Linkage disequilibrium maps constructed with common SNPs are useful for first-pass disease association screens

P. Taillon-Miller, S. F. Saccone, N. L. Saccone, S. Duan, E. F. Kloss, E. G. Lovins, R. Donaldson, A. Phong, C. Ha, L. Flagstad, S. Miller, A. Drendel, D. Lind, R. D. Miller, J. P. Rice, P. Y. Kwok

Research output: Contribution to journalArticlepeer-review

18 Scopus citations

Abstract

To develop an efficient strategy for mapping genetic factors associated with common diseases, we constructed linkage disequilibrium (LD) maps of human chromosomes 5, 7, 17, and X. These maps consist of common single nucleotide polymorphisms at an average intermarker distance of 100 kb. The genotype data from these markers in a panel of American samples of European descent were analyzed to produce blocks of markers in strong pair-wise LD. Power calculations were used to guide block definitions and predicted that high-level LD maps would be useful in initial genome scans for susceptibility alleles in case-control association studies of complex diseases. As anticipated, LD blocks on the X chromosome were larger and covered more of the chromosome than those found on the autosomes.

Original languageEnglish
Pages (from-to)899-912
Number of pages14
JournalGenomics
Volume84
Issue number6
DOIs
StatePublished - Dec 2004

Keywords

  • Genomics
  • Linkage disequilibrium
  • Polymorphism
  • Sample size
  • Single nucleotide

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