2020
DOI: 10.1186/s13052-020-00860-1
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Targeted re-sequencing for early diagnosis of genetic causes of childhood epilepsy: the Italian experience from the ‘beyond epilepsy’ project

Abstract: Background Childhood epilepsies are a heterogeneous group of conditions differing in diagnostic criteria, management, and outcome. Late-infantile neuronal ceroid lipofuscinosis type 2 (CLN2) is a neurodegenerative condition caused by biallelic TPP1 variants. This disorder presents with subtle and relatively non-specific symptoms, mimicking those observed in more common paediatric epilepsies and followed by rapid psychomotor deterioration and drug-resistant epilepsy. A prompt diagnosis is essential to adopt app… Show more

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Cited by 26 publications
(23 citation statements)
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“…Remarkably, patients with CLN2 disease in this study were diagnosed at a mean age of 38.7 months with a mean time from seizure onset to diagnosis of 10 months, a significantly shorter time compared to natural history diagnostic data [ 34 ], demonstrating that use of a comprehensive epilepsy gene panel can effectively and timely diagnose patients with CLN2 disease. Interestingly, consistent with our study, three other reports have recently shown TPP1 ( CLN2 ) pathogenic or likely pathogenic variants and CLN2 diagnosis being a relatively common finding when using NGS panels for diagnostics of pediatric seizure patients [ 10 , 26 ]. These findings stress the importance of the genes included in the selected panel when evaluating the diagnostic yield and appropriateness of the panel.…”
Section: Discussionsupporting
confidence: 92%
See 1 more Smart Citation
“…Remarkably, patients with CLN2 disease in this study were diagnosed at a mean age of 38.7 months with a mean time from seizure onset to diagnosis of 10 months, a significantly shorter time compared to natural history diagnostic data [ 34 ], demonstrating that use of a comprehensive epilepsy gene panel can effectively and timely diagnose patients with CLN2 disease. Interestingly, consistent with our study, three other reports have recently shown TPP1 ( CLN2 ) pathogenic or likely pathogenic variants and CLN2 diagnosis being a relatively common finding when using NGS panels for diagnostics of pediatric seizure patients [ 10 , 26 ]. These findings stress the importance of the genes included in the selected panel when evaluating the diagnostic yield and appropriateness of the panel.…”
Section: Discussionsupporting
confidence: 92%
“…To our knowledge, this represents one of the first studies in patients with epilepsy onset between 24 to 60 months of life with comprehensive genetic testing [ 26 ]. The inclusion criteria were selected according to common early findings of CLN2 disease: unprovoked seizure after 2 years of age and at least one of motor disturbance, speech delay, MRI abnormalities and abnormal EEG.…”
Section: Discussionmentioning
confidence: 99%
“…Particularly, patients harbouring the p.(D146N) EPM2B mutation invariably show atypical milder LD, with delayed disease onset and prolonged disease course [9][10][11]. Nowadays, next-generation sequencing technologies have shortened the time needed for the diagnosis of several neurological disorders, including LD [12]. Nevertheless, predicting the prognosis and the evolution of LD remains challenging in most patients.…”
Section: Introductionmentioning
confidence: 99%
“…An example of how panels may be used to identify patients with genetic epilepsies is a prospective, multicenter study of targeted resequencing using a 283-gene next-generation sequencing panel to analyze samples from 21 children with neurodevelopmental abnormalities (aged 24-60 months) after the first unprovoked seizure [74]. Four children were diagnosed with a genetic disorder, resulting in a diagnostic yield of 19%.…”
Section: Expert Opinionmentioning
confidence: 99%