Abstract

Development and application of mathematical and statistical methods for the genetic analysis of complex human traits is proposed. In particular, the primary focus is on developing methods for understanding complex patterns of inheritance through genetic linkage markers. The advent of restriction fragment length polymorphisms (RFLP's) spanning the entire genome now offers the power to achieve such analysis. Specifically, we intend to: elaborate models of inheritance involving multiple loci (for example, epistasis and genetic heterogeneity model); determine the power of detecting linkage for such complex models; determine the ability to establish complex patterns of inheritance with multiple linked markers. We will also examine variable age of onset as a potential indicator of genetic heterogeneity, and its impact on a linkage analysis. Finally, we will examine the application of linkage analysis for multivariate traits, and determine the power of linkage to explain genetic sources of correlation among traits. The methods that are developed will be applied to three major data sets. First, multivariate data including family history on idiopathic torsion dystonia will be examined with the goal of establishing genetic heterogeneity; this will have important ramifications for proposed family and linkage studies. Second, a large sample of family data on breast cancer (4700 probands) will be examined to determine the possibility of genetic heterogeneity as determined by age of onset and possibly other risk factors; these results will impact on linkage analyses of breast cancer. Third, an extensive set of data on immune response to twelve pneumococcal antigens and HLA, Gm and Km in South American Indian families will be analyzed from a multivariate-genetic standpoint to determine genetic patterns of correlation. The role of HLA, Gm and Km in the familial patterns will be determined. It is anticipated that the methods developed will have broad applicability beyond the specific projects described above. The results of this project will be of significant clinical and public health importance because they will offer a better understanding of disease etiology and the (possibly complex) genetic contribution to it, as well as provide avenues for treatment design, prevention, and accurate risk assessment.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Human Genome Research Institute (NHGRI)
Type
Research Project (R01)
Project #
5R01HG000348-04
Application #
3333489
Study Section
Special Emphasis Panel (SSS (E))
Project Start
1988-09-30
Project End
1993-08-31
Budget Start
1991-09-01
Budget End
1992-08-31
Support Year
4
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Yale University
Department
Type
Schools of Medicine
DUNS #
082359691
City
New Haven
State
CT
Country
United States
Zip Code
06520

  Publications

Spiker, D; Lotspeich, L J; Dimiceli, S et al. (2001) Birth order effects on nonverbal IQ scores in autism multiplex families. J Autism Dev Disord 31:449-60
Klein, C; Vieregge, P; Hagenah, J et al. (1999) Search for the PARK3 founder haplotype in a large cohort of patients with Parkinson's disease from northern Germany. Ann Hum Genet 63:285-91
Teng, J; Risch, N (1999) The relative power of family-based and case-control designs for linkage disequilibrium studies of complex human diseases. II. Individual genotyping. Genome Res 9:234-41
Klein, C; Ozelius, L J; Hagenah, J et al. (1998) Search for a founder mutation in idiopathic focal dystonia from Northern Germany. Am J Hum Genet 63:1777-82
Klein, C; Brin, M F; de Leon, D et al. (1998) De novo mutations (GAG deletion) in the DYT1 gene in two non-Jewish patients with early-onset dystonia. Hum Mol Genet 7:1133-6
Risch, N; Teng, J (1998) The relative power of family-based and case-control designs for linkage disequilibrium studies of complex human diseases I. DNA pooling. Genome Res 8:1273-88
Andrews, C; Devlin, B; Perlin, M et al. (1997) Binning clones by hybridization with complex probes: statistical refinement of an inner product mapping method. Genomics 41:141-54
Wildenauer, D B; Hallmayer, J; Schwab, S G et al. (1996) Searching for susceptibility genes in schizophrenia by genetic linkage analysis. Cold Spring Harb Symp Quant Biol 61:845-50
Zhang, H; Risch, N (1996) Mapping quantitative-trait loci in humans by use of extreme concordant sib pairs: selected sampling by parental phenotypes. Am J Hum Genet 59:951-7
Risch, N J; Zhang, H (1996) Mapping quantitative trait loci with extreme discordant sib pairs: sampling considerations. Am J Hum Genet 58:836-43

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