4.5 Article

Integrative and regularized principal component analysis of multiple sources of data

Journal

STATISTICS IN MEDICINE
Volume 35, Issue 13, Pages 2235-2250

Publisher

WILEY
DOI: 10.1002/sim.6866

Keywords

integrative clustering; PCA; tumor subtypes

Funding

  1. NIH [R01-GM081535, R01-GM113250, R01-HL105397]
  2. NSF [DMS-0906616, DMS-1207771]
  3. NSFC [11571068]
  4. Division Of Mathematical Sciences
  5. Direct For Mathematical & Physical Scien [1415500] Funding Source: National Science Foundation

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Integration of data of disparate types has become increasingly important to enhancing the power for new discoveries by combining complementary strengths of multiple types of data. One application is to uncover tumor subtypes in human cancer research in which multiple types of genomic data are integrated, including gene expression, DNA copy number, and DNA methylation data. In spite of their successes, existing approaches based on joint latent variable models require stringent distributional assumptions and may suffer from unbalanced scales (or units) of different types of data and non-scalability of the corresponding algorithms. In this paper, we propose an alternative based on integrative and regularized principal component analysis, which is distribution-free, computationally efficient, and robust against unbalanced scales. The new method performs dimension reduction simultaneously on multiple types of data, seeking data-adaptive sparsity and scaling. As a result, in addition to feature selection for each type of data, integrative clustering is achieved. Numerically, the proposed method compares favorably against its competitors in terms of accuracy (in identifying hidden clusters), computational efficiency, and robustness against unbalanced scales. In particular, compared with a popular method, the new method was competitive in identifying tumor subtypes associated with distinct patient survival patterns when applied to a combined analysis of DNA copy number, mRNA expression, and DNA methylation data in a glioblastoma multiforme study. Copyright (c) 2016 John Wiley & Sons, Ltd.

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