Literature DB >> 27859628

Longitudinal SNP-set association analysis of quantitative phenotypes.

Zhong Wang1,2,3, Ke Xu4,5, Xinyu Zhang4,5, Xiaowei Wu6, Zuoheng Wang1.   

Abstract

Many genetic epidemiological studies collect repeated measurements over time. This design not only provides a more accurate assessment of disease condition, but allows us to explore the genetic influence on disease development and progression. Thus, it is of great interest to study the longitudinal contribution of genes to disease susceptibility. Most association testing methods for longitudinal phenotypes are developed for single variant, and may have limited power to detect association, especially for variants with low minor allele frequency. We propose Longitudinal SNP-set/sequence kernel association test (LSKAT), a robust, mixed-effects method for association testing of rare and common variants with longitudinal quantitative phenotypes. LSKAT uses several random effects to account for the within-subject correlation in longitudinal data, and allows for adjustment for both static and time-varying covariates. We also present a longitudinal trait burden test (LBT), where we test association between the trait and the burden score in linear mixed models. In simulation studies, we demonstrate that LBT achieves high power when variants are almost all deleterious or all protective, while LSKAT performs well in a wide range of genetic models. By making full use of trait values from repeated measures, LSKAT is more powerful than several tests applied to a single measurement or average over all time points. Moreover, LSKAT is robust to misspecification of the covariance structure. We apply the LSKAT and LBT methods to detect association with longitudinally measured body mass index in the Framingham Heart Study, where we are able to replicate association with a circadian gene NR1D2.
© 2016 WILEY PERIODICALS, INC.

Entities:  

Keywords:  association testing; linear mixed model; longitudinal study; quantitative trait; variant set

Mesh:

Substances:

Year:  2016        PMID: 27859628      PMCID: PMC5154867          DOI: 10.1002/gepi.22016

Source DB:  PubMed          Journal:  Genet Epidemiol        ISSN: 0741-0395            Impact factor:   2.135


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