Abstract

Complex disorders arise from the actions and interaction of many genetic and non-genetic factors. Such disorders, including asthma, diabetes, cardiovascular disease, and psychiatric disorders, account for a huge proportion of public health care expenditures, and yet we remain largely ignorant of their basic defects. The identification of genetic variation influencing susceptibility to complex disorders would yield a better understanding of the basic defects, leading to more effective and specific treatments, and would also improve our ability to identify and characterize non-genetic risk factors that might prove cost-effective targets for prevention strategies. It is clear, however, that the paradigms that were used so successfully in the identification of genes for simple, Mendelian disorders must be modified for studies in complex disorders. In our initial cycle of funding, we proposed to develop approaches for the identification of genetic variation affecting susceptibility to complex disorders at three levels of resolution: linkage mapping, fine-scale linkage disequilibrium (LD) mapping, and positional cloning. We have published manuscripts describing approaches we developed at each of these levels of resolution and have made the resulting software freely available. These published manuscripts include description of an approach for identifying and characterizing gene-gene interaction in the context of robust multipoint linkage analysis (Cox et al., 1999), description of a likelihood-based method of LD mapping using the Decay in Haplotype Sharing (DHS) (McPeek and Strahs, 1999), and description of approaches for the analytic component to the positional cloning of complex disorders (Horikawa et al., 2000). We now propose to extend these studies.
Our specific aims are: (1) To extend the approaches we have developed for identifying and characterizing gene-gene interactions between unlinked regions to enable us to better model gene-gene and gene-environment interaction within the framework of robust, allele-sharing methods for multipoint linkage analysis; (2) To extend the DHS approach with (a) development of improved models of background LD that can be utilized in these analyses and (b) development of computationally-feasible algorithms that allow the use of genotypes in unrelated individuals (rather than unambiguously established haplotypes); and (3) To develop robust, flexible approaches that test whether genetic variation adequately accounts for the evidence for linkage in the context of realistically complex molecular genetic models. Our long-term research goal is to provide a robust statistical and analytic framework that can be integrated with molecular genetic studies to identify genetic variation influencing complex phenotypes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK055889-05
Application #
6524370
Study Section
Genome Study Section (GNM)
Program Officer
Mckeon, Catherine T
Project Start
1998-09-30
Project End
2005-08-31
Budget Start
2002-09-01
Budget End
2003-08-31
Support Year
5
Fiscal Year
2002
Total Cost
$264,250
Indirect Cost

  Institution

Name
University of Chicago
Department
Genetics
Type
Schools of Medicine
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Kawai, Toshihide; Ng, Maggie C Y; Hayes, M Geoffrey et al. (2009) Variation in the perilipin gene (PLIN) affects glucose and lipid metabolism in non-Hispanic white women with and without polycystic ovary syndrome. Diabetes Res Clin Pract 86:186-92
Hayes, M Geoffrey; Pluzhnikov, Anna; Miyake, Kazuaki et al. (2007) Identification of type 2 diabetes genes in Mexican Americans through genome-wide association studies. Diabetes 56:3033-44
Wittke-Thompson, Jacqueline K; Ambrose, Nicoline; Yairi, Ehud et al. (2007) Genetic studies of stuttering in a founder population. J Fluency Disord 32:33-50
Pan, Lin; Ober, Carole; Abney, Mark (2007) Heritability estimation of sex-specific effects on human quantitative traits. Genet Epidemiol 31:338-47
Tong, Liping; Mets, Laurens; McPeek, Mary Sara (2007) Likelihood-based inference for multi-color optical mapping. Stat Appl Genet Mol Biol 6:Article5
Voight, Benjamin F; Kudaravalli, Sridhar; Wen, Xiaoquan et al. (2006) A map of recent positive selection in the human genome. PLoS Biol 4:e72
Kurz, Thorsten; Hoffjan, Sabine; Hayes, M Geoffrey et al. (2006) Fine mapping and positional candidate studies on chromosome 5p13 identify multiple asthma susceptibility loci. J Allergy Clin Immunol 118:396-402
Achkar, Jean-Paul; Dassopoulos, Themistocles; Silverberg, Mark S et al. (2006) Phenotype-stratified genetic linkage study demonstrates that IBD2 is an extensive ulcerative colitis locus. Am J Gastroenterol 101:572-80
Nicolae, Dan L; Wu, Xiaolin; Miyake, Kazuaki et al. (2006) GEL: a novel genotype calling algorithm using empirical likelihood. Bioinformatics 22:1942-7
Nicolae, Dan L; Wen, Xiaoquan; Voight, Benjamin F et al. (2006) Coverage and characteristics of the Affymetrix GeneChip Human Mapping 100K SNP set. PLoS Genet 2:e67

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