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Quality assessment of whole genome mapping data in the refined familial spastic paraplegia interval on chromosome 14q
Authors:C Paternotte  D Rudnicki  C Fizames  CS Davoine  D Mavel  A Dürr  D Samson  C Marquette  D Muselet  N Vega-Czarny  N Drouot  T Voit  B Fontaine  G Gyapay  G Auburger  J Weissenbach  J Hazan
Affiliation:URA CNRS 1922, Généthon, 91000 Evry, France.
Abstract:Autosomal dominant familial spastic paraplegia (AD-FSP) is a genetically heterogeneous neurodegenerative disorder characterized by progressive spasticity of the lower limbs. Three loci on chromosome 14q (SPG3), 2p (SPG4), and 15q (SPG6) were shown to be responsible for AD-FSP. Analysis of recombination events in three SPG3-linked families allowed us to narrow the critical interval from 9 to 5 cM. An approximately 5-Mb YAC contig comprising 32 clones and 90 STSs was built from D14S301 to D14S991, encompassing this region of 14q21. Fifty-six ESTs assigned previously to this region with radiation hybrid (RH) panels Genebridge 4 and G3 were precisely localized on the YAC contig. The 90 STSs positioned on the contig were tested on the TNG RH panel to compare our YAC-based map with an RH map at a high level of resolution. Comparison between our map and the whole genome mapping data on this interval of chromosome 14q is discussed.
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