Your search keyword '"Gianpiero Cavalleri"' showing total 13 results

1. Whole exome sequencing studies in epilepsy: A deep analysis of the published literature

Author

Arif Shukralla, Robert Carton, Katherine A. Benson, Hany El Naggar, Austin Lacey, Gianpiero Cavalleri, and Norman Delanty

Subjects

Epilepsy, Exome Sequencing, Genetics, Humans, Genetics (clinical)

Abstract

To evaluate the quality of whole-exome sequencing (WES) reporting in the epilepsy literature. We aimed to assess the quality of reporting of WES in epilepsy. We compared studies based on journal type and if outcome reporting biases exist. We used a self-constructed benchmark to quantitatively analyze studies. We included 451 publications. Reporting was heterogeneous with poor reporting of (1) ACMG guideline application 13% and (2) Human Phenotype Ontology (HPO) numbers in 3% of studies, 3) VUS in 19%. Predictors of reporting included journal type and journal impact factor. Date of publication and publication type were not predictors of poor reporting. Pairwise comparisons of genetics versus neurology journals using relative risks yielded significant differences in reporting of ACMG guideline application (RR 1.88, 95% CI 1.04-3.38); HPO numbers (RR 8.62, 95% CI 1.08-63.37) and deposition of findings to ClinVar (RR 2.50, 95% CI 1.03-6.1). Reporting of WES literature is heterogeneous in quality, and poor reporting hinders collaboration and accession of data into large databases like OMIM and OrphaNet. This study highlights reporting bias in this area and, formal structural guidelines like the CONSORT guidelines used in the reporting of clinical trials are needed to address the issue.

Published

2022

2. Genome-wide meta-analysis of over 29,000 people with epilepsy reveals 26 loci and subtype-specific genetic architecture

Author

Andreas Schulze-Bonhage, Patrick May, Samuel Berkovic, Lorenzo Ferri, Monica Gagliardi, Adam Strzelczyk, Oluyomi Modupe Adesoji, Vytautas Kasiulevicius, Heidi Kirsch, Algirdas Utkus, Bobby Koeleman, and Gianpiero Cavalleri

Abstract

Epilepsy is a highly heritable disorder affecting over 50 million people worldwide, of which about one-third are resistant to current treatments. Here, we report a trans-ethnic GWAS including 29,944 cases, stratified into three broad- and seven sub-types of epilepsy, and 52,538 controls. We identify 26 genome-wide significant loci, 19 of which are specific to genetic generalized epilepsy (GGE). We implicate 29 likely causal genes underlying these 26 loci. SNP-based heritability analyses show that common variants substantially close the missing heritability gap for GGE. Subtype analysis revealed markedly different genetic architectures between focal and generalized epilepsies. Gene-set analysis of GGE signals implicate synaptic processes in both excitatory and inhibitory neurons in the brain. Prioritized candidate genes overlap with monogenic epilepsy genes and with targets of current anti-seizure medications. Finally, we leverage our results to identify alternate drugs with predicted efficacy if repurposed for epilepsy treatment.

Published

2022

3. Revealing the recent demographic history of Europe via haplotype sharing in the UK Biobank

Author

Edmund Gilbert, Ashwini Shanmugam, and Gianpiero Cavalleri

Subjects

Europe, Multidisciplinary, Haplotypes, Databases, Genetic, Population, Datasets as Topic, Genetic Variation, Demography

Abstract

Haplotype-based analyses have recently been leveraged to interrogate the fine-scale structure in specific geographic regions, notably in Europe, although an equivalent haplotype-based understanding across the whole of Europe with these tools is lacking. Furthermore, study of identity-by-descent (IBD) sharing in a large sample of haplotypes across Europe would allow a direct comparison between different demographic histories of different regions. The UK Biobank (UKBB) is a population-scale dataset of genotype and phenotype data collected from the United Kingdom, with established sampling of worldwide ancestries. The exact content of these non-UK ancestries is largely uncharacterized, where study could highlight valuable intracontinental ancestry references with deep phenotyping within the UKBB. In this context, we sought to investigate the sample of European ancestry captured in the UKBB. We studied the haplotypes of 5,500 UKBB individuals with a European birthplace; investigated the population structure and demographic history in Europe, showing in parallel the variety of footprints of demographic history in different genetic regions around Europe; and expand knowledge of the genetic landscape of the east and southeast of Europe. Providing an updated map of European genetics, we leverage IBD-segment sharing to explore the extent of population isolation and size across the continent. In addition to building and expanding upon previous knowledge in Europe, our results show the UKBB as a source of diverse ancestries beyond Britain. These worldwide ancestries sampled in the UKBB may complement and inform researchers interested in specific communities or regions not limited to Britain.

Published

2022

4. The Epilepsy Genetics Initiative: Systematic reanalysis of diagnostic exomes increases yield

Author

Ingrid Scheffer, Colleen Campbell, Samuel Berkovic, Laura Jansen, Susannah Cornes, Brenda Porter, Kristen Park, Gianpiero Cavalleri, Nicholas Stong, UCL - SSS/IREC/PEDI - Pôle de Pédiatrie, and UCL - (SLuc) Service de neurologie pédiatrique

Subjects

0301 basic medicine, Adult, Male, Parents, Delayed Diagnosis, Adolescent, data sharing, whole exome sequencing, 03 medical and health sciences, Epilepsy, Young Adult, 0302 clinical medicine, Data sequences, Seizures, Databases, Genetic, Exome Sequencing, Medicine, Humans, Exome, Medical diagnosis, Child, Exome sequencing, seizures, Retrospective Studies, Genetics, Family Health, business.industry, Information Dissemination, Siblings, Whole exome sequencing, Infant, Pathogenicity, medicine.disease, 030104 developmental biology, Neurology, Child, Preschool, Mutation, Full‐length Original Research, Data sharing, Female, Neurology (clinical), Genetic diagnosis, business, 030217 neurology & neurosurgery, Gene Discovery

Abstract

Summary Objective The Epilepsy Genetics Initiative (EGI) was formed in 2014 to create a centrally managed database of clinically generated exome sequence data. EGI performs systematic research‐based reanalysis to identify new molecular diagnoses that were not possible at the time of initial sequencing and to aid in novel gene discovery. Herein we report on the efficacy of this approach 3 years after inception. Methods One hundred sixty‐six individuals with epilepsy who underwent diagnostic whole exome sequencing (WES) were enrolled, including 139 who had not received a genetic diagnosis. Sequence data were transferred to the EGI and periodically reevaluated on a research basis. Results Eight new diagnoses were made as a result of updated annotations or the discovery of novel epilepsy genes after the initial diagnostic analysis was performed. In five additional cases, we provided new evidence to support or contradict the likelihood of variant pathogenicity reported by the laboratory. One novel epilepsy gene was discovered through dual interrogation of research and clinically generated WES. Significance EGI's diagnosis rate of 5.8% represents a considerable increase in diagnostic yield and demonstrates the value of periodic reinterrogation of whole exome data. The initiative's contributions to gene discovery underscore the importance of data sharing and the value of collaborative enterprises.

Published

2019

5. 252 Whole exome sequencing in epilepsy: quality of reporting in literature

Author

Arif Shukralla, Austin Lacey, Hany El Naggar, Gianpiero Cavalleri, and Norman Delanty

Subjects

Psychiatry and Mental health, Surgery, Neurology (clinical)

Abstract

PurposeWhole exome sequencing is a new rapid and cost effective tool for the diagnosis of the epilepsies.MethodOur primary aim was to assess the quality of reporting of WES. Secondary aims; to compare the quality of studies based on journal type if recent ACMG guideless have made influenced reporting quality; if any outcome reporting biases exist.We analysed studies of whole exome sequencing in epilepsy. We used a self-constructed benchmark to quantitatively analyse studies, explore retrospectively if reporting trends have changed.ResultsTotal of 307 studies was included. Reporting of data was heterogenous with poor reporting of diagnostic yield in 6% of studies, incidental findings in 11%, variants of undetermined significance in 19%. Predictors of poor reporting included: Journal type, proband status and case reports. Pairwise compari- sons of genetics journals versus other journals using relative risks yielded significant differences in reporting of consanguinity status (RR 1.27 CI 1.04–1.55); variant filtering (RR 1.95 CI 1.41–2.7) and determination of pathogenicity (RR 1.35 CI 1.17–1.56).ConclusionReporting of WES data in the medical literature is heterogenous, making comparisons across studies difficult. Formal structured guidelines similar to the CONSORT guidelines are needed to address this issue further.arifshukralla@gmail.com

Published

2022

6. A Rare Autosomal Dominant Variant in Regulator of Calcineurin Type 1 (

Author

Brandon M, Lane, Susan, Murray, Katherine, Benson, Agnieszka, Bierzynska, Megan, Chryst-Stangl, Liming, Wang, Guanghong, Wu, Gianpiero, Cavalleri, Brendan, Doyle, Neil, Fennelly, Anthony, Dorman, Shane, Conlon, Virginia, Vega-Warner, Damian, Fermin, Poornima, Vijayan, Mohammad Azfar, Qureshi, Shirlee, Shril, Moumita, Barua, Friedhelm, Hildebrandt, Martin, Pollak, David, Howell, Matthew G, Sampson, Moin, Saleem, Peter J, Conlon, Robert, Spurney, and Rasheed, Gbadegesin

Subjects

Basic Research

Abstract

BACKGROUND: Podocyte dysfunction is the main pathologic mechanism driving the development of FSGS and other morphologic types of steroid-resistant nephrotic syndrome (SRNS). Despite significant progress, the genetic causes of most cases of SRNS have yet to be identified. METHODS: Whole-genome sequencing was performed on 320 individuals from 201 families with familial and sporadic NS/FSGS with no pathogenic mutations in any known NS/FSGS genes. RESULTS: Two variants in the gene encoding regulator of calcineurin type 1 (RCAN1) segregate with disease in two families with autosomal dominant FSGS/SRNS. In vitro, loss of RCAN1 reduced human podocyte viability due to increased calcineurin activity. Cells expressing mutant RCAN1 displayed increased calcineurin activity and NFAT activation that resulted in increased susceptibility to apoptosis compared with wild-type RCAN1. Treatment with GSK-3 inhibitors ameliorated this elevated calcineurin activity, suggesting the mutation alters the balance of RCAN1 regulation by GSK-3β, resulting in dysregulated calcineurin activity and apoptosis. CONCLUSIONS: These data suggest mutations in RCAN1 can cause autosomal dominant FSGS. Despite the widespread use of calcineurin inhibitors in the treatment of NS, genetic mutations in a direct regulator of calcineurin have not been implicated in the etiology of NS/FSGS before this report. The findings highlight the therapeutic potential of targeting RCAN1 regulatory molecules, such as GSK-3β, in the treatment of FSGS.

Published

2020

7. Assessing the genetic association between vitamin B6 metabolism and genetic generalized epilepsy

Author

Graham Neil Thomas, Remi Stevelink, Ingrid Scheffer, Andreja Avbersek, Thomas Ferraro, Costin Leu, Krishna Chinthapalli, Claudia B. Catarino, Peter Widdess-Walsh, Colin Doherty, Anthony Marson, Michele Iacomino, Martin Krenn, Aarno Palotie, Heidi Kirsch, Stefan Wolking, Gianpiero Cavalleri, Clinicum, Research Programs Unit, Diabetes and Obesity Research Program, Johan Eriksson / Principal Investigator, Department of General Practice and Primary Health Care, University of Helsinki, Helsinki University Hospital Area, Faculty of Medicine, Centre of Excellence in Complex Disease Genetics, Aarno Palotie / Principal Investigator, Institute for Molecular Medicine Finland, and Genomics of Neurological and Neuropsychiatric Disorders

Subjects

PNPO, Genome-wide association study, Neurodegenerative, 3124 Neurology and psychiatry, 0302 clinical medicine, Endocrinology, PHOSPHATE, 2.1 Biological and endogenous factors, GWAS, Aetiology, lcsh:QH301-705.5, PYRIDOXINE RESPONSIVENESS, Genetics, International League Against Epilepsy Consortium on Complex Epilepsies, lcsh:R5-920, 0303 health sciences, GGE, Pharmacogenetics, Pyridoxine, SNP, 3. Good health, VIRUS-X-PROTEIN, lcsh:Medicine (General), medicine.drug, Research Paper, BIOMARKERS, Locus (genetics), Single-nucleotide polymorphism, Biology, CELL APOPTOSIS, 03 medical and health sciences, medicine, Molecular Biology, 030304 developmental biology, Genetic association, Nutrition, Epilepsy, MUTATIONS, Prevention, Human Genome, 3112 Neurosciences, Neurosciences, Brain Disorders, lcsh:Biology (General), SEIZURES, 3111 Biomedicine, Biochemistry and Cell Biology, 030217 neurology & neurosurgery

Abstract

Altered vitamin B6 metabolism due to pathogenic variants in the gene PNPO causes early onset epileptic encephalopathy, which can be treated with high doses of vitamin B6. We recently reported that single nucleotide polymorphisms (SNPs) that influence PNPO expression in the brain are associated with genetic generalized epilepsy (GGE). However, it is not known whether any of these GGE-associated SNPs influence vitamin B6 metabolite levels. Such an influence would suggest that vitamin B6 could play a role in GGE therapy. Here, we performed genome-wide association studies (GWAS) to assess the influence of GGE associated genetic variants on measures of vitamin B6 metabolism in blood plasma in 2232 healthy individuals. We also asked if SNPs that influence vitamin B6 were associated with GGE in 3122 affected individuals and 20,244 controls. Our GWAS of vitamin B6 metabolites reproduced a previous association and found a novel genome-wide significant locus. The SNPs in these loci were not associated with GGE. We found that 84 GGE-associated SNPs influence expression levels of PNPO in the brain as well as in blood. However, these SNPs were not associated with vitamin B6 metabolism in plasma. By leveraging polygenic risk scoring (PRS), we found suggestive evidence of higher catabolism and lower levels of the active and transport forms of vitamin B6 in GGE, although these findings require further replication. Keywords: Pyridoxine, GGE, GWAS, Genetics, SNP, Pharmacogenetics

Published

2019

8. Re-annotation of 191 developmental and epileptic encephalopathy-associated genes unmasks de novo variants in

Author

Charles A, Steward, Jolien, Roovers, Marie-Marthe, Suner, Jose M, Gonzalez, Barbara, Uszczynska-Ratajczak, Dmitri, Pervouchine, Stephen, Fitzgerald, Margarida, Viola, Hannah, Stamberger, Fadi F, Hamdan, Berten, Ceulemans, Patricia, Leroy, Caroline, Nava, Anne, Lepine, Electra, Tapanari, Don, Keiller, Stephen, Abbs, Alba, Sanchis-Juan, Detelina, Grozeva, Anthony S, Rogers, Mark, Diekhans, Roderic, Guigó, Robert, Petryszak, Berge A, Minassian, Gianpiero, Cavalleri, Dimitrios, Vitsios, Slavé, Petrovski, Jennifer, Harrow, Paul, Flicek, F, Lucy Raymond, Nicholas J, Lench, Peter De, Jonghe, Jonathan M, Mudge, Sarah, Weckhuysen, Sanjay M, Sisodiya, and Adam, Frankish

Subjects

Molecular medicine, Medical genomics, Article

Abstract

The developmental and epileptic encephalopathies (DEE) are a group of rare, severe neurodevelopmental disorders, where even the most thorough sequencing studies leave 60–65% of patients without a molecular diagnosis. Here, we explore the incompleteness of transcript models used for exome and genome analysis as one potential explanation for a lack of current diagnoses. Therefore, we have updated the GENCODE gene annotation for 191 epilepsy-associated genes, using human brain-derived transcriptomic libraries and other data to build 3,550 putative transcript models. Our annotations increase the transcriptional ‘footprint’ of these genes by over 674 kb. Using SCN1A as a case study, due to its close phenotype/genotype correlation with Dravet syndrome, we screened 122 people with Dravet syndrome or a similar phenotype with a panel of exon sequences representing eight established genes and identified two de novo SCN1A variants that now - through improved gene annotation - are ascribed to residing among our exons. These two (from 122 screened people, 1.6%) molecular diagnoses carry significant clinical implications. Furthermore, we identified a previously classified SCN1A intronic Dravet syndrome-associated variant that now lies within a deeply conserved exon. Our findings illustrate the potential gains of thorough gene annotation in improving diagnostic yields for genetic disorders.

Published

2019

9. Intestinal-Cell Kinase and Juvenile Myoclonic Epilepsy. Reply

Author

Josemir Sander, Patrick May, Rudi Balling, Eduardo Pérez-Palma, Karl Martin Klein, Ingrid Scheffer, Andreja Avbersek, Dheeraj Bobbili, Samuel Berkovic, Costin Leu, Rhys Thomas, Anthony Marson, Henrike Heyne, Janine Altmüller, Sarah Weckhuysen, Michael Nothnagel, Terence O'Brien, Martin Krenn, Aarno Palotie, Mahmoud Koko, Seo-Kyung Chung, Graeme Sills, Stefan Wolking, Antonio Gambardella, Gianpiero Cavalleri, Weckhuysen, Sarah, EuroEPINOMICS-CoGIE Consortium, EpiPGX Consortium, and Epi4K Consortium/Epilepsy Phenome/Genome Project

Subjects

medicine.medical_specialty, Protein-Serine-Threonine Kinases, business.industry, Myoclonic Epilepsy, Juvenile, Juvenile, Electroencephalography, General Medicine, Protein Serine-Threonine Kinases, medicine.disease, INTESTINAL CELL KINASE, Epilepsy, Endocrinology, Myoclonic Epilepsy, Internal medicine, medicine, Myoclonic epilepsy, Humans, Human medicine, Juvenile myoclonic epilepsy, business

Published

2019

10. Corrigendum to: Polygenic burden in focal and generalized epilepsies

Author

Remi Stevelink and Gianpiero Cavalleri

Subjects

Male, Multifactorial Inheritance, Databases, Factual, Genetic Variation, Corrigenda, Polymorphism, Single Nucleotide, White People, Cohort Studies, Cost of Illness, Humans, Epilepsy, Generalized, Female, Genetic Predisposition to Disease, Epilepsies, Partial, Neurology (clinical), Genome-Wide Association Study

Abstract

Rare genetic variants can cause epilepsy, and genetic testing has been widely adopted for severe, paediatric-onset epilepsies. The phenotypic consequences of common genetic risk burden for epilepsies and their potential future clinical applications have not yet been determined. Using polygenic risk scores (PRS) from a European-ancestry genome-wide association study in generalized and focal epilepsy, we quantified common genetic burden in patients with generalized epilepsy (GE-PRS) or focal epilepsy (FE-PRS) from two independent non-Finnish European cohorts (Epi25 Consortium, n = 5705; Cleveland Clinic Epilepsy Center, n = 620; both compared to 20 435 controls). One Finnish-ancestry population isolate (Finnish-ancestry Epi25, n = 449; compared to 1559 controls), two European-ancestry biobanks (UK Biobank, n = 383 656; Vanderbilt biorepository, n = 49 494), and one Japanese-ancestry biobank (BioBank Japan, n = 168 680) were used for additional replications. Across 8386 patients with epilepsy and 622 212 population controls, we found and replicated significantly higher GE-PRS in patients with generalized epilepsy of European-ancestry compared to patients with focal epilepsy (Epi25: P = 1.64×10-15; Cleveland: P = 2.85×10-4; Finnish-ancestry Epi25: P = 1.80×10-4) or population controls (Epi25: P = 2.35×10-70; Cleveland: P = 1.43×10-7; Finnish-ancestry Epi25: P = 3.11×10-4; UK Biobank and Vanderbilt biorepository meta-analysis: P = 7.99×10-4). FE-PRS were significantly higher in patients with focal epilepsy compared to controls in the non-Finnish, non-biobank cohorts (Epi25: P = 5.74×10-19; Cleveland: P = 1.69×10-6). European ancestry-derived PRS did not predict generalized epilepsy or focal epilepsy in Japanese-ancestry individuals. Finally, we observed a significant 4.6-fold and a 4.5-fold enrichment of patients with generalized epilepsy compared to controls in the top 0.5% highest GE-PRS of the two non-Finnish European cohorts (Epi25: P = 2.60×10-15; Cleveland: P = 1.39×10-2). We conclude that common variant risk associated with epilepsy is significantly enriched in multiple cohorts of patients with epilepsy compared to controls-in particular for generalized epilepsy. As sample sizes and PRS accuracy continue to increase with further common variant discovery, PRS could complement established clinical biomarkers and augment genetic testing for patient classification, comorbidity research, and potentially targeted treatment.

Published

2020

11. Long- and short-term outcomes in renal allografts with deceased donors: A large recipient and donor genome-wide association study

Author

Maria P, Hernandez-Fuentes, Christopher, Franklin, Irene, Rebollo-Mesa, Jennifer, Mollon, Florence, Delaney, Esperanza, Perucha, Caragh, Stapleton, Richard, Borrows, Catherine, Byrne, Gianpiero, Cavalleri, Brendan, Clarke, Menna, Clatworthy, John, Feehally, Susan, Fuggle, Sarah A, Gagliano, Sian, Griffin, Abdul, Hammad, Robert, Higgins, Alan, Jardine, Mary, Keogan, Timothy, Leach, Iain, MacPhee, Patrick B, Mark, James, Marsh, Peter, Maxwell, William, McKane, Adam, McLean, Charles, Newstead, Titus, Augustine, Paul, Phelan, Steve, Powis, Peter, Rowe, Neil, Sheerin, Ellen, Solomon, Henry, Stephens, Raj, Thuraisingham, Richard, Trembath, Peter, Topham, Robert, Vaughan, Steven H, Sacks, Peter, Conlon, Gerhard, Opelz, Nicole, Soranzo, Michael E, Weale, and Graham M, Lord

Subjects

Adult, DNA Replication, Male, basic (laboratory) research/science, Genotype, Histocompatibility Testing, Graft Survival, kidney transplantation/nephrology, kidney (allograft) function/dysfunction, Middle Aged, clinical research/practice, Kidney Transplantation, Polymorphism, Single Nucleotide, Tissue Donors, Transplant Recipients, immunogenetics, Humans, Transplantation, Homologous, informatics, Female, organ transplantation in general, rejection, Letters to the Editor, Letter to the Editor, Genome-Wide Association Study

Abstract

Improvements in immunosuppression have modified short-term survival of deceased-donor allografts, but not their rate of long-term failure. Mismatches between donor and recipient HLA play an important role in the acute and chronic allogeneic immune response against the graft. Perfect matching at clinically relevant HLA loci does not obviate the need for immunosuppression, suggesting that additional genetic variation plays a critical role in both short- and long-term graft outcomes. By combining patient data and samples from supranational cohorts across the United Kingdom and European Union, we performed the first large-scale genome-wide association study analyzing both donor and recipient DNA in 2094 complete renal transplant-pairs with replication in 5866 complete pairs. We studied deceased-donor grafts allocated on the basis of preferential HLA matching, which provided some control for HLA genetic effects. No strong donor or recipient genetic effects contributing to long- or short-term allograft survival were found outside the HLA region. We discuss the implications for future research and clinical application.

Published

2017

12. Ultra-rare genetic variation in common epilepsies: a case-control sequencing study

Author

Andrew S Allen, Susannah T Bellows, Samuel F Berkovic, Joshua Bridgers, Rosemary Burgess, Gianpiero Cavalleri, Seo-Kyung Chung, Patrick Cossette, Norman Delanty, Dennis Dlugos, Michael P Epstein, Catharine Freyer, David B Goldstein, Erin L Heinzen, Michael S Hildebrand, Michael R Johnson, Ruben Kuzniecky, Daniel H Lowenstein, Anthony G Marson, Richard Mayeux, Caroline Mebane, Heather C Mefford, Terence J O'Brien, Ruth Ottman, Steven Petrou, Slavgé Petrovski, William O Pickrell, Annapurna Poduri, Rodney A Radtke, Mark I Rees, Brigid M Regan, Zhong Ren, Ingrid E Scheffer, Graeme J Sills, Rhys H Thomas, Quanli Wang, Bassel Abou-Khalil, Brian K Alldredge, Dina Amrom, Eva Andermann, Frederick Andermann, Jocelyn F. Bautista, Judith Bluvstein, Alex Boro, Gregory D Cascino, Damian Consalvo, Patricia Crumrine, Orrin Devinsky, Miguel Fiol, Nathan B Fountain, Jacqueline French, Daniel Friedman, Eric B Geller, Tracy Glauser, Simon Glynn, Kevin Haas, Sheryl R Haut, Jean Hayward, Sandra L Helmers, Sucheta Joshi, Andres Kanner, Heidi E Kirsch, Robert C Knowlton, Eric H Kossoff, Rachel Kuperman, Paul V Motika, Edward J Novotny, Juliann M Paolicchi, Jack M Parent, Kristen Park, Lynette G Sadleir, Renée A. Shellhaas, Elliott H Sherr, Jerry J. Shih, Shlomo Shinnar, Rani K Singh, Joseph Sirven, Michael C Smith, Joseph Sullivan, Liu Lin Thio, Anu Venkat, Eileen P.G Vining, Gretchen K Von Allmen, Judith L Weisenberg, Peter Widdess-Walsh, Melodie R Winawer, and Imperial College Healthcare NHS Trust- BRC Funding

Subjects

0301 basic medicine, medicine.medical_specialty, Population, Disease, Bioinformatics, 03 medical and health sciences, Epilepsy, 0302 clinical medicine, Epilepsy Phenome/Genome Project, Genetic variation, medicine, Humans, Exome, Genetic Predisposition to Disease, education, Psychiatry, education.field_of_study, Neurology & Neurosurgery, business.industry, Genetic Variation, 1103 Clinical Sciences, Sequence Analysis, DNA, medicine.disease, Comorbidity, R1, 030104 developmental biology, Case-Control Studies, Epilepsy syndromes, Epilepsy, Generalized, Epilepsies, Partial, Neurology (clinical), 1109 Neurosciences, business, 030217 neurology & neurosurgery

Abstract

Summary Background Despite progress in understanding the genetics of rare epilepsies, the more common epilepsies have proven less amenable to traditional gene-discovery analyses. We aimed to assess the contribution of ultra-rare genetic variation to common epilepsies. Methods We did a case-control sequencing study with exome sequence data from unrelated individuals clinically evaluated for one of the two most common epilepsy syndromes: familial genetic generalised epilepsy, or familial or sporadic non-acquired focal epilepsy. Individuals of any age were recruited between Nov 26, 2007, and Aug 2, 2013, through the multicentre Epilepsy Phenome/Genome Project and Epi4K collaborations, and samples were sequenced at the Institute for Genomic Medicine (New York, USA) between Feb 6, 2013, and Aug 18, 2015. To identify epilepsy risk signals, we tested all protein-coding genes for an excess of ultra-rare genetic variation among the cases, compared with control samples with no known epilepsy or epilepsy comorbidity sequenced through unrelated studies. Findings We separately compared the sequence data from 640 individuals with familial genetic generalised epilepsy and 525 individuals with familial non-acquired focal epilepsy to the same group of 3877 controls, and found significantly higher rates of ultra-rare deleterious variation in genes established as causative for dominant epilepsy disorders (familial genetic generalised epilepsy: odd ratio [OR] 2·3, 95% CI 1·7–3·2, p=9·1 × 10 −8 ; familial non-acquired focal epilepsy 3·6, 2·7–4·9, p=1·1 × 10 −17 ). Comparison of an additional cohort of 662 individuals with sporadic non-acquired focal epilepsy to controls did not identify study-wide significant signals. For the individuals with familial non-acquired focal epilepsy, we found that five known epilepsy genes ranked as the top five genes enriched for ultra-rare deleterious variation. After accounting for the control carrier rate, we estimate that these five genes contribute to the risk of epilepsy in approximately 8% of individuals with familial non-acquired focal epilepsy. Our analyses showed that no individual gene was significantly associated with familial genetic generalised epilepsy; however, known epilepsy genes had lower p values relative to the rest of the protein-coding genes (p=5·8 × 10 −8 ) that were lower than expected from a random sampling of genes. Interpretation We identified excess ultra-rare variation in known epilepsy genes, which establishes a clear connection between the genetics of common and rare, severe epilepsies, and shows that the variants responsible for epilepsy risk are exceptionally rare in the general population. Our results suggest that the emerging paradigm of targeting of treatments to the genetic cause in rare devastating epilepsies might also extend to a proportion of common epilepsies. These findings might allow clinicians to broadly explain the cause of these syndromes to patients, and lay the foundation for possible precision treatments in the future. Funding National Institute of Neurological Disorders and Stroke (NINDS), and Epilepsy Research UK.

Published

2017

13. Molecular variation of human HSP90alpha and HSP90beta genes in Caucasians

Author

Passarino, G., Gianpiero Cavalleri, Stecconi, R., Franceschi, C., Altomare, K., Dato, S., Greco, V., Luca Cavalli Sforza, L., Underhill, P. A., and Benedictis, G.