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Publication : Fine mapping of polymorphic alcohol-related quantitative trait loci candidate genes using interval-specific congenic recombinant mice.

First Author  Ehringer MA Year  2002
Journal  Alcohol Clin Exp Res Volume  26
Issue  11 Pages  1603-8
PubMed ID  12436047 Mgi Jnum  J:80012
Mgi Id  MGI:2429399 Doi  10.1097/01.ALC.0000036921.33411.67
Citation  Ehringer MA, et al. (2002) Fine mapping of polymorphic alcohol-related quantitative trait Loci candidate genes using interval-specific congenic recombinant mice. Alcohol Clin Exp Res 26(11):1603-8
abstractText  BACKGROUND The inbred long-sleep (ILS) and inbred short-sleep (ISS) strains of mice are widely studied as a model of initial sensitivity to alcohol. Recently, a large comparative DNA sequencing study of candidate genes located within the four quantitative trait loci (QTLs) associated with the ethanol-induced loss of righting reflex in ILS and ISS mice has identified eight genes that contain coding region differences corresponding to amino acid changes. Here, recently developed interval-specific congenic recombinant mice (ISCRs) have been used to map these genes in relationship to newly narrowed QTL regions.METHODS Regions of candidate genes containing DNA differences corresponding to previously identified amino acid changes between ISS and ILS mice were amplified from either genomic DNA or complementary DNA from ISCR mice using polymerase chain reaction. The products were purified and directly sequenced to determine the genotypes for each polymorphism. On the basis of these genotypic data, each candidate gene was determined to be located either within or outside of recently narrowed QTL intervals.RESULTS Of these eight candidates with protein-coding differences, five are now excluded from their respective intervals. The other three (, and ) have been localized to the narrowed QTL intervals.CONCLUSIONS These three central nervous system genes (, and ) represent promising candidates for involvement in the differential sensitivity to alcohol exhibited between ILS and ISS mice. This study also demonstrates how the combination of high-throughput comparative gene sequencing and concomitant genetic fine mapping of QTL regions with ISCRs can be an effective tool for accelerating the process of moving from QTL to gene.
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