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Fine Mapping of the Gene for Carbohydrate-Deficient Glycoprotein Syndrome, Type I (CDG1): Linkage Disequilibrium and Founder Effect in Scandinavian Families
Authors:Cecilia Bjursell  Helena Stibler  Jan Wahlström  Bengt Kristiansson  Flemming Skovby  Petter Strömme  Gösta Blennow  Tommy Martinsson
Institution:aDepartment of Clinical Genetics, University of Gothenburg, East Hospital, S-41685, Gothenburg, Sweden;cDepartment of Pediatrics, University of Gothenburg, East Hospital, S-41685, Gothenburg, Sweden;bDepartment of Neurology, Karolinska Hospital, S-10401, Stockholm, Sweden;dDepartment of Clinical Genetics, Rigshospitalet, 2100, Copenhagen, Denmark;eDepartment of Pediatrics, Rikshospitalet, 0027, Oslo 1, Norway;fDepartment of Pediatrics, University Hospital, S-221 85, Lund, Sweden
Abstract:Carbohydrate-deficient glycoprotein syndrome type I (CDG I) is characterized clinically by severe nervous system involvement and biochemically by defects in the carbohydrate residues in a number of serum glycoproteins. The CDG1 gene was recently localized by us to a 13-cM interval in chromosome region 16p13. In this study 44 CDG I families from nine countries were analyzed with available markers in a region ranging from marker D16S495 to D16S497, and haplotype and linkage disequilibrium analyses were performed. One specific haplotype was found to be markedly overrepresented in CDG I patients from a geographically distinct region in Scandinavia, strongly indicating that CDG I families in this region share the same ancestral CDG1 mutation. Furthermore, analysis of the extent of the common haplotype in these families indicates that the CDG1 gene is located in the region defined by markers D16S513–AFMa284wd5–D16S768–D16S406–D16S502. The critical CDG1 region, in strong linkage disequilibrium with markers AFMa284wd5, D16S768, and D16S406, thus constitutes less than 1 Mb of DNA and less than 1 cM in the very distal part of the CDG1 region defined by us previously.
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