peer reviewedGermline and brain-specific somatic variants have been reported as an underlying cause in patients with epilepsy-associated neuropathologies, including focal cortical dysplasias (FCDs) and long-term epilepsy associated tumors (LEAT). However, evaluation of identified neuropathology associated variants in genetic screens is complex since not all observed variants contribute to the etiology of neuropathologies not even in genuinely disease-associated genes. Here, we critically reevaluated the pathogenicity of 12 previously published disease-related genes and of 79 neuropathology-associated missense variants listed in the PubMed and ClinVar databases. We (1) assessed the evolutionary gene constraint using the pLI and the missense...
Trio exome sequencing has been successful in identifying genes with de novo mutations (DNMs) causing...
BACKGROUND: Many genes are candidates for involvement in epileptic encephalopathy (EE) because one o...
Abstract The clinical diagnosis of neurodegenerative disorders based on phenotype is difficult in he...
Objective Increasing availability of surgically resected brain tissue from patients with focal epile...
Purpose: Increasing availability of surgically resected brain tissue from Focal Cortical Dysplasia a...
peer reviewedObjective: Increasing availability of surgically resected brain tissue from patients ...
It is challenging to estimate genetic variant burden across different subtypes of epilepsy. Herein, ...
Gene panel and exome sequencing have revealed a high rate of molecular diagnoses among diseases wher...
Missense variant interpretation is challenging. Essential regions for protein function are conserved...
OBJECTIVE: Copy number variations (CNVs) represent a significant genetic risk for several neurodevel...
Background: Classifying pathogenicity of missense variants represents a major challenge in clinical ...
Trio exome sequencing has been successful in identifying genes with de novo mutations (DNMs) causing...
Trio exome sequencing has been successful in identifying genes with de novo mutations (DNMs) causing...
BACKGROUND: Many genes are candidates for involvement in epileptic encephalopathy (EE) because one o...
Abstract The clinical diagnosis of neurodegenerative disorders based on phenotype is difficult in he...
Objective Increasing availability of surgically resected brain tissue from patients with focal epile...
Purpose: Increasing availability of surgically resected brain tissue from Focal Cortical Dysplasia a...
peer reviewedObjective: Increasing availability of surgically resected brain tissue from patients ...
It is challenging to estimate genetic variant burden across different subtypes of epilepsy. Herein, ...
Gene panel and exome sequencing have revealed a high rate of molecular diagnoses among diseases wher...
Missense variant interpretation is challenging. Essential regions for protein function are conserved...
OBJECTIVE: Copy number variations (CNVs) represent a significant genetic risk for several neurodevel...
Background: Classifying pathogenicity of missense variants represents a major challenge in clinical ...
Trio exome sequencing has been successful in identifying genes with de novo mutations (DNMs) causing...
Trio exome sequencing has been successful in identifying genes with de novo mutations (DNMs) causing...
BACKGROUND: Many genes are candidates for involvement in epileptic encephalopathy (EE) because one o...
Abstract The clinical diagnosis of neurodegenerative disorders based on phenotype is difficult in he...