Darrel J. Waggoner, Christopher A. Tan
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引用次数: 10
Abstract
Newborn screening (NBS), since its implementation in the 1960s, has traditionally been successful in reducing mortality and disability in children with a range of different conditions. Lysosomal storage disorders (LSD) are a heterogeneous group of inherited metabolic diseases that result from lysosomal dysfunction. Based on available treatment and suitable screening methods, the LSDs that are considered for NBS generally include Fabry, Gaucher, Krabbe, MPSI, MPSII, MPSV, Metachromatic leukodystrophy, Niemann-Pick, and Pompe. Utilizing traditional and expanded criteria for consideration of NBS leads to a set of fundamental questions that need to be explored when considering the opportunities and challenges of adding LSDs to NBS panels. © 2012 Wiley Periodicals, Inc. Dev Disabil Res Rev 2011; 17:9–14.
扩大新生儿溶酶体疾病筛查:机遇与挑战
新生儿筛查自20世纪60年代实施以来,传统上成功地降低了患有一系列不同疾病的儿童的死亡率和致残率。溶酶体贮积障碍(LSD)是一种由溶酶体功能障碍引起的异质性遗传代谢疾病。根据现有的治疗方法和合适的筛选方法,NBS考虑的lsd一般包括Fabry、Gaucher、Krabbe、MPSI、MPSII、MPSV、异色性脑白质营养不良、Niemann-Pick和Pompe。在考虑将lsd添加到NBS面板的机遇和挑战时,使用传统的和扩展的标准来考虑NBS会导致一系列需要探索的基本问题。©2012 Wiley期刊公司Dev disability Res Rev 2011;17:9-14。
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