.L146P is a missense mutation previously described only in one Italian patient, drastically changing the protein structure, and leading to a severe phenotype [ 33 ]. Neurodegeneration in mucopolysaccharidosis III has been demonstrated independently of the specific genetic mutation [ 34 36 ], being the result of axonal dystrophy with an accumulation of ubiquitin-positive lesions containing phosphorylated-tau, wildtype α-synuclein, APP and β-amyloid, as shown by clinical and preclinical evidence [ 37 39 ]. However, mice carrying heterozygous p.D31N mutation in SGSH did not show an increased presence of brain pathology or neurodegeneration compared to controls, nor a significant accumulation of heparan sulfate despite a 50% reduction in SGSH levels.…”
Section: Discussionmentioning
confidence: 99%