Deep congenic analysis identifies many strong, context-dependent QTLs, one of which, Slc35b4, regulates obesity and glucose homeostasis

  1. Joseph H Nadeau4,5
  1. 1 American University of Beirut;
  2. 2 University of Michigan;
  3. 3 CWRU;
  4. 4 Institute for Systems Biology
  1. * Corresponding author; email: jnadeau{at}systemsbiology.org

Abstract

Although central to many studies of phenotypic variation and disease susceptibility, characterizing the genetic architecture of complex traits has been unexpectedly difficult. For example, most of the susceptibility genes that contribute to highly heritable conditions such as obesity and type 2 diabetes (T2D) remain to be identified despite intensive study. We took advantage of mouse models of diet-induced metabolic disease in chromosome substitution strains (CSSs) both to characterize the genetic architecture of diet-induced obesity and glucose homeostasis, and to test feasibility of gene discovery. Beginning with a survey of CSSs, followed with genetic and phenotypic analysis of congenic, subcongenic and subsubcongenic strains, we identified a remarkable number of closely linked, phenotypically heterogeneous quantitative trait loci (QTLs) on mouse chromosome 6 that have unexpectedly large phenotypic effects. Although fine-mapping reduced the genomic intervals and gene content of these QTLs over 3,000-fold, the average phenotypic effect on body weight was reduced less than 3-fold, highlighting the 'fractal' nature of genetic architecture in mice. Despite this genetic complexity, we found evidence for 14 QTLs in only 32 recombination events in less than 3000 mice, and with an average of four genes located within the three body weight QTLs in the subsubcongenic strains. For Obrq2a1, genetic and functional studies collectively identified the solute receptor Slc35b4 as a regulator of obesity, insulin resistance, and gluconeogenesis. This work demonstrated the unique power of CSSs as a platform for studying complex genetic traits and identifying QTLs.

  • Received January 13, 2011.
  • Accepted April 12, 2011.

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  1. Published in Advance April 19, 2011, doi: 10.1101/gr.120741.111 Genome Res. gr.120741.111 Copyright © 2011, Cold Spring Harbor Laboratory Press

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