Literature DB >> 26189816

A Fast Method that Uses Polygenic Scores to Estimate the Variance Explained by Genome-wide Marker Panels and the Proportion of Variants Affecting a Trait.

Luigi Palla1, Frank Dudbridge2.   

Abstract

Several methods have been proposed to estimate the variance in disease liability explained by large sets of genetic markers. However, current methods do not scale up well to large sample sizes. Linear mixed models require solving high-dimensional matrix equations, and methods that use polygenic scores are very computationally intensive. Here we propose a fast analytic method that uses polygenic scores, based on the formula for the non-centrality parameter of the association test of the score. We estimate model parameters from the results of multiple polygenic score tests based on markers with p values in different intervals. We estimate parameters by maximum likelihood and use profile likelihood to compute confidence intervals. We compare various options for constructing polygenic scores, based on nested or disjoint intervals of p values, weighted or unweighted effect sizes, and different numbers of intervals, in estimating the variance explained by a set of markers, the proportion of markers with effects, and the genetic covariance between a pair of traits. Our method provides nearly unbiased estimates and confidence intervals with good coverage, although estimation of the variance is less reliable when jointly estimated with the covariance. We find that disjoint p value intervals perform better than nested intervals, but the weighting did not affect our results. A particular advantage of our method is that it can be applied to summary statistics from single markers, and so can be quickly applied to large consortium datasets. Our method, named AVENGEME (Additive Variance Explained and Number of Genetic Effects Method of Estimation), is implemented in R software.
Copyright © 2015 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.

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Year:  2015        PMID: 26189816      PMCID: PMC4573448          DOI: 10.1016/j.ajhg.2015.06.005

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


  32 in total

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Journal:  Am J Hum Genet       Date:  2007-07-25       Impact factor: 11.025

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4.  Uncovering the total heritability explained by all true susceptibility variants in a genome-wide association study.

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5.  Common SNPs explain a large proportion of the heritability for human height.

Authors:  Jian Yang; Beben Benyamin; Brian P McEvoy; Scott Gordon; Anjali K Henders; Dale R Nyholt; Pamela A Madden; Andrew C Heath; Nicholas G Martin; Grant W Montgomery; Michael E Goddard; Peter M Visscher
Journal:  Nat Genet       Date:  2010-06-20       Impact factor: 38.330

6.  Adaptation - not by sweeps alone.

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9.  The genetics of human adaptation: hard sweeps, soft sweeps, and polygenic adaptation.

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10.  Common polygenic variation contributes to risk of schizophrenia and bipolar disorder.

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  68 in total

1.  Extreme Polygenicity of Complex Traits Is Explained by Negative Selection.

Authors:  Luke J O'Connor; Armin P Schoech; Farhad Hormozdiari; Steven Gazal; Nick Patterson; Alkes L Price
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2.  Estimating SNP-Based Heritability and Genetic Correlation in Case-Control Studies Directly and with Summary Statistics.

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3.  Contrasting the Genetic Architecture of 30 Complex Traits from Summary Association Data.

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6.  Does Childhood Trauma Moderate Polygenic Risk for Depression? A Meta-analysis of 5765 Subjects From the Psychiatric Genomics Consortium.

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Journal:  Biol Psychiatry       Date:  2017-09-21       Impact factor: 13.382

7.  Concepts, estimation and interpretation of SNP-based heritability.

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Review 8.  Dissecting the genetics of complex traits using summary association statistics.

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9.  The Translational Potential of Neuroimaging Genomic Analyses To Diagnosis And Treatment In The Mental Disorders.

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