Dynamic incorporation of multiple in silico functional annotations empowers rare variant association analysis of large whole-genome sequencing studies at scale

Li, Xihao; Li, Fulin; Zhou, Hufeng; Gaynor, Sheila M.; Liu, Yaowu; Chen, Han; Sun, Ryan; Dey, Rounak; Arnett, Donna K.; Aslibekyan, Stella; Ballantyne, Christie M.; Bielak, Lawrence F.; Blangero, John; Boerwinkle, Eric; Bowden, Donald W.; Broome, Jai; Conomos, Matthew P.; Correa, Adolfo; Cupples, L. Adrienne; Curran, Joanne E.; Freedman, Barry I.; Guo, Xiuqing; Hindy, George; Irvin, Marguerite R.; Kardia, Sharon L.R.; Kathiresan, Sekar; Khan, Alyna; Kooperberg, Charles; Laurie, Cathy C.; Liu, X Shirley; Mahaney, Michael C.; Manichaikul, Ani; Martin, Lisa W.; Mathias, Rasika A.; McGarvey, Stephen T.; Mitchell, Braxton D.; Montasser, May E.; Moore, Jill E.; Morrison, Alanna C.; O’Connell, Jeffrey R.; Palmer, Nicholette D.; Pampana, Akhil; Peralta, Juan M.; Peyser, Patricia A.; Psaty, Bruce M.; Redline, Susan; Rice, Kenneth; Rich, Stephen S.; Smith, Jennifer A.; Tiwari, Hemant K.; Tsai, Michael Y.; Vasan, Ramachandran S.; Wang, Feifei; Weeks, Daniel E.; Weng, Zhiping; Wilson, James G.; Yanek, Lisa R.; Benjamin, Emelia J.; Sunyaev, Shamil; Abecasis, Gonçalo R.; Rotter, Jerome I.; Willer, Cristen J.; Peloso, Gina M.; Natarajan, Pradeep; Lin, Xihong

doi:10.1038/s41588-020-0676-4

Cited by 171 publications

(188 citation statements)

References 91 publications

(113 reference statements)

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“…The top hit in UKBB (rs157592, MAF = 18.7%, p-value = 1.87 x 10 -8 ) had LD r 2 = 0.7 with rs429358 as presented in the Supplementary Table 3. This variant is in the intergenic region and have no in-silico functions according to the FAVOR functional annotation online portal 56 (See URL).…”

Section: Resultsmentioning

confidence: 99%

“…Third, the current implementation of GATE is targeted to perform single-variant association analysis, which can suffer from low power to detect associations in extremely rare variants. With whole genome and whole exome sequencing data available, a possible future extension of this method can allow for mask-based or region-based association tests to improve power for the rare variants 56,59 . Finally, the current version of GATE does not incorporate left-truncated data, which may not be valid for early-onset phenotypes in biobanks with relatively older participants.…”

Section: Discussionmentioning

confidence: 99%

“…Manhattan plots, Q-Q plots, and regional association plots for each TTE phenotype as well as the PheWAS plots can be browsed at http://phewas.genohub.org/. The FAVOR 56 portal is accessed through favor.genohub.org.…”

Section: Urlsmentioning

confidence: 99%

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An efficient and accurate frailty model approach for genome-wide survival association analysis controlling for population structure and relatedness in large-scale biobanks

Dey

Zhou

Kiiskinen

et al. 2020

Preprint

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With decades of electronic health records linked to genetic data, large biobanks provide unprecedented opportunities for systematically understanding the genetics of the natural history of complex diseases. Genome-wide survival association analysis can identify genetic variants associated with ages of onset, disease progression and lifespan. We developed an efficient and accurate frailty (random effects) model approach for genome-wide survival association analysis of censored time-to-event (TTE) phenotypes in large biobanks by accounting for both population structure and relatedness. Our method utilizes state-of-the-art optimization strategies to reduce the computational cost. The saddlepoint approximation is used to allow for analysis of heavily censored phenotypes (>90%) and low frequency variants (down to minor allele count 20). We demonstrated the performance of our method through extensive simulation studies and analysis of five TTE phenotypes, including lifespan, with heavy censoring rates (90.9% to 99.8%) on ~400,000 UK Biobank participants with white British ancestry and ~180,000 samples in FinnGen, respectively. We further performed genome-wide association analysis for 871 TTE phenotypes in UK Biobank and presented the genome-wide scale phenome-wide association (PheWAS) results with the PheWeb browser.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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An efficient and accurate frailty model approach for genome-wide survival association analysis controlling for population structure and relatedness in large-scale biobanks

Dey

Zhou

Kiiskinen

et al. 2020

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“…We show that TOPMed WGS data provide a rich resource for developing and testing methods for surveying human variation, for inference of human demography and for exploring functional constraints on the genome 73 , 74 . In addition to these uses, we expect that TOPMed data will improve nearly all ongoing studies of common and rare disorders by providing both a deep catalogue of variation in healthy individuals and an imputation resource that enables array-based studies to achieve a completeness that was previously attainable only through direct sequencing.…”

Section: Conclusion and Future Prospectsmentioning

confidence: 99%

Sequencing of 53,831 diverse genomes from the NHLBI TOPMed Program

Taliun¹,

Harris²,

Kessler³

et al. 2021

Nature

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The Trans-Omics for Precision Medicine (TOPMed) programme seeks to elucidate the genetic architecture and biology of heart, lung, blood and sleep disorders, with the ultimate goal of improving diagnosis, treatment and prevention of these diseases. The initial phases of the programme focused on whole-genome sequencing of individuals with rich phenotypic data and diverse backgrounds. Here we describe the TOPMed goals and design as well as the available resources and early insights obtained from the sequence data. The resources include a variant browser, a genotype imputation server, and genomic and phenotypic data that are available through dbGaP (Database of Genotypes and Phenotypes)1. In the first 53,831 TOPMed samples, we detected more than 400 million single-nucleotide and insertion or deletion variants after alignment with the reference genome. Additional previously undescribed variants were detected through assembly of unmapped reads and customized analysis in highly variable loci. Among the more than 400 million detected variants, 97% have frequencies of less than 1% and 46% are singletons that are present in only one individual (53% among unrelated individuals). These rare variants provide insights into mutational processes and recent human evolutionary history. The extensive catalogue of genetic variation in TOPMed studies provides unique opportunities for exploring the contributions of rare and noncoding sequence variants to phenotypic variation. Furthermore, combining TOPMed haplotypes with modern imputation methods improves the power and reach of genome-wide association studies to include variants down to a frequency of approximately 0.01%.

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“…MACIE scores have already been used, for example, to identify and characterize inflammation and immune-related risk variants in squamous cell lung cancer41 . Finally, the proposed MACIE scores can be used as a weighting scheme to further empower variant-set analyses of rare variants42 .…”

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confidence: 99%

A multi-dimensional integrative scoring framework for predicting functional variants in the human genome

Yung

Zhou

et al. 2021

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Attempts to identify and prioritize functional DNA elements in coding and noncoding regions, particularly through use of in silico functional annotation data, continue to increase in popularity. However, specific functional roles may vary widely from one variant to another, making it challenging to summarize different aspects of variant function. Here we propose Multi-dimensional Annotation Class Integrative Estimation (MACIE), an unsupervised multivariate mixed model framework capable of integrating annotations of diverse origin to assess multi-dimensional functional roles for both coding and noncoding variants. Unlike existing one-dimensional scoring methods, MACIE views variant functionality as a composite attribute encompassing multiple different characteristics, and estimates the joint posterior functional probability vector of each genomic position, a quantity that offers richer and more interpretable information in the presence of multiple aspects of functionality. Applied to a variety of independent coding and non-coding datasets, MACIE demonstrates powerful and robust performance in discriminating between functional and non-functional variants. We also show an application of MACIE to fine-mapping using lipids GWAS summary statistics data from the European Network for Genetic and Genomic Epidemiology Consortium.

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Dynamic incorporation of multiple in silico functional annotations empowers rare variant association analysis of large whole-genome sequencing studies at scale

Cited by 171 publications

References 91 publications

An efficient and accurate frailty model approach for genome-wide survival association analysis controlling for population structure and relatedness in large-scale biobanks

An efficient and accurate frailty model approach for genome-wide survival association analysis controlling for population structure and relatedness in large-scale biobanks

Sequencing of 53,831 diverse genomes from the NHLBI TOPMed Program

A multi-dimensional integrative scoring framework for predicting functional variants in the human genome

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