Polygenic adaptation and negative selection across traits, years and environments in a long-lived plant species (Pinus pinaster Ait., Pinaceae)

AbstractA decade of association studies in multiple organisms suggests that most complex traits are polygenic; that is, they have a genetic architecture determined by numerous loci distributed across the genome, each with small effect-size. Thus, determining the degree of polygenicity and its variation across traits, environments and years is useful to understand the genetic basis of phenotypic variation. In this study, we applied multilocus approaches to estimate the degree of polygenicity of fitness-related traits in a long-lived plant (Pinus pinaster Ait., maritime pine) and to analyze how polygenicity changes across environments and years. To do so, we evaluated five categories of fitness-related traits (survival, height, phenology-related, functional, and biotic-stress response traits) in a clonal common garden network, planted in contrasted environments (over 12,500 trees). First, most of the analyzed traits showed evidence of local adaptation based on QST-FST comparisons. Second, we observed a remarkably stable degree of polygenicity, averaging 6% (range of 0-27%), across traits, environments and years. As previously suggested for humans, some of these traits showed also evidence of negative selection, which could explain, at least partially, the high degree of polygenicity. The observed genetic architecture of fitness-related traits in maritime pine supports the polygenic adaptation model. Because polygenic adaptation can occur rapidly, our study suggests that current predictions on the capacity of natural forest tree populations to adapt to new environments should be revised, which is of special relevance in the current context of climate change.

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Genetics of complex traits: prediction of phenotype, identification of causal polymorphisms and genetic architecture

Proceedings of The Royal Society B Biological Sciences ◽

10.1098/rspb.2016.0569 ◽

2016 ◽

Vol 283 (1835) ◽

pp. 20160569 ◽

Cited By ~ 52

Author(s):

M. E. Goddard ◽

K. E. Kemper ◽

I. M. MacLeod ◽

A. J. Chamberlain ◽

B. J. Hayes

Keyword(s):

Complex Traits ◽

Genetic Architecture ◽

Quantitative Traits ◽

Association Studies ◽

Genome Wide Association Studies ◽

Nucleotide Polymorphisms ◽

Crop Breeding ◽

Single Nucleotide ◽

Genome Wide ◽

Phenotype Identification

Complex or quantitative traits are important in medicine, agriculture and evolution, yet, until recently, few of the polymorphisms that cause variation in these traits were known. Genome-wide association studies (GWAS), based on the ability to assay thousands of single nucleotide polymorphisms (SNPs), have revolutionized our understanding of the genetics of complex traits. We advocate the analysis of GWAS data by a statistical method that fits all SNP effects simultaneously, assuming that these effects are drawn from a prior distribution. We illustrate how this method can be used to predict future phenotypes, to map and identify the causal mutations, and to study the genetic architecture of complex traits. The genetic architecture of complex traits is even more complex than previously thought: in almost every trait studied there are thousands of polymorphisms that explain genetic variation. Methods of predicting future phenotypes, collectively known as genomic selection or genomic prediction, have been widely adopted in livestock and crop breeding, leading to increased rates of genetic improvement.

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Better estimation of SNP heritability from summary statistics provides a new understanding of the genetic architecture of complex traits

10.1101/284976 ◽

2018 ◽

Cited By ~ 6

Author(s):

Doug Speed ◽

David J Balding

Keyword(s):

Complex Traits ◽

Genetic Architecture ◽

Large Scale ◽

Association Studies ◽

Genome Wide Association Studies ◽

Summary Statistics ◽

Confounding Bias ◽

Conserved Regions ◽

Genome Wide ◽

Variation Explained

LD Score Regression (LDSC) has been widely applied to the results of genome-wide association studies. However, its estimates of SNP heritability are derived from an unrealistic model in which each SNP is expected to contribute equal heritability. As a consequence, LDSC tends to over-estimate confounding bias, under-estimate the total phenotypic variation explained by SNPs, and provide misleading estimates of the heritability enrichment of SNP categories. Therefore, we present SumHer, software for estimating SNP heritability from summary statistics using more realistic heritability models. After demonstrating its superiority over LDSC, we apply SumHer to the results of 24 large-scale association studies (average sample size 121 000). First we show that these studies have tended to substantially over-correct for confounding, and as a result the number of genome-wide significant loci has under-reported by about 20%. Next we estimate enrichment for 24 categories of SNPs defined by functional annotations. A previous study using LDSC reported that conserved regions were 13-fold enriched, and found a further twelve categories with above 2-fold enrichment. By contrast, our analysis using SumHer finds that conserved regions are only 1.6-fold (SD 0.06) enriched, and that no category has enrichment above 1.7-fold. SumHer provides an improved understanding of the genetic architecture of complex traits, which enables more efficient analysis of future genetic data.

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TIGAR: An Improved Bayesian Tool for Transcriptomic Data Imputation Enhances Gene Mapping of Complex Traits

10.1101/507525 ◽

2018 ◽

Cited By ~ 3

Author(s):

Sini Nagpal ◽

Xiaoran Meng ◽

Michael P. Epstein ◽

Lam C. Tsoi ◽

Matthew Patrick ◽

...

Keyword(s):

Gene Expression ◽

Complex Traits ◽

Bayesian Model ◽

Genetic Architecture ◽

Bayesian Method ◽

Association Studies ◽

Gwas Data ◽

Nonparametric Bayesian ◽

Transcriptomic Data ◽

Special Cases

AbstractThe transcriptome-wide association studies (TWAS) that test for association between the study trait and the imputed gene expression levels from cis-acting expression quantitative trait loci (cis-eQTL) genotypes have successfully enhanced the discovery of genetic risk loci for complex traits. By using the gene expression imputation models fitted from reference datasets that have both genetic and transcriptomic data, TWAS facilitates gene-based tests with GWAS data while accounting for the reference transcriptomic data. The existing TWAS tools like PrediXcan and FUSION use parametric imputation models that have limitations for modeling the complex genetic architecture of transcriptomic data. Therefore, we propose an improved Bayesian method that assumes a data-driven nonparametric prior to impute gene expression. Our method is general and flexible and includes both the parametric imputation models used by PrediXcan and FUSION as special cases. Our simulation studies showed that the nonparametric Bayesian model improved both imputation R2 for transcriptomic data and the TWAS power over PrediXcan. In real applications, our nonparametric Bayesian method fitted transcriptomic imputation models for 2X number of genes with 1.7X average regression R2 over PrediXcan, thus improving the power of follow-up TWAS. Hence, the nonparametric Bayesian model is preferred for modeling the complex genetic architecture of transcriptomes and is expected to enhance transcriptome-integrated genetic association studies. We implement our Bayesian approach in a convenient software tool “TIGAR” (Transcriptome-Integrated Genetic Association Resource), which imputes transcriptomic data and performs subsequent TWAS using individual-level or summary-level GWAS data.

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GPA-MDS: A Visualization Approach to Investigate Genetic Architecture among Phenotypes Using GWAS Results

International Journal of Genomics ◽

10.1155/2016/6589843 ◽

2016 ◽

Vol 2016 ◽

pp. 1-6 ◽

Cited By ~ 2

Author(s):

Wei Wei ◽

Paula S. Ramos ◽

Kelly J. Hunt ◽

Bethany J. Wolf ◽

Gary Hardiman ◽

...

Keyword(s):

Complex Traits ◽

Genetic Architecture ◽

Association Studies ◽

Genetic Relationships ◽

Joint Analysis ◽

Genome Wide Association Studies ◽

Risk Variants ◽

Novel Approach ◽

Medical Benefits ◽

Rigorous Framework

Genome-wide association studies (GWAS) have identified tens of thousands of genetic variants associated with hundreds of phenotypes and diseases, which have provided clinical and medical benefits to patients with novel biomarkers and therapeutic targets. Recently, there has been accumulating evidence suggesting that different complex traits share a common risk basis, namely, pleiotropy. Previously, a statistical method, namely, GPA (Genetic analysis incorporating Pleiotropy and Annotation), was developed to improve identification of risk variants and to investigate pleiotropic structure through a joint analysis of multiple GWAS datasets. While GPA provides a statistically rigorous framework to evaluate pleiotropy between phenotypes, it is still not trivial to investigate genetic relationships among a large number of phenotypes using the GPA framework. In order to address this challenge, in this paper, we propose a novel approach, GPA-MDS, to visualize genetic relationships among phenotypes using the GPA algorithm and multidimensional scaling (MDS). This tool will help researchers to investigate common etiology among diseases, which can potentially lead to development of common treatments across diseases. We evaluate the proposed GPA-MDS framework using a simulation study and apply it to jointly analyze GWAS datasets examining 18 unique phenotypes, which helps reveal the shared genetic architecture of these phenotypes.

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A global overview of pleiotropy and genetic architecture in complex traits

10.1101/500090 ◽

2018 ◽

Cited By ~ 19

Author(s):

Kyoko Watanabe ◽

Sven Stringer ◽

Oleksandr Frei ◽

Maša Umićević Mirkov ◽

Tinca J.C. Polderman ◽

...

Keyword(s):

Genetic Variants ◽

Complex Traits ◽

Genetic Architecture ◽

Human Genetics ◽

Association Studies ◽

Regulatory Elements ◽

Genome Wide Association Studies ◽

Multiple Trait ◽

Current Availability ◽

Flanking Regions

ABSTRACTAfter a decade of genome-wide association studies (GWASs), fundamental questions in human genetics are still unanswered, such as the extent of pleiotropy across the genome, the nature of trait-associated genetic variants and the disparate genetic architecture across human traits. The current availability of hundreds of GWAS results provide the unique opportunity to gain insight into these questions. In this study, we harmonized and systematically analysed 4,155 publicly available GWASs. For a subset of well-powered GWAS on 558 unique traits, we provide an extensive overview of pleiotropy and genetic architecture. We show that trait associated loci cover more than half of the genome, and 90% of those loci are associated with multiple trait domains. We further show that potential causal genetic variants are enriched in coding and flanking regions, as well as in regulatory elements, and how trait-polygenicity is related to an estimate of the required sample size to detect 90% of causal genetic variants. Our results provide novel insights into how genetic variation contributes to trait variation. All GWAS results can be queried and visualized at the GWAS ATLAS resource (http://atlas.ctglab.nl).

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Polygenicity of complex traits is explained by negative selection

10.1101/420497 ◽

2018 ◽

Cited By ~ 6

Author(s):

Luke J. O’Connor ◽

Armin P. Schoech ◽

Farhad Hormozdiari ◽

Steven Gazal ◽

Nick Patterson ◽

...

Keyword(s):

Complex Traits ◽

Negative Selection ◽

Genetic Architecture ◽

Low Frequency ◽

Effect Sizes ◽

Common Disease ◽

Common Variants ◽

Robust Statistical Method ◽

Genetic Signal ◽

Definition Of

Complex traits and common disease are highly polygenic: thousands of common variants are causal, and their effect sizes are almost always small. Polygenicity could be explained by negative selection, which constrains common-variant effect sizes and may reshape their distribution across the genome. We refer to this phenomenon as flattening, as genetic signal is flattened relative to the underlying biology. We introduce a mathematical definition of polygenicity, the effective number of associated SNPs, and a robust statistical method to estimate it. This definition of polygenicity differs from the number of causal SNPs, a standard definition; it depends strongly on SNPs with large effects. In analyses of 33 complex traits (average N=361k), we determined that common variants are ∼4x more polygenic than low-frequency variants, consistent with pervasive flattening. Moreover, functionally important regions of the genome have increased polygenicity in proportion to their increased heritability, implying that heritability enrichment reflects differences in the number of associations rather than their magnitude (which is constrained by selection). We conclude that negative selection constrains the genetic signal of biologically important regions and genes, reshaping genetic architecture.

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Bench Research Informed by GWAS Results

Cells ◽

10.3390/cells10113184 ◽

2021 ◽

Vol 10 (11) ◽

pp. 3184

Author(s):

Nikolay V. Kondratyev ◽

Margarita V. Alfimova ◽

Arkadiy K. Golov ◽

Vera E. Golimbet

Keyword(s):

Complex Traits ◽

Genetic Architecture ◽

Reverse Genetics ◽

Genetic Factors ◽

Association Studies ◽

Genome Wide Association ◽

Genome Wide Association Studies ◽

Genome Wide

Scientifically interesting as well as practically important phenotypes often belong to the realm of complex traits. To the extent that these traits are hereditary, they are usually ‘highly polygenic’. The study of such traits presents a challenge for researchers, as the complex genetic architecture of such traits makes it nearly impossible to utilise many of the usual methods of reverse genetics, which often focus on specific genes. In recent years, thousands of genome-wide association studies (GWAS) were undertaken to explore the relationships between complex traits and a large number of genetic factors, most of which are characterised by tiny effects. In this review, we aim to familiarise ‘wet biologists’ with approaches for the interpretation of GWAS results, to clarify some issues that may seem counterintuitive and to assess the possibility of using GWAS results in experiments on various complex traits.

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Sexual differences in genetic architecture in UK Biobank

10.1101/2020.07.20.211813 ◽

2020 ◽

Author(s):

Elena Bernabeu ◽

Oriol Canela-Xandri ◽

Konrad Rawlik ◽

Andrea Talenti ◽

James Prendergast ◽

...

Keyword(s):

Sexual Dimorphism ◽

Complex Traits ◽

Genetic Architecture ◽

Molecular Mechanisms ◽

Association Studies ◽

Mammalian Species ◽

Genetic Correlations ◽

European Ancestry ◽

Genome Wide Association Studies ◽

Uk Biobank

ABSTRACTSex is arguably the most important differentiating characteristic in most mammalian species, separating populations into different groups, with varying behaviors, morphologies, and physiologies based on their complement of sex chromosomes. In humans, despite males and females sharing nearly identical genomes, there are differences between the sexes in complex traits and in the risk of a wide array of diseases. Gene by sex interactions (GxS) are thought to account for some of this sexual dimorphism. However, the extent and basis of these interactions are poorly understood.Here we provide insights into both the scope and mechanism of GxS across the genome of circa 450,000 individuals of European ancestry and 530 complex traits in the UK Biobank. We found small yet widespread differences in genetic architecture across traits through the calculation of sex-specific heritability, genetic correlations, and sex-stratified genome-wide association studies (GWAS). We also found that, in some cases, sex-agnostic GWAS efforts might be missing loci of interest, and looked into possible improvements in the prediction of high-level phenotypes. Finally, we studied the potential functional role of the dimorphism observed through sex-biased eQTL and gene-level analyses.This study marks a broad examination of the genetics of sexual dimorphism. Our findings parallel previous reports, suggesting the presence of sexual genetic heterogeneity across complex traits of generally modest magnitude. Our results suggest the need to consider sex-stratified analyses for future studies in order to shed light into possible sex-specific molecular mechanisms.

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SparsePro: an efficient genome-wide fine-mapping method integrating summary statistics and functional annotations

10.1101/2021.10.04.463133 ◽

2021 ◽

Author(s):

Wenmin Zhang ◽

Hamed S Najafabadi ◽

Yue Li

Keyword(s):

Fine Mapping ◽

Complex Traits ◽

Genetic Architecture ◽

Association Studies ◽

Computational Cost ◽

Mapping Method ◽

Genome Wide Association Studies ◽

Functional Annotations ◽

Genome Wide ◽

Causal Variants

Identifying causal variants from genome-wide association studies (GWASs) is challenging due to widespread linkage disequilibrium (LD). Functional annotations of the genome may help prioritize variants that are biologically relevant and thus improve fine-mapping of GWAS results. However, classical fine-mapping methods have a high computational cost, particularly when the underlying genetic architecture and LD patterns are complex. Here, we propose a novel approach, SparsePro, to efficiently conduct functionally informed statistical fine-mapping. Our method enjoys two major innovations: First, by creating a sparse low-dimensional projection of the high-dimensional genotype, we enable a linear search of causal variants instead of an exponential search of causal configurations used in existing methods; Second, we adopt a probabilistic framework with a highly efficient variational expectation-maximization algorithm to integrate statistical associations and functional priors. We evaluate SparsePro through extensive simulations using resources from the UK Biobank. Compared to state-of-the-art methods, SparsePro achieved more accurate and well-calibrated posterior inference with greatly reduced computation time. We demonstrate the utility of SparsePro by investigating the genetic architecture of five functional biomarkers of vital organs. We identify potential causal variants contributing to the genetically encoded coordination mechanisms between vital organs and pinpoint target genes with potential pleiotropic effects. In summary, we have developed an efficient genome-wide fine-mapping method with the ability to integrate functional annotations. Our method may have wide utility in understanding the genetics of complex traits as well as in increasing the yield of functional follow-up studies of GWASs.

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Polygenic Adaptation has Impacted Multiple Anthropometric Traits

10.1101/167551 ◽

2017 ◽

Cited By ~ 30

Author(s):

Jeremy J. Berg ◽

Xinjun Zhang ◽

Graham Coop

Keyword(s):

Complex Traits ◽

Association Studies ◽

Gwas Data ◽

Human Populations ◽

Genome Wide Association Studies ◽

Uk Biobank ◽

Link Type ◽

Polygenic Scores ◽

Polygenic Adaptation ◽

The Uk

AbstractOur understanding of the genetic basis of human adaptation is biased toward loci of large pheno-typic effect. Genome wide association studies (GWAS) now enable the study of genetic adaptation in polygenic phenotypes. We test for polygenic adaptation among 187 world-wide human populations using polygenic scores constructed from GWAS of 34 complex traits. We identify signals of polygenic adaptation for anthropometric traits including height, infant head circumference (IHC), hip circumference and waist-to-hip ratio (WHR). Analysis of ancient DNA samples indicates that a north-south cline of height within Europe and and a west-east cline across Eurasia can be traced to selection for increased height in two late Pleistocene hunter gatherer populations living in western and west-central Eurasia. Our observation that IHC and WHR follow a latitudinal cline in Western Eurasia support the role of natural selection driving Bergmann’s Rule in humans, consistent with thermoregulatory adaptation in response to latitudinal temperature variation.Author’s Note on Failure to ReplicateAfter this preprint was posted, the UK Biobank dataset was released, providing a new and open GWAS resource. When attempting to replicate the height selection results from this preprint using GWAS data from the UK Biobank, we discovered that we could not. In subsequent analyses, we determined that both the GIANT consortium height GWAS data, as well as another dataset that was used for replication, were impacted by stratification issues that created or at a minimum substantially inflated the height selection signals reported here. The results of this second investigation, written together with additional coauthors, have now been published (https://elifesciences.org/articles/39725 along with another paper by a separate group of authors, showing similar issues https://elifesciences.org/articles/39702). A preliminary investigation shows that the other non-height based results may suffer from similar issues. We stand by the theory and statistical methods reported in this paper, and the paper can be cited for these results. However, we have shown that the data on which the major empirical results were based are not sound, and so should be treated with caution until replicated.

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