Literature DB >> 16984977

Bayesian method for gene detection and mapping, using a case and control design and DNA pooling.

Toby Johnson1.   

Abstract

Association mapping studies aim to determine the genetic basis of a trait. A common experimental design uses a sample of unrelated individuals classified into 2 groups, for example cases and controls. If the trait has a complex genetic basis, consisting of many quantitative trait loci (QTLs), each group needs to be large. Each group must be genotyped at marker loci covering the region of interest; for dense coverage of a large candidate region, or a whole-genome scan, the number of markers will be very large. The total amount of genotyping required for such a study is formidable. A laboratory effort efficient technique called DNA pooling could reduce the amount of genotyping required, but the data generated are less informative and require novel methods for efficient analysis. In this paper, a Bayesian statistical analysis of the classic model of McPeek and Strahs is proposed. In contrast to previous work on this model, I assume that data are collected using DNA pooling, so individual genotypes are not directly observed, and also account for experimental errors. A complete analysis can be performed using analytical integration, a propagation algorithm for a hidden Markov model, and quadrature. The method developed here is both statistically and computationally efficient. It allows simultaneous detection and mapping of a QTL, in a large-scale association mapping study, using data from pooled DNA. The method is shown to perform well on data sets simulated under a realistic coalescent-with-recombination model, and is shown to outperform classical single-point methods. The method is illustrated on data consisting of 27 markers in an 880-kb region around the CYP2D6 gene.

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Year:  2006        PMID: 16984977     DOI: 10.1093/biostatistics/kxl028

Source DB:  PubMed          Journal:  Biostatistics        ISSN: 1465-4644            Impact factor:   5.899


  7 in total

1.  Multimarker analysis and imputation of multiple platform pooling-based genome-wide association studies.

Authors:  Nils Homer; Waibhav D Tembe; Szabolcs Szelinger; Margot Redman; Dietrich A Stephan; John V Pearson; Stanley F Nelson; David Craig
Journal:  Bioinformatics       Date:  2008-07-10       Impact factor: 6.937

2.  The allostatic impact of chronic ethanol on gene expression: A genetic analysis of chronic intermittent ethanol treatment in the BXD cohort.

Authors:  Andrew D van der Vaart; Jennifer T Wolstenholme; Maren L Smith; Guy M Harris; Marcelo F Lopez; Aaron R Wolen; Howard C Becker; Robert W Williams; Michael F Miles
Journal:  Alcohol       Date:  2016-11-01       Impact factor: 2.405

3.  Methodological Issues in Multistage Genome-wide Association Studies.

Authors:  Duncan C Thomas; Graham Casey; David V Conti; Robert W Haile; Juan Pablo Lewinger; Daniel O Stram
Journal:  Stat Sci       Date:  2009-11-01       Impact factor: 2.901

4.  FHL2 interacts with CALM and is highly expressed in acute erythroid leukemia.

Authors:  Z Pašaliç; P A Greif; V Jurinoviç; M Mulaw; P M Kakadia; B Tizazu; L Fröhlich-Archangelo; A Krause; S K Bohlander
Journal:  Blood Cancer J       Date:  2011-11-11       Impact factor: 11.037

5.  High-resolution genetic mapping with pooled sequencing.

Authors:  Matthew D Edwards; David K Gifford
Journal:  BMC Bioinformatics       Date:  2012-04-19       Impact factor: 3.169

6.  Genetic Linkage Analysis of 15 DFNB Loci in a Group of Iranian Families with Autosomal Recessive Hearing Loss.

Authors:  Ma Tabatabaiefar; F Alasti; M Montazer Zohour; L Shariati; E Farrokhi; Dd Farhud; Gv Camp; Mr Noori-Daloii; M Hashemzadeh Chaleshtori
Journal:  Iran J Public Health       Date:  2011-06-30       Impact factor: 1.429

Review 7.  Two-phase and family-based designs for next-generation sequencing studies.

Authors:  Duncan C Thomas; Zhao Yang; Fan Yang
Journal:  Front Genet       Date:  2013-12-13       Impact factor: 4.599

  7 in total

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