1. Founder effect in a Belgian-Dutch fragile X population.
- Author
-
Buyle S, Reyniers E, Vits L, De Boulle K, Handig I, Wuyts FL, Deelen W, Halley DJ, Oostra BA, and Willems PJ
- Subjects
- Alleles, Belgium epidemiology, Chi-Square Distribution, Female, Fragile X Syndrome epidemiology, Humans, Linkage Disequilibrium, Male, Molecular Epidemiology, Mutation, Netherlands epidemiology, Prevalence, Repetitive Sequences, Nucleic Acid, Fragile X Syndrome ethnology, Fragile X Syndrome genetics, Gene Frequency
- Abstract
For many years, the high prevalence of the fragile X syndrome was thought to be caused by a high mutation frequency. The recent isolation of the FMR1 gene and identification of the most prevalent mutation enable a more precise study of the fragile X mutation. As the vast majority of fragile X patients show amplification of an unstable trinucleotide repeat, DNA studies can now trace back the origin of the fragile X mutation. To date, de novo mutations leading to amplification of the CGG repeat have not yet been detected. Recently, linkage disequilibrium was found in the Australian and US populations between the fragile X mutation and adjacent polymorphic markers, suggesting a founder effect of the fragile X mutation. We present here a molecular study of Belgian and Dutch fragile X families. No de novo mutations could be found in 54 of these families. Moreover, we found significant (P < 0.0001) linkage disequilibrium in 68 unrelated fragile X patients between the fragile X mutation and an adjacent polymorphic microsatellite at DXS548. This suggests that a founder effect of the fragile X mutation also exists in the Belgian and Dutch populations. Both the absence of new mutations and the presence of linkage disequilibrium suggest that a few ancestral mutations are responsible for most of the patients with fragile X syndrome.
- Published
- 1993
- Full Text
- View/download PDF