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The mosaic structure of variation in the laboratory mouse genome

Author

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  • Claire M. Wade

    (Whitehead Institute for Biomedical Research and Whitehead/MIT Center for Genome Research
    The University of Queensland)

  • Edward J. Kulbokas

    (Whitehead Institute for Biomedical Research and Whitehead/MIT Center for Genome Research)

  • Andrew W. Kirby

    (Whitehead Institute for Biomedical Research and Whitehead/MIT Center for Genome Research)

  • Michael C. Zody

    (Whitehead Institute for Biomedical Research and Whitehead/MIT Center for Genome Research)

  • James C. Mullikin

    (The Sanger Centre, The Wellcome Trust Genome Campus)

  • Eric S. Lander

    (Whitehead Institute for Biomedical Research and Whitehead/MIT Center for Genome Research)

  • Kerstin Lindblad-Toh

    (Whitehead Institute for Biomedical Research and Whitehead/MIT Center for Genome Research)

  • Mark J. Daly

    (Whitehead Institute for Biomedical Research and Whitehead/MIT Center for Genome Research)

Abstract

Most inbred laboratory mouse strains are known to have originated from a mixed but limited founder population in a few laboratories1,2. However, the effect of this breeding history on patterns of genetic variation among these strains and the implications for their use are not well understood. Here we present an analysis of the fine structure of variation in the mouse genome, using single nucleotide polymorphisms (SNPs). When the recently assembled genome sequence from the C57BL/6J strain3 is aligned with sample sequence from other strains, we observe long segments of either extremely high (∼40 SNPs per 10 kb) or extremely low (∼0.5 SNPs per 10 kb) polymorphism rates. In all strain-to-strain comparisons examined, only one-third of the genome falls into long regions (averaging >1 Mb) of a high SNP rate, consistent with estimated divergence rates between Mus musculus domesticus and either M. m. musculus or M. m. castaneus. These data suggest that the genomes of these inbred strains are mosaics with the vast majority of segments derived from domesticus and musculus sources. These observations have important implications for the design and interpretation of positional cloning experiments.

Suggested Citation

  • Claire M. Wade & Edward J. Kulbokas & Andrew W. Kirby & Michael C. Zody & James C. Mullikin & Eric S. Lander & Kerstin Lindblad-Toh & Mark J. Daly, 2002. "The mosaic structure of variation in the laboratory mouse genome," Nature, Nature, vol. 420(6915), pages 574-578, December.
  • Handle: RePEc:nat:nature:v:420:y:2002:i:6915:d:10.1038_nature01252
    DOI: 10.1038/nature01252
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