Center for Inherited Metabolic Disorders, Department of Clinical Genetics, Copenhagen University Hospital, Copenhagen, Denmark.
Mol Genet Metab. 2012 Nov;107(3):281-93. doi: 10.1016/j.ymgme.2012.06.006. Epub 2012 Jun 21.
Expanded newborn screening for selected inborn errors of metabolism (IEM) in Denmark, the Faroe Islands and Greenland was introduced in 2002. We now present clinical, biochemical, and statistical results of expanded screening (excluding PKU) of 504,049 newborns during nine years as well as diagnoses and clinical findings in 82,930 unscreened newborns born in the same period. The frequencies of diagnoses made within the panel of disorders screened for are compared with the frequencies of the disorders in the decade preceding expanded newborn screening. The expanded screening was performed as a pilot study during the first seven years, and the experience obtained during these years was used in the development of the routine neonatal screening program introduced in 2009. Methods for screening included tandem mass spectrometry and an assay for determination of biotinidase activity. A total of 310 samples from 504,049 newborns gave positive screening results. Of the 310 results, 114 were true positive, including results from 12 newborns in which the disease in question was subsequently diagnosed in their mothers. Thus, the overall frequency of an IEM in the screening panel was 1:4942 (mothers excluded) or 1:4421 (mothers included). The false positive rate was 0.038% and positive predictive value 37%. Overall specificity was 99.99%. All patients with true positive results were followed in The Center for Inherited Metabolic Disorders in Copenhagen, and the mean follow-up period was 45 months (range 2109 months). There were no deaths among the 102 children, and 94% had no clinically significant sequelae at last follow-up. Our study confirms the higher frequency of selected IEM after implementation of expanded newborn screening and suggests an improved outcome for several disorders. We argue that newborn screening for these disorders should be standard of care, though unresolved issues remain, e.g. about newborns with a potential for remaining asymptomatic throughout life. Well organized logistics of the screening program from screening laboratory to centralized, clinical management is important.
丹麦、法罗群岛和格陵兰于 2002 年开始对部分先天性代谢缺陷(IEM)进行扩展新生儿筛查。本文现介绍 9 年间 504049 例新生儿扩展筛查(不包括苯丙酮尿症)的临床、生化和统计结果,以及同期未经筛查的 82930 例新生儿的诊断和临床发现。所筛查疾病组的诊断频率与扩展新生儿筛查前 10 年的疾病频率进行比较。扩展筛查最初 7 年作为试点研究进行,在此期间获得的经验用于 2009 年推出的常规新生儿筛查计划。筛查方法包括串联质谱法和生物蝶呤酶活性测定。从 504049 例新生儿中总共 310 例标本筛查结果阳性。310 例结果中,114 例为真阳性,包括 12 例患儿,其疾病随后在其母亲中得到诊断。因此,在筛查组中 IEM 的总体发生率为 1:4942(排除母亲)或 1:4421(包括母亲)。假阳性率为 0.038%,阳性预测值为 37%。总体特异性为 99.99%。所有真阳性结果的患者均在哥本哈根遗传性代谢紊乱中心接受随访,平均随访时间为 45 个月(范围 2109 个月)。102 例患儿中无死亡病例,最后一次随访时 94%的患儿无明显临床后遗症。本研究证实,扩大新生儿筛查后,某些 IEM 的发病率更高,且一些疾病的预后得到改善。我们认为,对这些疾病进行新生儿筛查应该成为标准治疗方法,尽管仍存在一些未解决的问题,例如对那些终生无症状的新生儿。从筛查实验室到集中化临床管理的筛查计划的良好组织物流非常重要。
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