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Literature DB >> 8128969

Maximum-likelihood estimation of gene location by linkage disequilibrium.

Abstract

Linkage disequilibrium, D, between a polymorphic disease and mapped markers can, in principle, be used to help find the map position of the disease gene. Likelihoods are therefore derived for the value of D conditional on the observed number of haplotypes in the sample and on the population parameter Nc, where N is the effective population size and c the recombination fraction between the disease and marker loci. The likelihood is computed explicitly for the case of two loci with heterozygote superiority and, more generally, by computer simulations assuming a steady state of constant population size and selective pressures or neutrality. It is found that the likelihood is, in general, not very dependent on the degree of selection at the loci and is very flat. This suggests that precise information on map position will not be obtained from estimates of linkage disequilibrium.

Mesh：

Year: 1994 PMID： 8128969 PMCID： PMC1918089

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

9 in total

1. Expected behavior of conditional linkage disequilibrium.

Authors: N Kaplan; B S Weir
Journal: Am J Hum Genet Date: 1992-08 Impact factor: 11.025

2. The end in sight for Huntington disease?

Authors: C Pritchard; D R Cox; R M Myers
Journal: Am J Hum Genet Date: 1991-07 Impact factor: 11.025

3. Human genetics: the molecular challenge.

Authors: W F Bodmer
Journal: Cold Spring Harb Symp Quant Biol Date: 1986

4. Variances and covariances of squared linkage disequilibria in finite populations.

Authors: W G Hill; B S Weir
Journal: Theor Popul Biol Date: 1988-02 Impact factor: 1.570

5. Correlation and probability methods for one and two loci.

Authors: J A Sved; M W Feldman
Journal: Theor Popul Biol Date: 1973-03 Impact factor: 1.570

6. The sampling distribution of linkage disequilibrium under an infinite allele model without selection.

Authors: R R Hudson
Journal: Genetics Date: 1985-03 Impact factor: 4.562

7. A candidate for the cystic fibrosis locus isolated by selection for methylation-free islands.

Authors: X Estivill; M Farrall; P J Scambler; G M Bell; K M Hawley; N J Lench; G P Bates; H C Kruyer; P A Frederick; P Stanier
Journal: Nature Date: 1987 Apr 30-May 6 Impact factor: 49.962

8. 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

Review 9. The Huntington's disease candidate region exhibits many different haplotypes.

Authors: M E MacDonald; A Novelletto; C Lin; D Tagle; G Barnes; G Bates; S Taylor; B Allitto; M Altherr; R Myers
Journal: Nat Genet Date: 1992-05 Impact factor: 38.330

9 in total

65 in total

10. The structure of linkage disequilibrium at the DBH locus strongly influences the magnitude of association between diallelic markers and plasma dopamine beta-hydroxylase activity.

Authors: Cyrus P Zabetian; Sarah G Buxbaum; Robert C Elston; Michael D Köhnke; George M Anderson; Joel Gelernter; Joseph F Cubells
Journal: Am J Hum Genet Date: 2003-04-30 Impact factor: 11.025

Maximum-likelihood estimation of gene location by linkage disequilibrium.

1. Expected behavior of conditional linkage disequilibrium.

2. The end in sight for Huntington disease?

3. Human genetics: the molecular challenge.

4. Variances and covariances of squared linkage disequilibria in finite populations.

5. Correlation and probability methods for one and two loci.

6. The sampling distribution of linkage disequilibrium under an infinite allele model without selection.

7. A candidate for the cystic fibrosis locus isolated by selection for methylation-free islands.

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

Review 9. The Huntington's disease candidate region exhibits many different haplotypes.

1. The power of association studies to detect the contribution of candidate genetic loci to variation in complex traits.

2. Estimation of effective population size and migration rate from one- and two-locus identity measures.

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

4. Fine mapping of quantitative trait loci using linkage disequilibria with closely linked marker loci.

5. Two-locus sampling distributions and their application.

6. Joint linkage and linkage disequilibrium mapping of quantitative trait loci in natural populations.

7. Inferring linkage disequilibrium between a polymorphic marker locus and a trait locus in natural populations.

8. The effect of genotyping errors on the robustness of composite linkage disequilibrium measures.

9. A haplotype map of the human genome.

10. The structure of linkage disequilibrium at the DBH locus strongly influences the magnitude of association between diallelic markers and plasma dopamine beta-hydroxylase activity.