Analysis of FMR1 (CGG)(n) alleles and FRAXA microsatellite haplotypes in the population of Greenland: Implications for the population of the New World from Asia

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Abstract

The fragile X syndrome is caused by the expansion of a polymorphic (CGG)(n) tract in the promoter region of the FMR1 gene. Apparently the incidence of fragile X syndrome is rare in the population of Greenland. In order to examine population-related factors involved in stability of the (CGG)(n) sequence, DNA samples obtained randomly from the Greenlandic population were analysed for size and AGG interspersion pattern of the FMR1 (CGG)(n) region and associated DXS548-FRAXAC1 haplotypes. In addition a large Greenland family with unstable transmission in the premutation range was analysed. The (CGG)(n) allele sizes in the Greenland population showed a narrow distribution similar to that reported for Asian populations. DNA sequencing of alleles with 36 CGG repeats revealed an AGG(CGG)6 insertion previously reported exclusively in Asian populations and a high frequency of alleles with a (CGG)10AGG(CGG)9AGG(CGG)9 or (CGG)9AGG(CGG)9AGG(CGG)6AGG(CGG)9 sequence pattern was found. Thus the data confirm the Asian origin of the Greenlandic (Eskimo) population and indicates that some (CGG)(n) alleles have remained stable for 15-30,000 years, since the population of the New World arrived from Asia via the Bering Strait.

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Larsen, L. A., Armstrong, J. S. M., Grønskov, K., Hjalgrim, H., Brøndum-Nielsen, K., Hasholt, L., … Vuust, J. (1999). Analysis of FMR1 (CGG)(n) alleles and FRAXA microsatellite haplotypes in the population of Greenland: Implications for the population of the New World from Asia. European Journal of Human Genetics, 7(7), 771–777. https://doi.org/10.1038/sj.ejhg.5200374

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