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Literature DB >> 7887434

A powerful likelihood method for the analysis of linkage disequilibrium between trait loci and one or more polymorphic marker loci.

Abstract

Historically, most methods for detecting linkage disequilibrium were designed for use with diallelic marker loci, for which the analysis is straightforward. With the advent of polymorphic markers with many alleles, the normal approach to their analysis has been either to extend the methodology for two-allele systems (leading to an increase in df and to a corresponding loss of power) or to select the allele believed to be associated and then collapse the other alleles, reducing, in a biased way, the locus to a diallelic system. I propose a likelihood-based approach to testing for linkage disequilibrium, an approach that becomes more conservative as the number of alleles increases, and as the number of markers considered jointly increases in a multipoint test for linkage disequilibrium, while maintaining high power. Properties of this method for detecting associations and fine mapping the location of disease traits are investigated. It is found to be, in general, more powerful than conventional methods, and it provides a tractable framework for the fine mapping of new disease loci. Application to the cystic fibrosis data of Kerem et al, is included to illustrate the method.

Entities: Disease

Mesh：

Substances：
Genetic Markers

Year: 1995 PMID： 7887434 PMCID： PMC1801166

Source DB: PubMed Journal: Am J Hum Genet ISSN： 0002-9297 Impact factor: 11.025

6 in total

1. A haplotype-based 'haplotype relative risk' approach to detecting allelic associations.

Authors: J D Terwilliger; J Ott
Journal: Hum Hered Date: 1992 Impact factor: 0.444

2. Identification of the cystic fibrosis gene: genetic analysis.

Authors: B Kerem; J M Rommens; J A Buchanan; D Markiewicz; T K Cox; A Chakravarti; M Buchwald; L C Tsui
Journal: Science Date: 1989-09-08 Impact factor: 47.728

3. Maximum-likelihood estimation of gene location by linkage disequilibrium.

Authors: W G Hill; B S Weir
Journal: Am J Hum Genet Date: 1994-04 Impact factor: 11.025

4. On the lod score method in linkage analysis.

Authors: J Chotai
Journal: Ann Hum Genet Date: 1984-10 Impact factor: 1.670

5. Linkage disequilibrium mapping in isolated founder populations: diastrophic dysplasia in Finland.

Authors: J Hästbacka; A de la Chapelle; I Kaitila; P Sistonen; A Weaver; E Lander
Journal: Nat Genet Date: 1992-11 Impact factor: 38.330

6. Haplotype relative risks: an easy reliable way to construct a proper control sample for risk calculations.

Authors: C T Falk; P Rubinstein
Journal: Ann Hum Genet Date: 1987-07 Impact factor: 1.670

6 in total

118 in total

1. Assessment of linkage disequilibrium by the decay of haplotype sharing, with application to fine-scale genetic mapping.

Authors: M S McPeek; A Strahs
Journal: Am J Hum Genet Date: 1999-09 Impact factor: 11.025

2. Fine mapping of the chromosome 3p susceptibility locus in inflammatory bowel disease.

Authors: J Hampe; N J Lynch; S Daniels; S Bridger; A J Macpherson; P Stokkers; A Forbes; J E Lennard-Jones; C G Mathew; M E Curran; S Schreiber
Journal: Gut Date: 2001-02 Impact factor: 23.059

3. Multipoint linkage-disequilibrium-mapping approach based on the case-parent trio design.

Authors: K Y Liang; F C Hsu; T H Beaty; K C Barnes
Journal: Am J Hum Genet Date: 2001-03-15 Impact factor: 11.025

4. Linkage analysis in the presence of errors IV: joint pseudomarker analysis of linkage and/or linkage disequilibrium on a mixture of pedigrees and singletons when the mode of inheritance cannot be accurately specified.

Authors: H H Göring; J D Terwilliger
Journal: Am J Hum Genet Date: 2000-03-23 Impact factor: 11.025

A powerful likelihood method for the analysis of linkage disequilibrium between trait loci and one or more polymorphic marker loci.

1. A haplotype-based 'haplotype relative risk' approach to detecting allelic associations.

2. Identification of the cystic fibrosis gene: genetic analysis.

3. Maximum-likelihood estimation of gene location by linkage disequilibrium.

4. On the lod score method in linkage analysis.

5. Linkage disequilibrium mapping in isolated founder populations: diastrophic dysplasia in Finland.

6. Haplotype relative risks: an easy reliable way to construct a proper control sample for risk calculations.

1. Assessment of linkage disequilibrium by the decay of haplotype sharing, with application to fine-scale genetic mapping.

2. Fine mapping of the chromosome 3p susceptibility locus in inflammatory bowel disease.

3. Multipoint linkage-disequilibrium-mapping approach based on the case-parent trio design.

4. Linkage analysis in the presence of errors IV: joint pseudomarker analysis of linkage and/or linkage disequilibrium on a mixture of pedigrees and singletons when the mode of inheritance cannot be accurately specified.

5. Linkage analysis in the presence of errors III: marker loci and their map as nuisance parameters.

6. The trimmed-haplotype test for linkage disequilibrium.

7. Bayesian fine-scale mapping of disease loci, by hidden Markov models.

8. Data mining applied to linkage disequilibrium mapping.

9. Haplotype fine mapping by evolutionary trees.

10. Genetic analyses of chromosome 12 loci in Crohn's disease.