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Genome-Wide Pathway Association Studies of Multiple Correlated Quantitative Phenotypes Using Principle Component Analyses

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  • Feng Zhang
  • Xiong Guo
  • Shixun Wu
  • Jing Han
  • Yongjun Liu
  • Hui Shen
  • Hong-Wen Deng

Abstract

Genome-wide pathway association studies provide novel insight into the biological mechanism underlying complex diseases. Current pathway association studies primarily focus on single important disease phenotype, which is sometimes insufficient to characterize the clinical manifestations of complex diseases. We present a multi-phenotypes pathway association study(MPPAS) approach using principle component analysis(PCA). In our approach, PCA is first applied to multiple correlated quantitative phenotypes for extracting a set of orthogonal phenotypic components. The extracted phenotypic components are then used for pathway association analysis instead of original quantitative phenotypes. Four statistics were proposed for PCA-based MPPAS in this study. Simulations using the real data from the HapMap project were conducted to evaluate the power and type I error rates of PCA-based MPPAS under various scenarios considering sample sizes, additive and interactive genetic effects. A real genome-wide association study data set of bone mineral density (BMD) at hip and spine were also analyzed by PCA-based MPPAS. Simulation studies illustrated the performance of PCA-based MPPAS for identifying the causal pathways underlying complex diseases. Genome-wide MPPAS of BMD detected associations between BMD and KENNY_CTNNB1_TARGETS_UP as well as LONGEVITYPATHWAY pathways in this study. We aim to provide a applicable MPPAS approach, which may help to gain deep understanding the potential biological mechanism of association results for complex diseases.

Suggested Citation

  • Feng Zhang & Xiong Guo & Shixun Wu & Jing Han & Yongjun Liu & Hui Shen & Hong-Wen Deng, 2012. "Genome-Wide Pathway Association Studies of Multiple Correlated Quantitative Phenotypes Using Principle Component Analyses," PLOS ONE, Public Library of Science, vol. 7(12), pages 1-7, December.
  • Handle: RePEc:plo:pone00:0053320
    DOI: 10.1371/journal.pone.0053320
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    References listed on IDEAS

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    1. Timothy G Lesnick & Spiridon Papapetropoulos & Deborah C Mash & Jarlath Ffrench-Mullen & Lina Shehadeh & Mariza de Andrade & John R Henley & Walter A Rocca & J Eric Ahlskog & Demetrius M Maraganore, 2007. "A Genomic Pathway Approach to a Complex Disease: Axon Guidance and Parkinson Disease," PLOS Genetics, Public Library of Science, vol. 3(6), pages 1-12, June.
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    Cited by:

    1. Yamin Deng & Shiman Wu & Huifang Fan, 2020. "Genome-wide pathway-based quantitative multiple phenotypes analysis," PLOS ONE, Public Library of Science, vol. 15(11), pages 1-13, November.

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