Linkage to chromosome 1p36 for attention-deficit/hyperactivity disorder traits in school and home settings.

نویسندگان

  • Kaixin Zhou
  • Philip Asherson
  • Pak Sham
  • Barbara Franke
  • Richard J L Anney
  • Jan Buitelaar
  • Richard Ebstein
  • Michael Gill
  • Keeley Brookes
  • Cathelijne Buschgens
  • Desmond Campbell
  • Wai Chen
  • Hanna Christiansen
  • Ellen Fliers
  • Isabel Gabriëls
  • Lena Johansson
  • Rafaela Marco
  • Fernando Mulas
  • Ueli Müller
  • Aisling Mulligan
  • Benjamin M Neale
  • Fruhling Rijsdijk
  • Nanda Rommelse
  • Henrik Uebel
  • Lamprini Psychogiou
  • Xiaohui Xu
  • Tobias Banaschewski
  • Edmund Sonuga-Barke
  • Jacques Eisenberg
  • Iris Manor
  • Ana Miranda
  • Robert D Oades
  • Herbert Roeyers
  • Aribert Rothenberger
  • Joseph Sergeant
  • Hans-Christoph Steinhausen
  • Eric Taylor
  • Margaret Thompson
  • Stephen V Faraone
چکیده

BACKGROUND Limited success has been achieved through previous attention-deficit/hyperactivity disorder (ADHD) linkage scans, which were all designed to map genes underlying the dichotomous phenotype. The International Multi-centre ADHD Genetics (IMAGE) project performed a whole genome linkage scan specifically designed to map ADHD quantitative trait loci (QTL). METHODS A set of 1094 single selected Caucasian ADHD nuclear families was genotyped on a highly accurate and informative single nucleotide polymorphism (SNP) panel. Two quantitative traits measuring the children's symptoms in home and school settings were collected and standardized according to a population sample of 8000 children to reflect the developmental nature and gender prevalence difference of ADHD. Univariate linkage test was performed on both traits and their mean score. RESULTS A significant common linkage locus was found at chromosome 1p36 with a locus-specific heritability of 5.1% and a genomewide empirical p < .04. Setting-specific suggestive linkage signals were also found: logarithm of odds (LOD) = 2.2 at 9p23 for home trait and LOD = 2.6 at 11q21 for school trait. CONCLUSIONS These results indicate that given large samples with proper phenotypic measures, searching for ADHD genes with a QTL strategy is an important alternative to using the clinical diagnosis. The fact that our linkage region 1p36 overlaps with the dyslexia QTL DYX8 further suggests it is potentially a pleiotropic locus for ADHD and dyslexia.

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عنوان ژورنال:
  • Biological psychiatry

دوره 64 7  شماره 

صفحات  -

تاریخ انتشار 2008