Mostrar el registro sencillo del ítem

A Missense Mutation in KCTD17 Causes Autosomal Dominant Myoclonus-Dystonia

dc.contributor.authorMencacci, Niccolo E.
dc.contributor.authorBandrés Ciga, Sara
dc.date.accessioned2020-07-29T11:10:17Z
dc.date.available2020-07-29T11:10:17Z
dc.date.issued2015-06-04
dc.identifier.citationMencacci, N. E., Rubio-Agusti, I., Zdebik, A., Asmus, F., Ludtmann, M. H., Ryten, M., ... & Forabosco, P. (2015). A missense mutation in KCTD17 causes autosomal dominant myoclonus-dystonia. The American Journal of Human Genetics, 96(6), 938-947. [https://doi.org/10.1016/j.ajhg.2015.04.008]es_ES
dc.identifier.urihttp://hdl.handle.net/10481/63188
dc.descriptionWe would like to extend our thanks to the individuals whose participation made this research possible. This work was supported financially by a Medical Research Council/Wellcome Trust Strategic Award (WT089698/Z/09/Z) and a grant from the Bachman-Strauss Dystonia Parkinsonism Foundation. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. The work was undertaken at University College London Hospitals (UCLH) and University College London (UCL), who receive support from the Department of Health's NIHR Biomedical Research Center's funding streams. E.L. and T.G. are supported by a grant from the Dystonia Medical Research Foundation (DMRF). C.K. is the recipient of a career development award from the Herman and Lilly Schilling Foundation. A.M.P. is funded by the Reta Lila Weston Trust. S.B.C. held a FPU fellowship from the Spanish Ministry of Education and Science jointly with a short-term stay grant by Cei-BioTic and University of Granada. Next Generation Sequencing was performed at the UCL Institute of Neurology Sequencing Facility. We thank the UCL-Exomes Consortium for providing the exome sequencing data of UK population controls. Expression data was provided by the UK Human Brain Expression Consortium (UKBEC), which comprises J.H., M.R., Michael Weale, D.T., Adaikalavan Ramasamy, Colin Smith, and Robert Walker. UKBEC members are affiliated with UCL Institute of Neurology (J.H., M.R., D.T.), King's College London (M.R., Adaikalavan Ramasamy, and Michael Weale), and the University of Edinburgh (Colin Smith and Robert Walker). We thank Miss Elisavet Preza for providing help with the skin biopsy preparation.es_ES
dc.description.abstractMyoclonus-dystonia (M-D) is a rare movement disorder characterized by a combination of non-epileptic myoclonic jerks and dystonia. SGCE mutations represent a major cause for familial M-D being responsible for 30%–50% of cases. After excluding SGCE mutations, we identified through a combination of linkage analysis and whole-exome sequencing KCTD17 c.434 G>A p.(Arg145His) as the only segregating variant in a dominant British pedigree with seven subjects affected by M-D. A subsequent screening in a cohort of M-D cases without mutations in SGCE revealed the same KCTD17 variant in a German family. The clinical presentation of the KCTD17-mutated cases was distinct from the phenotype usually observed in M-D due to SGCE mutations. All cases initially presented with mild myoclonus affecting the upper limbs. Dystonia showed a progressive course, with increasing severity of symptoms and spreading from the cranio-cervical region to other sites. KCTD17 is abundantly expressed in all brain regions with the highest expression in the putamen. Weighted gene co-expression network analysis, based on mRNA expression profile of brain samples from neuropathologically healthy individuals, showed that KCTD17 is part of a putamen gene network, which is significantly enriched for dystonia genes. Functional annotation of the network showed an over-representation of genes involved in post-synaptic dopaminergic transmission. Functional studies in mutation bearing fibroblasts demonstrated abnormalities in endoplasmic reticulum-dependent calcium signaling. In conclusion, we demonstrate that the KCTD17 c.434 G>A p.(Arg145His) mutation causes autosomal dominant M-D. Further functional studies are warranted to further characterize the nature of KCTD17 contribution to the molecular pathogenesis of M-D.es_ES
dc.description.sponsorshipMedical Research Council UK (MRC) Wellcome Trust WT089698/Z/09/Zes_ES
dc.description.sponsorshipBachman-Strauss Dystonia Parkinsonism Foundationes_ES
dc.description.sponsorshipDepartment of Health's NIHR Biomedical Research Centeres_ES
dc.description.sponsorshipDystonia Medical Research Foundation (DMRF)es_ES
dc.description.sponsorshipHerman and Lilly Schilling Foundationes_ES
dc.description.sponsorshipReta Lila Weston Trustes_ES
dc.description.sponsorshipSpanish Governmentes_ES
dc.description.sponsorshipCei-BioTices_ES
dc.description.sponsorshipUniversity of Granadaes_ES
dc.description.sponsorshipAcademy of Medical Sciences (AMS) AMS-SGCL11-Pealles_ES
dc.description.sponsorshipMedical Research Council UK (MRC) MR/L501554/1 G1100643 MC_G1000735 MC_PC_09003 G0700943 MC_G0901330es_ES
dc.description.sponsorshipNational Institute for Health Research (NIHR) 2042 NF-SI-0513-10064 NF-SI-0507-10376es_ES
dc.description.sponsorshipParkinson's UK H-1006es_ES
dc.language.isoenges_ES
dc.publisherElsevieres_ES
dc.rightsAtribución 3.0 España*
dc.rights.urihttp://creativecommons.org/licenses/by/3.0/es/*
dc.titleA Missense Mutation in KCTD17 Causes Autosomal Dominant Myoclonus-Dystoniaes_ES
dc.typeinfo:eu-repo/semantics/articlees_ES
dc.rights.accessRightsinfo:eu-repo/semantics/openAccesses_ES
dc.identifier.doi10.1016/j.ajhg.2015.04.008
dc.type.hasVersioninfo:eu-repo/semantics/publishedVersiones_ES


Ficheros en el ítem

[PDF]
Nombre:
1-s2.0-S0002929715001457-main.pdf
Tamaño:
1.533Mb
Formato:
PDF

Este ítem aparece en la(s) siguiente(s) colección(ones)

Mostrar el registro sencillo del ítem

Atribución 3.0 España
Excepto si se señala otra cosa, la licencia del ítem se describe como Atribución 3.0 España