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Publication year
2010Source
Movement Disorders, 25, 14, (2010), pp. 2420-7ISSN
Publication type
Article / Letter to editor
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Organization
Neurology
Journal title
Movement Disorders
Volume
vol. 25
Issue
iss. 14
Page start
p. 2420
Page end
p. 7
Subject
DCN 2: Functional NeurogenomicsAbstract
Mutations in THAP1, a gene encoding a nuclear pro-apoptotic protein, have been associated with DYT6 dystonia. First reports on the phenotype of DYT6 dystonia show an early onset dystonia with predominant cranio-cervical and laryngeal involvement. Here we assessed the frequency and phenotype of THAP1 mutation carriers in a large Dutch cohort of adult-onset (>/=26 years) dystonia (n = 388) and early-onset dystonia (n = 67) patients. We describe the phenotype of DYT6 dystonia patients and their response on GPi DBS. Overall, 3 nonsynonymous heterozygous mutations were detected in the early-onset group (4.5%). Two DYT6 families were identified, showing a heterozygous phenotype. All patients had segmental or generalized dystonia, often associated with profound oromandibular and laryngeal involvement. No nonsynonymous mutations were found in patients with adult-onset focal dystonia. Rare synonymous variants were identified in conserved regions of THAP1, two in the adult-onset cervical dystonia group and one in the control group. Four DYT6 dystonia patients were treated with GPi DBS with moderate to good response on motor function but marginal benefit on speech.
This item appears in the following Collection(s)
- Academic publications [246515]
- Electronic publications [134121]
- Faculty of Medical Sciences [93308]
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