Genome-wide association data classification and SNPs selection using two-stage quality-based Random Forests

Single-nucleotide polymorphisms (SNPs) selection and identification are the most important tasks in Genome-wide association data analysis. The problem is difficult because genome-wide association data is very high dimensional and a large portion of SNPs in the data is irrelevant to the disease. Adva...

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Bibliographic Details
Published in:BMC genomics 2015-01, Vol.16 Suppl 2 (S2), p.S5-S5, Article S5
Main Authors: Nguyen, Thanh-Tung, Huang, Joshua, Wu, Qingyao, Nguyen, Thuy, Li, Mark
Format: Article
Language:English
Subjects:
Algorithms
Alzheimer Disease - genetics
Computational Biology - methods
Genetic Predisposition to Disease - genetics
Genome-Wide Association Study - classification
Genome-Wide Association Study - methods
Genome-Wide Association Study - statistics & numerical data
Humans
Machine Learning
Models, Genetic
Parkinson Disease - genetics
Polymorphism, Single Nucleotide
Proceedings
Reproducibility of Results
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Summary:Single-nucleotide polymorphisms (SNPs) selection and identification are the most important tasks in Genome-wide association data analysis. The problem is difficult because genome-wide association data is very high dimensional and a large portion of SNPs in the data is irrelevant to the disease. Advanced machine learning methods have been successfully used in Genome-wide association studies (GWAS) for identification of genetic variants that have relatively big effects in some common, complex diseases. Among them, the most successful one is Random Forests (RF). Despite of performing well in terms of prediction accuracy in some data sets with moderate size, RF still suffers from working in GWAS for selecting informative SNPs and building accurate prediction models. In this paper, we propose to use a new two-stage quality-based sampling method in random forests, named ts-RF, for SNP subspace selection for GWAS. The method first applies p-value assessment to find a cut-off point that separates informative and irrelevant SNPs in two groups. The informative SNPs group is further divided into two sub-groups: highly informative and weak informative SNPs. When sampling the SNP subspace for building trees for the forest, only those SNPs from the two sub-groups are taken into account. The feature subspaces always contain highly informative SNPs when used to split a node at a tree. This approach enables one to generate more accurate trees with a lower prediction error, meanwhile possibly avoiding overfitting. It allows one to detect interactions of multiple SNPs with the diseases, and to reduce the dimensionality and the amount of Genome-wide association data needed for learning the RF model. Extensive experiments on two genome-wide SNP data sets (Parkinson case-control data comprised of 408,803 SNPs and Alzheimer case-control data comprised of 380,157 SNPs) and 10 gene data sets have demonstrated that the proposed model significantly reduced prediction errors and outperformed most existing the-state-of-the-art random forests. The top 25 SNPs in Parkinson data set were identified by the proposed model including four interesting genes associated with neurological disorders. The presented approach has shown to be effective in selecting informative sub-groups of SNPs potentially associated with diseases that traditional statistical approaches might fail. The new RF works well for the data where the number of case-control objects is much smaller than the number of SNPs, wh
ISSN:1471-2164
1471-2164
DOI:10.1186/1471-2164-16-S2-S5