GAA repeat polymorphism in Turkish Friedreich's ataxia patients


Yilmaz M. B., Koc A. F., Kasap H., Guzel A. I., Sarica Y., Suleymanova D.

INTERNATIONAL JOURNAL OF NEUROSCIENCE, vol.116, no.5, pp.565-574, 2006 (SCI-Expanded) identifier identifier identifier

Abstract

Friedreich's ataxia ( FRDA), the most common subtype of early onset hereditary spinocerebellar ataxia ( SCA), is an autosomal recessive neurodegenerative disorder caused by unstable GAA tri- nucleotide expansions in the first intron of FRDA gene located at 9q13- q21.1 position. Results of GAA repeat polymorphism in 80 Turkish SCA patients and 38 family members of 11 typical FRDA patients were reported. GAA triplet repeat size ranged from similar to 7 to 34 in normal alleles and from similar to 66 to 1300 in mutant alleles. Twenty six patients were homozygous for GAA expansion and size of expanded alleles differed from similar to 425 to 1300 repeats. Children 2 and 6 years old ( showing no ataxia symptoms) of one family had homozygous GAA expansions reaching similar to 925 repeats. All 11 families studied had at least 1 afflicted child and 9 parents and 2 siblings were carrier ( heterozygous) with mutant alleles ranging from 66 to 850 repeats. Family studies confirmed the meiotic instability and stronger effect of expansion in the smaller alleles on phenotype and a negative correlation between GAA repeat expansion size and onset- age of the disease.