An integrated haplotype map of the human major histocompatibility complex

Author:

Walsh, E. C.

Mather, K. A.

Schaffner, S. F.

Farwell, L.

Daly, M. J.

Patterson, N.

Cullen, M.

Carrington, M.

Bugawan, T. L.

Erlich, H.

Campbell, J.

Barrett, J.

Miller, K.

Thomson, G.

Lander, E. S.

Rioux, J. D.
Author Address

MIT, Whitehead Inst, Ctr Genome Res, 1 Kendall Sq,Bldg 300, Cambridge, MA 02139 USA Whitehead Inst Biomed Res, Ctr Genome Res, Cambridge, MA 02142 USA Univ Calif Berkeley, Dept Integrat Biol, Berkeley, CA 94720 USA NCI, Basic Res Program, Sci Applicat Int Corp, Lab Genom Divers, Frederick, MD 21701 USA Roche Mol Syst, Dept Human Genet, Alameda, CA USA Rioux JD MIT, Whitehead Inst, Ctr Genome Res, 1 Kendall Sq,Bldg 300, Cambridge, MA 02139 USA

Abstract:

Numerous studies have clearly indicated a role for the major histocompatibility complex (MHC) in susceptibility to autoimmune diseases. Such studies have focused on the genetic variation of a small number of classical human-leukocyte- antigen (HLA) genes in the region. Although these genes represent good candidates, given their immunological roles, linkage disequilibrium (LD) surrounding these genes has made it difficult to rule out neighboring genes, many with immune function, as influencing disease susceptibility. It is likely that a comprehensive analysis of the patterns of LD and variation, by using a high-density map of single-nucleotide polymorphisms ( SNPs), would enable a greater understanding of the nature of the observed associations, as well as lead to the identification of causal variation. We present herein an initial analysis of this region, using 201 SNPs, nine classical HLA loci, two TAP genes, and 18 microsatellites. This analysis suggests that LD and variation in the MHC, aside from the classical HLA loci, are essentially no different from those in the rest of the genome. Furthermore, these data show that multi-SNP haplotypes will likely be a valuable means for refining association signals in this region.

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