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Genetic diversity within the R408W phenylketonuria mutation lineages in Europe
Authors:Tighe Orna  Dunican Donncha  O'Neill Charles  Bertorelle Giorgio  Beattie Diane  Graham Colin  Zschocke Johannes  Cali Francesco  Romano Valentino  Hrabincova Eva  Kozak Libor  Nechyporenko Marina  Livshits Ludmilla  Guldberg Per  Jurkowska Monika  Zekanowski Cezary  Perez Belen  Desviat Lourdes Ruiz  Ugarte Magdalena  Kucinskas Vaidutis  Knappskog Per  Treacy Eileen  Naughten Eileen  Tyfield Linda  Byck Susan  Scriver Charles R  Mayne Philip D  Croke David T
Affiliation:Department of Pathology and National Centre for Newborn Screening, The Children's University Hospital, Dublin, Ireland.
Abstract:The R408W phenylketonuria mutation in Europe has arisen by recurrent mutation in the human phenylalanine hydroxylase (PAH) locus and is associated with two major PAH haplotypes. R408W-2.3 exhibits a west-to-east cline of relative frequency reaching its maximum in the Balto-Slavic region, while R408W-1.8 exhibits an east-to-west cline peaking in Connacht, the most westerly province of Ireland. Spatial autocorrelation analysis has demonstrated that the R408W-2.3 cline, like that of R408W-1.8, is consistent with a pattern likely to have been established by human dispersal. Genetic diversity within wild-type and R408W chromosomes in Europe was assessed through variable number tandem repeat (VNTR) nucleotide sequence variation and tetranucleotide short tandem repeat (STR) allelic associations. Wild-type VNTR-8 chromosomes exhibited two major cassette sequence organizations: (a1)5-b3-b2-c1 and (a1)5-b5-b2-c1. R408W-1.8 was predominantly associated with (a1)5-B5-B2-C1. Both wild-type vntr-3 and r408w-2.3 chromosomes exhibited a single invariant cassette sequence organization, a2-b2-c1. STR allele distributions associated with the cassette variants were consistent with greater diversity in the wild-type VNTR-8 lineage and were suggestive of different levels of diversity between R408W-1.8 and R408W-2.3. The finding of greater genetic diversity within the wild-type VNTR-8 lineage compared to VNTR-3 suggests that VNTR-8 may be older within the European population. However, in the absence of a more extensive STR data-set, no such conclusions are possible for the respective R408W mutant lineages.
Keywords:phenylketonuria  PKU  phenylalanine hydroxylase  PAH  Europe  population genetics  VNTR  STR
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