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A pilot newborn screening program for Mucopolysaccharidosis type I in Taiwan

机译:台湾一型黏多糖贮积病的新生儿筛查试验计划

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Background Mucopolysaccharidosis type I (MPS I) is a genetic disease caused by the deficiency of α-L-iduronidase (IDUA) activity. MPS I is classified into three clinical phenotypes called Hurler, Scheie, and Hurler-Scheie syndromes according to their clinical severity. Treatments for MPS I are available. Better outcomes are associated with early treatment, which suggests a need for newborn screening for MPS I. The goal of this study was to determine whether measuring IDUA activity in dried blood on filter paper was effective in newborn screening for MPS I. Methods We conducted a newborn screening pilot program for MPS I from October 01, 2008 to April 30, 2013. Screening involved measuring IDUA activity in dried blood spots from 35,285 newborns using a fluorometric assay. Results Of the 35,285 newborns screened, 19 did not pass the tests and had been noticed for a recall examination. After completing further recheck process, 3 were recalled again for leukocyte IDUA enzyme activity testing. Two of the three had deficient leukocyte IDUA activity. Molecular DNA analyses confirmed the diagnosis of MPS I in these two newborns. Conclusions It is feasible to use the IDUA enzyme assay for newborn screening. The incidence of MPS I in Taiwan estimated from this study is about 1/17,643.
机译:背景I型粘多糖贮积病(MPS I)是由α-L-艾杜糖醛酸酶(IDUA)活性不足引起的遗传性疾病。根据其严重程度,MPS I被分为三种临床表型,分别称为Hurler,Scheie和Hurler-Scheie综合征。提供MPS I治疗。更好的结局与早期治疗相关,这表明需要对MPS I进行新生儿筛查。本研究的目的是确定测量滤纸上干血中IDUA活性是否对MPS I新生儿筛查有效。从2008年10月1日至2013年4月30日进行MPS I新生儿筛查先导计划。筛查涉及使用荧光测定法测量35285例新生儿的干血斑中IDUA活性。结果在筛查的35285例新生儿中,有19例未通过测试并且被召回检查。完成进一步的复核过程后,再次召回3名进行白细胞IDUA酶活性测试。三分之二的白细胞IDUA活性不足。分子DNA分析证实了这两个新生儿中MPS I的诊断。结论将IDUA酶测定用于新生儿筛查是可行的。根据这项研究,台湾地区MPS I的发病率约为1 / 17,643。

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