Newborn screening of primary carnitine deficiency: clinical and molecular genetic characteristics.

IF 3.1 3区医学 Q1 PEDIATRICS Italian Journal of Pediatrics Pub Date : 2025-03-11 DOI:10.1186/s13052-025-01911-1

Haili Hu, Qingqing Ma, Yan Wang, Wangsheng Song, Hongyu Xu

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Abstract

Background: Primary carnitine deficiency (PCD) is a rare autosomal recessive fatty acid oxidation disorder caused by variants in the SLC22A5 gene, with its prevalence and the spectrum of mutations in SLC22A5 varying across races and regions. This study aimed to analyze the clinical and genetic characteristics of PCD patients, including newborns and their mothers, identified by newborn screening (NBS) in Hefei, China.

Methods: The dried blood spot samples from newborns were analyzed using tandem mass spectrometry (MS/MS) from July 2015 to December 2024. Newborns and their mothers with low free carnitine (C0) levels identified during initial screening were subsequently recalled. Next-generation sequencing was employed to analyze gene mutations in patients whose rescreening results indicated that C0 levels remained below the critical reference value.

Results: A total of 897,050 newborns were screened for PCD, and 46 cases were diagnosed, resulting in an incidence rate of 1 in 19,501. Among the screened population, 34 mothers were identified as PCD patients. A total of 26 different variants were detected in the SLC22A5 gene, including four novel variants found in both PCD newborns and their mothers (c.253 C > T, c.976_977delinsAGCAGT, c.384dup, and c.236_271del). Of the 44 PCD newborns tested at our center, seven exhibited homozygous mutations, 35 exhibited compound heterozygous mutations, and two cases showed no detectable gene mutation. The most common mutation was c.1400 C > G (45.88%), followed by c.51 C > G (16.47%) and c.760 C > T (8.24%). Among the 34 PCD mothers, 15 had homozygous mutations and 19 had compound heterozygous mutations; 60.29% of the mutations were c.1400 C > G. The C0 levels in patients with SLC22A5 truncation mutations were significantly lower than those in the non-truncation mutation group (P < 0.05). Furthermore, within the truncation mutation group, the C0 levels of patients with the S467C mutation were higher than those of patients without the S467C mutation (P < 0.05).

Conclusions: MS/MS combined with genetic testing could effectively enhance the diagnostic accuracy of PCD. Our study identified four novel mutations, expanding the variant spectrum of the SLC22A5 gene.

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新生儿原发性肉碱缺乏症的筛查：临床和分子遗传学特征。

背景：原发性肉碱缺乏症（Primary carnitine deficiency， PCD）是一种罕见的常染色体隐性脂肪酸氧化疾病，由SLC22A5基因变异引起，其患病率和SLC22A5基因突变谱在不同种族和地区存在差异。本研究旨在分析合肥市新生儿筛查（NBS）发现的PCD患者（包括新生儿及其母亲）的临床和遗传特征。方法：采用串联质谱法（MS/MS）对2015年7月~ 2024年12月采集的新生儿干血斑标本进行分析。在最初的筛查中发现的游离肉碱（C0）水平低的新生儿及其母亲随后被召回。采用新一代测序技术分析重筛结果显示C0水平低于临界参考值的患者的基因突变。结果：共筛查新生儿PCD 897,050例，确诊46例，发病率为1 / 19,501。在筛查人群中，34名母亲被确定为PCD患者。SLC22A5基因共检测到26种不同的变异，包括在PCD新生儿及其母亲中发现的4种新变异（c.253）C b> T, C . 976_977delinsagcagt, C .384dup和C .236_271del)。在我们中心检测的44例PCD新生儿中，7例出现纯合突变，35例出现复合杂合突变，2例未检测到基因突变。最常见的突变发生在公元1400年C > G占45.88%,C .51次之C > G（16.47%）和C 760C > t（8.24%）。34例PCD母亲中，纯合突变15例，复合杂合突变19例；c.1400突变占60.29%c b> g。SLC22A5截断突变患者的C0水平明显低于非截断突变组(P)结论：MS/MS联合基因检测可有效提高PCD的诊断准确性。我们的研究发现了四个新的突变，扩大了SLC22A5基因的变异谱。

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来源期刊

Italian Journal of Pediatrics PEDIATRICS-

CiteScore

6.10

自引率

13.90%

发文量

192

审稿时长

6-12 weeks

期刊介绍： Italian Journal of Pediatrics is an open access peer-reviewed journal that includes all aspects of pediatric medicine. The journal also covers health service and public health research that addresses primary care issues. The journal provides a high-quality forum for pediatricians and other healthcare professionals to report and discuss up-to-the-minute research and expert reviews in the field of pediatric medicine. The journal will continue to develop the range of articles published to enable this invaluable resource to stay at the forefront of the field. Italian Journal of Pediatrics, which commenced in 1975 as Rivista Italiana di Pediatria, provides a high-quality forum for pediatricians and other healthcare professionals to report and discuss up-to-the-minute research and expert reviews in the field of pediatric medicine. The journal will continue to develop the range of articles published to enable this invaluable resource to stay at the forefront of the field.