Affiliation:
1. Universidade Federal do Paraná, Brazil
2. University of Toronto, Canada
3. Laboratório Genetika, Brazil
Abstract
Spinocerebellar ataxia type 3 (SCA3) involves cerebellar, pyramidal, extrapyramidal, motor neuron and oculomotor systems with strong phenotypic heterogeneity, that lead us to classify the disorder into different clinical subtypes according to the predominantly affected motor systems. Method The series comprises 167 SCA3 patients belonging to 68 pedigrees, studied from 1989-2013. These patients were categorized into seven different subphenotypes. Results SCA3 cases were clustered according to the predominant clinical features. Three most common forms were subphenotype 2, characterized by ataxia and pyramidal symptom was observed in 67.5%, subphenotype 3 with ataxia and peripheral signs in 13.3%, and subphenotype 6 with pure cerebellar syndrome in 7.2%. Conclusion Our study was the first to systematically classify SCA3 into seven subphenotypes. This classification may be particularly useful for determination of a more specific and direct phenotype/genotype correlation in future studies.
Subject
Neurology,Clinical Neurology
Reference25 articles.
1. Autosomal dominant cerebellar ataxias: clinical features, genetics, and pathogenesis;Schols L;Lancet Neurol,2004
2. Spinocerebellar ataxias;Teive HAG;Arq Neuropsiquiatr,2009
3. Spinocerebellar ataxias: an update;Soong BW;Curr Opin Neurol,2007
4. Recent advances in degenerative ataxias;Klockgether T;Curr Opin Neurol,2000
5. A survey of spinocerebellar ataxia in South Brazil-66 new cases with Machado-Joseph disease, SCA7, SCA8, or unidentified disease-causing mutations;Jardim LB;J Neurol,2001
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