Region-Based Association Test for Familial Data under Functional Linear Models

Svishcheva, G. R.; Belonogova, Nadezhda M.; Axenovich, Tatiana I.

doi:10.1371/journal.pone.0128999

Cited by 20 publications

(31 citation statements)

References 33 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In prior studies, fixed effect functional regression models were found to outperform SKAT, its optimal unified test (SKAT‐O), and a combined sum test of rare and common variant effect (SKAT‐C) in most cases (Fan et al., , , , ,b,c; Luo et al., , , ; Svishcheva et al., ; Vsevolozhskaya et al., , ). In Fan et al.…”

Section: Discussionmentioning

confidence: 99%

A comparison study of multivariate fixed models and Gene Association with Multiple Traits (GAMuT) for next‐generation sequencing

Chiu

Jung

Wang

et al. 2016

Genetic Epidemiology

View full text Add to dashboard Cite

In this paper, extensive simulations are performed to compare two statistical methods to analyze multiple correlated quantitative phenotypes: (1) approximate F-distributed tests of multivariate functional linear models (MFLM) and additive models of multivariate analysis of variance (MANOVA), and (2) Gene Association with Multiple Traits (GAMuT) for association testing of high-dimensional genotype data. It is shown that approximate F-distributed tests of MFLM and MANOVA have higher power and are more appropriate for major gene association analysis (i.e., scenarios in which some genetic variants have relatively large effects on the phenotypes); GAMuT has higher power and is more appropriate for analyzing polygenic effects (i.e., effects from a large number of genetic variants each of which contributes a small amount to the phenotypes). MFLM and MANOVA are very flexible and can be used to perform association analysis for: (i) rare variants, (ii) common variants, and (iii) a combination of rare and common variants. Although GAMuT was designed to analyze rare variants, it can be applied to analyze a combination of rare and common variants and it performs well when (1) the number of genetic variants is large and (2) each variant contributes a small amount to the phenotypes (i.e., polygenes). MFLM and MANOVA are fixed effect models which perform well for major gene association analysis. GAMuT can be viewed as an extension of sequence kernel association tests (SKAT). Both GAMuT and SKAT are more appropriate for analyzing polygenic effects and they perform well not only in the rare variant case, but also in the case of a combination of rare and common variants. Data analyses of European cohorts and the Trinity Students Study are presented to compare the performance of the two methods.

show abstract

Section: Discussionmentioning

confidence: 99%

A comparison study of multivariate fixed models and Gene Association with Multiple Traits (GAMuT) for next‐generation sequencing

Chiu

Jung

Wang

et al. 2016

Genetic Epidemiology

View full text Add to dashboard Cite

show abstract

“…A genotypic function is obtained by either (i) a cubic B‐spline basis expansion over a dense set of knots,

κ_{1}, ..., κ_{K}

, over the range of the variant's genomic positions

t_{i}

's (in the one‐base coordinate system) or (ii) penalized spline smoothing that avoids the knot selection problem completely [e.g., Luo et al., , Vsevolozhskaya et al., ]. Earlier investigations of FLMs designed for genetic association testing include comprehensive coverage of the estimation procedure for the genotypic functions

G (t)

's [Fan et al., , ; Lee et al., ; Luo et al., , , b; Svishcheva et al., ; Vsevolozhskaya et al., ; Wang et al., ; Zhu and Xiong, ].…”

Section: Methodsmentioning

confidence: 99%

“…As discussed elsewhere [e.g., Svishcheva et al., ; Vsevolozhskaya et al., ], statistical power of functional methods may depend on the quality of genotype data smoothing. To obtain smooth genotypic functions, we first coded allelic dosage based on the minor allele counts (i.e., either 0, 1, or 2) and applied the “flipping algorithm” [Vsevolozhskaya et al., ] to minimize the number of 0‐2 (or 2‐0) patterns in every two subsequent variant positions.…”

Section: Application To Real Data: Angprl4 Association With Tgmentioning

confidence: 99%

Uncovering Local Trends in Genetic Effects of Multiple Phenotypes via Functional Linear Models

et al. 2016

View full text Add to dashboard Cite

Recent technological advances equipped researchers with capabilities that go beyond traditional genotyping of loci known to be polymorphic in a general population. Genetic sequences of study participants can now be assessed directly. This capability removed technology-driven bias toward scoring predominantly common polymorphisms and let researchers reveal a wealth of rare and sample-specific variants. While the relative contributions of rare and common polymorphisms to trait variation are being debated, researchers are faced with the need for new statistical tools for simultaneous evaluation of all variants within a region. Several research groups demonstrated flexibility and good statistical power of the functional linear model approach. In this work we extend previous developments to allow inclusion of multiple traits and adjustment for additional covariates. Our functional approach is unique in that it provides a nuanced depiction of effects and interactions for the variables in the model by representing them as curves varying over a genetic region. We demonstrate flexibility and competitive power of our approach by contrasting its performance with commonly used statistical tools and illustrate its potential for discovery and characterization of genetic architecture of complex traits using sequencing data from the Dallas Heart Study.

show abstract

“…10,[16][17][18][19][20][21][22][23][24][25][26][27][28][29] In most cases, it was shown that the functional regression test statistics perform better than sequence kernel association test (SKAT), its optimal unified test (SKAT-O), and a combined sum test of rare and common variant effect (SKAT-C) of mixed models. 4,[16][17][18][19][20][21][22][23][24][25][26][27][30][31][32][33] Specifically, mixed model-based SKAT/SKATO/ SKAT-C performs well when (a) the number of causal variants is large and (b) each causal variant contributes a small amount to the traits, as the assumption of mixed models is satisfied under these circumstances. 7,21,34 In most cases, however, fixed models perform better since the causal variants of complex disorders can be common or rare or a combination of the two and some causal variants may have relatively large effects.…”

Section: Introductionmentioning

confidence: 99%

“…7,21,34 In most cases, however, fixed models perform better since the causal variants of complex disorders can be common or rare or a combination of the two and some causal variants may have relatively large effects. 10,[16][17][18][19][20][21][22][23][24][25][26][27] If the number of causal variants is large and each causal variant contributes a small amount to the traits, it would be hard to show association as the power of a test can be low. 35 One may want to note that SKAT and SKAT-O were shown to have higher power than burden tests, which is another main method to analyze rare variants.…”

Section: Introductionmentioning

confidence: 99%

Meta-analysis of quantitative pleiotropic traits for next-generation sequencing with multivariate functional linear models

Chiu¹,

Jung²,

Chen³

et al. 2016

Eur J Hum Genet

View full text Add to dashboard Cite

To analyze next-generation sequencing data, multivariate functional linear models are developed for a meta-analysis of multiple studies to connect genetic variant data to multiple quantitative traits adjusting for covariates. The goal is to take the advantage of both meta-analysis and pleiotropic analysis in order to improve power and to carry out a unified association analysis of multiple studies and multiple traits of complex disorders. Three types of approximate F -distributions based on Pillai-Bartlett trace, HotellingLawley trace, and Wilks's Lambda are introduced to test for association between multiple quantitative traits and multiple genetic variants. Simulation analysis is performed to evaluate false-positive rates and power of the proposed tests. The proposed methods are applied to analyze lipid traits in eight European cohorts. It is shown that it is more advantageous to perform multivariate analysis than univariate analysis in general, and it is more advantageous to perform meta-analysis of multiple studies instead of analyzing the individual studies separately. The proposed models require individual observations. The value of the current paper can be seen at least for two reasons: (a) the proposed methods can be applied to studies that have individual genotype data; (b) the proposed methods can be used as a criterion for future work that uses summary statistics to build test statistics to meta-analyze the data. INTRODUCTION Meta-analysis of multiple studies and pleiotropy analysis of multiple traits are two areas in association studies that recently have received extensive attention in the literature. 1-10 To our knowledge, metaanalysis and pleiotropy analysis have been performed separately so far, and there are no gene-based meta-analysis methods for combining multiple studies together and for carrying out a unified pleiotropy analysis. Here, multivariate functional linear models (MFLM) are developed to connect genetic variant data to multiple quantitative traits adjusting for covariates in a meta-analysis context. The goal is to take the advantage of both meta-analysis and pleiotropy analysis in order to improve power and to carry out a unified analysis of multiple studies and multiple quantitative traits of complex disorders.A noticeable feature of next-generation sequencing data is that dense panels of genetic variants are available via high-throughput sequencing technology, and so we face high-dimension genetic data. [11][12][13][14] The genetic data can consist of rare variants, or common variants, or a combination of the two, where the rare variants' minor allele frequencies (MAFs) are less than 0.01 ∼ 0.05. The high dimensionality of genetic data and the presence of dense rare variants raise

show abstract

Region-Based Association Test for Familial Data under Functional Linear Models

Cited by 20 publications

References 33 publications

A comparison study of multivariate fixed models and Gene Association with Multiple Traits (GAMuT) for next‐generation sequencing

A comparison study of multivariate fixed models and Gene Association with Multiple Traits (GAMuT) for next‐generation sequencing

Uncovering Local Trends in Genetic Effects of Multiple Phenotypes via Functional Linear Models

Meta-analysis of quantitative pleiotropic traits for next-generation sequencing with multivariate functional linear models

Contact Info

Product

Resources

About