A Study of the Relationship Between Clinical Phenotypes and Plasma Iduronate-2-sulfatase Enzyme Activities in Hunter Syndrome Patients

Overview

Journal Korean J Pediatr

Specialty Pediatrics

Date 2012 Apr 5

PMID 22474463

Citations 3

Authors

Ok Jeong Lee

Su-Jin Kim

Young Bae Sohn

Hyung-Doo Park

Soo-Youn Lee

Chi-Hwa Kim

Ah-Ra Ko

Yeon-Joo Yook

Su-Jin Lee

Sung Won Park

Se-Hwa Kim

Sung-Yoon Cho

Eun-Kyung Kwon

Sun Ju Han

Dong-Kyu Jin

Affiliations

Soon will be listed here.

Abstract

Purpose: Mucopolysaccharidosis type II (MPS II or Hunter syndrome) is a rare lysosomal storage disorder caused by iduronate-2-sulfatase (IDS) deficiency. MPS II causes a wide phenotypic spectrum of symptoms ranging from mild to severe. IDS activity, which is measured in leukocyte pellets or fibroblasts, was reported to be related to clinical phenotype by Sukegawa-Hayasaka et al. Measurement of residual plasma IDS activity using a fluorometric assay is simpler than conventional measurements using skin fibroblasts or peripheral blood mononuclear cells. This is the first study to describe the relationship between plasma IDS activity and clinical phenotype of MPS II.

Methods: We hypothesized that residual plasma IDS activity is related to clinical phenotype. We classified 43 Hunter syndrome patients as having attenuated or severe disease types based on clinical characteristics, especially intellectual and cognitive status. There were 27 patients with the severe type and 16 with the attenuated type. Plasma IDS activity was measured by a fluorometric enzyme assay using 4-methylumbelliferyl-α-iduronate 2-sulphate.

Results: Plasma IDS activity in patients with the severe type was significantly lower than that in patients with the attenuated type (P=0.006). The optimal cut-off value of plasma IDS activity for distinguishing the severe type from the attenuated type was 0.63 nmol·4 hr(-1)·mL(-1). This value had 88.2% sensitivity, 65.4% specificity, and an area under receiver-operator characteristics (ROC) curve of 0.768 (ROC curve analysis; P=0.003).

Conclusion: These results show that the mild phenotype may be related to residual lysosomal enzyme activity.

Citing Articles

Validation and Implementation of a Highly Sensitive and Efficient Newborn Screening Assay for Mucopolysaccharidosis Type II.

Bilyeu H, Washburn J, Vermette L, Klug T Int J Neonatal Screen. 2020; 6(4).

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Clinical, biochemical and molecular characteristics of Filipino patients with mucopolysaccharidosis type II - Hunter syndrome.

Chiong M, Canson D, Abacan M, Baluyot M, Cordero C, Silao C Orphanet J Rare Dis. 2017; 12(1):7.

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Impact of enzyme replacement therapy on linear growth in Korean patients with mucopolysaccharidosis type II (Hunter syndrome).

Cho S, Huh R, Chang M, Lee J, Kwun Y, Maeng S J Korean Med Sci. 2014; 29(2):254-60.

PMID: 24550654 PMC: 3924006. DOI: 10.3346/jkms.2014.29.2.254.

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