Please use this identifier to cite or link to this item: https://ahro.austin.org.au/austinjspui/handle/1/9850
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dc.contributor.authorBerkovic, Samuel Fen
dc.contributor.authorMazarib, Azizen
dc.contributor.authorWalid, Simrien
dc.contributor.authorNeufeld, Miriam Yen
dc.contributor.authorManelis, Judithen
dc.contributor.authorNevo, Yoramen
dc.contributor.authorKorczyn, Amos Den
dc.contributor.authorYin, Jinggangen
dc.contributor.authorXiong, Lanen
dc.contributor.authorPandolfo, Massimoen
dc.contributor.authorMulley, John Cen
dc.contributor.authorWallace, Robyn Hen
dc.date.accessioned2015-05-15T23:06:48Z
dc.date.available2015-05-15T23:06:48Z
dc.date.issued2005-01-05en
dc.identifier.citationBrain : A Journal of Neurology 2005; 128(Pt 3): 652-8en
dc.identifier.govdoc15634728en
dc.identifier.otherPUBMEDen
dc.identifier.urihttps://ahro.austin.org.au/austinjspui/handle/1/9850en
dc.description.abstractProgressive myoclonus epilepsy (PME) has a number of causes, of which Unverricht-Lundborg disease (ULD) is the most common. ULD has previously been mapped to a locus on chromosome 21 (EPM1). Subsequently, mutations in the cystatin B gene have been found in most cases. In the present work we identified an inbred Arab family with a clinical pattern compatible with ULD, but mutations in the cystatin B gene were absent. We sought to characterize the clinical and molecular features of the disorder. The family was studied by multiple field trips to their town to clarify details of the complex consanguineous relationships and to personally examine the family. DNA was collected for subsequent molecular analyses from 21 individuals. A genome-wide screen was performed using 811 microsatellite markers. Homozygosity mapping was used to identify loci of interest. There were eight affected individuals. Clinical onset was at 7.3 +/- 1.5 years with myoclonic or tonic-clonic seizures. All had myoclonus that progressed in severity over time and seven had tonic-clonic seizures. Ataxia, in addition to myoclonus, occurred in all. Detailed cognitive assessment was not possible, but there was no significant progressive dementia. There was intrafamily variation in severity; three required wheelchairs in adult life; the others could walk unaided. MRI, muscle and skin biopsies on one individual were unremarkable. We mapped the family to a 15-megabase region at the pericentromeric region of chromosome 12 with a maximum lod score of 6.32. Although the phenotype of individual subjects was typical of ULD, the mean age of onset (7.3 years versus 11 years for ULD) was younger. The locus on chromosome 12 does not contain genes for any other form of PME, nor does it have genes known to be related to cystatin B. This represents a new form of PME and we have designated the locus as EPM1B.en
dc.language.isoenen
dc.subject.otherAdolescenten
dc.subject.otherAdulten
dc.subject.otherChromosome Mapping.methodsen
dc.subject.otherChromosomes, Human, Pair 12.geneticsen
dc.subject.otherDisease Progressionen
dc.subject.otherElectroencephalographyen
dc.subject.otherFemaleen
dc.subject.otherGenotypeen
dc.subject.otherHomozygoteen
dc.subject.otherHumansen
dc.subject.otherLod Scoreen
dc.subject.otherMagnetic Resonance Imagingen
dc.subject.otherMaleen
dc.subject.otherPedigreeen
dc.subject.otherUnverricht-Lundborg Syndrome.genetics.pathology.physiopathologyen
dc.titleA new clinical and molecular form of Unverricht-Lundborg disease localized by homozygosity mapping.en
dc.typeJournal Articleen
dc.identifier.journaltitleBrainen
dc.identifier.affiliationEpilepsy Research Centre and Department of Medicine (Neurology), University of Melbourne, Austin Health, Heidelberg West, Victoria, Australiaen
dc.identifier.doi10.1093/brain/awh377en
dc.description.pages652-8en
dc.relation.urlhttps://pubmed.ncbi.nlm.nih.gov/15634728en
dc.type.austinJournal Articleen
local.name.researcherBerkovic, Samuel F
item.languageiso639-1en-
item.cerifentitytypePublications-
item.fulltextWith Fulltext-
item.grantfulltextopen-
item.openairetypeJournal Article-
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
crisitem.author.deptEpilepsy Research Centre-
crisitem.author.deptNeurology-
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