Prevalence and clinical prediction of mitochondrial disorders in a large neuropediatric cohort.
Friedhelm HildebrandtJessika JohannsenFanny KortümMatias WagnerKonstantinos TsiakasTatjana BierhalsDavor LesselTheresia HergetKatja KlothJasmin LisfeldTasja ScholzNadia ObiSaskia WortmannHolger ProkischChristian KubischJonas DeneckeRené SanterMaja HempelPublished in: Clinical genetics (2021)
Neurological symptoms are frequent and often a leading feature of childhood-onset mitochondrial disorders (MD) but the exact incidence of MD in unselected neuropediatric patients is unknown. Their early detection is desirable due to a potentially rapid clinical decline and the availability of management options. In 491 children with neurological symptoms, a comprehensive diagnostic work-up including exome sequencing was performed. The success rate in terms of a molecular genetic diagnosis within our cohort was 51%. Disease-causing variants in a mitochondria-associated gene were detected in 12% of solved cases. In order to facilitate the clinical identification of MDs within neuropediatric cohorts, we have created an easy-to-use bedside-tool, the MDC-NP. In our cohort, the MDC-NP predicted disease conditions related to MDs with a sensitivity of 0.83, and a specificity of 0.96.
Keyphrases
- copy number
- risk factors
- oxidative stress
- end stage renal disease
- genome wide
- newly diagnosed
- chronic kidney disease
- cell death
- gene expression
- physical activity
- peritoneal dialysis
- molecular dynamics
- sleep quality
- dna methylation
- prognostic factors
- young adults
- blood brain barrier
- reactive oxygen species
- single molecule
- quantum dots