BMC Genetics (Apr 2007)

A single nucleotide mutation in <it>Nppc </it>is associated with a long bone abnormality in <it>lbab </it>mice

  • Roe Bruce A,
  • Li Xinmin,
  • Donahue Leah,
  • Yang HongBin,
  • Yan Jian,
  • Jiao Feng,
  • Jiao Yan,
  • Stuart John,
  • Gu Weikuan

DOI
https://doi.org/10.1186/1471-2156-8-16
Journal volume & issue
Vol. 8, no. 1
p. 16

Abstract

Read online

Abstract Background The long bone abnormality (lbab) mouse is a new autosomal recessive mutant characterized by overall smaller body size with proportionate dwarfing of all organs and shorter long bones. Previous linkage analysis has located the lbab mutation on chromosome 1 between the markers D1Mit9 and D1Mit488. Results A genome-based positional approach was used to identify a mutation associated with lbab disease. A total of 122 genes and expressed sequence tags at the lbab region were screened for possible mutation by using genomic DNA from lbabl/lbab, lbab/+, and +/+ B6 mice and high throughput temperature gradient capillary electrophoresis. A sequence difference was identified in one of the amplicons of gene Nppc between lbab/lbab and +/+ mice. One-step reverse transcriptase polymerase chain reaction was performed to validate the difference of Nppc in different types of mice at the mRNA level. The mutation of Nppc was unique in lbab/lbab mice among multiple mouse inbred strains. The mutation of Nppc is co-segregated with lbab disease in 200 progenies produced from heterozygous lbab/+ parents. Conclusion A single nucleotide mutation of Nppc is associated with dwarfism in lbab/lbab mice. Current genome information and technology allow us to efficiently identify single nucleotide mutations from roughly mapped disease loci. The lbab mouse is a useful model for hereditary human achondroplasia.