Transcriptome network component analysis with limited microarray data

doi:10.1093/bioinformatics/btl279

Bioinformatics Advance Access originally published online on June 9, 2006
Bioinformatics 2006 22(15):1886-1894; doi:10.1093/bioinformatics/btl279

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Transcriptome network component analysis with limited microarray data

Simon J. Galbraith ¹^,2^,, Linh M. Tran ²^, and James C. Liao ²^,*

¹ Department of Computer Science, University of California Los Angeles, CA, USA
² Department of Chemical Engineering, University of California Los Angeles, CA, USA

^*To whom correspondence should be addressed.

Summary: Network component analysis (NCA) is a method to deducetranscription factor (TF) activities and TF-gene regulationcontrol strengths from gene expression data and a TF-gene bindingconnectivity network. Previously, this method could analyzea maximum number of regulators equal to the total sample sizebecause of the identifiability limit in data decomposition.As such, the total number of source signal components was limitedto the total number of experiments rather than the total numberof biological regulators. However, networks that have less transcriptomedata points than the number of regulators are of interest. Thusit is imperative to develop a theoretical basis that allowsrealistic source signal extraction based on relatively few datapoints. On the other hand, such methods would inherently increasenumerical challenges leading to multiple solutions. Therefore,solutions to both the problems are needed.

Results: We have improved NCA for transcription factor activity(TFA) estimation, based on the observation that most genes areregulated by only a few TFs. This observation leads to the derivationof a new identifiability criterion which is tested during numericaliteration that allows us to decompose data when the number ofTFs is greater than the number of experiments. To show thatour method works with real microarray data and has biologicalutility, we analyze Saccharomyces cerevisiae cell cycle microarraydata (73 experiments) using a TF-gene connectivity network (96TFs) derived from ChIP-chip binding data. We compare the resultsof NCA analysis with the results obtained from ChIP-chip regressionmethods, and we show that NCA and regression produce TFAs thatare qualitatively similar, but the NCA TFAs outperform regressionin statistical tests. We also show that NCA can extract subtleTFA signals that correlate with known cell cycle TF functionand cell cycle phase. Overall we determined that 31 TFs havestatistically periodic TFAs in one or more experiments, 75%of which are known cell cycle regulators. In addition, we findthat the 12 TFAs that are periodic in two or more experimentscorrespond to well-known cell cycle regulators. We also investigatedTFA sensitivity to the choice of connectivity network we constructedtwo networks using different ChIP-chip p-value cut-offs.

Availability: The NCA Toolbox for MATLAB is available at http://www.seas.ucla.edu/~liaoj/download.htm

Contact: liaoj{at}seas.ucla.edu

Received on May 27, 2006; accepted on June 2, 2006

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