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Default NMR-based urinalysis for rapid diagnosis of ?-ureidopropionase deficiency in a patient with Dravet syndrome.

NMR-based urinalysis for rapid diagnosis of ?-ureidopropionase deficiency in a patient with Dravet syndrome.

Related Articles NMR-based urinalysis for rapid diagnosis of ?-ureidopropionase deficiency in a patient with Dravet syndrome.

Clin Chim Acta. 2015 Feb 2;440:201-4

Authors: Lam CW, Law CY, Leung KF, Lai CK, Pak-lam Chen S, Chan B, Chan KY, Yuen YP, Mak CM, Yan-wo Chan A

Abstract
BACKGROUND: Beta-ureidopropionase deficiency is a rare inborn error of metabolism (IEM) affecting pyrimidine metabolism. To-date, about 30 genetically confirmed cases had been reported. The clinical phenotypes of this condition are variable; some patients were asymptomatic while some may present with developmental delay or autistic features. In severe cases, patients may present with profound neurological deficit including hypotonia, seizures and mental retardation. Using NMR-based urinalysis, this condition can be rapidly diagnosed within 15 min.
CASE: An 11-month-old Chinese boy had dual molecular diagnoses, ?-ureidopropionase deficiency and Dravet syndrome. He presented with intractable and recurrent convulsions, global developmental delay and microcephaly. Urine organic acid analysis using GC-MS and NMR-based urinalysis showed excessive amount of ?-ureidopropionic acid and ?-ureidoisobutyric acid, the two disease-specific markers for ?-ureidopropionase deficiency. Genetic analysis confirmed homozygous known disease-causing mutation UPB1 NM_016327.2: c.977G>A; NP_057411.1:p.R326Q. In addition, genetic analysis for Dravet syndrome showed the presence of heterozygous disease-causing mutation SCN1A NM_001165963.1:c.4494delC; NP_001159435.1:p.F1499Lfs*2.
CONCLUSIONS: The differentiation between Dravet syndrome and ?-ureidopropionase deficiency is clinically challenging since both conditions share overlapping clinical features. The detection of urine ?-ureidoisobutyric and ?-ureidopropionic acids using NMR or GC-MS is helpful in laboratory diagnosis of ?-ureidopropionase deficiency. The disease-causing mutation, c.977G>A of ?-ureidopropionase deficiency, is highly prevalent in Chinese population (allele frequency=1.7%); ?-ureidopropionase deficiency screening test should be performed for any patients with unexplained neurological deficit, developmental delay or autism.


PMID: 25445412 [PubMed - indexed for MEDLINE]



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