Literature DB >> 23175758

A Lasso multi-marker mixed model for association mapping with population structure correction.

Barbara Rakitsch1, Christoph Lippert, Oliver Stegle, Karsten Borgwardt.   

Abstract

MOTIVATION: Exploring the genetic basis of heritable traits remains one of the central challenges in biomedical research. In traits with simple Mendelian architectures, single polymorphic loci explain a significant fraction of the phenotypic variability. However, many traits of interest seem to be subject to multifactorial control by groups of genetic loci. Accurate detection of such multivariate associations is non-trivial and often compromised by limited statistical power. At the same time, confounding influences, such as population structure, cause spurious association signals that result in false-positive findings.
RESULTS: We propose linear mixed models LMM-Lasso, a mixed model that allows for both multi-locus mapping and correction for confounding effects. Our approach is simple and free of tuning parameters; it effectively controls for population structure and scales to genome-wide datasets. LMM-Lasso simultaneously discovers likely causal variants and allows for multi-marker-based phenotype prediction from genotype. We demonstrate the practical use of LMM-Lasso in genome-wide association studies in Arabidopsis thaliana and linkage mapping in mouse, where our method achieves significantly more accurate phenotype prediction for 91% of the considered phenotypes. At the same time, our model dissects the phenotypic variability into components that result from individual single nucleotide polymorphism effects and population structure. Enrichment of known candidate genes suggests that the individual associations retrieved by LMM-Lasso are likely to be genuine. AVAILABILITY: Code available under http://webdav.tuebingen. mpg.de/u/karsten/Forschung/research.html. CONTACT: rakitsch@tuebingen.mpg.de, ippert@microsoft.com or stegle@ebi.ac.uk SUPPLEMENTARY INFORMATION: Supplementary data are available at Bioinformatics online.

Entities:  

Mesh:

Year:  2012        PMID: 23175758     DOI: 10.1093/bioinformatics/bts669

Source DB:  PubMed          Journal:  Bioinformatics        ISSN: 1367-4803            Impact factor:   6.937


  46 in total

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4.  A random forest approach to capture genetic effects in the presence of population structure.

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5.  Evaluation of multi-locus models for genome-wide association studies: a case study in sugar beet.

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6.  Inference on the Genetic Basis of Eye and Skin Color in an Admixed Population via Bayesian Linear Mixed Models.

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7.  easyGWAS: A Cloud-Based Platform for Comparing the Results of Genome-Wide Association Studies.

Authors:  Dominik G Grimm; Damian Roqueiro; Patrice A Salomé; Stefan Kleeberger; Bastian Greshake; Wangsheng Zhu; Chang Liu; Christoph Lippert; Oliver Stegle; Bernhard Schölkopf; Detlef Weigel; Karsten M Borgwardt
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8.  Analyzing Association Mapping in Pedigree-Based GWAS Using a Penalized Multitrait Mixed Model.

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Review 9.  Fine-mapping QTLs in advanced intercross lines and other outbred populations.

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Review 10.  Finding the Genomic Basis of Local Adaptation: Pitfalls, Practical Solutions, and Future Directions.

Authors:  Sean Hoban; Joanna L Kelley; Katie E Lotterhos; Michael F Antolin; Gideon Bradburd; David B Lowry; Mary L Poss; Laura K Reed; Andrew Storfer; Michael C Whitlock
Journal:  Am Nat       Date:  2016-08-15       Impact factor: 3.926

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