| Literature DB >> 28899997 |
Jungsoo Gim1, Wonji Kim2, Soo Heon Kwak3, Hosik Choi4, Changyi Park5, Kyong Soo Park3, Sunghoon Kwon6, Taesung Park7, Sungho Won8.
Abstract
Despite the many successes of genome-wide association studies (GWAS), the known susceptibility variants identified by GWAS have modest effect sizes, leading to notable skepticism about the effectiveness of building a risk prediction model from large-scale genetic data. However, in contrast to genetic variants, the family history of diseases has been largely accepted as an important risk factor in clinical diagnosis and risk prediction. Nevertheless, the complicated structures of the family history of diseases have limited their application in clinical practice. Here, we developed a new method that enables incorporation of the general family history of diseases with a liability threshold model, and propose a new analysis strategy for risk prediction with penalized regression analysis that incorporates both large numbers of genetic variants and clinical risk factors. Application of our model to type 2 diabetes in the Korean population (1846 cases and 1846 controls) demonstrated that single-nucleotide polymorphisms accounted for 32.5% of the variation explained by the predicted risk scores in the test data set, and incorporation of family history led to an additional 6.3% improvement in prediction. Our results illustrate that family medical history provides valuable information on the variation of complex diseases and improves prediction performance.Entities:
Keywords: Genetic variability in complex binary traits; Liability threshold model; family history; penalized prediction model; risk prediction in complex disease
Mesh:
Year: 2017 PMID: 28899997 PMCID: PMC5676245 DOI: 10.1534/genetics.117.300283
Source DB: PubMed Journal: Genetics ISSN: 0016-6731 Impact factor: 4.562