The molecular diagnosis of spinocerebellar ataxia type 1 in patients with ataxia

Abstract

Spinocerebellar ataxia type 1 (SCA1) is an autosomal dominant neurodegenerative disease caused by an expanded CAG trinucleotide repeat in the SCA1 gene on chromosome 6. We screened 40 probands with ataxia for the CAG repeat expansion and found five probands with SCA1 representing five different families. The SCA1 gene was analysed in 50 members of these families, and the CAG repeat expansion was found in all 17 affected persons and in 14 unaffected at‐risk individuals. The range of expansion was 41–53 repeat units, while the range of normal alleles was 22–36 repeat units. We found pronounced inter‐ and intrafamilial phenotypical variation. One of the families had a comparatively mild phenotype which correlates with a CAG repeat length in the low end of the range of expansions and a late age at onset. With few exceptions, normal alleles of the SCA1 gene have one to three CAT interruptions in the middle of the CAG repeat, while all expanded alleles are uninterrupted. We report the hitherto longest normal uninterrupted allele of 22 repeat units and stress the importance of analysis for the presence of CAT interruptions in the diagnosis of SCA1.