Genetic diagnosis of 10 neonates with primary carnitine deficiency.

Jian-qiang Tan; Da-yu Chen; Zhe-tao LI; Ti-zhen Yan; Ji-wei Huang; Ren Cai

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Genetic diagnosis of 10 neonates with primary carnitine deficiency.

Author: Jian-Qiang TAN ¹ ; Da-Yu CHEN ; Zhe-Tao LI ; Ti-Zhen YAN ; Ji-Wei HUANG ; Ren CAI
Author Information

1. Department of Medical Genetics, Liuzhou Maternal and Child Health Care Hospital, Liuzhou, Guangxi 545001, China. lzcairen@126.com.
Publication Type:Journal Article
MeSH: Cardiomyopathies; diagnosis; genetics; Carnitine; deficiency; genetics; Computational Biology; Genetic Counseling; Humans; Hyperammonemia; diagnosis; genetics; Infant, Newborn; Muscular Diseases; diagnosis; genetics; Mutation; Solute Carrier Family 22 Member 5; genetics; Tandem Mass Spectrometry
From: Chinese Journal of Contemporary Pediatrics 2017;19(11):1150-1154
CountryChina
Language:Chinese
Abstract:
OBJECTIVETo study the gene mutation profile of primary carnitine deficiency (PCD) in neonates, and to provide a theoretical basis for early diagnosis and treatment, genetic counseling, and prenatal diagnosis of PCD.
METHODSAcylcarnitine profile analysis was performed by tandem mass spectrometry using 34 167 dry blood spots on filter paper. The SLC22A5 gene was sequenced and analyzed in neonates with free carnitine (C0) levels lower than 10 μmol/L as well as their parents.
RESULTSIn the acylcarnitine profile analysis, a C0 level lower than 10 μmol/L was found in 10 neonates, but C0 level was not reduced in their mothers. The 10 neonates had 10 types of mutations at 20 different sites in the SLC22A5 gene, which included 4 previously unreported mutations: c.976C>T, c.919delG, c.517delC, and c.338G>A. Bioinformatics analysis showed that the four new mutations were associated with a risk of high pathogenicity.
CONCLUSIONSTandem mass spectrometry combined with SLC22A5 gene sequencing may be useful for the early diagnosis of PCD. Identification of new mutations enriches the SLC22A5 gene mutation profile.