1. Identification and functional analysis of novel THAP1 mutations
- Author
-
Alev Erogullari, Christoph Kamm, Vladimir S. Kostic, Andreas Dendorfer, Jens Volkmann, Nils Uflacker, Marina Svetel, Alexander Schmidt, Norbert Brüggemann, Elena Moro, Eckart Altenmüller, Katja Lohmann, Andrea A. Kühn, Christine Klein, Andreas Ferbert, Susanne A. Schneider, Andreas Kupsch, Matthias Wittstock, Simone Zittel, Frank J. Kaiser, Alma Osmanovic, Alexander Münchau, Thora Lohnau, and Susen Winkler
- Subjects
Adult ,Male ,Untranslated region ,Adolescent ,Genotype ,Biology ,medicine.disease_cause ,Article ,Young Adult ,Gene Frequency ,Genetics ,medicine ,Humans ,Missense mutation ,Age of Onset ,Nuclear protein ,Mutation frequency ,Child ,Allele frequency ,Genetic Association Studies ,Genetics (clinical) ,Aged ,Dystonia ,Mutation ,Polymorphism, Genetic ,Nuclear Proteins ,Middle Aged ,medicine.disease ,Molecular biology ,DNA-Binding Proteins ,Protein Transport ,Child, Preschool ,Female ,Apoptosis Regulatory Proteins - Abstract
Mutations in THAP1 have been associated with dystonia 6 (DYT6). THAP1 encodes a transcription factor that represses the expression of DYT1. To further evaluate the mutational spectrum of THAP1 and its associated phenotype, we sequenced THAP1 in 567 patients with focal (n = 461), segmental (n = 68), or generalized dystonia (n = 38). We identified 10 novel variants, including six missense substitutions within the DNA-binding Thanatos-associated protein domain (Arg13His, Lys16Glu, His23Pro, Lys24Glu, Pro26Leu, Ile80Val), a 1bp-deletion downstream of the nuclear localization signal (Asp191Thrfs*9), and three alterations in the untranslated regions. The effect of the missense variants was assessed using prediction tools and luciferase reporter gene assays. This indicated the Ile80Val substitution as a benign variant. The subcellular localization of Asp191Thrfs*9 suggests a disturbed nuclear import for this mutation. Thus, we consider six of the 10 novel variants as pathogenic mutations accounting for a mutation frequency of 1.1%. Mutation carriers presented mainly with early onset dystonia (12 years in five of six patients). Symptoms started in an arm or neck and spread to become generalized in three patients or segmental in two patients. Speech was affected in four mutation carriers. In conclusion, THAP1 mutations are rare in unselected dystonia patients and functional analysis is necessary to distinguish between benign variants and pathogenic mutations.
- Published
- 2011
- Full Text
- View/download PDF