The Epilepsy Phenome/Genome Project

McGovern, Kathleen R.; Stillman, Nora; McKenna, Kevin E.; Mays, Vickie M.; Williams, Michael; Carpenter, Alan; Miller, Kevin F.; Agarwal, Prashant; Ayala, Jennifer; Bakey, Cate; Borkowski, Thomas; Boyd, Riann; Camuto, Alicia; Carrasco, Cendy; Cassarly, Jennifer A.; Collins, Yong; Collon, Kevin; Collon, Sean; Eckman, Heather; Fogarty, Susan; Morón, Dolores González; Grayson, La June; Hagopian, Samantha; Hayden, Emily M.; Heggeli, Kristin; Hennessy, Rachel; Hessling, Jody; Hirschfield, Emily; Howell, J. Christina; Klingerman, Sherry; Lopez, Maritza E.; Marinelli, Heather; Maschhaupt, Brandy; Minnick, Jennie; Misajon, Jade; Monahan, Jennifer L.; Oliver, Karen; Parulkar, Isha; Przepiorka, Laura; Pyzik, Paula L.; Regan, Brigid M.; Shain, Catherine; Slingerland, Lexie; Stanton, Caitlin R.; Taylor, Kelly; Thompson, Stacy D.; Turczyk, Jennifer; Vara, Alexander D.; Wesolowski, Cindy; Yourich, Andrew

doi:10.1177/1740774513484392

Cited by 41 publications

(24 citation statements)

References 41 publications

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“…Individual 3 (Coriell ND27062) was ascertained by the Epilepsy Phenome/Genome Project 13 as part of a patient cohort with infantile spasms and/or Lennox-Gastaut syndrome. 5 Seizure onset occurred during the first year of life and seizure types include tonic-clonic, atypical absence, atonic, infantile spasms and focal dyscognitive (Table 4).…”

Section: Methodsmentioning

confidence: 99%

De novo KCNB1 mutations in epileptic encephalopathy

Torkamani

Bersell

Jorge

et al. 2014

Annals of Neurology

126

181

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Background Numerous studies have demonstrated increased load of de novo copy number variants (CNVs) or single nucleotide variants (SNVs) in individuals with neurodevelopmental disorders, including epileptic encephalopathies, intellectual disability and autism. Methods We searched for de novo mutations in a family quartet with a sporadic case of epileptic encephalopathy with no known etiology to determine the underlying cause using high coverage whole exome sequencing (WES) and lower coverage whole genome sequencing (WGS). Mutations in additional patients were identified by WES. The effect of mutations on protein function was assessed in a heterologous expression system. Results We identified a de novo missense mutation in KCNB1 that encodes the KV2.1 voltage-gated potassium channel. Functional studies demonstrated a deleterious effect of the mutation on KV2.1 function leading to a loss of ion selectivity and gain of a depolarizing inward cation conductance. Subsequently, we identified two additional patients with epileptic encephalopathy and de novo KCNB1 missense mutations that cause a similar pattern of KV2.1 dysfunction. Interpretation Our genetic and functional evidence demonstrate that KCNB1 mutation can result in early onset epileptic encephalopathy. This expands the locus heterogeneity associated with epileptic encephalopathies and suggests that clinical WES may be useful for diagnosis of epileptic encephalopathies of unknown etiology.

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Section: Methodsmentioning

confidence: 99%

De novo KCNB1 mutations in epileptic encephalopathy

Torkamani

Bersell

Jorge

et al. 2014

Annals of Neurology

126

181

View full text Add to dashboard Cite

show abstract

“…Participants were identified through a combination of prospective screening of clinic patients, retrospective review of medical records, and education and recruitment of colleagues within the primary EPGP institutions and neighboring institutions. [23] After obtaining informed consent from the subject, all clinical and demographic data were gathered prospectively through semi-structured interviews as well as review of medical records, EEG, and imaging data. Figure 1 depicts the data collection and review processes and the three points at which eligibility was re-assessed following obtaining informed consent.…”

Section: Methodsmentioning

confidence: 99%

“…If the EEG was normal, there had to be clear clinical history and the data were sent for review and adjudication. [23] For NAFE, subjects had neuroimaging which was either normal or demonstrated mesial temporal sclerosis or focal cortical dysplasia and an unambiguous clinical semiology consistent with focal seizures and/or focal EEG abnormalities. Patients with benign rolandic epilepsy based upon clinical presentation were not required to have neuroimaging.…”

Section: Methodsmentioning

confidence: 99%

“…[23] The interview was modified from a previously validated instrument. [25, 26] When necessary, data were reviewed and adjudicated by the Phenotype Core.…”

Section: Methodsmentioning

confidence: 99%

“…Systematic quality reviews were conducted to identify and correct errors in phenotypic data[23]. All data were stored electronically in a central repository[27].…”

Section: Methodsmentioning

confidence: 99%

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Sex differences in seizure types and symptoms

Carlson¹,

Dugan²,

Kirsch³

et al. 2014

Epilepsy & Behavior

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Background Despite the increasing interest in sex differences in disease manifestations and responses to treatment, very few data are available on sex differences in seizure types and semiology. The Epilepsy Phenome/Genome Project (EPGP) is a large-scale, multi-institutional, collaborative study that aims to create a comprehensive repository of detailed clinical information and DNA samples from a large cohort of people with epilepsy. We used this well-characterized cohort to explore differences in seizure types as well as focal seizure symptoms between males and females. Methods We reviewed the EPGP database and identified individuals with generalized epilepsy of unknown etiology (GE) (n=760; female 446, male 314), non-acquired focal epilepsy (NAFE) (n=476; female 245, male 231), or both (n=64; female 33, male 31). Demographic data along with characterization of seizure type and focal seizure semiologies were examined. Results In GE, males reported atonic seizures more frequently than females (6.5% vs. 1.7%; p<0.001). No differences were observed in other generalized seizure types. In NAFE, no sex differences were seen for seizure types with or without alteration of consciousness or progression to secondary generalization. Autonomic (16.4% vs. 26.6%; p=0.005), psychic (26.7% vs. 40.3%; p=0.001), and visual symptoms (10.3% vs. 19.9%; p=0.002) were more frequently reported in females than males. Specifically, of psychic symptoms, more females than males endorsed déjà vu (p=0.001), but not forced thoughts, derealization/depersonalization, jamais vu, or fear. With corrections for multiple comparisons, there were no significant differences in aphasic, motor, somatosensory, gustatory, olfactory, auditory, vertiginous, or ictal headache symptoms between sexes. Conclusions Significant differences between the sexes were observed in the reporting of atonic seizures, which was more common in males with GE, and for autonomic, visual, and psychic symptoms associated with NAFE, which were more common in females.

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Copy number variant analysis from exome data in 349 patients with epileptic encephalopathy

Allen¹,

Coe²,

Cook³

et al. 2015

Annals of Neurology

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Infantile spasms (IS) and Lennox Gastaut syndrome (LGS) are epileptic encephalopathies characterized by early-onset, intractable seizures and poor developmental outcomes. De novo sequence mutations and copy number variants (CNVs) are causative in a subset of cases. We used exome sequence data in 349 trios with IS or LGS to identify putative de novo CNVs. We confirm 18 de novo CNVs in 17 patients (4.8%), 10 of which are likely pathogenic, giving a firm genetic diagnosis for 2.9% of patients. Confirmation of exome-predicted CNVs by array-based methods is still required due to false positive rates of prediction algorithms. Our exome-based results are consistent with recent array-based studies in similar cohorts and highlight novel candidate genes for IS and LGS.

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The Epilepsy Phenome/Genome Project

Cited by 41 publications

References 41 publications

De novo KCNB1 mutations in epileptic encephalopathy

De novo KCNB1 mutations in epileptic encephalopathy

Sex differences in seizure types and symptoms

Copy number variant analysis from exome data in 349 patients with epileptic encephalopathy

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