Your search keyword '"Berkovic, Samuel F."' showing total 34 results

1. Familial aggregation of seizure outcomes in four familial epilepsy cohorts.

Author

Ellis, Colin A., Tu, Danni, Oliver, Karen L., Mefford, Heather C., Hauser, W. Allen, Buchhalter, Jeffrey, Epstein, Michael P., Cao, Quy, Berkovic, Samuel F., and Ottman, Ruth

Subjects

EPILEPSY, SEIZURES (Medicine), INTRACLASS correlation, PEOPLE with epilepsy

Abstract

Objective: To assess the possible effects of genetics on seizure outcome by estimating the familial aggregation of three outcome measures: seizure remission, history of ≥4 tonic–clonic seizures, and seizure control for individuals taking antiseizure medication. Methods: We analyzed families containing multiple persons with epilepsy in four previously collected retrospective cohorts. Seizure remission was defined as being 5 and 10 years seizure‐free at last observation. Total number of tonic–clonic seizures was dichotomized at <4 and ≥4 seizures. Seizure control in patients taking antiseizure medication was defined as no seizures for 1, 2, and 3 years. We used Bayesian generalized linear mixed‐effects model (GLMM) to estimate the intraclass correlation coefficient (ICC) of the family‐specific random effect, controlling for epilepsy type, age at epilepsy onset, and age at last data collection as fixed effects. We analyzed each cohort separately and performed meta‐analysis using GLMMs. Results: The combined cohorts included 3644 individuals with epilepsy from 1463 families. A history of ≥4 tonic–clonic seizures showed strong familial aggregation in three separate cohorts and meta‐analysis (ICC.28, 95% confidence interval [CI].21–.35, Bayes factor 8 × 1016). Meta‐analyses did not reveal significant familial aggregation of seizure remission (ICC.08, 95% CI.01–.17, Bayes factor 1.46) or seizure control for individuals taking antiseizure medication (ICC.13, 95% CI 0–.35, Bayes factor 0.94), with heterogeneity among cohorts. Significance: A history of ≥4 tonic–clonic seizures aggregated strongly in families, suggesting a genetic influence, whereas seizure remission and seizure control for individuals taking antiseizure medications did not aggregate consistently in families. Different seizure outcomes may have different underlying biology and risk factors. These findings should inform the future molecular genetic studies of seizure outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

2. Recognition and epileptology of protracted CLN3 disease.

Author

Cameron, Jillian M., Damiano, John A., Grinton, Bronwyn, Carney, Patrick W., McKelvie, Penny, Silbert, Peter, Lawn, Nicholas, Scheffer, Ingrid E., Oliver, Karen L., Hildebrand, Michael S., and Berkovic, Samuel F.

Subjects

EPILEPSY, SEIZURES (Medicine), EPILEPTIFORM discharges, PARTIAL epilepsy, HAPLOTYPES, CLINICAL deterioration

Abstract

Objective: This study was undertaken to analyze phenotypic features of a cohort of patients with protracted CLN3 disease to improve recognition of the disorder. Methods: We analyzed phenotypic data of 10 patients from six families with protracted CLN3 disease. Haplotype analysis was performed in three reportedly unrelated families. Results: Visual impairment was the initial symptom, with onset at 5–9 years, similar to classic CLN3 disease. Mean time from onset of visual impairment to seizures was 12 years (range = 6–41 years). Various seizure types were reported, most commonly generalized tonic–clonic seizures; focal seizures were present in four patients. Progressive myoclonus epilepsy was not seen. Interictal electroencephalogram revealed mild background slowing and 2.5–3.5‐Hz spontaneous generalized spike–wave discharges. Additional interictal focal epileptiform discharges were noted in some patients. Age at death for the three deceased patients was 31, 31, and 52 years. Molecular testing revealed five individuals were homozygous for c.461‐280_677 + 382del966, the "common 1‐kb" CLN3 deletion. The remaining individuals were compound heterozygous for various combinations of recurrent pathogenic CLN3 variants. Haplotype analysis demonstrated evidence of a common founder for the common 1‐kb deletion. Dating analysis suggested the deletion arose approximately 1500 years ago and thus did not represent cryptic familial relationship in this Australian cohort. Significance: We highlight the protracted phenotype of a disease generally associated with death in adolescence, which is a combined focal and generalized epilepsy syndrome with progressive neurological deterioration. The disorder should be suspected in an adolescent or adult patient presenting with generalized or focal seizures preceded by progressive visual loss. The common 1‐kb deletion has been typically associated with classic CLN3 disease, and the protracted phenotype has not previously been reported with this genotype. This suggests that modifying genetic factors may be important in determining this somewhat milder phenotype and identification of these factors should be the subject of future research. [ABSTRACT FROM AUTHOR]

Published

2023

3. Extended follow‐up after anterior temporal lobectomy demonstrates seizure recurrence 20+ years postsurgery.

Author

McIntosh, Anne M., Wynd, Alex W., and Berkovic, Samuel F.

Subjects

TEMPORAL lobectomy, SEIZURES (Medicine), TEMPORAL lobe, FREE will & determinism, LOG-rank test, EPILEPSY

Abstract

Objective: Anterior temporal lobectomy (ATL) for medication‐resistant localized epilepsy results in ablation or reduction of seizures for most patients. However, some individuals who attain an initial extended period of postsurgical seizure freedom will experience a later seizure recurrence. In this study, we examined the prevalence and some risk factors for late recurrence in an ATL cohort with extensive regular follow‐up. Methods: Included were 449 patients who underwent ATL at Austin Health, Australia, from 1978 to 2008. Postsurgical follow‐up was undertaken 2–3 yearly. Seizure recurrence was tested using Kaplan–Meier analysis, log‐rank test, and Cox regression. Late recurrence was qualified as a first disabling seizure >2 years postsurgery. We examined risks within the ATL cohort according to broad pathology groups and tested whether late recurrence differed for the ATL cohort compared to patients who had resections outside the temporal lobe (n = 98). Results: Median post‐ATL follow‐up was 22 years (range =.1–38.6), 6% were lost to follow‐up, and 12% had died. Probabilities for remaining completely seizure‐free after surgery were 51% (95% confidence interval [CI] = 53–63) at 2 postoperative years, 36% (95% CI = 32–41) at 10 years, 32% (95% CI = 27–36) at 20 years, and 30% (95% CI = 25–34) at 25 years. Recurrences were reported up to 23 years postoperatively. Late seizures occurred in all major ATL pathology groups, with increased risk in the "normal" and "distant lesion" groups (p ≤.03). Comparison between the ATL cohort and patients who underwent extratemporal resection demonstrated similar patterns of late recurrence (p =.74). Significance: Some first recurrences were very late, reported decades after ATL. Late recurrences were not unique to any broad ATL pathology group and did not differ according to whether resections were ATL or extratemporal. Reports of these events by patients with residual pathology suggest that potentially epileptogenic abnormalities outside the area of resection may be implicated as one of several possible underlying mechanisms. [ABSTRACT FROM AUTHOR]

Published

2023

4. Newly diagnosed seizures assessed at two established first seizure clinics: Clinic characteristics, investigations, and findings over 11 years.

Author

McIntosh, Anne M., Tan, K. Meng, Hakami, Tahir M., Newton, Mark R., Carney, Patrick W., Yang, Mengjiazhi, Saya, Sibel, Marco, David J. T., Perucca, Piero, Kwan, Patrick, O'Brien, Terence J., and Berkovic, Samuel F.

Subjects

CLINICS, SEIZURES (Medicine), DIAGNOSIS of epilepsy, BRAIN injuries, PUBLIC hospitals, BRAIN tumors

Abstract

Objective: 'First seizure' clinics (FSCs) aim to achieve early expert assessment for individuals with possible new‐onset epilepsy. These clinics also have substantial potential for research into epilepsy evolution, outcomes, and costs. However, a paucity of FSCs details has implications for interpretation and utilization of this research. Methods: We reviewed investigation findings over 11 years (2000‐2010) from two established independent FSCs at Austin Health (AH) and Royal Melbourne Hospital (RMH), Australia. These adult clinics are in major public hospitals and operate with similar levels of expertise. Organizational differences include screening and dedicated administration at AH. Included were N = 1555 patients diagnosed with new‐onset unprovoked seizures/epilepsy (AH n = 901, RMH n = 654). Protocol‐driven interviews and investigations had been recorded prospectively and were extracted from medical records for study. Results: Median patient age was 37 (IQR 26‐52, range 18‐94) years (AH 34 vs RMH 42 years; P <.001). Eighty‐six percent of patients attended FSC within three weeks postindex seizure (median AH 12 vs RMH 25 days; P <.01). By their first appointment, 42% had experienced ≥2 seizures. An EEG was obtained within three weeks postindex seizure in 73% of patients, demonstrating epileptiform discharges in 25% (AH 33% vs RMH 15%). Seventy‐six percent of patients had an MRI within 6 weeks. Of those with imaging (n = 1500), 19% had potentially epileptogenic abnormalities (RMH 28% vs AH 12%; P <.01). At both sites, changes due to previous stroke/hemorrhage were the commonest lesions, followed by traumatic brain injury. ≥WHO level 1 brain tumors diagnosed at presentation comprised a very small proportion (<1%) at each clinic. At both sites, epilepsy type could be determined in 60% of patients; RMH had more focal and AH more generalized epilepsy diagnoses. Significance: Differences between the clinics' administrative and screening practices may contribute to differences in investigation findings. Insight into these differences will facilitate interpretation and utilization, and planning of future research. [ABSTRACT FROM AUTHOR]

Published

2021

5. The severe epilepsy syndromes of infancy: A population‐based study.

Author

Howell, Katherine B., Freeman, Jeremy L., Mackay, Mark T., Fahey, Michael C., Archer, John, Berkovic, Samuel F., Chan, Eunice, Dabscheck, Gabriel, Eggers, Stefanie, Hayman, Michael, Holberton, James, Hunt, Rodney W., Jacobs, Susan E., Kornberg, Andrew J., Leventer, Richard J., Mandelstam, Simone, McMahon, Jacinta M., Mefford, Heather C., Panetta, Julie, and Riseley, Jessica

Subjects

SEIZURES (Medicine), INFANTS, SYNDROMES, INFANTILE spasms, BRAIN imaging, EPILEPSY, NEUROCYSTICERCOSIS

Abstract

Objective: To study the epilepsy syndromes among the severe epilepsies of infancy and assess their incidence, etiologies, and outcomes. Methods: A population‐based cohort study was undertaken of severe epilepsies with onset before age 18 months in Victoria, Australia. Two epileptologists reviewed clinical features, seizure videos, and electroencephalograms to diagnose International League Against Epilepsy epilepsy syndromes. Incidence, etiologies, and outcomes at age 2 years were determined. Results: Seventy‐three of 114 (64%) infants fulfilled diagnostic criteria for epilepsy syndromes at presentation, and 16 (14%) had "variants" of epilepsy syndromes in which there was one missing or different feature, or where all classical features had not yet emerged. West syndrome (WS) and "WS‐like" epilepsy (infantile spasms without hypsarrhythmia or modified hypsarrhythmia) were the most common syndromes, with a combined incidence of 32.7/100 000 live births/year. The incidence of epilepsy of infancy with migrating focal seizures (EIMFS) was 4.5/100 000 and of early infantile epileptic encephalopathy (EIEE) was 3.6/100 000. Structural etiologies were common in "WS‐like" epilepsy (100%), unifocal epilepsy (83%), and WS (39%), whereas single gene disorders predominated in EIMFS, EIEE, and Dravet syndrome. Eighteen (16%) infants died before age 2 years. Development was delayed or borderline in 85 of 96 (89%) survivors, being severe–profound in 40 of 96 (42%). All infants with EIEE or EIMFS had severe–profound delay or were deceased, but only 19 of 64 (30%) infants with WS, "WS‐like," or "unifocal epilepsy" had severe–profound delay, and only two of 64 (3%) were deceased. Significance: Three quarters of severe epilepsies of infancy could be assigned an epilepsy syndrome or "variant syndrome" at presentation. In this era of genomic testing and advanced brain imaging, diagnosing epilepsy syndromes at presentation remains clinically useful for guiding etiologic investigation, initial treatment, and prognostication. [ABSTRACT FROM AUTHOR]

Published

2021

6. Inherited RORB pathogenic variants: Overlap of photosensitive genetic generalized and occipital lobe epilepsy.

Author

Sadleir, Lynette G., de Valles‐Ibáñez, Guillem, King, Chontelle, Coleman, Matthew, Mossman, Stuart, Paterson, Sarah, Nguyen, John, Berkovic, Samuel F., Mullen, Saul, Bahlo, Melanie, Hildebrand, Michael S., Mefford, Heather C., and Scheffer, Ingrid E.

Subjects

OCCIPITAL lobe, EPILEPSY, SLOW wave sleep, SEIZURES (Medicine), NUCLEOTIDE sequencing, AGE of onset, GAIN-of-function mutations

Abstract

Variants in RORB have been reported in eight individuals with epilepsy, with phenotypes ranging from eyelid myoclonia with absence epilepsy to developmental and epileptic encephalopathies. We identified novel RORB variants in 11 affected individuals from four families. One was from whole genome sequencing and three were from RORB screening of three epilepsy cohorts: developmental and epileptic encephalopathies (n = 1021), overlap of generalized and occipital epilepsy (n = 84), and photosensitivity (n = 123). Following interviews and review of medical records, individuals' seizure and epilepsy syndromes were classified. Three novel missense variants and one exon 3 deletion were predicted to be pathogenic by in silico tools, not found in population databases, and located in key evolutionary conserved domains. Median age at seizure onset was 3.5 years (0.5‐10 years). Generalized, predominantly absence and myoclonic, and occipital seizures were seen in all families, often within the same individual (6/11). All individuals with epilepsy were photosensitive, and seven of 11 had cognitive abnormalities. Electroencephalograms showed generalized spike and wave and/or polyspike and wave. Here we show a striking RORB phenotype of overlap of photosensitive generalized and occipital epilepsy in both individuals and families. This is the first report of a gene associated with this overlap of epilepsy syndromes. [ABSTRACT FROM AUTHOR]

Published

2020

7. SCN1A Variants in vaccine-related febrile seizures: A prospective study.

Author

Damiano, John A., Deng, Lucy, Li, Wenhui, Burgess, Rosemary, Schneider, Amy L., Crawford, Nigel W., Buttery, Jim, Gold, Michael, Richmond, Peter, Macartney, Kristine K., Hildebrand, Michael S., Scheffer, Ingrid E., Wood, Nicholas, and Berkovic, Samuel F.

Subjects

FEBRILE seizures, SODIUM channels, LONGITUDINAL method, CHILDREN'S hospitals, SEIZURES (Medicine), LENNOX-Gastaut syndrome, BRUGADA syndrome, RESEARCH, VACCINES, GENETIC mutation, RESEARCH methodology, CASE-control method, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, MEMBRANE transport proteins, DISEASE susceptibility

Abstract

Objective: Febrile seizures may follow vaccination. Common variants in the sodium channel gene, SCN1A, are associated with febrile seizures, and rare pathogenic variants in SCN1A cause the severe developmental and epileptic encephalopathy Dravet syndrome. Following vaccination, febrile seizures may raise the specter of poor outcome and inappropriately implicate vaccination as the cause. We aimed to determine the prevalence of SCN1A variants in children having their first febrile seizure either proximal to vaccination or unrelated to vaccination compared to controls.Methods: We performed SCN1A sequencing, blind to clinical category, in a prospective cohort of children presenting with their first febrile seizure as vaccine proximate (n = 69) or as non-vaccine proximate (n = 75), and children with no history of seizures (n = 90) recruited in Australian pediatric hospitals.Results: We detected 2 pathogenic variants in vaccine-proximate cases (p.R568X and p.W932R), both of whom developed Dravet syndrome, and 1 in a non-vaccine-proximate case (p.V947L) who had febrile seizures plus from 9 months. All had generalized tonic-clonic seizures lasting >15 minutes. We also found enrichment of a reported risk allele, rs6432860-T, in children with febrile seizures compared to controls (odds ratio = 1.91, 95% confidence interval = 1.31-2.81).Interpretation: Pathogenic SCN1A variants may be identified in infants with vaccine-proximate febrile seizures. As early diagnosis of Dravet syndrome is essential for optimal management and outcome, SCN1A sequencing in infants with prolonged febrile seizures, proximate to vaccination, should become routine. ANN NEUROL 2020;87:281-288. [ABSTRACT FROM AUTHOR]

Published

2020

8. Quantitative analysis of phenotypic elements augments traditional electroclinical classification of common familial epilepsies.

Author

Abou‐Khalil, Bassel, Afawi, Zaid, Allen, Andrew S., Bautista, Jocelyn F., Bellows, Susannah T., Berkovic, Samuel F., Bluvstein, Judith, Burgess, Rosemary, Cascino, Gregory, Cossette, Patrick, Cristofaro, Sabrina, Crompton, Douglas E., Delanty, Norman, Devinsky, Orrin, Dlugos, Dennis, Ellis, Colin A., Epstein, Michael P., Fountain, Nathan B., Freyer, Catharine, and Geller, Eric B.

Subjects

PARTIAL epilepsy, FEBRILE seizures, QUANTITATIVE research, SEIZURES (Medicine), CLASSIFICATION

Abstract

Objective: Classification of epilepsy into types and subtypes is important for both clinical care and research into underlying disease mechanisms. A quantitative, data‐driven approach may augment traditional electroclinical classification and shed new light on existing classification frameworks. Methods: We used latent class analysis, a statistical method that assigns subjects into groups called latent classes based on phenotypic elements, to classify individuals with common familial epilepsies from the Epi4K Multiplex Families study. Phenotypic elements included seizure types, seizure symptoms, and other elements of the medical history. We compared class assignments to traditional electroclinical classifications and assessed familial aggregation of latent classes. Results: A total of 1120 subjects with epilepsy were assigned to five latent classes. Classes 1 and 2 contained subjects with generalized epilepsy, largely reflecting the distinction between absence epilepsies and younger onset (class 1) versus myoclonic epilepsies and older onset (class 2). Classes 3 and 4 contained subjects with focal epilepsies, and in contrast to classes 1 and 2, these did not adhere as closely to clinically defined focal epilepsy subtypes. Class 5 contained nearly all subjects with febrile seizures plus or unknown epilepsy type, as well as a few subjects with generalized epilepsy and a few with focal epilepsy. Family concordance of latent classes was similar to or greater than concordance of clinically defined epilepsy types. Significance: Quantitative classification of epilepsy has the potential to augment traditional electroclinical classification by (1) combining some syndromes into a single class, (2) splitting some syndromes into different classes, (3) helping to classify subjects who could not be classified clinically, and (4) defining the boundaries of clinically defined classifications. This approach can guide future research, including molecular genetic studies, by identifying homogeneous sets of individuals that may share underlying disease mechanisms. [ABSTRACT FROM AUTHOR]

Published

2019

9. Metabolic patterns and seizure outcomes following anterior temporal lobectomy.

Author

Cahill, Varduhi, Sinclair, Benjamin, Malpas, Charles B., McIntosh, Anne M., Chen, Zhibin, Vivash, Lucy E., O'Shea, Marie F., Wilson, Sarah J., Desmond, Patricia M., Berlangieri, Salvatore U., Hicks, Rodney J., Rowe, Christopher C., Morokoff, Andrew P., King, James A., Fabinyi, Gavin C., Kaye, Andrew H., Kwan, Patrick, Berkovic, Samuel F., and O'Brien, Terence J.

Subjects

TEMPORAL lobectomy, SEIZURES (Medicine), POSITRON emission tomography, FOLLOW-up studies (Medicine), METABOLISM, MAGNETIC resonance imaging, ODDS ratio, CONFIDENCE intervals

Abstract

Objective: We investigated the relationship between the interictal metabolic patterns, the extent of resection of 18 F-fluorodeoxyglucose positron emission tomography (18 FDG-PET) hypometabolism, and seizure outcomes in patients with unilateral drug-resistant mesial temporal lobe epilepsy (MTLE) following anterior temporal lobe (TL) resection.Methods: Eighty-two patients with hippocampal sclerosis or normal magnetic resonance imaging (MRI) findings, concordant 18 FDG-PET hypometabolism, and at least 2 years of postoperative follow-up were included in this 2-center study. The hypometabolic regions in each patient were identified with reference to 20 healthy controls (p < 0.005). The resected TL volume and the volume of resected TL PET hypometabolism (TLH) were calculated from the pre- and postoperative MRI scans coregistered with interictal 18 FDG-PET.Results: Striking differences in metabolic patterns were observed depending on the lateralization of the epileptogenic TL. The extent of the ipsilateral TLH was significantly greater in left MTLE patients (p < 0.001), whereas right MTLE patients had significantly higher rates of contralateral (CTL) TLH (p = 0.016). In right MTLE patients, CTL hypometabolism was the strongest predictor of an unfavorable seizure outcome, associated with a 5-fold increase in the likelihood of seizure recurrence (odds ratio [OR] = 4.90, 95% confidence interval [CI] = 1.07-22.39, p = 0.04). In left MTLE patients, greater extent of resection of ipsilateral TLH was associated with lower rates of seizure recurrence (p = 0.004) in univariate analysis; however, its predictive value did not reach statistical significance (OR = 0.96, 95% CI = 0.90-1.02, p = 0.19).Interpretation: The difference in metabolic patterns depending on the lateralization of MTLE may represent distinct epileptic networks in patients with right versus left MTLE, and can guide preoperative counseling and surgical planning. Ann Neurol 2019; 1-10 ANN NEUROL 2019;85:241-250. [ABSTRACT FROM AUTHOR]

Published

2019

10. A case series of lacosamide as adjunctive therapy in refractory sleep‐related hypermotor epilepsy (previously nocturnal frontal lobe epilepsy).

Author

Samarasekera, Shanika R., Berkovic, Samuel F., and Scheffer, Ingrid E.

Subjects

*VIMPAT, *EPILEPSY, *SPASMS, *ANTICONVULSANTS, *SEIZURES (Medicine)

Abstract

Summary: The aim of this study was to evaluate the efficacy and tolerability of open‐label lacosamide in patients with refractory sleep‐related hypermotor epilepsy. The study was a case review of eight patients with refractory sleep‐related hypermotor epilepsy treated with lacosamide. Seizure diaries compared the mean baseline seizure frequency with the most recent 3 months of follow‐up. Five (62.5%) patients were responders, defined as ≥50% reduction in seizure frequency, over a mean duration of exposure of 21.5 months. The mean maintenance dose of lacosamide was 400 mg/day. No‐one reported worsening of seizures. Lacosamide was well tolerated with initial fatigue being the main side‐effect. Lacosamide is a potentially efficacious adjunctive therapy in patients with refractory sleep‐related hypermotor epilepsy. A double‐blind placebo‐controlled study would determine its efficacy. [ABSTRACT FROM AUTHOR]

Published

2018

11. Dynamic action potential clamp predicts functional separation in mild familial and severe de novo forms of SCN2A epilepsy.

Author

Berecki, Géza, Howell, Katherine B., Deerasooriya, Yadeesha H., Cilio, Maria Roberta, Oliva, Megan K., Kaplan, David, Scheffer, Ingrid E., Berkovic, Samuel F., and Petrou, Steven

Subjects

EPILEPSY, SEIZURES (Medicine), ION channels, INFANTILE spasms, REDUCTION potential

Abstract

De novo variants in SCN2A developmental and epileptic encephalopathy (DEE) show distinctive genotype–phenotype correlations. The two most recurrent SCN2A variants in DEE, R1882Q and R853Q, are associated with different ages and seizure types at onset. R1882Q presents on day 1 of life with focal seizures, while infantile spasms is the dominant seizure type seen in R853Q cases, presenting at a median age of 8 months. Voltage clamp, which characterizes the functional properties of ion channels, predicted gain-of-function for R1882Q and loss-of-function for R853Q. Dynamic action potential clamp, that we implement here as a method for modeling neurophysiological consequences of a given epilepsy variant, predicted that the R1882Q variant would cause a dramatic increase in firing, whereas the R853Q variant would cause a marked reduction in action potential firing. Dynamic clamp was also able to functionally separate the L1563V variant, seen in benign familial neonatal–infantile seizures from R1882Q, seen in DEE, suggesting a diagnostic potential for this type of analysis. Overall, the study shows a strong correlation between clinical phenotype, SCN2A genotype, and functional modeling. Dynamic clamp is well positioned to impact our understanding of pathomechanisms and for development of disease mechanism-targeted therapies in genetic epilepsy. [ABSTRACT FROM AUTHOR]

Published

2018

12. Familial mesial temporal lobe epilepsy and the borderland of déjà vu.

Author

Perucca, Piero, Crompton, Douglas E., Bellows, Susannah T., McIntosh, Anne M., Kalincik, Tomas, Newton, Mark R., Vajda, Frank J. E., Scheffer, Ingrid E., Kwan, Patrick, O'Brien, Terence J., Tan, K. Meng, and Berkovic, Samuel F.

Subjects

EPILEPSY, TEMPORAL lobe, SEIZURES (Medicine), MAGNETIC resonance imaging, BRAIN diseases

Abstract

Objective: The cause of mesial temporal lobe epilepsy (MTLE) is often unknown. We ascertained to what extent newly diagnosed nonlesional MTLE actually represents familial MTLE (FMTLE).Methods: We identified all consecutive patients presenting to the Austin Health First Seizure Clinic with MTLE and normal magnetic resonance imaging (MRI) or MRI evidence of hippocampal sclerosis over a 10-year period. Patients' first-degree relatives and pairwise age- and sex-matched controls underwent a comprehensive epilepsy interview. Each interview transcript was reviewed independently by 2 epileptologists, blinded to relative or control status. Reviewers classified each subject as follows: epilepsy, specifying if MTLE; manifestations suspicious for epilepsy; or unaffected. Physiological déjà vu was noted.Results: Forty-four patients were included. At the Clinic, MTLE had been recognized to be familial in 2 patients only. Among 242 subjects interviewed, MTLE was diagnosed in 9 of 121 relatives versus 0 of 121 controls (p = 0.008). All affected relatives had seizures with intense déjà vu and accompanying features; 6 relatives had not been previously diagnosed. Déjà vu experiences that were suspicious, but not diagnostic, of MTLE occurred in 6 additional relatives versus none of the controls (p = 0.04). Physiological déjà vu was common, and did not differ significantly between relatives and controls. After completing the relatives' interviews, FMTLE was diagnosed in 8 of 44 patients (18.2%).Interpretation: FMTLE accounts for almost one-fifth of newly diagnosed nonlesional MTLE, and it is largely unrecognized without direct questioning of relatives. Relatives of patients with MTLE may experience déjà vu phenomena that clinically lie in the "borderland" between epileptic seizures and physiological déjà vu. Ann Neurol 2017;82:166-176. [ABSTRACT FROM AUTHOR]

Published

2017

13. Frequency of CNKSR2 mutation in the X-linked epilepsy-aphasia spectrum.

Author

Damiano, John A., Burgess, Rosemary, Kivity, Sara, Lerman‐Sagie, Tally, Afawi, Zaid, Scheffer, Ingrid E., Berkovic, Samuel F., and Hildebrand, Michael S.

Subjects

SEIZURES (Medicine), FEBRILE seizures, GENETIC counseling, X-linked genetic disorders, GENETIC disorders, HEPATIC encephalopathy

Abstract

Synaptic proteins are critical to neuronal function in the brain, and their deficiency can lead to seizures and cognitive impairments. CNKSR2 (connector enhancer of KSR2) is a synaptic protein involved in Ras signaling-mediated neuronal proliferation, migration and differentiation. Mutations in the X-linked gene CNKSR2 have been described in patients with seizures and neurodevelopmental deficits, especially those affecting language. In this study, we sequenced 112 patients with phenotypes within the epilepsy-aphasia spectrum ( EAS) to determine the frequency of CNKSR2 mutation within this complex set of disorders. We detected a novel nonsense mutation (c.2314 C>T; p.Arg712*) in one Ashkenazi Jewish family, the male proband of which had a severe epileptic encephalopathy with continuous spike-waves in sleep ( ECSWS). His affected brother also had ECSWS with better outcome, whereas the sister had childhood epilepsy with centrotemporal spikes. This mutation segregated in the three affected siblings in an X-linked manner, inherited from their mother who had febrile seizures. Although the frequency of point mutation is low, CNKSR2 sequencing should be considered in families with suspected X-linked EAS because of the specific genetic counseling implications. [ABSTRACT FROM AUTHOR]

Published

2017

14. A retrospective population-based study on seizures related to childhood vaccination.

Author

von Spiczak, Sarah, Helbig, Ingo, Drechsel-Baeuerle, Ursula, Muhle, Hiltrud, van Baalen, Andreas, van Kempen, Marjan J., Lindhout, Dick, Scheffer, Ingrid E., Berkovic, Samuel F., Stephani, Ulrich, and Keller-Stanislawski, Brigitte

Subjects

EPILEPSY, SEIZURES (Medicine), VACCINATION, ETIOLOGY of diseases, IMMUNIZATION, VACCINES

Abstract

Summary Purpose: Cases of severe childhood epilepsies in temporal association with vaccination have great impact on the acceptance of vaccination programs by parents and health care providers. However, little is known about the type and frequency of seizures and epilepsy syndromes following vaccination. This study aims to describe the clinical features of children presenting with seizures after vaccination using a register-based cohort. Methods: We surveyed the national German database of adverse events following immunization (AEFI) for reported seizures and epilepsies in children aged 0-6 years. All cases reported in 2006-2008 were analyzed retrospectively; available clinical information was reevaluated and classified by seizure type and epilepsy syndrome. Key Findings: In total, 328 cases reported between 2006 and 2008 were included. Data supportive of seizures or epilepsy were present in 247 (75.3%) of 328 patients with a mean interval between the vaccination and the epileptic event of 24 h and 7.5 days for inactivated and attenuated vaccines, respectively. Fifty-one (15.5%) of 328 patients presented with syncope, hypotonic-hyporesponsive episodes, or other nonepileptic events. Information was insufficient for classification into epileptic versus nonepileptic events in 30 (11.3%) of 328 patients. For cases with confirmed seizures, febrile seizures were present in 121 (49%) of 247 cases, and 38 (15.4%) of 247 patients had single afebrile seizures. Status epilepticus was described in 21 (8.5%) of 247 patients. Thirty-one (12.6%) of 247 patients presented with various pediatric epilepsy syndromes. Severe childhood epilepsies (Dravet syndrome, West syndrome, Lennox-Gastaut syndrome, or Doose syndrome) were diagnosed in 29 (11.7%) of 247 patients, with the vaccination-associated event being the first documented seizure in 15 (51.7%) of 29 patients. Significance: Vaccination-associated seizures present in the setting of various epilepsy syndromes, including severe childhood epilepsies in >10% of cases. Early diagnosis of the corresponding epilepsy syndromes and confirmation of an underlying etiology is important for treatment decisions, genetic counseling, and public health evaluation of vaccine safety. [ABSTRACT FROM AUTHOR]

Published

2011

15. Mild adolescent/adult onset epilepsy and paroxysmal exercise-induced dyskinesia due to GLUT1 deficiency.

Author

Afawi, Zaid, Suls, Arvid, Ekstein, Dana, Kivity, Sara, Neufeld, Miriam Y, Oliver, Karen, De Jonghe, Peter, Korczyn, Amos D., and Berkovic, Samuel F.

Subjects

EPILEPSY, PAROXYSMAL hemoglobinuria, MOVEMENT disorders, SEIZURES (Medicine), GENETIC mutation

Abstract

Paroxysmal exercise-induced dyskinesia (PED) and epilepsy without intellectual disability have recently been recognized as manifestations of deficiency of the glucose transporter GLUT1, due to mutations in the gene SLC2A1. We describe a family with six definitely affected members in two generations. Two had PED, three had epilepsy, and one had both. A missense mutation in SLC2A1 (c.950A>C; p.N317T) was detected in five living affected members, but absent in three nonaffected first-degree members and in one subject believed to be a phenocopy. The clinical picture of mild epilepsy with onset in adolescence or early adulthood plus PED should raise a suspicion of GLUT1 deficiency. [ABSTRACT FROM AUTHOR]

Published

2010

16. Can changes in cortical excitability distinguish progressive from juvenile myoclonic epilepsy?

Author

Badawy, Radwa A.B., Macdonell, Richard A.L., Jackson, Graeme D, and Berkovic, Samuel F.

Subjects

MYOCLONUS, TRANSCRANIAL magnetic stimulation, GABA, SOMATOSENSORY evoked potentials, SEIZURES (Medicine), ANTICONVULSANTS, MOTOR cortex, PATIENTS

Abstract

We used transcranial magnetic stimulation (TMS) to investigate whether there were any characteristic cortical excitability changes in progressive myoclonic epilepsy (PME) compared to juvenile myoclonic epilepsy (JME). Six patients with PME were studied. Motor threshold (MT) at rest and recovery curve analysis using paired-pulse stimulation at a number of interstimulus intervals (ISIs) was determined. Results were compared to those of 9 patients with chronic refractory JME and 10 with chronic well-controlled JME. PME showed a marked increase in cortical excitability at all the long ISIs (p < 0.01), compared to refractory JME (effect sizes ranging from 1.4 to 1.9) and well-controlled JME (effect sizes ranging from 2.0 to 2.4). Significant differences at the short ISIs 2-5 ms were seen only on comparison with the well-controlled group (p < 0.05, effect size 0.6, 0.7). There were no significant differences in MTs of PME compared to either JME groups. Our findings demonstrate specific differences in cortical excitability using TMS between PME and those with JME, particularly at long latencies in the paired-pulse paradigm, implicating a role for γ-aminobutyric acid (GABA)B-mediated networks. [ABSTRACT FROM AUTHOR]

Published

2010

17. Clinical features of seizures associated with parahippocampal/inferior temporal lesions compared to those with hippocampal sclerosis.

Author

Mirandola, Laura, Badawy, Radwa A., Saunders, Ann M., McIntosh, Anne, Berkovic, Samuel F., and Jackson, Graeme D.

Subjects

FRONTAL lobe diseases, TEMPORAL lobe epilepsy, TEMPORAL lobectomy, BRAIN diseases, SPASMS, SEIZURES (Medicine)

Abstract

Temporal lobe epilepsy (TLE) is not a unitary electroclinical imaging syndrome. We asked if seizures arising from the parahippocampal-inferior temporal (PIT) region differ from those associated with hippocampal sclerosis (HS). The electroclinical features of 22 patients with HS and 14 patients with lesions in the PIT region who underwent epilepsy surgery and were seizure free for at least 2 years postoperatively were analyzed retrospectively. Patients with PIT lesions had a higher frequency of hypermotor and bilateral features and a lower frequency of behavioral arrest at the onset of seizure compared to cases with HS, suggesting that TLE originating in the PIT area can mimic frontal lobe epilepsy or contralateral mesial TLE. [ABSTRACT FROM AUTHOR]

Published

2010

18. Familial Lennox-Gastaut syndrome in male siblings with a novel DCX mutation and anterior pachygyria.

Author

Lawrence, Kate M., Mei, Davide, Newton, Mark R., Leventer, Richard J., Guerrini, Renzo, and Berkovic, Samuel F.

Subjects

BRAIN diseases, EPILEPSY, LENNOX-Gastaut syndrome, CHILDHOOD epilepsy, ELECTROENCEPHALOGRAPHY, DEVELOPMENTAL disabilities, SEIZURES (Medicine)

Abstract

Lennox-Gastaut syndrome (LGS) has numerous causes, but only rarely has familial recurrence been observed. We studied a family in which three male members had severe epilepsy and intellectual disability. The proband had seizure onset at 7 years of age with atonic, myoclonic, atypical absence, and tonic seizures with slow spike-wave on electroencephalography (EEG). One living sibling had a similar clinical pattern. One deceased sibling was known to have had seizures with intellectual disability. Neuroimaging revealed anterior predominant pachygyria. DNA sequencing of the gene doublecortin ( DCX) on the X chromosome revealed a novel missense mutation in the two living affected male siblings. The occurrence of three affected male family members with proven or suspected LGS in this family was puzzling and only solved by a combination of magnetic resonance (MR) and molecular genetics evaluations. This finding provided essential information for genetic counseling. [ABSTRACT FROM AUTHOR]

Published

2010

19. The Epilepsy Genetic Association Database (epiGAD): Analysis of 165 genetic association studies, 1996–2008.

Author

Tan, Nigel C. K. and Berkovic, Samuel F.

Subjects

*EPILEPSY, *SPASMS, *PHARMACOGENOMICS, *SEIZURES (Medicine), *DEVELOPMENTAL disabilities, *SOCIETIES

Abstract

We have created the Epilepsy Genetic Association Database (epiGAD, , an online database of epilepsy genetic association studies. A systematic search using several search engines identified 165 studies. Herein we analyze the types of studies available, the sample sizes used, and the strength of the findings. Common questions examined were susceptibility to idiopathic generalized epilepsy, focal epilepsy, or febrile seizures, and pharmacogenomic approaches to drug-resistant epilepsy. Sample sizes were generally small; 80% of studies had 200 or fewer cases, although more recent studies published from 2005–2008 incorporated slightly larger sample sizes. No association was judged as “strong” using current criteria for assessing genetic associations—this is probably due to inadequate sample sizes. Sample sizes need to increase, either by research collaboration or via systematic reviews and meta-analyses. We believe epiGAD will facilitate future meta-analyses. [ABSTRACT FROM AUTHOR]

Published

2010

20. Parahippocampal epilepsy with subtle dysplasia: A cause of “imaging negative” partial epilepsy.

Author

Pillay, Neelan, Fabinyi, Gavin C. A., Myles, Terry S., Fitt, Gregory J., Berkovic, Samuel F., and Jackson, Graeme D.

Subjects

EPILEPSY, SEIZURES (Medicine), SPASMS, DYSPLASIA, MEDICAL imaging systems

Abstract

Lesion-negative refractory partial epilepsy is a major challenge in the assessment of patients for potential surgery. Finding a potential epileptogenic lesion simplifies assessment and is associated with good outcome. Here we describe imaging features of subtle parahippocampal dysplasia in five cases that were initially assessed as having imaging-negative frontal or temporal lobe epilepsy. We analyzed the clinical and imaging features of five patients with seizures from the parahippocampal region. Five patients had subtle but distinctive magnetic resonance imaging (MRI) abnormalities in the parahippocampal gyrus. This was a unilateral signal abnormality in the parahippocampal white matter extending into gray matter on heavily T1- and T2-weighted images with relative preservation of the gray–white matter boundary on T1-weighted volume sequences. Only one of these patients had typical electroclinical unilateral temporal lobe epilepsy (TLE); one mimicked frontal lobe epilepsy, two showed bitemporal seizures, and one had unlocalized partial seizures. All have had surgery; four are seizure-free (one has occasional auras only, follow-up 6 months to 10 years), and one has a >50% seizure reduction. Histopathologic evaluation suggested dysplastic features in the surgical specimens in all. In patients with lesion-negative partial epilepsy with frontal or temporal semiology, or in cases with apparent bitemporal seizures, subtle parahippocampal abnormalities should be carefully excluded. Recognizing the MRI findings of an abnormal parahippocampal gyrus can lead to successful surgery without invasive monitoring, despite apparently incongruent electroclinical features. [ABSTRACT FROM AUTHOR]

Published

2009

21. Multidrug-resistant genotype ( ABCB1) and seizure recurrence in newly treated epilepsy: Data from international pharmacogenetic cohorts.

Author

Szoeke, Cassandra, Sills, Graeme J., Kwan, Patrick, Petrovski, Slave, Newton, Mark, Hitiris, Nikolas, Baum, Larry, Berkovic, Samuel F., Brodie, Martin J., Sheffield, Leslie J., and O'Brien, Terence J.

Subjects

TREATMENT of epilepsy, SEIZURES (Medicine), GENETIC polymorphisms, PHARMACOGENOMICS, BIOCHEMICAL genetics, GENOTYPE-environment interaction, P-glycoprotein

Abstract

The association between a specific polymorphism ( 3435C> T) in the ABCB1 gene, coding for the membrane drug transporter P-glycoprotein (PgP), and pharmacoresistance to seizure control is controversial. Studies have been limited by multiple drug use, chronic cohorts with varying definitions, and retrospective clinical data. Herein we examine the relationship of this polymorphism with seizure recurrence in three independent international cohorts of patients newly treated for epilepsy. Data were collected on demographics, medication details, and seizure control after 12 months of treatment. The distribution of ABCB1 3435C>T genotypes was compared between patients with and without recurrent unprovoked seizures. Five hundred forty-two newly treated patients were enrolled (212 from Australia, 285 from Scotland, and 45 from Hong Kong). A total of 38.4% had recurrent unprovoked seizures after starting antiepileptic drug (AED) treatment. Genotype frequencies and ethnicity did not differ between the Scottish and Australian cohorts, but both were significantly different in the Hong Kong cohort. There was no significant relationship between the ABCB1 3435C> T genotype and the rate of recurrence of unprovoked seizures in the three cohorts individually or combined; however the epilepsy syndrome and a greater number of seizures pretreatment was associated with an increased risk of seizure recurrence. The ABCB1 3435C> T genotype does not have a major role in determining the efficacy of seizure control with initial AED therapy. The study highlights issues that arise in combining pharmacogenetic datasets from different ethnic regions and health systems, an approach that is essential to advance this field. [ABSTRACT FROM AUTHOR]

Published

2009

22. Cognitive complaints after a first seizure in adulthood: Influence of psychological adjustment.

Author

Velissaris, Sarah L., Wilson, Sarah J., Newton, Mark R., Berkovic, Samuel F., and Saling, Michael M.

Subjects

SEIZURES (Medicine), BRAIN diseases, ANXIETY, MOOD (Psychology), MENTAL depression

Abstract

To examine the nature and determinants (biologic and psychological) of cognitive complaints in first-seizure patients. We analyzed this in the context of our previous findings that a sense of loss of control after a newly diagnosed seizure (limited or pervasive) predicts subsequent psychological adjustment trajectories. Eighty-five consecutive First Seizure Clinic patients were assessed at 1 and 3 months. Cognitive complaints were evaluated qualitatively, with a semistructured interview, and quantitatively, with the A-B Neuropsychological Assessment Schedule (ABNAS). Objective attentional processing was assessed with reaction time tasks and the Wechsler Adult Intelligence Scale-3rd edition (WAIS-III) Processing Speed Index. Mood was assessed with the Hospital Anxiety and Depression Scale (HADS). Psychological adjustment trajectories were represented by previous classification of patients into limited and pervasive groups, as derived from semistructured interview. Cognitive complaints at 1 and 3 months were strongly associated with mood, and unrelated to objective attentional processing. Psychological adjustment trajectories influenced the longitudinal course of cognitive complaints, and these effects were partially mediated by mood differences between the limited and pervasive groups. The course of cognitive complaints was also altered by commencing antiepileptic drugs. Patients experiencing seizure recurrence reported greater cognitive complaints, even before their seizure recurred. Mediation analyses showed this effect was likely attributable to increased mood disturbance in the seizure recurrence group, and was unrelated to objective attentional processing. Understanding cognitive complaints in first-seizure patients requires a longitudinal perspective that takes into account the patients’ changing psychological and medical contexts. Patients presenting with extensive cognitive complaints may warrant assessment for mood and adjustment issues. [ABSTRACT FROM AUTHOR]

Published

2009

23. Epileptic encephalopathies of infancy: welcome advances.

Author

Berkovic, Samuel F

Subjects

*INFANTS, *LENNOX-Gastaut syndrome, *SPINAL muscular atrophy, *GENETIC disorders, *SEIZURES (Medicine), *EPILEPSY, *SEROTONIN uptake inhibitors, *SPASMS, *INFANTILE spasms, *BLIND experiment

Abstract

Until recently, infants with severe epilepsy and intellectual disability often received a diagnosis of not much more than that - the cause was usually unknown, treatment was supportive, and families often felt disempowered due to lack of information about the condition. A number of therapies are currently under investigation for Dravet syndrome and other epileptic encephalopathies. 5 AS Schoonjans, L Lagae, B Ceulemans, Low-dose fenfluramine in the treatment of neurologic disorders: experience in Dravet syndrome. [Extracted from the article]

Published

2019

24. Is Photosensitive Epilepsy Less Common in Males Due to Variation in X Chromosome Photopigment Genes?

Author

Taylor, Isabella, Hodgson, Bree, Scheffer, Ingrid E., Mulley, John, Berkovic, Samuel F., and Dibbens, Leanne

Subjects

EPILEPSY, SEIZURES (Medicine), PHOTOSENSITIVITY disorders, X chromosome, BIOLOGICAL pigments, GENETIC polymorphisms

Abstract

Photosensitive epilepsy is less frequent among males than females. Red is the most epileptogenic color. The X-linked red pigment gene contains the polymorphism Ser180Ala; the Ser180 allele increases red sensitivity. We hypothesized that the paucity of males with photosensitive epilepsy is explained by the distribution of this sex-linked allele, and predicted photosensitive males would have a low frequency of this allele. We genotyped 35 males with photosensitive epilepsy and 84 male controls. Allele frequencies did not differ between these groups. The hypothesis was not supported, so alternate reasons for the sex bias in photosensitive epilepsy must be sought. [ABSTRACT FROM AUTHOR]

Published

2007

25. Novel Missense CACNA1G Mutations Associated with Infantile-Onset Developmental and Epileptic Encephalopathy.

Author

Berecki, Géza, Helbig, Katherine L., Ware, Tyson L., Grinton, Bronwyn, Skraban, Cara M., Marsh, Eric D., Berkovic, Samuel F., and Petrou, Steven

Subjects

MISSENSE mutation, COGNITION disorders, CEREBELLAR ataxia, DEVELOPMENTAL delay, CALCIUM channels, SEIZURES (Medicine), CHILDREN with epilepsy, GAIN-of-function mutations

Abstract

The CACNA1G gene encodes the low-voltage-activated Cav3.1 channel, which is expressed in various areas of the CNS, including the cerebellum. We studied two missense CACNA1G variants, p.L208P and p.L909F, and evaluated the relationships between the severity of Cav3.1 dysfunction and the clinical phenotype. The presentation was of a developmental and epileptic encephalopathy without evident cerebellar atrophy. Both patients exhibited axial hypotonia, developmental delay, and severe to profound cognitive impairment. The patient with the L909F mutation had initially refractory seizures and cerebellar ataxia, whereas the L208P patient had seizures only transiently but was overall more severely affected. In transfected mammalian cells, we determined the biophysical characteristics of L208P and L909F variants, relative to the wild-type channel and a previously reported gain-of-function Cav3.1 variant. The L208P mutation shifted the activation and inactivation curves to the hyperpolarized direction, slowed the kinetics of inactivation and deactivation, and reduced the availability of Ca2+ current during repetitive stimuli. The L909F mutation impacted channel function less severely, resulting in a hyperpolarizing shift of the activation curve and slower deactivation. These data suggest that L909F results in gain-of-function, whereas L208P exhibits mixed gain-of-function and loss-of-function effects due to opposing changes in the biophysical properties. Our study expands the clinical spectrum associated with CACNA1G mutations, corroborating further the causal association with distinct complex phenotypes. [ABSTRACT FROM AUTHOR]

Published

2020

26. The borderland of epilepsy: A clinical and molecular view, 100 years on.

Author

Berkovic, Samuel F. and Crompton, Douglas E.

Subjects

*EPILEPSY, *SYNCOPE, *SEIZURES (Medicine), *MOLECULAR genetics, *MIGRAINE

Abstract

The article presents clinical and molecular advancements made in epilepsy. It revisits the syncope, migraine, parasomnias, and some rarer disorders including the paroxysmal dyskinesias and organic causes of nonepileptic convulsions. It mentions that a major advancement made possible by molecular genetics is that epilepsies are a family of channelopathies. It also discusses about the paradox related to migraine and epilepsy.

Published

2010

27. Treatment of new-onset epilepsy: seizures beget discussion.

Author

McIntosh, Anne M. and Berkovic, Samuel F.

Subjects

*SEIZURES (Medicine), *EPILEPSY, *BRAIN diseases, *RESEARCH, *MEDICAL research

Abstract

Looks at developments in the treatment of epileptic seizures. Question of when to start patients on antiepileptic medication; Authors' view that the decision requires doctors to consider a complex arrangement of medical, psychological and sociological factors; Review of research into the long-term control of seizures performed by Anthony Marson and colleagues; Conclusion by Marson's research that delaying medication did not increase the risk of chronic epilepsy.

Published

2005

28. Prediction of seizure likelihood with a long-term, implanted seizure advisory system in patients with drug-resistant epilepsy: a first-in-man study.

Author

Cook, Mark J, O'Brien, Terence J, Berkovic, Samuel F, Murphy, Michael, Morokoff, Andrew, Fabinyi, Gavin, D'Souza, Wendyl, Yerra, Raju, Archer, John, Litewka, Lucas, Hosking, Sean, Lightfoot, Paul, Ruedebusch, Vanessa, Sheffield, W Douglas, Snyder, David, Leyde, Kent, and Himes, David

Subjects

*SEIZURES diagnosis, *ELECTROENCEPHALOGRAPHY, *PATIENT monitoring, *ALGORITHMS, *CLINICAL trials, *SEIZURES (Medicine), *ELECTRODES, *ARTIFICIAL implants, *LONGITUDINAL method, *HEALTH outcome assessment, *RESEARCH funding, *SAFETY, *SPASMS, *TIME, *PILOT projects, *EQUIPMENT & supplies, *TREATMENT effectiveness, *DIAGNOSIS

Abstract

Summary: Background: Seizure prediction would be clinically useful in patients with epilepsy and could improve safety, increase independence, and allow acute treatment. We did a multicentre clinical feasibility study to assess the safety and efficacy of a long-term implanted seizure advisory system designed to predict seizure likelihood and quantify seizures in adults with drug-resistant focal seizures. Methods: We enrolled patients at three centres in Melbourne, Australia, between March 24, 2010, and June 21, 2011. Eligible patients had between two and 12 disabling partial-onset seizures per month, a lateralised epileptogenic zone, and no history of psychogenic seizures. After devices were surgically implanted, patients entered a data collection phase, during which an algorithm for identification of periods of high, moderate, and low seizure likelihood was established. If the algorithm met performance criteria (ie, sensitivity of high-likelihood warnings greater than 65% and performance better than expected through chance prediction of randomly occurring events), patients then entered an advisory phase and received information about seizure likelihood. The primary endpoint was the number of device-related adverse events at 4 months after implantation. Our secondary endpoints were algorithm performance at the end of the data collection phase, clinical effectiveness (measures of anxiety, depression, seizure severity, and quality of life) 4 months after iniation of the advisory phase, and longer-term adverse events. This trial is registered with ClinicalTrials.gov, number NCT01043406. Findings: We implanted 15 patients with the advisory system. 11 device-related adverse events were noted within four months of implantation, two of which were serious (device migration, seroma); an additional two serious adverse events occurred during the first year after implantation (device-related infection, device site reaction), but were resolved without further complication. The device met enabling criteria in 11 patients upon completion of the data collection phase, with high likelihood performance estimate sensitivities ranging from 65% to 100%. Three patients' algorithms did not meet performance criteria and one patient required device removal because of an adverse event before sufficient training data were acquired. We detected no significant changes in clinical effectiveness measures between baseline and 4 months after implantation. Interpretation: This study showed that intracranial electroencephalographic monitoring is feasible in ambulatory patients with drug-resistant epilepsy. If these findings are replicated in larger, longer studies, accurate definition of preictal electrical activity might improve understanding of seizure generation and eventually lead to new management strategies. Funding: NeuroVista. [Copyright &y& Elsevier]

Published

2013

29. SCN1A clinical spectrum includes the self-limited focal epilepsies of childhood.

Author

Kivity, Sara, Oliver, Karen L., Afawi, Zaid, Damiano, John A., Arsov, Todor, Bahlo, Melanie, and Berkovic, Samuel F.

Subjects

*EPILEPSY, *GENETIC disorders, *SEIZURES (Medicine), *SYNDROMES, *FEVER

Abstract

Introduction Amongst autosomal dominant genetic epilepsy with febrile seizures plus (GEFS+) families, SCN1A variants are the most common genetic cause. Initially regarded as a generalized form of epilepsy, the GEFS+ spectrum is now known to include some focal epilepsies, but it is generally not conceptualized as extending to the self-limited focal epilepsies of childhood, such as Panayiotopoulos syndrome. There are, however, three reports of SCN1A variants in Panayiotopoulos syndrome. We describe the variable clinical phenotypes that include the self-limited focal epilepsies of childhood, present in a large GEFS+ family, segregating a heterozygous SCN1A missense variant. Material and methods Electro-clinical details on all putatively affected family members were sought and blood samples were taken for genetic analysis. Two individuals were chosen for SCN1A testing. All 26 exons and exon–intron junctions were amplified, sequenced and analyzed. This was followed by pedigree segregation analysis of the variant identified. Results A pathogenic heterozygous SCN1A (c.2624C>A; p.Thr875Lys) variant was identified. Sixteen of the 18 variant positive family members were affected (88% penetrance): 8 with febrile seizures, 2 febrile seizures plus, 1 unclassified seizures and 5 with self-limited focal epilepsy of childhood. Of these, one was diagnosed with atypical childhood epilepsy with centrotemporal spikes and four with Panayiotopoulos syndrome. Discussion By characterizing the heterogeneous clinical phenotypes in a large, SCN1A mutation positive GEFS+ family, we conclude that the GEFS+ spectrum can extend to the self-limited focal epilepsies of childhood, including Panayiotopoulos syndrome, and in turn highlight the complex genotype-phenotype correlations associated with SCN1A -related epilepsies. [ABSTRACT FROM AUTHOR]

Published

2017

30. Real-world utility of whole exome sequencing with targeted gene analysis for focal epilepsy.

Author

Perucca, Piero, Scheffer, Ingrid E., Harvey, A. Simon, James, Paul A., Lunke, Sebastian, Thorne, Natalie, Gaff, Clara, Regan, Brigid M., Damiano, John A., Hildebrand, Michael S., Berkovic, Samuel F., O’Brien, Terence J., and Kwan, Patrick

Subjects

*GENOMICS, *NUCLEOTIDE sequence, *EPILEPSY, *EXOMES, *SEIZURES (Medicine)

Abstract

Objective Driven by advances in genomic technology and reduction in costs, next-generation sequencing (NGS) is venturing into routine clinical care. The ‘real-world’ clinical utility of NGS remains to be determined in focal epilepsies, which account for 60% of all epilepsies and for which the importance of genetic factors is just beginning to emerge. We investigated the diagnostic yield and management implications of whole exome sequencing (WES)-based screening of selected genes in the routine care of common focal epilepsies suspected to have a genetic basis. Methods We performed WES, followed by targeted analysis of 64 epilepsy genes, on 40 consecutive children and adults enrolled prospectively from routine clinical practice who had MRI-negative focal epilepsy and a family history of febrile seizures or any type of epilepsy in at least one first- or second-degree relative. Exclusion criteria were previous genetic testing, severe intellectual disability and benign focal epilepsies of childhood. Results 5/40 (12.5%) patients had a pathogenic or likely pathogenic variant, detected in SCN1A , DEPDC5 , PCDH19, GABRG2 or NPRL2 . Identifying a pathogenic SCN1A variant in a patient with drug-resistant epilepsy prompted to halt presurgical investigations due to concern of unfavorable post-surgical outcome. It also led in the same patient to discontinue long-standing carbamazepine therapy (a potentially aggravating drug in epilepsies due to SCN1A mutations), resulting in complete seizure control. Patients with pathogenic or likely pathogenic variants had a younger median age of seizure onset (range) compared to those without [18 months (8 months-18 years) vs 18 years (18 months-70 years), p = 0.02]. Significance Our data demonstrate that WES with targeted gene analysis is an effective diagnostic tool for patients with common focal epilepsies in whom a genetic etiology is suspected. It can also influence clinical decision-making, including antiepileptic drug selection and consideration of epilepsy surgery, hence supporting its incorporation in the routine clinical care of this patient group. [ABSTRACT FROM AUTHOR]

Published

2017

31. Parental Mosaicism in "De Novo" Epileptic Encephalopathies.

Author

Myers, Candace T., Hollingsworth, Georgina, Muir, Alison M., Schneider, Amy L., Thuesmunn, Zoe, Knupp, Allison, King, Chontelle, Lacroix, Amy, Mehaffey, Michele G., Berkovic, Samuel F., Carvill, Gemma L., Sadleir, Lynette G., Scheffer, Ingrid E., and Mefford, Heather C.

Subjects

*SEIZURES (Medicine), *EPILEPSY, *MOSAICISM, *GENETIC mutation, *PARENTS, *SPASMS

Published

2018

32. The psychological impact of a newly diagnosed seizure: Losing and restoring perceived control

Author

Velissaris, Sarah L., Wilson, Sarah J., Saling, Michael M., Newton, Mark R., and Berkovic, Samuel F.

Subjects

*SEIZURES (Medicine), *DEVELOPMENTAL disabilities, *NEUROLOGICAL disorders, *SPASMS

Abstract

Abstract: This study aimed to characterize the process of psychosocial adjustment following a newly diagnosed seizure. Eighty-five adult patients were assessed 1 and 3 months after a first seizure presentation with a purpose-developed semistructured interview, the NEWQOL, and the COPE. Among a broad range of patient concerns, psychological issues were paramount, representing a process of losing and restoring perceived control. Two psychological adjustment trajectories were identified, which hinged on the experience of a limited (n =37) or pervasive (n =48) loss of control. These adjustment trajectories were predicted by demographic and clinical factors. The pervasive group described a more extensive process of reevaluation, leading to an improved sense of self at 3 months. Pervasive loss of control, anxiety, and depression predicted subsequent seizure recurrence. Overall, a first seizure can trigger a complex adjustment process, which might require therapeutic management in some patients. [Copyright &y& Elsevier]

Published

2007

33. Update on pharmacogenetics in epilepsy: a brief review

Author

Szoeke, Cassandra EI, Newton, Mark, Wood, Julie M, Goldstein, David, Berkovic, Samuel F, OBrien, Terrence J, and Sheffield, Les J

Subjects

*ANTICONVULSANTS, *EPILEPSY, *BRAIN diseases, *SEIZURES (Medicine), *CENTRAL nervous system depressants

Abstract

Summary: Recent developments in the pharmacogenetics of antiepileptic drugs provide new prospects for predicting the efficacy of treatment and potential side-effects. Epilepsy is a common, serious, and treatable neurological disorder, yet current treatment is limited by high rates of adverse drug reactions and lack of complete seizure control in a significant proportion of patients. The disorder is especially suitable for pharmacogenetic investigation because treatment response can be quantified and side-effects can be assessed with validated measures. Additionally, there is substantial knowledge of the pharmacodynamics and kinetics of antiepileptic drugs, and some candidate genes implicated in the disorder have been identified. However, recent studies of the association of particular genes and their genetic variants with seizure control and adverse drug reactions have not provided unifying conclusions. This article reviews the published work and summarises the state of research in this area. Future directions for research and the application of this technology to the clinical practice of individualising treatment for epilepsy are discussed. [Copyright &y& Elsevier]

Published

2006

34. Proconvulsant-induced seizures in α4 nicotinic acetylcholine receptor subunit knockout mice

Author

Wong, John Y. F., Ross, Shelley A., McColl, Craig, Massalas, Jim S., Powney, Emma, Finkelstein, David I., Clark, Malcolm, Horne, Malcolm K., Berkovic, Samuel F., and Drago, John

Subjects

*SEIZURES (Medicine), *CHOLINERGIC receptors, *GABA

Abstract

The genetic basis of a number of epilepsy syndromes has been identified but the precise mechanism whereby these mutations produce seizures is unknown. Three mutations of the α4 subunit of the neuronal nicotinic acetylcholine receptor (nAChR) have been identified in autosomal dominant nocturnal frontal lobe epilepsy. In vitro studies of two mutations suggest an alteration of receptor function resulting in decreased ion channel current flow. We investigated the response of α4 nAChR subunit knockout mice to the γ-aminobutyric acid (GABA) receptor antagonists; pentylenetetrazole (PTZ) and bicuculline (BIC), the glutamate receptor agonist kainic acid (KA), the glycine receptor antagonist strychnine and the K+ channel blocker 4-aminopyridine (4-AP). Mutant (Mt) mice had a greater sensitivity to PTZ and BIC, with an increase in major motor seizures and seizure-related deaths. Furthermore, Mt mice were more sensitive to KA and strychnine, but the effects were much smaller compared to those seen with the GABA receptor antagonists. Paradoxically, Mt mice appeared to be relatively protected from 4-AP-induced major motor seizures and death.The results show that a functional deletion of the α4 nAChR subunit in vivo is associated with a major increase in sensitivity to GABA receptor blockers. [Copyright &y& Elsevier]

Published

2002