De Novo Mutations in Moderate or Severe Intellectual Disability

Hamdan, Fadi F.; Srour, Myriam; Capo‐Chichi, José‐Mario; Daoud, Hussein; Nassif, Christina; Patry, Lysanne; Massicotte, Christine; Ambalavanan, Amirthagowri; Spiegelman, Dan; Diallo, Ousmane; Henrion, Édouard; Dionne‐Laporte, Alexandre; Fougerat, Anne; Pshezhetsky, Alexey V.; Venkateswaran, Sunita; Rouleau, Guy A.; Michaud, Jacques L.

doi:10.1371/journal.pgen.1004772

Cited by 352 publications

(338 citation statements)

References 61 publications

Supporting

Mentioning

315

Contrasting

Unclassified

Order By: Relevance

“…To date, five other cases of GABRB3 early infantile epileptic encephalopathy have been reported,10, 13 to our knowledge (Table 1). We postulate that there are several features common in all these cases, including: (1) seizure onset in infancy, <10months of age, (2) multiple seizure types including infantile spasms, (3) variable EEG abnormalities, and (4) associated comorbidities such as neurodevelopmental delay, attention‐deficit–hyperactivity disorder, autistic features, and intellectual disability.…”

Section: Discussionmentioning

confidence: 91%

GABRB3 mutations: a new and emerging cause of early infantile epileptic encephalopathy

Papandreou

McTague²,

Trump

et al. 2015

Develop Med Child Neuro

View full text Add to dashboard Cite

The gamma‐aminobutyric acid type A receptor β3 gene (GABRB3) encodes the β3‐subunit of the gamma‐aminobutyric acid type A (GABAA) receptor, which mediates inhibitory signalling within the central nervous system. Recently, GABRB3 mutations have been identified in a few patients with infantile spasms and Lennox–Gastaut syndrome. We report the clinical and electrographic features of a novel case of GABRB3‐related early‐onset epileptic encephalopathy. Our patient presented with neonatal hypotonia and feeding difficulties, then developed pharmacoresistant epileptic encephalopathy, characterized by multiple seizure types from 3 months of age. Electroencephalography demonstrated ictal generalized and interictal multifocal epileptiform abnormalities. Using a SureSelectXT custom multiple gene panel covering 48 early infantile epileptic encephalopathy/developmental delay genes, a novel de novo GABRB3 heterozygous missense mutation, c.860C>T (p.Thr287Ile), was identified and confirmed on Sanger sequencing. GABRB3 is an emerging cause of early‐onset epilepsy. Novel genetic technologies, such as whole‐exome/genome sequencing and multiple gene panels, will undoubtedly identify further cases, allowing more detailed electroclinical delineation of the GABRB3‐related genotypic and phenotypic spectra.

show abstract

Section: Discussionmentioning

confidence: 91%

GABRB3 mutations: a new and emerging cause of early infantile epileptic encephalopathy

Papandreou

McTague²,

Trump

et al. 2015

Develop Med Child Neuro

View full text Add to dashboard Cite

show abstract

“…The value of 1.88 validated de novo variants per patient in our study is consistent with the 1.71-1.98 validated de novo variants per patient previously reported in larger intellectual-disability cohorts, thereby validating our sequencing and analysis pipeline. 19,20 Autosomal recessive, X-linked recessive, and compound heterozygous inheritance models were also investigated, but no variants that could explain the patients' phenotype were detected. The lack of homozygous autosomal recessive causal variants was in accordance with our initial selection of only patients whose parents were nonconsanguineous.…”

Section: Wes Yieldmentioning

confidence: 99%

Effectiveness of whole-exome sequencing and costs of the traditional diagnostic trajectory in children with intellectual disability

Monroe

Frederix

Savelberg

et al. 2016

Genetics in Medicine

151

140

View full text Add to dashboard Cite

Purpose: This study investigated whole-exome sequencing (WES) yield in a subset of intellectually disabled patients referred to our clinical diagnostic center and calculated the total costs of these patients' diagnostic trajectory in order to evaluate early WES implementation. Methods:We compared 17 patients' trio-WES yield with the retrospective costs of diagnostic procedures by comprehensively examining patient records and collecting resource use information for each patient, beginning with patient admittance and concluding with WES initiation. We calculated cost savings using scenario analyses to evaluate the costs replaced by WES when used as a first diagnostic tool.Results: WES resulted in diagnostically useful outcomes in 29.4% of patients. The entire traditional diagnostic trajectory average cost was $16,409 per patient, substantially higher than the $3,972 trio-WES cost. WES resulted in average cost savings of $3,547 for genetic and metabolic investigations in diagnosed patients and $1,727 for genetic investigations in undiagnosed patients. Conclusion:The increased causal variant detection yield by WES and the relatively high costs of the entire traditional diagnostic trajectory suggest that early implementation of WES is a relevant and costefficient option in patient diagnostics. This information is crucial for centers considering implementation of WES and serves as input for future value-based research into diagnostics. Genet Med advance online publication 4 February 2016

show abstract

“…8,9 Previously, we and others separately reported on an individual with a de novo mutation in the 'WW domain-containing adapter with coiled-coil' (WAC) gene using trio-based exome sequencing. 1, 10 The mutations were reported as potential cause of disease, based on mutation severity, protein function, its expression in fetal stages and high expression in adult brain. 1,10,11 WAC encodes a protein-regulating transcription-coupled histone H2B ubiquitination and contains two evolutionary conserved domains, including an N-terminal WW domain interacting with RNA polymerase II and a C-terminal coiled-coil domain promoting the RNF20/RNF40's E3 ligase activity for ubiquitination at active transcription sites.…”

Section: Introductionmentioning

confidence: 99%

De novo loss-of-function mutations in WAC cause a recognizable intellectual disability syndrome and learning deficits in Drosophila

et al. 2016

View full text Add to dashboard Cite

Recently WAC was reported as a candidate gene for intellectual disability (ID) based on the identification of a de novo mutation in an individual with severe ID. WAC regulates transcription-coupled histone H2B ubiquitination and has previously been implicated in the 10p12p11 contiguous gene deletion syndrome. In this study, we report on 10 individuals with de novo WAC mutations which we identified through routine (diagnostic) exome sequencing and targeted resequencing of WAC in 2326 individuals with unexplained ID. All but one mutation was expected to lead to a loss-of-function of WAC. Clinical evaluation of all individuals revealed phenotypic overlap for mild ID, hypotonia, behavioral problems and distinctive facial dysmorphisms, including a square-shaped face, deep set eyes, long palpebral fissures, and a broad mouth and chin. These clinical features were also previously reported in individuals with 10p12p11 microdeletion syndrome. To investigate the role of WAC in ID, we studied the importance of the Drosophila WAC orthologue (CG8949) in habituation, a non-associative learning paradigm. Neuronal knockdown of Drosophila CG8949 resulted in impaired learning, suggesting that WAC is required in neurons for normal cognitive performance. In conclusion, we defined a clinically recognizable ID syndrome, caused by de novo loss-of-function mutations in WAC. Independent functional evidence in Drosophila further supported the role of WAC in ID. On the basis of our data WAC can be added to the list of ID genes with a role in transcription regulation through histone modification.

show abstract

De Novo Mutations in Moderate or Severe Intellectual Disability

Cited by 352 publications

References 61 publications

GABRB3 mutations: a new and emerging cause of early infantile epileptic encephalopathy

GABRB3 mutations: a new and emerging cause of early infantile epileptic encephalopathy

Effectiveness of whole-exome sequencing and costs of the traditional diagnostic trajectory in children with intellectual disability

De novo loss-of-function mutations in WAC cause a recognizable intellectual disability syndrome and learning deficits in Drosophila

Contact Info

Product

Resources

About