A Five-Year Review of Newborn Screening for Spinal Muscular Atrophy in the State of Utah: Lessons Learned.

IF 4 Q1 GENETICS & HEREDITY
Kristen N Wong, Melissa McIntyre, Sabina Cook, Kim Hart, Amelia Wilson, Sarah Moldt, Andreas Rohrwasser, Russell J Butterfield
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Abstract

Spinal muscular atrophy (SMA) is an autosomal recessive condition characterized by alpha motor neuron degeneration in the spinal cord anterior horn. Clinical symptoms manifest in the first weeks to months of life in the most severe cases, resulting in progressive symmetrical weakness and atrophy of the proximal voluntary muscles. Approximately 95% of SMA patients present with homozygous deletion of the SMN1 gene. With multiple available therapies preventing symptom development and slowing disease progression, newborn screening for SMA is essential to identify at-risk individuals. From 2018 to 2023, a total of 239,844 infants were screened. 13 positive screens were confirmed to have SMA. An additional case was determined to be a false positive. We are not aware of any false-negative cases. All patients were seen promptly, with diagnosis confirmed within 1 week of the initial clinical visit. Patients were treated with nusinersen or onasemnogene abeparvovec. Treated patients with two copies of SMN2 are meeting important developmental milestones inconsistent with the natural history of type 1 SMA. Patients with 3-4 copies of SMN2 follow normal developmental timelines. Newborn screening is an effective tool for the early identification and treatment of patients with SMA. Presymptomatic treatment dramatically shifts the natural history of SMA, with most patients meeting appropriate developmental milestones. Patients with two copies of SMN2 identified through newborn screening constitute a neurogenetic emergency. Due to the complexities of follow-up, a multidisciplinary team, including close communication with the newborn screening program, is required to facilitate timely diagnosis and treatment.

犹他州新生儿脊髓性肌肉萎缩症筛查五年回顾:经验教训。
脊髓性肌萎缩症(SMA)是一种常染色体隐性遗传病,以脊髓前角α运动神经元变性为特征。在最严重的病例中,临床症状表现为出生后最初几周到几个月,导致近端自主肌肉进行性对称性无力和萎缩。约 95% 的 SMA 患者表现为 SMN1 基因同源缺失。现有多种疗法可预防症状发展和减缓疾病进展,因此新生儿SMA筛查对于识别高危人群至关重要。从 2018 年到 2023 年,共有 239844 名婴儿接受了筛查。13 例筛查结果呈阳性的婴儿被证实患有 SMA。另有一例被确定为假阳性。我们未发现任何假阴性病例。所有患者都得到了及时诊治,并在首次临床就诊后一周内确诊。患者接受了纽西奈森或onasemnogene abeparvovec治疗。经治疗后,有两个SMN2拷贝的患者达到了重要的发育里程碑,这与1型SMA的自然病史不符。有3-4个SMN2拷贝的患者遵循正常的发育时间表。新生儿筛查是早期识别和治疗 SMA 患者的有效工具。无症状治疗可显著改变 SMA 的自然病史,使大多数患者达到适当的发育里程碑。通过新生儿筛查发现 SMN2 有两个拷贝的患者属于神经遗传急症。由于随访的复杂性,需要一个多学科团队,包括与新生儿筛查项目的密切沟通,以促进及时诊断和治疗。
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来源期刊
International Journal of Neonatal Screening
International Journal of Neonatal Screening Medicine-Pediatrics, Perinatology and Child Health
CiteScore
6.70
自引率
20.00%
发文量
56
审稿时长
11 weeks
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