Statistical analysis strategies for association studies involving rare variants.

paper Cited Public

Authors: Bansal, Vikas; Libiger, Ondrej; Torkamani, Ali; Schork, Nicholas J
Year: 2010
Journal: Nature reviews. Genetics
PMID: 20940738
DOI: 10.1038/nrg2867
PMCID: PMC3743540

Figure 1

Sample size requirements and statistical power for variants of different frequencies(A). Sample sizes necessary to detect an association between an allele with a specific effect size and a binary trait. The plots assume a standard z-test for the difference in the frequency of the allele between the two phenotypic categories. A genome-wide type I error rate of 10−9 was assumed, under the assumption that one may perform 2 orders of magnitude more tests in a complete sequence-based GWAS than a standard GWAS. (B). Similar setting to that provided in Figure 1A except the effect size depicted on the x axis gives the ratio of the frequency of the allele in the case vs. control groups. These curves give insight into the power gains associated with the collapsing strategy. Consider the black line in Figure 1B and testing a single rare variant with a frequency of 0.01 in the controls and 0.02 in the cases. This difference would require approximately 250,000 cases and controls to detect with 80% power at a super genome-wide level of significance. However, if one were to test 5 such variants with the same frequencies after collapsing them (assuming they are independent and no individual has more than one such variant), then one would effectively be testing a 0.05 frequency among the controls and a 0.10 frequency among the cases. From the red line in Figure 1B this difference would require only 3000 cases and controls. (C). Power to detect a quantitative trait locus with a sample of 1000 individuals as a function of fraction of phenotypic variation explained by the locus via standard linear regression analysis. A genome-wide type I error rate of 10−9 was assumed.

Figure 2

Scenarios in which DNA sequence variants distinguish cases and controlsBlue lines indicate genomic regions; red boxes indicate variants. A. Variants at a single locus with common alleles are more frequent in cases then controls. B. Multiple rare variations contribute to the phenotype such that the collective frequency of these variations is greater in cases. This would create a greater diversity of haplotypes or DNA sequences among the cases. C. Multiple rare variations contribute to the phenotype, but act in a synergistic fashion such that cases are likely to have more similar DNA sequences compared to controls. D. Multiple rare variations contribute to a phenotype, but the variations contributing to the phenotype reside in specific genomic regions. This situation would create greater sequence diversity among the cases, as in setting B, but only within the genomic regions of relevance.

#	Section	Preview
0	Introduction	Despite the success of genome wide association (GWA) studies in identifying common single nucleotide…
1	Introduction	There are many reasons to believe that multiple rare variants, both within the same gene and across…
2	Introduction	To comprehensively characterize the contribution of rare variants to phenotypic expression, one…
3	Introduction	In addition to a sequencing technology and an appropriate sampling and study design, bioinformatic…
4	Introduction	There are many settings in which a collection of rare variants might exhibit an association with a…
5	Capturing the Effects of Rare Variants — The nature of the effect of rare variants	As noted, rare variants are likely to influence a trait along with common variants.4, 14 In…
6	Capturing the Effects of Rare Variants — The nature of the effect of rare variants	Of these possible settings, the one receiving the most attention by statistical geneticists is the…
7	Capturing the Effects of Rare Variants — Single locus tests vs. ‘collapsing’ sets of rare variants	The simplest approach to testing rare variants for association with a trait is to test them…
8	Capturing the Effects of Rare Variants — Single locus tests vs. ‘collapsing’ sets of rare variants	control groups, and then testing the two groups for frequency differences. This strategy forms the…
9	Capturing the Effects of Rare Variants — Quantitative Traits and Conditional Analysis	Regression-based collapsed variant and conditional tests can greatly enhance association studies…
10	Capturing the Effects of Rare Variants — Quantitative Traits and Conditional Analysis	as covariate effects, the effects of previously identified common variants, or other collapsed sets…
11	Capturing the Effects of Rare Variants — Defining Collapsing Sets of Rare Variants via Function or Proximity	The collapsing strategy makes important assumptions. First, some formulations of collapsed tests…
12	Capturing the Effects of Rare Variants — Defining Collapsing Sets of Rare Variants via Function or Proximity	Although there are a number of ways to leverage functional annotations to guide the collapsing of…
13	Capturing the Effects of Rare Variants — Defining Collapsing Sets of Rare Variants via Function or Proximity	It is important to note the distinction between leveraging functional annotations to collapse a set…
14	Specific analysis models	There are a number of statistical analysis strategies that can be used to test the hypothesis that…
15	Specific analysis models — Methods based on summary statistics	Morgenthaler and Thilly30 were the first to describe a version of the collapsing approach in which…
16	Specific analysis models — Methods based on summary statistics	between groups. This testing could potentially be done simultaneously with frequency differences at…
17	Specific analysis models — Methods based on summary statistics	Madsen and Browning proposed a statistic for testing a prespecified collapsed set of variants that…
18	Specific analysis models — Methods based on summary statistics	Recently, Price et al.35 implemented a method for testing rare coding variants that considers…
19	Specific analysis models — Methods based on summary statistics	Another way of exploiting summary statistics for rare variant analysis involves comparing haplotype…

Name	Type
1000 Genomes Project	cohort
1000 individuals	cohort
BRCA1	gene
BRCA2	gene
breast cancer	phenotype
candidate disease genes local	gene
case group	cohort
cases	cohort
cases and controls local	cohort
Collapsed Set of Variants local	variant
common SNVs local	variant
common variants	cohort
Common variations local	variant
complex diseases	phenotype
complex traits	phenotype
Congenital disease local	phenotype
control	cohort
control group	cohort
controls	cohort
copy number variations	variant
cystic fibrosis	phenotype
disease	phenotype
EAH situation local	cohort
exonic variant local	variant
extreme obesity	phenotype
extreme phenotype values local	phenotype
FAAH	gene
families	cohort
genic variant local	variant
GWA study	cohort
haplotype	variant
human geoethnic groups local	cohort
MGLL	gene
neuropsychiatric disorders	phenotype
non-synonymous coding variant local	variant
non-synonymous coding variant in active site local	variant
phenotype	phenotype
phenotypic expression local	phenotype
population	cohort
quantitative phenotypes	phenotype
rare CNVs	variant
rare coding variant local	variant
rare SNVs local	variant
rare variant	cohort
SNP	cohort
structural variant	cohort
trait	phenotype
tumorigenesis	phenotype

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In this knowledge base

Title	Year	PMID
On the association of common and rare genetic variation influencing body mass index: a combined SNP and CNV analysis.	2014	24884913
Rare nonsynonymous exonic variants in addiction and behavioral disinhibition.	2014	24094508
Exome sequencing and the genetic basis of complex traits.	2012	22641211
Rare and common variants: twenty arguments.	2012	22251874

External

Title	Authors	Journal	Year	Link
cellSTAAR: incorporating single-cell-sequencing-based functional data to boost power in rare variant association testing of noncoding regions.	Van Buren E et al.	—	2026	→
Scalable and accurate rare-variant association tests for whole genome sequencing time-to-event analysis in large biobanks.	Song S et al.	—	2026	→
Adapting PRISMA Guidelines to Enhance Reporting Quality in Genetic Association Studies: A Framework Proposal.	Nezameslami R et al.	—	2025	→
Advancements and challenges in using AI for biomarker detection in early Alzheimer's disease.	Beheshti I et al.	—	2025	→
Assessment of the functionality and usability of open-source rare variant analysis pipelines.	Riccio C et al.	—	2025	→
Neurodevelopment Genes Encoding Olduvai Domains Link Myalgic Encephalomyelitis to Neuropsychiatric Disorders.	Arcos-Burgos M et al.	—	2025	→
Biostatistical Aspects of Whole Genome Sequencing Studies: Preprocessing and Quality Control.	Betschart RO et al.	—	2024	→
DYNATE: Localizing rare-variant association regions via multiple testing embedded in an aggregation tree.	Li X et al.	—	2024	→
Exome Analysis Points<i>APOE4</i>Haplotype as Major Risk to Develop Mesoamerican Nephropathy	Landires I et al.	—	2024	—
Genetic modifiers of cognitive decline in PSEN1 E280A Alzheimer's disease.	Sepulveda-Falla D et al.	—	2024	→
Genomic analysis reveals the association of KIT and MITF variants with the white spotting in swamp buffaloes.	Dai D et al.	—	2024	→
TRIO RVEMVS: A Bayesian framework for rare variant association analysis with expectation-maximization variable selection using family trio data.	Yu D et al.	—	2024	→
A genotype-to-phenotype approach suggests under-reporting of single nucleotide variants in nephrocystin-1 (NPHP1) related disease (UK 100,000 Genomes Project).	Leggatt G et al.	—	2023	→
Common and rare variant associations with latent traits underlying depression, bipolar disorder, and schizophrenia.	Dattani S et al.	—	2023	→
Relationship between the TGFBR1 Gene and Molar Incisor Hypomineralization.	Georgina-Pérez L et al.	—	2023	→
A framework for detecting noncoding rare-variant associations of large-scale whole-genome sequencing studies.	Li Z et al.	—	2022	→
Genetic and functional analyses implicate microRNA 499A in bipolar disorder development.	Tielke A et al.	—	2022	→
Pedigree investigation, clinical characteristics, and prognosis analysis of haematological disease patients with germline TET2 mutation.	Wu X et al.	—	2022	→
Performing Genome-Wide Association Studies Using rMVP.	Liu X et al.	—	2022	→
Simulation Research on the Methods of Multi-Gene Region Association Analysis Based on a Functional Linear Model.	Li S et al.	—	2022	→
Simultaneous Detection of Signal Regions Using Quadratic Scan Statistics With Applications to Whole Genome Association Studies.	Li Z et al.	—	2022	→
The Genetic Architecture of Non-Syndromic Rhegmatogenous Retinal Detachment.	Moledina M et al.	—	2022	→
A fast and powerful aggregated Cauchy association test for joint analysis of multiple phenotypes.	Chen L et al.	—	2021	→
A two-stage testing strategy for detecting genes×environment interactions in association studies.	Zhou J et al.	—	2021	→
Controlling for human population stratification in rare variant association studies.	Bouaziz M et al.	—	2021	→
Gene-Based Association Testing of Dichotomous Traits With Generalized Functional Linear Mixed Models Using Extended Pedigrees: Applications to Age-Related Macular Degeneration.	Jiang Y et al.	—	2021	→
Genome-wide association study and its applications in the non-model crop Sesamum indicum.	Berhe M et al.	—	2021	→
Identification of Influential Variants in Significant Aggregate Rare Variant Tests.	Blumhagen RZ et al.	—	2021	→
Identification of Novel Genomic-Variant Patterns of OR56A5, OR52L1, and CTSD in Retinitis Pigmentosa Patients by Whole-Exome Sequencing.	Lin TY et al.	—	2021	→
Integrative analysis of multi-omics data for discovering low-frequency variants associated with low-density lipoprotein cholesterol levels.	Yang T et al.	—	2021	→
Interplay between IL6 and CRIM1 in thiopurine intolerance due to hematological toxicity in leukemic patients with wild-type NUDT15 and TPMT.	Kim H et al.	—	2021	→
VCSEL: PRIORITIZING SNP-SET BY PENALIZED VARIANCE COMPONENT SELECTION.	Kim J et al.	—	2021	→
Whole-genome sequencing reveals KRTAP1-1 as a novel genetic variant associated with antidepressant treatment outcomes.	Park JH et al.	—	2021	→
Dynamic incorporation of multiple in silico functional annotations empowers rare variant association analysis of large whole-genome sequencing studies at scale.	Li X et al.	—	2020	→
Familial Alzheimer's Disease and Recessive Modifiers.	Vélez JI et al.	—	2020	→
Identifying rare variants for quantitative traits in extreme samples of population via Kullback-Leibler distance.	Xiang Y et al.	—	2020	→
Novel exomic rare variants associated with venous thrombosis.	Deguchi H et al.	—	2020	→
Views on GWAS statistical analysis.	Cao X et al.	—	2020	→
Whole-exome sequencing of 81 individuals from 27 multiply affected bipolar disorder families.	Forstner AJ et al.	—	2020	→
A general statistic to test an optimally weighted combination of common and/or rare variants.	Zhang J et al.	—	2019	→
A modified association test for rare and common variants based on affected sib-pair design.	Guo Y et al.	—	2019	→
Association mapping in plants in the post-GWAS genomics era.	Gupta PK et al.	—	2019	→
Association score testing for rare variants and binary traits in family data with shared controls.	Saad M et al.	—	2019	→
Determining population stratification and subgroup effects in association studies of rare genetic variants for nicotine dependence.	Hsieh AR et al.	—	2019	→
Dynamic Scan Procedure for Detecting Rare-Variant Association Regions in Whole-Genome Sequencing Studies.	Li Z et al.	—	2019	→
Genetic Variation Underpinning ADHD Risk in a Caribbean Community.	Puentes-Rozo PJ et al.	—	2019	→
Pathway enrichment analysis and visualization of omics data using g:Profiler, GSEA, Cytoscape and EnrichmentMap.	Reimand J et al.	—	2019	→
Real world scenarios in rare variant association analysis: the impact of imbalance and sample size on the power in silico.	Zhang X et al.	—	2019	→
Rediscovering the value of families for psychiatric genetics research.	Glahn DC et al.	—	2019	→
Regulation of glucose and lipid metabolism in health and disease.	Chen L et al.	—	2019	→
Star Allele-Based Haplotyping versus Gene-Wise Variant Burden Scoring for Predicting 6-Mercaptopurine Intolerance in Pediatric Acute Lymphoblastic Leukemia Patients.	Park Y et al.	—	2019	→
Targeting Neuroplasticity, Cardiovascular, and Cognitive-Associated Genomic Variants in Familial Alzheimer's Disease.	Vélez JI et al.	—	2019	→
Telomerase Variants in Patients with Cirrhosis Awaiting Liver Transplantation.	Chiu V et al.	—	2019	→
The Role of ERRFI1+808T/G Polymorphism in Diabetic Nephropathy.	Asgarbeik S et al.	—	2019	→
Whole genome sequencing and rare variant analysis in essential tremor families.	Odgerel Z et al.	—	2019	→
Advances in the Genetics of Hypertension: The Effect of Rare Variants.	Russo A et al.	—	2018	→
A model-free test for detecting disease association signals with multiple genetic variants and covariates.	Lee JY et al.	—	2018	→
Assessing Rare Variation in Complex Traits.	Kuchenbaecker K et al.	—	2018	→
Association analysis of multiple traits by an approach of combining P values.	Chen L et al.	—	2018	→
Association analysis of rare and common variants with multiple traits based on variable reduction method.	Chen L et al.	—	2018	→
A subregion-based burden test for simultaneous identification of susceptibility loci and subregions within.	Zhu B et al.	—	2018	→
BRCA1/2-negative, high-risk breast cancers (BRCAX) for Asian women: genetic susceptibility loci and their potential impacts.	Lee JY et al.	—	2018	→
Evaluation of Gene-Based Family-Based Methods to Detect Novel Genes Associated With Familial Late Onset Alzheimer Disease.	Fernández MV et al.	—	2018	→
Functional annotation of genomic variants in studies of late-onset Alzheimer's disease.	Butkiewicz M et al.	—	2018	→
Genetic architecture: the shape of the genetic contribution to human traits and disease.	Timpson NJ et al.	—	2018	→
Genome-Wide Association Analyses in the Model Rhizobium <i>Ensifer meliloti</i>.	Epstein B et al.	—	2018	→
GIGI-Quick: a fast approach to impute missing genotypes in genome-wide association family data.	Kunji K et al.	—	2018	→
Methods and results from the genome-wide association group at GAW20.	Wang X et al.	—	2018	→
Resequencing Epithelial Sodium Channel Genes Identifies Rare Variants Associated With Blood Pressure Salt-Sensitivity: The GenSalt Study.	Gu X et al.	—	2018	→
Bayesian longitudinal low-rank regression models for imaging genetic data from longitudinal studies.	Lu ZH et al.	—	2017	→
Common and rare genetic markers of lipid variation in subjects with type 2 diabetes from the ACCORD clinical trial.	Marvel SW et al.	—	2017	→
Detecting disease association with rare variants in case-parents studies.	Li YM et al.	—	2017	→
Genetics of neurodegenerative diseases: an overview.	Pihlstrøm L et al.	—	2017	→
Genome-based exome sequencing analysis identifies GYG1, DIS3L and DDRGK1 are associated with myocardial infarction in Koreans.	Lee JY et al.	—	2017	→
Genomic determinants of long-term cardiometabolic complications in childhood acute lymphoblastic leukemia survivors.	England J et al.	—	2017	→
Longitudinal data analysis for rare variants detection with penalized quadratic inference function.	Cao H et al.	—	2017	→
Meta-analysis of quantitative pleiotropic traits for next-generation sequencing with multivariate functional linear models.	Chiu CY et al.	—	2017	→
Microbial genome-wide association studies: lessons from human GWAS.	Power RA et al.	—	2017	→
On the association analysis of CNV data: a fast and robust family-based association method.	Liu M et al.	—	2017	→
Opportunities and challenges of whole-genome and -exome sequencing.	Petersen BS et al.	—	2017	→
PreCimp: Pre-collapsing imputation approach increases imputation accuracy of rare variants in terms of collapsed variables.	Kim YJ et al.	—	2017	→
Resequencing Study Identifies Rare Renin-Angiotensin-Aldosterone System Variants Associated With Blood Pressure Salt-Sensitivity: The GenSalt Study.	Kelly TN et al.	—	2017	→
SweGen: a whole-genome data resource of genetic variability in a cross-section of the Swedish population.	Ameur A et al.	—	2017	→
The screening of the functional microRNA binding site SNPs in sporadic colorectal cancer genes.	He H et al.	—	2017	→
What is the probability of replicating a statistically significant association in genome-wide association studies?	Jiang W et al.	—	2017	→
Whole exome sequencing implicates eye development, the unfolded protein response and plasma membrane homeostasis in primary open-angle glaucoma.	Zhou T et al.	—	2017	→
A new structural approach to genomic discovery of disease: example of adult-onset diabetes.	Sirovich L	—	2016	→
APOE*E2 allele delays age of onset in PSEN1 E280A Alzheimer's disease.	Vélez JI et al.	—	2016	→
Association Tests for Rare Variants.	Nicolae DL	—	2016	→
Detecting the Common and Individual Effects of Rare Variants on Quantitative Traits by Using Extreme Phenotype Sampling.	Zhou YJ et al.	—	2016	→
Discovery of rare variants for complex phenotypes.	Kosmicki JA et al.	—	2016	→
Gene-set association tests for next-generation sequencing data.	Lee J et al.	—	2016	→
Genetics of movement disorders in the next-generation sequencing era.	Olgiati S et al.	—	2016	→
Genetic Studies of Endophenotypes From Spine CT Scans Provide Novel Insights Into the Contribution of Mechanosensory Pathways to Vertebral Fractures and Spinal Curvature.	Tobias JH et al.	—	2016	→
Genetic variations underlying Alzheimer's disease: evidence from genome-wide association studies and beyond.	Cuyvers E et al.	—	2016	→
In Silico Functional Annotation of Genomic Variation.	Butkiewicz M et al.	—	2016	→
Meta-Analysis of Rare Variant Association Tests in Multiethnic Populations.	Mensah-Ablorh A et al.	—	2016	→
On Robust Association Testing for Quantitative Traits and Rare Variants.	Wei P et al.	—	2016	→
Post hoc Analysis for Detecting Individual Rare Variant Risk Associations Using Probit Regression Bayesian Variable Selection Methods in Case-Control Sequencing Studies.	Larson NB et al.	—	2016	→
Power estimation and sample size determination for replication studies of genome-wide association studies.	Jiang W et al.	—	2016	→
Progress in methods for rare variant association.	Santorico SA et al.	—	2016	→
Targeted deep resequencing of <i>ALOX5</i> and <i>ALOX5AP</i> in patients with diabetes and association of rare variants with leukotriene pathways.	Postula M et al.	—	2016	→
Techniques and Approaches to Genetic Analyses in Nephrological Disorders.	Willig LK	—	2016	→
The genetic architecture of resistance to virus infection in Drosophila.	Cogni R et al.	—	2016	→
Transmission and decorrelation methods for detecting rare variants using sequencing data from related individuals.	Darst BF et al.	—	2016	→
A New Method for Detecting Associations with Rare Copy-Number Variants.	Tzeng JY et al.	—	2015	→
A new strategy for enhancing imputation quality of rare variants from next-generation sequencing data via combining SNP and exome chip data.	Kim YJ et al.	—	2015	→
A powerful approach to test an optimally weighted combination of rare variants in admixed populations.	Wang X et al.	—	2015	→
Associating rare genetic variants with human diseases.	Zhang Q	—	2015	→
Detecting association of rare and common variants by adaptive combination of P-values.	Zhou Y et al.	—	2015	→
Detecting the Genomic Signature of Divergent Selection in Presence of Gene Flow.	Zeng P et al.	—	2015	→
ESPRESSO: taking into account assessment errors on outcome and exposures in power analysis for association studies.	Gaye A et al.	—	2015	→
Excess of rare variants in genes that are key epigenetic regulators of spermatogenesis in the patients with non-obstructive azoospermia.	Li Z et al.	—	2015	→
Generation of sequence-based data for pedigree-segregating Mendelian or Complex traits.	Li B et al.	—	2015	→
Genetics and brain morphology.	Strike LT et al.	—	2015	→
Genomic medicine and risk prediction across the disease spectrum.	Kotze MJ et al.	—	2015	→
HaploShare: identification of extended haplotypes shared by cases and evaluation against controls.	Ying D et al.	—	2015	→
Mendelian genes for Parkinson's disease contribute to the sporadic forms of the disease.	Spataro N et al.	—	2015	→
Peripartum Anesthetic Management and Genomic Analysis of Rare Variants in a Patient with Familial Pulmonary Fibrosis.	Sugino S et al.	—	2015	→
Permutation-based variance component test in generalized linear mixed model with application to multilocus genetic association study.	Zeng P et al.	—	2015	→
Phenome-Wide Association Studies: Embracing Complexity for Discovery.	Pendergrass SA et al.	—	2015	→
Rare variant association studies: considerations, challenges and opportunities.	Auer PL et al.	—	2015	→
Rare variants analysis using penalization methods for whole genome sequence data.	Yazdani A et al.	—	2015	→
Region-Based Association Test for Familial Data under Functional Linear Models.	Svishcheva GR et al.	—	2015	→
Renin, genes, microRNAs, and renal mechanisms involved in hypertension.	Morris BJ	—	2015	→
Scripps Genome ADVISER: Annotation and Distributed Variant Interpretation SERver.	Pham PH et al.	—	2015	→
Single-tube, highly parallel mutation enrichment in cancer gene panels by use of temperature-tolerant COLD-PCR.	Castellanos-Rizaldos E et al.	—	2015	→
Statistical analysis for genome-wide association study.	Zeng P et al.	—	2015	→
Strategies to improve the performance of rare variant association studies by optimizing the selection of controls.	Zhu N et al.	—	2015	→
The group exponential lasso for bi-level variable selection.	Breheny P	—	2015	→
The mini-driver model of polygenic cancer evolution.	Castro-Giner F et al.	—	2015	→
Using Hamming Distance as Information for SNP-Sets Clustering and Testing in Disease Association Studies.	Wang C et al.	—	2015	→
Accuracy of allele frequency estimation using pooled RNA-Seq.	Konczal M et al.	—	2014	→
A comparison of two collapsing methods in different approaches.	Dering C et al.	—	2014	→
Adaptive combination of P-values for family-based association testing with sequence data.	Lin WY	—	2014	→
Adjustment of familial relatedness in association test for rare variants.	Li C et al.	—	2014	→
A method to incorporate prior information into score test for genetic association studies.	Zakharov S et al.	—	2014	→
A powerful and adaptive association test for rare variants.	Pan W et al.	—	2014	→
A powerful association test of multiple genetic variants using a random-effects model.	Cheng KF et al.	—	2014	→
Approach to clinical and genetic characterization of statin-induced myopathy.	Feng Q	—	2014	→
Assessing multivariate gene-metabolome associations with rare variants using Bayesian reduced rank regression.	Marttinen P et al.	—	2014	→
Association mapping in crop plants: opportunities and challenges.	Gupta PK et al.	—	2014	→
Association testing of clustered rare causal variants in case-control studies.	Lin WY	—	2014	→
Bayesian Generalized Low Rank Regression Models for Neuroimaging Phenotypes and Genetic Markers.	Zhu H et al.	—	2014	→
Bioinformatics challenges in genome-wide association studies (GWAS).	De R et al.	—	2014	→
Chip-based direct genotyping of coding variants in genome wide association studies: utility, issues and prospects.	Nievergelt CM et al.	—	2014	→
Combining family- and population-based imputation data for association analysis of rare and common variants in large pedigrees.	Saad M et al.	—	2014	→
Correction for multiple testing in a gene region.	Hendricks AE et al.	—	2014	→
Epistasis analysis for quantitative traits by functional regression model.	Zhang F et al.	—	2014	→
Evaluating the impact of genotype errors on rare variant tests of association.	Cook K et al.	—	2014	→
Evidence for the role of EPHX2 gene variants in anorexia nervosa.	Scott-Van Zeeland AA et al.	—	2014	→
Family-based tests applied to extended pedigrees identify rare variants related to hypertension.	Xu M et al.	—	2014	→
Gene-based rare allele analysis identified a risk gene of Alzheimer's disease.	Kim JH et al.	—	2014	→
Genetic Analysis Workshop 18 single-nucleotide variant prioritization based on protein impact, sequence conservation, and gene annotation.	Nalpathamkalam T et al.	—	2014	→
Genetic dissection of the Drosophila melanogaster female head transcriptome reveals widespread allelic heterogeneity.	King EG et al.	—	2014	→
Genetic studies of Crohn's disease: past, present and future.	Liu JZ et al.	—	2014	→
Genotype imputation accuracy with different reference panels in admixed populations.	Huang GH et al.	—	2014	→
Germline variation in cancer-susceptibility genes in a healthy, ancestrally diverse cohort: implications for individual genome sequencing.	Bodian DL et al.	—	2014	→
GrabBlur--a framework to facilitate the secure exchange of whole-exome and -genome SNV data using VCF files.	Stade B et al.	—	2014	→
Identifying rare and common disease associated variants in genomic data using Parkinson's disease as a model.	Lin YC et al.	—	2014	→
Integrating EMR-linked and in vivo functional genetic data to identify new genotype-phenotype associations.	Mosley JD et al.	—	2014	→
Investigation of the involvement of MIR185 and its target genes in the development of schizophrenia.	Forstner AJ et al.	—	2014	→
Kernel-machine testing coupled with a rank-truncation method for genetic pathway analysis.	Yan Q et al.	—	2014	→
Likelihood ratio tests in rare variant detection for continuous phenotypes.	Zeng P et al.	—	2014	→
Logistic Principal Component Analysis for Rare Variants in Gene-Environment Interaction Analysis.	Lu M et al.	—	2014	→
Methods for collapsing multiple rare variants in whole-genome sequence data.	Sung YJ et al.	—	2014	→
More powerful genetic association testing via a new statistical framework for integrative genomics.	Zhao SD et al.	—	2014	→
Next Generation Statistical Genetics: Modeling, Penalization, and Optimization in High-Dimensional Data.	Lange K et al.	—	2014	→
Novel genetic susceptibility loci for diabetic end-stage renal disease identified through robust naive Bayes classification.	Sambo F et al.	—	2014	→
On the association of common and rare genetic variation influencing body mass index: a combined SNP and CNV analysis.	Peterson RE et al.	—	2014	→
Protective variant associated with alcohol dependence in a Mexican American cohort.	Norden-Krichmar TM et al.	—	2014	→
Rare and low-frequency variants in human common diseases and other complex traits.	Lettre G	—	2014	→
Rare nonsynonymous exonic variants in addiction and behavioral disinhibition.	Vrieze SI et al.	—	2014	→
Rare variant analysis of blood pressure phenotypes in the Genetic Analysis Workshop 18 whole genome sequencing data using sequence kernel association test.	Mallaney C et al.	—	2014	→
Rare variant association testing by adaptive combination of P-values.	Lin WY et al.	—	2014	→
Rare variants detection with kernel machine learning based on likelihood ratio test.	Zeng P et al.	—	2014	→
Regularized rare variant enrichment analysis for case-control exome sequencing data.	Larson NB et al.	—	2014	→
Statistical power and significance testing in large-scale genetic studies.	Sham PC et al.	—	2014	→
Targeted next-generation sequencing on Hirschsprung disease: a pilot study exploits DNA pooling.	Gui H et al.	—	2014	→
The interaction of a single-nucleotide polymorphism with age on response to interferon-α and ribavirin therapy in female patients with hepatitis C infection.	Nishino J et al.	—	2014	→
Using population isolates in genetic association studies.	Hatzikotoulas K et al.	—	2014	→
Whole genome sequencing data from pedigrees suggests linkage disequilibrium among rare variants created by population admixture.	Feng T et al.	—	2014	→
Adjustment for population stratification via principal components in association analysis of rare variants.	Zhang Y et al.	—	2013	→
Advances in the genetic dissection of plant cell walls: tools and resources available in Miscanthus.	Slavov G et al.	—	2013	→
A geometric framework for evaluating rare variant tests of association.	Liu K et al.	—	2013	→
A hybrid likelihood model for sequence-based disease association studies.	Chen YC et al.	—	2013	→
A powerful and efficient set test for genetic markers that handles confounders.	Listgarten J et al.	—	2013	→
Assessing the impact of population stratification on association studies of rare variation.	Jiang Y et al.	—	2013	→
Cancer pharmacogenomics: strategies and challenges.	Wheeler HE et al.	—	2013	→
Combined genotype and haplotype tests for region-based association studies.	Zakharov S et al.	—	2013	→
Comparison of similarity-based tests and pooling strategies for rare variants.	Zakharov S et al.	—	2013	→
Copy number variation analysis implicates the cell polarity gene glypican 5 as a human spina bifida candidate gene.	Bassuk AG et al.	—	2013	→
Detecting genomic clustering of risk variants from sequence data: cases versus controls.	Schaid DJ et al.	—	2013	→
Detecting rare variant effects using extreme phenotype sampling in sequencing association studies.	Barnett IJ et al.	—	2013	→
Detecting rare variants for psychiatric disorders using next generation sequencing: a methods primer.	Altmann A et al.	—	2013	→
Determination of genotype combinations that can predict the outcome of the treatment of alcohol dependence using the 5-HT(3) antagonist ondansetron.	Johnson BA et al.	—	2013	→
Exome sequencing-driven discovery of coding polymorphisms associated with common metabolic phenotypes.	Albrechtsen A et al.	—	2013	→
Exome sequencing identifies novel rheumatoid arthritis-susceptible variants in the BTNL2.	Mitsunaga S et al.	—	2013	→
Fine-scale patterns of population stratification confound rare variant association tests.	O'Connor TD et al.	—	2013	→
From genome-wide association studies to functional genomics: new insights into cardiovascular disease.	McPherson R	—	2013	→
Functional coding variants in SLC6A15, a possible risk gene for major depression.	Quast C et al.	—	2013	→
Functional linear models for association analysis of quantitative traits.	Fan R et al.	—	2013	→
Gene-environment interactions in genome-wide association studies: current approaches and new directions.	Winham SJ et al.	—	2013	→
Genetic variants and their interactions in disease risk prediction - machine learning and network perspectives.	Okser S et al.	—	2013	→
Has discovery-based cancer research been a bust?	Epstein RJ	—	2013	→
Identification of grouped rare and common variants via penalized logistic regression.	Ayers KL et al.	—	2013	→
Identification of single nucleotide polymorphisms in genes involved in digestive and metabolic processes associated with feed efficiency and performance traits in beef cattle.	Abo-Ismail MK et al.	—	2013	→
Identifying rare variants associated with complex traits via sequencing.	Li B et al.	—	2013	→
Integrated model of de novo and inherited genetic variants yields greater power to identify risk genes.	He X et al.	—	2013	→
Knowledge-constrained K-medoids Clustering of Regulatory Rare Alleles for Burden Tests.	Sivley RM et al.	—	2013	→
Multiple genetic variant association testing by collapsing and kernel methods with pedigree or population structured data.	Schaid DJ et al.	—	2013	→
On rare-variant analysis in population-based designs: decomposing the likelihood to two informative components.	Won S et al.	—	2013	→
Pathway-based approaches for sequencing-based genome-wide association studies.	Wu G et al.	—	2013	→
Poor Man's 1000 Genome Project: Recent Human Population Expansion Confounds the Detection of Disease Alleles in 7,098 Complete Mitochondrial Genomes.	Kim HL et al.	—	2013	→
Rare genomic structural variants in complex disease: lessons from the replication of associations with obesity.	Walters RG et al.	—	2013	→
Rare variant analysis for family-based design.	De G et al.	—	2013	→
Recursive organizer (ROR): an analytic framework for sequence-based association analysis.	Zhao LP et al.	—	2013	→
Robust and powerful tests for rare variants using Fisher's method to combine evidence of association from two or more complementary tests.	Derkach A et al.	—	2013	→
Screening for rare variants in the coding region of ALS-associated genes at 9p21.2 and 19p13.3.	Koppers M et al.	—	2013	→
Sequencing studies in human genetics: design and interpretation.	Goldstein DB et al.	—	2013	→
Single Nucleotide Polymorphism (SNP) Detection and Genotype Calling from Massively Parallel Sequencing (MPS) Data.	Li Y et al.	—	2013	→
Smoothed functional principal component analysis for testing association of the entire allelic spectrum of genetic variation.	Luo L et al.	—	2013	→
Targeted resequencing identifies defective variants of decoy receptor 3 in pediatric-onset inflammatory bowel disease.	Cardinale CJ et al.	—	2013	→
The genetic architecture of methotrexate toxicity is similar in Drosophila melanogaster and humans.	Kislukhin G et al.	—	2013	→
The impact of copy number deletions on general cognitive ability and ventricle size in patients with schizophrenia and healthy control subjects.	Yeo RA et al.	—	2013	→
A beginners guide to SNP calling from high-throughput DNA-sequencing data.	Altmann A et al.	—	2012	→
A comparison of gene region simulation methods.	Hendricks AE et al.	—	2012	→
Adaptive ridge regression for rare variant detection.	Zhan H et al.	—	2012	→
A fast and noise-resilient approach to detect rare-variant associations with deep sequencing data for complex disorders.	Cheung YH et al.	—	2012	→
A genome-wide meta-analysis of association studies of Cloninger's Temperament Scales.	Service SK et al.	—	2012	→
An evaluation of different meta-analysis approaches in the presence of allelic heterogeneity.	Asimit J et al.	—	2012	→
A novel genome-information content-based statistic for genome-wide association analysis designed for next-generation sequencing data.	Luo L et al.	—	2012	→
A permutation procedure to correct for confounders in case-control studies, including tests of rare variation.	Epstein MP et al.	—	2012	→
Characterisation and validation of insertions and deletions in 173 patient exomes.	Lescai F et al.	—	2012	→
Clinical implications of human population differences in genome-wide rates of functional genotypes.	Torkamani A et al.	—	2012	→
Comprehensive evaluation of imputation performance in African Americans.	Chanda P et al.	—	2012	→
Confluence of genes, environment, development, and behavior in a post Genome-Wide Association Study world.	Vrieze SI et al.	—	2012	→
Deep sequencing of the LRRK2 gene in 14,002 individuals reveals evidence of purifying selection and independent origin of the p.Arg1628Pro mutation in Europe.	Rubio JP et al.	—	2012	→
Detecting association of rare and common variants by testing an optimally weighted combination of variants.	Sha Q et al.	—	2012	→
Detecting rare variants for quantitative traits using nuclear families.	Guo W et al.	—	2012	→
Differential confounding of rare and common variants in spatially structured populations.	Mathieson I et al.	—	2012	→
Evidence for a role of the rare p.A152T variant in MAPT in increasing the risk for FTD-spectrum and Alzheimer's diseases.	Coppola G et al.	—	2012	→
Excess of rare variants in non-genome-wide association study candidate genes in patients with hypertriglyceridemia.	Johansen CT et al.	—	2012	→
Exome sequencing and the genetic basis of complex traits.	Kiezun A et al.	—	2012	→
Family-based association studies for next-generation sequencing.	Zhu Y et al.	—	2012	→
Finding genes and variants for lipid levels after genome-wide association analysis.	Willer CJ et al.	—	2012	→
Genetic adaptation of fatty-acid metabolism: a human-specific haplotype increasing the biosynthesis of long-chain omega-3 and omega-6 fatty acids.	Ameur A et al.	—	2012	→
Genetic influences in childhood obesity: recent progress and recommendations for experimental designs.	Fernandez JR et al.	—	2012	→
Genetics of coronary artery disease: genome-wide association studies and beyond.	Prins BP et al.	—	2012	→
Genetic Studies of Complex Diseases in the Sequence Era.	Xiong M	—	2012	→
Genome-wide association analysis of imputed rare variants: application to seven common complex diseases.	Mägi R et al.	—	2012	→
Genomic research to identify novel pathways in the development of abdominal aortic aneurysm.	Harrison SC et al.	—	2012	→
Handling the data management needs of high-throughput sequencing data: SpeedGene, a compression algorithm for the efficient storage of genetic data.	Qiao D et al.	—	2012	→
Hidradenitis suppurativa: viewpoint on clinical phenotyping, pathogenesis and novel treatments.	van der Zee HH et al.	—	2012	→
Identification of IGF1, SLC4A4, WWOX, and SFMBT1 as hypertension susceptibility genes in Han Chinese with a genome-wide gene-based association study.	Yang HC et al.	—	2012	→
Imputation of rare variants in next-generation association studies.	Asimit JL et al.	—	2012	→
Individualized risk for statin-induced myopathy: current knowledge, emerging challenges and potential solutions.	Feng Q et al.	—	2012	→
Integration of biological networks and pathways with genetic association studies.	Sun YV	—	2012	→
Interpreting noncoding genetic variation in complex traits and human disease.	Ward LD et al.	—	2012	→
Lessons from genome-wide association studies findings in Alzheimer's disease.	Moraes CF et al.	—	2012	→
Localization of association signal from risk and protective variants in sequencing studies.	Brisbin A et al.	—	2012	→
Multiple regression methods show great potential for rare variant association tests.	Xu C et al.	—	2012	→
Next generation analytic tools for large scale genetic epidemiology studies of complex diseases.	Mechanic LE et al.	—	2012	→
Not just genomewide association studies: rare variants in genes not identified through genomewide association studies also contribute to hypertriglyceridemia.	Evans D et al.	—	2012	→
Osteoarthritis year 2011 in review: genetics.	Meulenbelt I	—	2012	→
Pooled DNA resequencing of 68 myocardial infarction candidate genes in French canadians.	Beaudoin M et al.	—	2012	→
Predicting signatures of "synthetic associations" and "natural associations" from empirical patterns of human genetic variation.	Chang D et al.	—	2012	→
Promises and challenges of pharmacogenetics: an overview of study design, methodological and statistical issues.	Ross S et al.	—	2012	→
Properties and power of the Drosophila Synthetic Population Resource for the routine dissection of complex traits.	King EG et al.	—	2012	→
Quantitative trait locus analysis for next-generation sequencing with the functional linear models.	Luo L et al.	—	2012	→
Rare and common variants: twenty arguments.	Gibson G	—	2012	→
Rare and low frequency variant stratification in the UK population: description and impact on association tests.	Babron MC et al.	—	2012	→
Rare copy number variations in adults with tetralogy of Fallot implicate novel risk gene pathways.	Silversides CK et al.	—	2012	→
Rare variants in ischemic stroke: an exome pilot study.	Cole JW et al.	—	2012	→
Rare variants in TMEM132D in a case-control sample for panic disorder.	Quast C et al.	—	2012	→
Rare versus common variants in pharmacogenetics: SLCO1B1 variation and methotrexate disposition.	Ramsey LB et al.	—	2012	→
Resolving the variable genome and epigenome in human disease.	Knight JC	—	2012	→
Statistical guidance for experimental design and data analysis of mutation detection in rare monogenic mendelian diseases by exome sequencing.	Zhi D et al.	—	2012	→
Statistical tests for detecting rare variants using variance-stabilising transformations.	Wang K et al.	—	2012	→
Surrogate genetics and metabolic profiling for characterization of human disease alleles.	Mayfield JA et al.	—	2012	→
Testing rare variants for association with diseases: a Bayesian marker selection approach.	Zhang L et al.	—	2012	→
The genetics of sudden cardiac death.	Arking DE et al.	—	2012	→
The next generation of complex lung genetic studies.	Yang IV et al.	—	2012	→
Toll-like receptor gene polymorphisms are associated with allergic rhinitis: a case control study.	Nilsson D et al.	—	2012	→
Two adaptive weighting methods to test for rare variant associations in family-based designs.	Fang S et al.	—	2012	→
Ultrasensitive detection of rare mutations using next-generation targeted resequencing.	Flaherty P et al.	—	2012	→
Unraveling the genetic component of systemic sclerosis.	Martín JE et al.	—	2012	→
U-statistics in genetic association studies.	Li H	—	2012	→
Weighted pedigree-based statistics for testing the association of rare variants.	Shugart YY et al.	—	2012	→
Whole-genome and whole-exome sequencing in neurological diseases.	Foo JN et al.	—	2012	→
Adaptive tests for association analysis of rare variants.	Pan W et al.	—	2011	→
An application and empirical comparison of statistical analysis methods for associating rare variants to a complex phenotype.	Bansal V et al.	—	2011	→
A new expectation-maximization statistical test for case-control association studies considering rare variants obtained by high-throughput sequencing.	Gordon D et al.	—	2011	→
Angiogenin variants in Parkinson disease and amyotrophic lateral sclerosis.	van Es MA et al.	—	2011	→
Annotating individual human genomes.	Torkamani A et al.	—	2011	→
Assessing the impact of non-differential genotyping errors on rare variant tests of association.	Powers S et al.	—	2011	→
Association analysis identifies ZNF750 regulatory variants in psoriasis.	Birnbaum RY et al.	—	2011	→
Association studies for next-generation sequencing.	Luo L et al.	—	2011	→
Association tests for rare and common variants based on genotypic and phenotypic measures of similarity between individuals.	Thalamuthu A et al.	—	2011	→
Breakthroughs in the genetics of orofacial clefting.	Mangold E et al.	—	2011	→
Comparison of statistical tests for disease association with rare variants.	Basu S et al.	—	2011	→
Computational and statistical approaches to analyzing variants identified by exome sequencing.	Stitziel NO et al.	—	2011	→
Confounded by sequencing depth in association studies of rare alleles.	Garner C	—	2011	→
Design considerations for massively parallel sequencing studies of complex human disease.	Feng BJ et al.	—	2011	→
Detecting rare and common variants for complex traits: sibpair and odds ratio weighted sum statistics (SPWSS, ORWSS).	Feng T et al.	—	2011	→
Dietary unsaturated fatty acids affect the mammary gland integrity and health in lactating dairy cows.	Mach N et al.	—	2011	→
Different approaches for dealing with rare variants in family-based genetic studies: application of a Genetic Analysis Workshop 17 problem.	Alfonso de Almeida MA et al.	—	2011	→
Disease risk prediction with rare and common variants.	Wu C et al.	—	2011	→
Estimation of allele frequency and association mapping using next-generation sequencing data.	Kim SY et al.	—	2011	→
Exome sequencing as a tool for Mendelian disease gene discovery.	Bamshad MJ et al.	—	2011	→
Family-based designs for genome-wide association studies.	Ott J et al.	—	2011	→
From sequence to function: Insights from natural variation in budding yeasts.	Nieduszynski CA et al.	—	2011	→
Hierarchical generalized linear models for multiple groups of rare and common variants: jointly estimating group and individual-variant effects.	Yi N et al.	—	2011	→
Human genetics and genomics a decade after the release of the draft sequence of the human genome.	Naidoo N et al.	—	2011	→
Incorporating model uncertainty in detecting rare variants: the Bayesian risk index.	Quintana MA et al.	—	2011	→
Integrating Rare-Variant Testing, Function Prediction, and Gene Network in Composite Resequencing-Based Genome-Wide Association Studies (CR-GWAS).	Zhu C et al.	—	2011	→
Mapping rare and common causal alleles for complex human diseases.	Raychaudhuri S	—	2011	→
Methods for adjusting population structure and familial relatedness in association test for collective effect of multiple rare variants on quantitative traits.	Zhang Q et al.	—	2011	→
Mining the LIPG allelic spectrum reveals the contribution of rare and common regulatory variants to HDL cholesterol.	Khetarpal SA et al.	—	2011	→
Multi-ethnic studies in complex traits.	Fu J et al.	—	2011	→
New insights into old methods for identifying causal rare variants.	Wang H et al.	—	2011	→
On the Aggregation of Multimarker Information for Marker-Set and Sequencing Data Analysis: Genotype Collapsing vs. Similarity Collapsing.	Pongpanich M et al.	—	2011	→
On the analysis of sequence data: testing for disease susceptibility loci using patterns of linkage disequilibrium.	Lipman PJ et al.	—	2011	→
Optimum designs for next-generation sequencing to discover rare variants for common complex disease.	Shi G et al.	—	2011	→
Population-based and family-based designs to analyze rare variants in complex diseases.	Kazma R et al.	—	2011	→
Rare variant density across the genome and across populations.	Raska P et al.	—	2011	→
Renin, genes, and beyond: 40 years of molecular discoveries in the hypertension field.	Morris BJ	—	2011	→
Statistical analysis of rare sequence variants: an overview of collapsing methods.	Dering C et al.	—	2011	→
Study designs for identification of rare disease variants in complex diseases: the utility of family-based designs.	Ionita-Laza I et al.	—	2011	→
Tests of association for rare variants: case control mutation screening.	Tavtigian SV et al.	—	2011	→
The relative importance of common and rare genetic variants in the development of hypertriglyceridemia.	Evans D et al.	—	2011	→
Using extreme phenotype sampling to identify the rare causal variants of quantitative traits in association studies.	Li D et al.	—	2011	→
Voxelwise gene-wide association study (vGeneWAS): multivariate gene-based association testing in 731 elderly subjects.	Hibar DP et al.	—	2011	→
Three ways of combining genotyping and resequencing in case-control association studies.	Longmate JA et al.	—	2010	→