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. 2012;7(6):e38365.
doi: 10.1371/journal.pone.0038365. Epub 2012 Jun 19.

Detection of simultaneous group effects in microRNA expression and related target gene sets

Affiliations

Detection of simultaneous group effects in microRNA expression and related target gene sets

Stephan Artmann et al. PLoS One. 2012.

Abstract

Expression levels of mRNAs are among other factors regulated by microRNAs. A particular microRNA can bind specifically to several target mRNAs and lead to their degradation. Expression levels of both, mRNAs and microRNAs, can be obtained by microarray experiments. In order to increase the power of detecting microRNAs that are differentially expressed between two different groups of samples, we incorporate expression levels of their related target gene sets. Group effects are determined individually for each microRNA, and by enrichment tests and global tests for target gene sets. The resulting lists of p-values from individual and set-wise testing are combined by means of meta analysis. We propose a new approach to connect microRNA-wise and gene set-wise information by means of p-value combination as often used in meta-analysis. In this context, we evaluate the usefulness of different approaches of gene set tests. In a simulation study we reveal that our combination approach is more powerful than microRNA-wise testing alone. Furthermore, we show that combining microRNA-wise results with 'competitive' gene set tests maintains a pre-specified false discovery rate. In contrast, a combination with 'self-contained' gene set tests can harm the false discovery rate, particularly when gene sets are not disjunct.

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Conflict of interest statement

Competing Interests: The authors have declared that no competing interests exist.

Figures

Figure 1
Figure 1. Flow chart of combining expression levels of miRNAs and their related target mRNAs.
The links between microRNAs and their target mRNAs are taken from public databases. MicroRNAs and target sets are first analysed separately and obtained p-values are combined as final result.
Figure 2
Figure 2. Effect of overlapping target gene sets on the simulated .
Effects are presented for component-wise testing (dotted line), target set-wise testing (dashed line) and the combination approach (solid line). While the competitive approaches such as the ‘Wilcoxon’-based gene set test (top) still maintained the pre-specified formula image-level of 5formula image when target gene sets overlapped, the formula image increased dramatically when employing the self-contained approaches such as the ‘globaltest’ procedure (bottom).
Figure 3
Figure 3. Simulated average power rates with respect to the log fold change .
Left: component-wise testing (dotted line), target testing with ‘ROAST’ (dashed line) and the combination approach (solid line), each in the case of an autoregressive covariance structure and non-overlapping target sets. Right: combination approach based on ‘globaltest’ (dotted line), ‘Wilcoxon’ (dashed line) and ‘Romer’ (solid line), each in the case of an unstructured covariance matrix and overlapping target sets.

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