@article {121, title = {A fast and scalable framework for large-scale and ultrahigh-dimensional sparse regression with application to the UK Biobank.}, journal = {PLoS Genet}, volume = {16}, year = {2020}, month = {2020 10}, pages = {e1009141}, abstract = {

The UK Biobank is a very large, prospective population-based cohort study across the United Kingdom. It provides unprecedented opportunities for researchers to investigate the relationship between genotypic information and phenotypes of interest. Multiple regression methods, compared with genome-wide association studies (GWAS), have already been showed to greatly improve the prediction performance for a variety of phenotypes. In the high-dimensional settings, the lasso, since its first proposal in statistics, has been proved to be an effective method for simultaneous variable selection and estimation. However, the large-scale and ultrahigh dimension seen in the UK Biobank pose new challenges for applying the lasso method, as many existing algorithms and their implementations are not scalable to large applications. In this paper, we propose a computational framework called batch screening iterative lasso (BASIL) that can take advantage of any existing lasso solver and easily build a scalable solution for very large data, including those that are larger than the memory size. We introduce snpnet, an R package that implements the proposed algorithm on top of glmnet and optimizes for single nucleotide polymorphism (SNP) datasets. It currently supports l1-penalized linear model, logistic regression, Cox model, and also extends to the elastic net with l1/l2 penalty. We demonstrate results on the UK Biobank dataset, where we achieve competitive predictive performance for all four phenotypes considered (height, body mass index, asthma, high cholesterol) using only a small fraction of the variants compared with other established polygenic risk score methods.

}, keywords = {Algorithms, Asthma, Biological Specimen Banks, Body Height, Body Mass Index, Cholesterol, Cohort Studies, Genetics, Population, Genome-Wide Association Study, Genotype, Humans, Logistic Models, Phenotype, Polymorphism, Single Nucleotide, Proportional Hazards Models, United Kingdom}, issn = {1553-7404}, doi = {10.1371/journal.pgen.1009141}, author = {Qian, Junyang and Tanigawa, Yosuke and Du, Wenfei and Aguirre, Matthew and Chang, Chris and Tibshirani, Robert and Rivas, Manuel A and Hastie, Trevor} }