Literature DB >> 12421764

SNPSTRs: empirically derived, rapidly typed, autosomal haplotypes for inference of population history and mutational processes.

Joanna L Mountain1, Alec Knight, Matthew Jobin, Christopher Gignoux, Adam Miller, Alice A Lin, Peter A Underhill.   

Abstract

Each independently evolving segment of the genomes of a sexually reproducing organism has a separate history reflecting part of the evolutionary history of that organism. Uniparentally or clonally inherited DNA segments such as the mitochondrial and chloroplast genomes and the nonrecombining portion of the Y chromosome have provided, to date, most of the known data regarding compound haplotypic variation within and among populations. These comparatively small segments include numerous polymorphic sites and undergo little or no recombination. Recombining autosomes, however, comprise the major repository of genetic variation. Technical challenges and recombination have limited large-scale application of autosomal haplotypes. We have overcome this barrier through development of a general approach to the assessment of short autosomal DNA segments. Each such segment includes one or more single nucleotide polymorphisms (SNPs) and exactly one short tandem repeat (STR) locus. With dramatically different mutation rates, these two types of genetic markers provide complementary evolutionary information. We call the combination of a SNP and a STR polymorphism a SNPSTR, and have developed a simple, rapid method for empirically determining gametic phase for double and triple heterozygotes. Here, we illustrate the approach with two SNPSTR systems. Although even one system provides insight into population history, the power of the approach lies in combining results from multiple SNPSTR systems.

Mesh:

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Year:  2002        PMID: 12421764      PMCID: PMC187554          DOI: 10.1101/gr.238602

Source DB:  PubMed          Journal:  Genome Res        ISSN: 1088-9051            Impact factor:   9.043


  31 in total

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Journal:  Nat Genet       Date:  2001-10       Impact factor: 38.330

4.  Intensely punctate meiotic recombination in the class II region of the major histocompatibility complex.

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5.  Linkage disequilibrium in the human genome.

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6.  Lower-than-expected linkage disequilibrium between tightly linked markers in humans suggests a role for gene conversion.

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  18 in total

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8.  A genomewide comparison of population structure at STRPs and nearby SNPs in humans.

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Review 9.  Linkage disequilibrium--understanding the evolutionary past and mapping the medical future.

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