Incidence, disease onset and short-term outcome in urea cycle disorders –cross-border surveillance in Germany, Austria and Switzerland

Nettesheim, Susanne; Kölker, Stefan; Häberle, Johannes; Posset, Roland; Hoffmann, Georg F.; Heinrich, B.; Gleich, Florian; Garbade, Sven F.

doi:10.1186/s13023-017-0661-x

Cited by 46 publications

(55 citation statements)

References 36 publications

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“…Except for selected UCDs such as ASL-D, showing progressive neurological and hepatic disease, 18 this is unexpected and not consistent with previous studies. 1,3,4,12 This is substantiated by a study demonstrating that cumulative exposures to disease-specific neurotoxic biomarkers (ie, plasma ammonium, L-glutamine, L-citrulline, and L-arginine) appear to be sensitive predictors of global neuropsychological outcome in ASS1-D, ASL-D, and ARG1-D. 18 Recently, ASS1, the deficient enzyme in individuals with ASS1-D, has been identified as an RNA-binding protein and as such could potentially interfere with RNA metabolism. 2,8,9 However, ascertainment bias does not seem to fully explain the observed discrepancy in outcomes, and alternative pathomechanisms are also to be considered.…”

Section: Discussionmentioning

confidence: 99%

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Impact of Diagnosis and Therapy on Cognitive Function in Urea Cycle Disorders

Posset

Gropman

Nagamani

et al. 2019

Annals of Neurology

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Objective: Individuals with urea cycle disorders (UCDs) often present with intellectual and developmental disabilities. The major aim of this study was to evaluate the impact of diagnostic and therapeutic interventions on cognitive outcomes in UCDs. Methods: This prospective, observational, multicenter study includes data from 503 individuals with UCDs who had comprehensive neurocognitive testing with a cumulative follow-up of 702 patient-years. Results: The mean cognitive standard deviation score (cSDS) was lower in symptomatic than in asymptomatic (p < 0.001, t test) individuals with UCDs. Intellectual disability (intellectual quotient < 70, cSDS < −2.0) was associated with the respective subtype of UCD and early disease onset, whereas height of the initial peak plasma ammonium concentration was inversely associated with neurocognitive outcomes in mitochondrial (proximal) rather than cytosolic (distal) UCDs. In ornithine transcarbamylase and argininosuccinate synthetase 1 deficiencies, we did not find evidence that monoscavenger therapy with sodium or glycerol phenylbutyrate was superior to sodium benzoate in providing cognitive protection. Early liver transplantation appears to be beneficial for UCDs. It is noteworthy that individuals with argininosuccinate synthetase 1 and argininosuccinate lyase deficiencies identified by newborn screening had better neurocognitive outcomes than those diagnosed after the manifestation of first symptoms. Interpretation: Cognitive function is related to interventional and non-interventional variables. Early detection by newborn screening and early liver transplantation appear to offer greater cognitive protection, but none of the currently used nitrogen scavengers was superior with regard to long-term neurocognitive outcome. Further confirmation could determine these variables as important clinical indicators of neuroprotection for individuals with UCDs.

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Section: Discussionmentioning

confidence: 99%

“…1 Individuals with UCDs are often affected by morbidity due to neurocognitive deficits and reduced life expectancy. 1 Individuals with UCDs are often affected by morbidity due to neurocognitive deficits and reduced life expectancy.…”

mentioning

confidence: 99%

Impact of Diagnosis and Therapy on Cognitive Function in Urea Cycle Disorders

Posset

Gropman

Nagamani

et al. 2019

Annals of Neurology

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“…Males with hypomorphic OTC alleles that retain residual enzyme activity, or female heterozygotes with skewed lyonization (Caldovic, Abdikarim, Narain, Tuchman, & Morizono, ; McCullough et al., ) typically present symptomatically after the first week of life (Caldovic et al., ; Numata et al., ). The true prevalence of OTCD is unknown, but it has been estimated to be between one in 14,000 and one in 76,000 (Balasubramaniam et al., ; Brusilow & Maestri, ; Dionisi‐Vici et al., ; Nettesheim et al., ; Summar et al., ). In 85%–90% of patients with the biochemical phenotype of OTCD, a mutation can be identified through commercially available sequencing or deletion/duplication testing.…”

Section: Introductionmentioning

confidence: 99%

Disease-causing mutations in the promoter and enhancer of the ornithine transcarbamylase gene

et al. 2018

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The ornithine transcarbamylase (OTC) gene is on the X chromosome and its product catalyzes the formation of citrulline from ornithine and carbamylphosphate in the urea cycle. About 10%-15% of patients, clinically diagnosed with OTC deficiency (OTCD), lack identifiable mutations in the coding region or splice junctions of the OTC gene on routine molecular testing. We collected DNA from such patients via retrospective review and by prospective enrollment. In nine of 38 subjects (24%), we identified a sequence variant in the OTC regulatory regions. Eight subjects had unique sequence variants in the OTC promoter and one subject had a novel sequence variant in the OTC enhancer. All sequence variants affect positions that are highly conserved in mammalian OTC genes. Functional studies revealed reduced reporter gene expression with all sequence variants. Two sequence variants caused decreased binding of the HNF4 transcription factor to its mutated binding site. Bioinformatic analyses combined with functional assays can be used to identify and authenticate pathogenic sequence variants in regulatory regions of the OTC gene, in other urea cycle disorders or other inborn errors of metabolism.

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“…The time of onset presents as either in neonates or in a more insidious late‐onset. The morbidity of CPS1D is estimated 1:50 000‐1:300 000 in worldwide, of which 1:800 000 in Japan and 1:50 000‐1:100 000 in European population . To our knowledge, the frequency of CPS1D has not been observed in Chinese cohorts and only three Chinese patients with CPS1D were reported …”

Section: Introductionmentioning

confidence: 80%

“…The morbidity of CPS1D is estimated 1:50 000-1:300 000 in worldwide, of which 1:800 000 in Japan and 1:50 000-1:100 000 in European population. 1,[3][4][5][6] To our knowledge, the frequency of CPS1D has not been observed in Chinese cohorts and only three Chinese patients with CPS1D were reported. 1,3 The pathogenic gene of CPS1D is CPS1 (CPS1; NC_000002.12), which encodes carbamoyl phosphate synthetase 1 (CPS1).…”

Section: Introductionmentioning

confidence: 83%

Two novel CPS1 mutations in a case of carbamoyl phosphate synthetase 1 deficiency causing hyperammonemia and leukodystrophy

Chen

Yuan

Sun

et al. 2018

Clinical Laboratory Analysis

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This study described the specific clinical characteristics and the variations of physiological and biochemical indices in a Chinese neonatal patient with CPS1D, which facilitated the diagnosis and mechanism research of the disease. Two novel causative missense mutations were identified, which enriched the mutation spectrum of CPS1D in China and worldwide. Advice of prenatal diagnosis was given to the family for a new pregnancy.

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Incidence, disease onset and short-term outcome in urea cycle disorders –cross-border surveillance in Germany, Austria and Switzerland

Cited by 46 publications

References 36 publications

Impact of Diagnosis and Therapy on Cognitive Function in Urea Cycle Disorders

Impact of Diagnosis and Therapy on Cognitive Function in Urea Cycle Disorders

Disease-causing mutations in the promoter and enhancer of the ornithine transcarbamylase gene

Two novel CPS1 mutations in a case of carbamoyl phosphate synthetase 1 deficiency causing hyperammonemia and leukodystrophy

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