| dc.contributor.author | DOHERTY, COLIN | en |
| dc.date.accessioned | 2015-05-19T14:57:02Z | |
| dc.date.available | 2015-05-19T14:57:02Z | |
| dc.date.issued | 2010 | en |
| dc.date.submitted | 2010 | en |
| dc.identifier.citation | Heinzen, E.L. Radtke, R.A. Urban, T.J. Cavalleri, G.L. Depondt, C. Need, A.C. Walley, N.M. Nicoletti, P. Ge, D. Catarino, C.B. Duncan, J.S. Kasperavi-iute, D. Tate, S.K. Caboclo, L.O. Sander, J.W. Clayton, L. Linney, K.N. Shianna, K.V. Gumbs, C.E. Smith, J. Cronin, K.D. Maia, J.M. Doherty, C.P. Pandolfo, M. Leppert, D. Middleton, L.T. Gibson, R.A. Johnson, M.R. Matthews, P.M. Hosford, D. Kälviäinen, R. Eriksson, K. Kantanen, A.-M. Dorn, T. Hansen, J. Krämer, G. Steinhoff, B.J. Wieser, H.-G. Zumsteg, D. Ortega, M. Wood, N.W. Huxley-Jones, J. Mikati, M. Gallentine, W.B. Husain, A.M. Buckley, P.G. Stallings, R.L. Podgoreanu, M.V. Delanty, N. Sisodiya, S.M. Goldstein, D.B., Rare Deletions at 16p13.11 Predispose to a Diverse Spectrum of Sporadic Epilepsy Syndromes, AJHG, 86, 5, 2010, 707 - 718 | en |
| dc.identifier.other | Y | en |
| dc.description | PUBLISHED | en |
| dc.description.abstract | Deletions at 16p13.11 are associated with schizophrenia, mental retardation, and most recently idiopathic generalized epilepsy. To evaluate the role of 16p13.11 deletions, as well as other structural variation, in epilepsy disorders, we used genome-wide screens to identify copy number variation in 3812 patients with a diverse spectrum of epilepsy syndromes and in 1299 neurologically-normal controls. Large deletions (> 100 kb) at 16p13.11 were observed in 23 patients, whereas no control had a deletion greater than 16 kb. Patients, even those with identically sized 16p13.11 deletions, presented with highly variable epilepsy phenotypes. For a subset of patients with a 16p13.11 deletion, we show a consistent reduction of expression for included genes, suggesting that haploinsufficiency might contribute to pathogenicity. We also investigated another possible mechanism of pathogenicity by using hybridization-based capture and next-generation sequencing of the homologous chromosome for ten 16p13.11-deletion patients to look for unmasked recessive mutations. Follow-up genotyping of suggestive polymorphisms failed to identify any convincing recessive-acting mutations in the homologous interval corresponding to the deletion. The observation that two of the 16p13.11 deletions were larger than 2 Mb in size led us to screen for other large deletions. We found 12 additional genomic regions harboring deletions > 2 Mb in epilepsy patients, and none in controls. Additional evaluation is needed to characterize the role of these exceedingly large, non-locus-specific deletions in epilepsy. Collectively, these data implicate 16p13.11 and possibly other large deletions as risk factors for a wide range of epilepsy disorders, and they appear to point toward haploinsufficiency as a contributor to the pathogenicity of deletions | en |
| dc.description.sponsorship | This work was supported by grants from the UK Medical Research Council (G0400126), The Wellcome Trust (084730), the National Institute for Health Research (NIHR) (08-08-SCC), University College London Hospitals Clinical Research and Development Committee (F136), and the National Society for Epilepsy, UK. This work was partly undertaken at University College London Hospitals/University College London, which received a proportion of funding from the Department of Health's NIHR Biomedical Research Centres funding scheme. The collection of the Belgian patients was supported by the Fonds National de la Recherche Scientifique and the Fondation Erasme, Université Libre de Bruxelles. The collection of the Irish patient cohort was supported as part of the Programme for Human Genomics and the Programme for Research in Third Level Institutions (PRTLI3) funded by the Irish Higher Education Authority and in part by the Children's Medical and Research Foundation and the Irish Research Council for Science, Engineering and Technology. GlaxoSmithKline funded the recruitment and the phenotypic data collection of the GenEpA Consortium samples used in this study and contributed to the genotyping costs associated with their study.
We also acknowledge Leslie Hall, Siwan Oldham, Linda Surh, Rachel Taylor (GlaxoSmithKline), and Dan Lowenstein (University of California, San Francisco) for contributing to the GenEpA steering committee. T.J.U. was supported by the American Epilepsy Society postdoctoral research fellowship. | en |
| dc.format.extent | 707 | en |
| dc.format.extent | 718 | en |
| dc.relation.ispartofseries | AJHG | en |
| dc.relation.ispartofseries | 86 | en |
| dc.relation.ispartofseries | 5 | en |
| dc.rights | Y | en |
| dc.subject | schizophrenia, mental retardation | en |
| dc.subject.lcsh | schizophrenia, mental retardation | en |
| dc.title | Rare Deletions at 16p13.11 Predispose to a Diverse Spectrum of Sporadic Epilepsy Syndromes | en |
| dc.type | Journal Article | en |
| dc.type.supercollection | scholarly_publications | en |
| dc.type.supercollection | refereed_publications | en |
| dc.identifier.peoplefinderurl | http://people.tcd.ie/cdohert | en |
| dc.identifier.rssinternalid | 102987 | en |
| dc.identifier.doi | http://dx.doi.org/10.1016/j.ajhg.2010.03.018 | en |
| dc.rights.ecaccessrights | openAccess | |
| dc.identifier.rssuri | http://www.scopus.com/inward/record.url?eid=2-s2.0-77952096810&partnerID=40&md5=82a7b157a589ceeb89fa323c23c1ddb1 | en |
| dc.identifier.uri | http://hdl.handle.net/2262/73953 | |
