A First-generation Linkage Disequilibrium Map of Human Chromosome 22

Overview

Journal Nature

Specialty Science

Date 2002 Jul 12

PMID 12110843

Citations 134

Authors

Elisabeth Dawson

Goncalo R Abecasis

Suzannah Bumpstead

Yuan Chen

Sarah Hunt

David M Beare

Jagjit Pabial

Thomas Dibling

Emma Tinsley

Susan Kirby

David Carter

Marianna Papaspyridonos

Simon Livingstone

Rocky Ganske

Elin Lohmussaar

Jana Zernant

Neeme Tonisson

Maido Remm

Reedik Magi

Tarmo Puurand

Jaak Vilo

Ants Kurg

Kate Rice

Panos Deloukas

Richard Mott

Andres Metspalu

David R Bentley

Lon R Cardon

Ian Dunham

Affiliations

Soon will be listed here.

Abstract

DNA sequence variants in specific genes or regions of the human genome are responsible for a variety of phenotypes such as disease risk or variable drug response. These variants can be investigated directly, or through their non-random associations with neighbouring markers (called linkage disequilibrium (LD)). Here we report measurement of LD along the complete sequence of human chromosome 22. Duplicate genotyping and analysis of 1,504 markers in Centre d'Etude du Polymorphisme Humain (CEPH) reference families at a median spacing of 15 kilobases (kb) reveals a highly variable pattern of LD along the chromosome, in which extensive regions of nearly complete LD up to 804 kb in length are interspersed with regions of little or no detectable LD. The LD patterns are replicated in a panel of unrelated UK Caucasians. There is a strong correlation between high LD and low recombination frequency in the extant genetic map, suggesting that historical and contemporary recombination rates are similar. This study demonstrates the feasibility of developing genome-wide maps of LD.

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