Idursulfase Beta (Hunterase) Therapeutic Experience in a Patient with Mucopolysaccharidosis Type II

N. Vashakmadze, N. Zhurkova, E. Zakharova, Ludmila K. Mikhaylova, Marina A. Babaykina
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Abstract

Background. Mucopolysaccharidosis type II (MPS II, Hunter syndrome) is an X-linked recessive disease caused by lysosomal enzyme iduronate-2-sulfatase deficiency resulting in progressive glycosaminoglycans (GAG) accumulation in tissues (dermatan sulfate and heparan sulfate). GAG accumulation in cells leads to the development of progressive pathological disorders, malfunction of various organs and systems, early disability, and decrease in life expectancy. Enzyme replacement therapy (ERT) reduces the rate of life-threatening conditions development in patient. ERT would be more effective if it is prescribed early, especially at preclinical stage. This is the time when there are no severe irreversible changes in the cell, thus, pathogenetic therapy will decrease GAG accumulation in lysosomes, slow down the pathological process, and improve patient's condition. Clinical case description. Male patient diagnosed with MPS II was administrated with ERT idursulfase beta at the age of 6 months. It led to milder disease course compared to proband uncle who had similar mutation in the IDS gene, severe disease phenotype, and later initiation of ERT (at the age of 2.5 years). Conclusion. Early ERT initiation in patients with MPS II significantly slows down development of severe and life-threatening complications, increases the duration and improves the quality of life.
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ⅱ型粘多糖病1例伊杜硫酶治疗体会
背景。粘多糖病II型(MPS II, Hunter综合征)是一种x连锁隐性疾病,由溶酶体伊杜醛酸-2-硫酸酯酶缺乏引起,导致组织(硫酸皮聚糖和硫酸肝素)中糖胺聚糖(GAG)的进行性积累。GAG在细胞中的积累导致进行性病理疾病的发展,各种器官和系统功能障碍,早期残疾和预期寿命降低。酶替代疗法(ERT)降低了患者危及生命的疾病发展的速度。如果在早期,特别是在临床前阶段开ERT会更有效。此时细胞内还没有发生严重的不可逆变化,因此病理学治疗可以减少GAG在溶酶体中的积累,减缓病理过程,改善患者的病情。临床病例描述。诊断为MPS II的男性患者在6个月大时给予ERT idursulase β。与IDS基因相似突变的先证者叔叔相比,其病程较轻,疾病表型严重,ERT开始较晚(2.5岁)。结论。MPS II患者早期启动ERT可显著减缓严重和危及生命的并发症的发展,增加持续时间并改善生活质量。
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