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Multi†subgroup gene screening using semi†parametric hierarchical mixture models and the optimal discovery procedure: Application to a randomized clinical trial in multiple myeloma

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  • Shigeyuki Matsui
  • Hisashi Noma
  • Pingping Qu
  • Yoshio Sakai
  • Kota Matsui
  • Christoph Heuck
  • John Crowley

Abstract

This article proposes an efficient approach to screening genes associated with a phenotypic variable of interest in genomic studies with subgroups. In order to capture and detect various association profiles across subgroups, we flexibly estimate the underlying effect size distribution across subgroups using a semi†parametric hierarchical mixture model for subgroup†specific summary statistics from independent subgroups. We then perform gene ranking and selection using an optimal discovery procedure based on the fitted model with control of false discovery rate. Efficiency of the proposed approach, compared with that based on standard regression models with covariates representing subgroups, is demonstrated through application to a randomized clinical trial with microarray gene expression data in multiple myeloma, and through a simulation experiment.

Suggested Citation

  • Shigeyuki Matsui & Hisashi Noma & Pingping Qu & Yoshio Sakai & Kota Matsui & Christoph Heuck & John Crowley, 2018. "Multi†subgroup gene screening using semi†parametric hierarchical mixture models and the optimal discovery procedure: Application to a randomized clinical trial in multiple myeloma," Biometrics, The International Biometric Society, vol. 74(1), pages 313-320, March.
  • Handle: RePEc:bla:biomet:v:74:y:2018:i:1:p:313-320
    DOI: 10.1111/biom.12716
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    References listed on IDEAS

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    2. John D. Storey, 2007. "The optimal discovery procedure: a new approach to simultaneous significance testing," Journal of the Royal Statistical Society Series B, Royal Statistical Society, vol. 69(3), pages 347-368, June.
    3. Lu Tian & Ash A. Alizadeh & Andrew J. Gentles & Robert Tibshirani, 2014. "A Simple Method for Estimating Interactions Between a Treatment and a Large Number of Covariates," Journal of the American Statistical Association, Taylor & Francis Journals, vol. 109(508), pages 1517-1532, December.
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    Cited by:

    1. Shonosuke Sugasawa & Hisashi Noma, 2021. "Efficient screening of predictive biomarkers for individual treatment selection," Biometrics, The International Biometric Society, vol. 77(1), pages 249-257, March.

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