The GAA triplet-repeat sequence in Friedreich ataxia shows a high level of somatic instability in vivo, with a significant predilection for large contractions

doi:10.1093/hmg/11.18.2175

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Human Molecular Genetics, 2002, Vol. 11, No. 18 2175-2187
© 2002 Oxford University Press

The GAA triplet-repeat sequence in Friedreich ataxia shows a high level of somatic instability in vivo, with a significant predilection for large contractions

Rajesh Sharma¹, Saeeda Bhatti¹, Mariluz Gomez¹, Rhonda M. Clark¹, Cynthia Murray³, Tetsuo Ashizawa⁴^,5 and Sanjay I. Bidichandani¹^,2^,*

¹Department of Biochemistry and Molecular Biology, and ²Department of Pediatrics, University of Oklahoma Health Sciences Center, Oklahoma City, OK, USA, ³Department of Mathematics and Statistics, University of Central Oklahoma, Edmond, OK, USA, and ⁴Department of Neurology and ⁵VA Medical Center, Baylor College of Medicine, Houston, TX, USA

Received May 14, 2002; Accepted June 28, 2002

Friedreich ataxia is commonly caused by large expansions ofa GAA triplet-repeat (GAA-TR) sequence in the first intron ofthe FRDA gene. We used small-pool PCR to analyze somatic variabilityamong 7190 individual FRDA molecules from peripheral blood DNAof subjects carrying 12 different expanded alleles, rangingin size from 241 to 1105 triplets. Expanded alleles showed alength-dependent increase in somatic variability, with mutationloads ranging from 47% to 78%. We noted a strong contractionbias among long alleles (>500 triplets), which showed a 4-foldhigher frequency of large contractions versus expansions. Somecontractions were very large; of all somatic mutations scored, $~$ 5% involved contractions of >50% of the original allele length,and 0.29% involved complete reversion to the normal/premutationlength ( $<=$ 60 triplets). These observations contrast sharply withthe strong expansion bias seen in expanded CTG triplet repeatsin myotonic dystrophy. No somatic variability was detected in>6000 individual FRDA molecules analyzed from 15 normal alleles(8–25 triplets). A premutation allele with 44 uninterruptedGAA repeats was found to be unstable, ranging in size from 6to 113 triplets, thus establishing the threshold for somaticinstability between 26 and 44 GAA triplets. Analysis of an additional7850 FRDA molecules from serially passaged lymphoblastoid celllines carrying nine expanded alleles (132–933 triplets)showed very low mutation loads, ranging from 0% to 6.2%. Ourdata indicate that expanded GAA-TR alleles in Friedreich ataxiaare highly mutable and have a natural tendency to contract invivo, and that these properties depend on multiple factors,including DNA sequence, triplet-repeat length and unknown cell-type-specificfactors.

^* To whom correspondence should be addressed at: Department ofBiochemistry and Molecular Biology, University of Oklahoma HealthSciences Center, 975 N.E., 10th, BRC458, Oklahoma City, OK 73104,USA. Tel: +1 4052711360; Fax: +1 4052713910; Email: sanjay-bidichandani{at}ouhsc.edu

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