Incidence and phenotypes of childhood-onset genetic epilepsies: a prospective population-based national cohort

Symonds, Joseph D.; Zuberi, Sameer M.; Stewart, Kirsty; McLellan, Ailsa; O’Regan, Mary; MacLeod, S. M.; Jollands, Alice; Joss, Shelagh; Kirkpatrick, Martin; Brunklaus, Andreas; Pilz, Daniela T.; Shetty, Jay; Dorris, Liam; Abu‐Arafeh, Ishaq; Andrew, Jamie; Brink, Philip; Callaghan, Mary; Cruden, Jamie; Diver, Louise A; Findlay, Christine; Gardiner, Sarah L.; Grattan, Rosemary; Lang, Bethan; MacDonnell, Jane; McKnight, Jean; Morrison, Calum A.; Nairn, Lesley; Slean, Meghan M.; Stephen, Elma; Webb, Alan; Vincent, Angela; Wilson, Margaret T.

doi:10.1093/brain/awz195

Cited by 271 publications

(266 citation statements)

References 80 publications

Supporting

Mentioning

243

Contrasting

Unclassified

Order By: Relevance

“…In the present study, a genetic etiology for nearly half of the patients (47.3%) with infantile-onset epilepsy was identified. The higher diagnostic yield in this age group was recently demonstrated in a prospective population-based study by Symonds et al (26). They prospectively recruited patients whose seizure onset was before 36 months of age.…”

Section: Discussionmentioning

confidence: 91%

Diagnostic Yield of Epilepsy Panel Testing in Patients With Seizure Onset Within the First Year of Life

Jang

Kim

et al. 2019

Front. Neurol.

View full text Add to dashboard Cite

Purpose: We aimed to evaluate the diagnostic yield of epilepsy gene panel testing in epilepsy patients whose seizures began within the first year after birth. We included 112 patients with seizure onset before 12 months and no known etiology.Methods: Deep targeted sequencing with a custom-designed capture probe was performed to ensure the detection of germline or mosaic sequence variants and copy number variations (CNVs).Results: We identified pathogenic or likely pathogenic variants in 53 patients (47.3%, 53/112), including five with pathogenic CNVs. Two putative pathogenic mosaic variants in SCN8A and KCNQ2 were also detected and validated. Those with neonatal onset (61.5%, 16/26) or early infantile onset (50.0%, 29/58) showed higher diagnostic rates than those with late infantile onset (28.5%, 8/28). The diagnostic rate was similar between patients with a specific syndrome (51.9%, 27/52) and those with no recognizable syndrome (43.3%, 26/60).Conclusion: Epilepsy gene panel testing identified a genetic cause in nearly half of the infantile onset epilepsy patients. Since the phenotypic spectrum is expanding and characterizing it at seizure onset is difficult, this group should be prioritized for epilepsy gene panel testing.

show abstract

Section: Discussionmentioning

confidence: 91%

Diagnostic Yield of Epilepsy Panel Testing in Patients With Seizure Onset Within the First Year of Life

Jang

Kim

et al. 2019

Front. Neurol.

View full text Add to dashboard Cite

show abstract

“…At this early stage, genetic testing results are often not yet available and may take weeks or months to conclude. However, there is robust population‐ and cohort‐based evidence showing that the genetic epilepsies commonly presenting at this early age (<3 months) are KCNQ2 , KCNQ3 , CDKL5 , SCN2A, and STXBP1 , but not SCN1A . These young infants will in the majority of cases respond to SCBs without the expectation for seizures to worsen when SCBs are given.…”

Section: Discussionmentioning

confidence: 99%

“…However, there is robust population-and cohort-based evidence showing that the genetic epilepsies commonly presenting at this early age (<3 months) are KCNQ2, KCNQ3, CDKL5, SCN2A, and STXBP1, but not SCN1A. 54,55 These young infants will in the majority of cases respond to SCBs without the expectation for seizures to worsen when SCBs are given. The theoretical risk of seizure exacerbation due to SCBs is comparatively low, because we show how unlikely SCN1A variants are to present at this young age.…”

Section: Clinical Relevance and Implications For Precision Medicinementioning

confidence: 99%

Biological concepts in human sodium channel epilepsies and their relevance in clinical practice

Brunklaus

Steckler

et al. 2020

Epilepsia

Self Cite

View full text Add to dashboard Cite

Objective Voltage‐gated sodium channels (SCNs) share similar amino acid sequence, structure, and function. Genetic variants in the four human brain‐expressed SCN genes SCN1A/2A/3A/8A have been associated with heterogeneous epilepsy phenotypes and neurodevelopmental disorders. To better understand the biology of seizure susceptibility in SCN‐related epilepsies, our aim was to determine similarities and differences between sodium channel disorders, allowing us to develop a broader perspective on precision treatment than on an individual gene level alone. Methods We analyzed genotype‐phenotype correlations in large SCN‐patient cohorts and applied variant constraint analysis to identify severe sodium channel disease. We examined temporal patterns of human SCN expression and correlated functional data from in vitro studies with clinical phenotypes across different sodium channel disorders. Results Comparing 865 epilepsy patients (504 SCN1A, 140 SCN2A, 171 SCN8A, four SCN3A, 46 copy number variation [CNV] cases) and analysis of 114 functional studies allowed us to identify common patterns of presentation. All four epilepsy‐associated SCN genes demonstrated significant constraint in both protein truncating and missense variation when compared to other SCN genes. We observed that age at seizure onset is related to SCN gene expression over time. Individuals with gain‐of‐function SCN2A/3A/8A missense variants or CNV duplications share similar characteristics, most frequently present with early onset epilepsy (<3 months), and demonstrate good response to sodium channel blockers (SCBs). Direct comparison of corresponding SCN variants across different SCN subtypes illustrates that the functional effects of variants in corresponding channel locations are similar; however, their clinical manifestation differs, depending on their role in different types of neurons in which they are expressed. Significance Variant function and location within one channel can serve as a surrogate for variant effects across related sodium channels. Taking a broader view on precision treatment suggests that in those patients with a suspected underlying genetic epilepsy presenting with neonatal or early onset seizures (<3 months), SCBs should be considered.

show abstract

“…The raw data from Whole Exome Sequencing (WES) were screened using an in-house pipeline as previously described [6] allowing for filtering of synonymous and common variants to which a panel of approximately 1300 genes known to be implicated in developmental delay and seizure disorders was applied. The original analysis failed to yield any variant that might be plausibly linked to an intellectual disability or epilepsy phenotype [7]. The data were reanalyzed six months later using an updated panel that (at that point) contained the gene UBTF, that had just been published in connection with an intellectual disability phenotype by Edvardson et al [1].…”

Section: Case Presentationmentioning

confidence: 99%

Childhood neurodegeneration associated with a specific UBTF variant: a new case report and review of the literature

et al. 2020

View full text Add to dashboard Cite

Background: A new monogenic neurodegenerative disease affecting ribosomal metabolism has recently been identified in association with a monoallelic UBTF putative gain of function variant (NM_001076683.1:c.628G>A, hg19). Phenotype is consistent among these probands with progressive motor, cognitive, and behavioural regression in early to middle childhood. Case presentation: We report on a child with this monoallelic UBTF variant who presented with progressive disease including regression, episodes of subacute deterioration during febrile illnesses and a remarkable EEG pattern with a transient pattern of semi-periodic slow waves. Conclusions: This case further supports the phenotype-genotype correlation of neurodegeneration associated with UBTF c.628G>A. Moreover, it brings new insights into the clinical features and EEG that could possibly serve as diagnostic markers of this otherwise nonspecific phenotype.

show abstract

Incidence and phenotypes of childhood-onset genetic epilepsies: a prospective population-based national cohort

Cited by 271 publications

References 80 publications

Diagnostic Yield of Epilepsy Panel Testing in Patients With Seizure Onset Within the First Year of Life

Diagnostic Yield of Epilepsy Panel Testing in Patients With Seizure Onset Within the First Year of Life

Biological concepts in human sodium channel epilepsies and their relevance in clinical practice

Childhood neurodegeneration associated with a specific UBTF variant: a new case report and review of the literature

Contact Info

Product

Resources

About