Application of homozygosity haplotype analysis to genetic mapping with high-density SNP genotype data.

Application of homozygosity haplotype analysis to genetic mapping with high-density SNP genotype data.

BACKGROUND: In families segregating a monogenic genetic disorder with a single disease gene introduction, patients share a mutation-carrying chromosomal interval with identity-by-descent (IBD). Such a shared chromosomal interval or haplotype, surrounding the actual pathogenic mutation, is typically...

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Main Authors: Haiyan Jiang, Andrew Orr, Duane L Guernsey, Johane Robitaille, Géraldine Asselin, Mark E Samuels, Marie-Pierre Dubé
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2009-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2670504?pdf=render
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spelling doaj-c5a29d9e3369428b85cf5537ae1881d42020-11-25T01:46:42ZengPublic Library of Science (PLoS)PLoS ONE1932-62032009-01-0144e528010.1371/journal.pone.0005280Application of homozygosity haplotype analysis to genetic mapping with high-density SNP genotype data.Haiyan JiangAndrew OrrDuane L GuernseyJohane RobitailleGéraldine AsselinMark E SamuelsMarie-Pierre DubéBACKGROUND: In families segregating a monogenic genetic disorder with a single disease gene introduction, patients share a mutation-carrying chromosomal interval with identity-by-descent (IBD). Such a shared chromosomal interval or haplotype, surrounding the actual pathogenic mutation, is typically detected and defined by multipoint linkage and phased haplotype analysis using microsatellite or SNP genotype data. High-density SNP genotype data presents a computational challenge for conventional genetic analyses. A novel non-parametric method termed Homozygosity Haplotype (HH) was recently proposed for the genome-wide search of the autosomal segments shared among patients using high density SNP genotype data. METHODOLOGY/PRINCIPAL FINDINGS: The applicability and the effectiveness of HH in identifying the potential linkage of disease causative gene with high-density SNP genotype data were studied with a series of monogenic disorders ascertained in eastern Canadian populations. The HH approach was validated using the genotypes of patients from a family affected with a rare autosomal dominant disease Schnyder crystalline corneal dystrophy. HH accurately detected the approximately 1 Mb genomic interval encompassing the causative gene UBIAD1 using the genotypes of only four affected subjects. The successful application of HH to identify the potential linkage for a family with pericentral retinal disorder indicates that HH can be applied to perform family-based association analysis by treating affected and unaffected family members as cases and controls respectively. A new strategy for the genome-wide screening of known causative genes or loci with HH was proposed, as shown the applications to a myoclonus dystonia and a renal failure cohort. CONCLUSIONS/SIGNIFICANCE: Our study of the HH approach demonstrates that HH is very efficient and effective in identifying potential disease linked region. HH has the potential to be used as an efficient alternative approach to sequencing or microsatellite-based fine mapping for screening the known causative genes in genetic disease study.http://europepmc.org/articles/PMC2670504?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Haiyan Jiang
Andrew Orr
Duane L Guernsey
Johane Robitaille
Géraldine Asselin
Mark E Samuels
Marie-Pierre Dubé
spellingShingle Haiyan Jiang
Andrew Orr
Duane L Guernsey
Johane Robitaille
Géraldine Asselin
Mark E Samuels
Marie-Pierre Dubé
Application of homozygosity haplotype analysis to genetic mapping with high-density SNP genotype data.
PLoS ONE
author_facet Haiyan Jiang
Andrew Orr
Duane L Guernsey
Johane Robitaille
Géraldine Asselin
Mark E Samuels
Marie-Pierre Dubé
author_sort Haiyan Jiang
title Application of homozygosity haplotype analysis to genetic mapping with high-density SNP genotype data.
title_short Application of homozygosity haplotype analysis to genetic mapping with high-density SNP genotype data.
title_full Application of homozygosity haplotype analysis to genetic mapping with high-density SNP genotype data.
title_fullStr Application of homozygosity haplotype analysis to genetic mapping with high-density SNP genotype data.
title_full_unstemmed Application of homozygosity haplotype analysis to genetic mapping with high-density SNP genotype data.
title_sort application of homozygosity haplotype analysis to genetic mapping with high-density snp genotype data.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2009-01-01
description BACKGROUND: In families segregating a monogenic genetic disorder with a single disease gene introduction, patients share a mutation-carrying chromosomal interval with identity-by-descent (IBD). Such a shared chromosomal interval or haplotype, surrounding the actual pathogenic mutation, is typically detected and defined by multipoint linkage and phased haplotype analysis using microsatellite or SNP genotype data. High-density SNP genotype data presents a computational challenge for conventional genetic analyses. A novel non-parametric method termed Homozygosity Haplotype (HH) was recently proposed for the genome-wide search of the autosomal segments shared among patients using high density SNP genotype data. METHODOLOGY/PRINCIPAL FINDINGS: The applicability and the effectiveness of HH in identifying the potential linkage of disease causative gene with high-density SNP genotype data were studied with a series of monogenic disorders ascertained in eastern Canadian populations. The HH approach was validated using the genotypes of patients from a family affected with a rare autosomal dominant disease Schnyder crystalline corneal dystrophy. HH accurately detected the approximately 1 Mb genomic interval encompassing the causative gene UBIAD1 using the genotypes of only four affected subjects. The successful application of HH to identify the potential linkage for a family with pericentral retinal disorder indicates that HH can be applied to perform family-based association analysis by treating affected and unaffected family members as cases and controls respectively. A new strategy for the genome-wide screening of known causative genes or loci with HH was proposed, as shown the applications to a myoclonus dystonia and a renal failure cohort. CONCLUSIONS/SIGNIFICANCE: Our study of the HH approach demonstrates that HH is very efficient and effective in identifying potential disease linked region. HH has the potential to be used as an efficient alternative approach to sequencing or microsatellite-based fine mapping for screening the known causative genes in genetic disease study.
url http://europepmc.org/articles/PMC2670504?pdf=render
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