Department of Metabolic Diseases, The Children's Memorial Health Institute, Warsaw, Polandd.
Am J Med Genet A. 2012 Feb;158A(2):450-4. doi: 10.1002/ajmg.a.34415. Epub 2012 Jan 13.
Mucopolysaccharidosis type II (MPS II, Hunter syndrome) is an X-linked lysosomal storage disease caused by a deficiency of iduronate-2-sulfatase (IDS). Two affected girls with moderate and severe forms of MPS II with normal karyotypes and increased urinary dermatan sulphate and heparin sulphate excretion and marked deficiencies of IDS activity are reported. Molecular studies showed that case 1 has a heterozygous mutation c.1568A > G (p.Y523C) associated with almost totally skewed inactivation of the normal maternal X chromosome, and case 2 has a heterozygous deletion that includes exons 1-4 of IDS (minimal deletion range c.1-103_184del). The multi-exon deletion correlated with early onset of the disease and severe phenotype with intellectual disability, whereas the missense mutation was associated with moderate developmental delay. Although genotype-phenotype correlation in MPS II is difficult, gene deletions seem to correlate with more severe clinical manifestation of the disease. Enzyme replacement therapy (ERT) in these two females resulted in disease stabilization in both.
黏多糖贮积症 II 型(MPS II,亨特综合征)是一种 X 连锁溶酶体贮积病,由艾度糖-2-硫酸酯酶(IDS)缺乏引起。报道了两名患有中度和重度 MPS II 的女性患者,她们的核型正常,尿硫酸皮肤素和硫酸乙酰肝素排泄增加,IDS 活性显著缺乏。分子研究表明,病例 1 存在杂合突变 c.1568A>G(p.Y523C),与正常母系 X 染色体几乎完全偏置失活相关,病例 2 存在包含 IDS 外显子 1-4 的杂合缺失(最小缺失范围 c.1-103_184del)。这种多外显子缺失与疾病的早发和严重表型相关,伴有智力残疾,而错义突变与中度发育迟缓相关。尽管 MPS II 中的基因型-表型相关性很困难,但基因缺失似乎与疾病更严重的临床表现相关。在这两名女性中进行的酶替代治疗(ERT)导致疾病稳定。
