Muccopolysaccharidosis Type II, Two Novel Mutations
Sedky, N., Fateen, E., Khalil, M., Ibrahim, N., Ibrahim, M., Aglan, M., Hassan, H., Essawi, M. (2024). Muccopolysaccharidosis Type II, Two Novel Mutations. EKB Journal Management System, 13(2), 1-7. doi: 10.21608/mxe.2025.362691.1037
Nouran Mohamed Sedky; Ekram Fateen; Mona Salem Khalil; Nahed Mohamed Ibrahim; Mona Mohamed Ibrahim; Mona Aglan; Heba Amin Hassan; Mona Essawi. "Muccopolysaccharidosis Type II, Two Novel Mutations". EKB Journal Management System, 13, 2, 2024, 1-7. doi: 10.21608/mxe.2025.362691.1037
Sedky, N., Fateen, E., Khalil, M., Ibrahim, N., Ibrahim, M., Aglan, M., Hassan, H., Essawi, M. (2024). 'Muccopolysaccharidosis Type II, Two Novel Mutations', EKB Journal Management System, 13(2), pp. 1-7. doi: 10.21608/mxe.2025.362691.1037
Sedky, N., Fateen, E., Khalil, M., Ibrahim, N., Ibrahim, M., Aglan, M., Hassan, H., Essawi, M. Muccopolysaccharidosis Type II, Two Novel Mutations. EKB Journal Management System, 2024; 13(2): 1-7. doi: 10.21608/mxe.2025.362691.1037

Muccopolysaccharidosis Type II, Two Novel Mutations

Middle East Journal of Medical Genetics
Volume 13, Issue 2, July 2024, Pages 1-7    PDF (465.89 K)
Document Type: Original Article
DOI: 10.21608/mxe.2025.362691.1037
Authors
Nouran Mohamed Sedky* 1; Ekram Fateen2; Mona Salem Khalil3; Nahed Mohamed Ibrahim3; Mona Mohamed Ibrahim4; Mona Aglan2; Heba Amin Hassan2; Mona Essawi2
1Medical Molecular Genetics, National Research Centre, Cairo, Egypt
2National Research Centre
3Clinical and Chemical Chemistry, Faculty of medicine, Ksr Eleny Cairo University, Cairo, Egypt
4Biochemical Genetics, Division of Human Genetics and Genome Research, National Research Centre, Dokki12311, Cairo, Egypt
Abstract
Background: Mucopolysaccharidosis type II (Hunter syndrome; MPS II) is an X-linked lysosomal disorder caused by mutations detected in the gene that controls production of the enzyme iduronate-2-sulfatase (IDS). MPS II is considered to be a rare disease worldwide, with an incidence of 0.3–0.7 per 100,000 among live births. The primary defect of the disease is caused by a mutation on the IDS gene which disrupts the activity of the IDS lysosomal enzyme. The enzyme IDS catalyzes one of the steps in the catabolism of the glycosaminoglycans (GAGs), leading to accumulation of both heparan and dermatan sulphate in different tissues and organs of the body with excretion of large amounts of them in the urine. The clinical spectrum of MPS II includes mild, intermediate, and severe variants affecting mainly the connective tissues, skeletal system, brain, liver and spleen. To date, 792 variants have been reported by the HGMD associated with MPS type II have been identified.
This study was done for two Egyptian male patients with MPS type 2 which revealed 2 novel mutations in the two different patients with successful segregation of their mothers aligning with X-linked recessive mode of inheritance. We recommend a genotype phenotype correlation using larger cohorts of patients in the future studies.
Keywords
Glycosaminoglycans; IDS gene; lysosomal; mucopolysaccharidosis
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