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beyond missing heritability prediction of complex traits除了遗传缺失预测复杂的特征
Beyond Missing Heritability: Prediction of Complex Traits
¤
Robert Makowsky*, Nicholas M. Pajewski , Yann C. Klimentidis, Ana I. Vazquez, Christine W. Duarte,
David B. Allison, Gustavo de los Campos
Department of Biostatistics, University of Alabama at Birmingham, Birmingham, Alabama, United States of America
Abstract
Despite rapid advances in genomic technology, our ability to account for phenotypic variation using genetic information
remains limited for many traits. This has unfortunately resulted in limited application of genetic data towards preventive
and personalized medicine, one of the primary impetuses of genome-wide association studies. Recently, a large proportion
of the ‘‘missing heritability’’ for human height was statistically explained by modeling thousands of single nucleotide
polymorphisms concurrently. However, it is currently unclear how gains in explained genetic variance will translate to the
prediction of yet-to-be observed phenotypes. Using data from the Framingham Heart Study, we explore the genomic
prediction of human height in training and validation samples while varying the statistical approach used, the number of
SNPs included in the model, the validation scheme, and the number of subjects used to train the model. In our training
datasets, we are able to explain a large proportion of the variation in height (h2 up to 0.83, R2 up to 0.96). However, the
proportion of variance accounted for in validation samples is much smaller (ranging from 0.15 to 0.36 depending on the
degree of familial information used in the training dataset). While such R2 values vastly exceed what has been previously
reported using a reduced number of pre-selected markers (,0.10), given the heritability of the trait (,0.80), substantial
room for improvement rem
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