Please use this identifier to cite or link to this item: http://hdl.handle.net/2440/93781
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dc.contributor.authorKlein, K.en
dc.contributor.authorBromhead, C.en
dc.contributor.authorSmith, K.en
dc.contributor.authorO'Callaghan, C.en
dc.contributor.authorCorcoran, S.en
dc.contributor.authorHeron, S.en
dc.contributor.authorIona, X.en
dc.contributor.authorHodgson, B.en
dc.contributor.authorMcMahon, J.en
dc.contributor.authorLawrence, K.en
dc.contributor.authorScheffer, I.en
dc.contributor.authorDibbens, L.en
dc.contributor.authorBahlo, M.en
dc.contributor.authorBerkovic, S.en
dc.date.issued2013en
dc.identifier.citationNeurology, 2013; 80(16):1485-1493en
dc.identifier.issn0028-3878en
dc.identifier.issn1526-632Xen
dc.identifier.urihttp://hdl.handle.net/2440/93781-
dc.description.abstractOBJECTIVE: To establish the occurrence of an autosomal dominant form of vasovagal syncope (VVS) by detailed phenotyping of multiplex families and identification of the causative locus. METHODS: Patients with VVS and a family history of syncope were recruited. A standardized questionnaire was administered to all available family members and medical records were reviewed. Of 44 families recruited, 6 were suggestive of autosomal dominant inheritance. Genome-wide linkage was performed in family A using single nucleotide polymorphism genotyping microarrays. Targeted analysis of chromosome 15q26 with microsatellite markers was implemented in 4 families; 1 family was too small for analysis. RESULTS: Family A contained 30 affected individuals over 3 generations with a median onset of 8 to 9 years. The other families comprised 4 to 14 affected individuals. Affected individuals reported typical triggers of VVS (sight of blood, injury, medical procedures, prolonged standing, pain, frightening thoughts). The triggers varied considerably within the families. Significant linkage to chromosome 15q26 (logarithm of odds score 3.28) was found in family A. Linkage to this region was excluded in 2 medium-sized families but not in 2 smaller families. Sequence analysis of the candidate genes SLCO3A1, ST8SIA2, and NR2F2 within the linkage interval did not reveal any mutations. CONCLUSIONS: Familial VVS, inherited in an autosomal dominant manner, may not be rare and has similar features to sporadic VVS. The chromosome 15q26 locus in family A increases the susceptibility to VVS but does not predispose to a particular vasovagal trigger. Linkage analysis in the remaining families established likely genetic heterogeneity.en
dc.description.statementofresponsibilityKarl Martin Klein, Catherine J. Bromhead, Katherine R. Smith, Christopher J. O’Callaghan, Susan J. Corcoran, Sarah E. Heron, Xenia Iona, Bree L. Hodgson, Jacinta M. McMahon, Kate M. Lawrence, Ingrid E. Scheffer, Leanne M. Dibbens, Melanie Bahlo, Samuel F. Berkovicen
dc.language.isoenen
dc.publisherAmerican Academy of Neurologyen
dc.rights© 2013 American Academy of Neurologyen
dc.subjectElectroencephalographyen
dc.titleAutosomal dominant vasovagal syncope: clinical features and linkage to chromosome 15q26en
dc.typeJournal articleen
dc.identifier.rmid0030031833en
dc.identifier.doi10.1212/WNL.0b013e31828cfad0en
dc.identifier.pubid109319-
pubs.library.collectionMedicine publicationsen
pubs.library.teamDS02en
pubs.verification-statusVerifieden
pubs.publication-statusPublisheden
dc.identifier.orcidHeron, S. [0000-0001-8759-6748]en
Appears in Collections:Medicine publications

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