BMC Bioinformatics (Jan 2009)

ModuleDigger: an itemset mining framework for the detection of <it>cis</it>-regulatory modules

  • Verstuyf Annemieke,
  • Lemmens Karen,
  • Dhollander Thomas,
  • Fu Qiang,
  • Storms Valerie,
  • De Bie Tijl,
  • Sun Hong,
  • De Moor Bart,
  • Marchal Kathleen

DOI
https://doi.org/10.1186/1471-2105-10-S1-S30
Journal volume & issue
Vol. 10, no. Suppl 1
p. S30

Abstract

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Abstract Background The detection of cis-regulatory modules (CRMs) that mediate transcriptional responses in eukaryotes remains a key challenge in the postgenomic era. A CRM is characterized by a set of co-occurring transcription factor binding sites (TFBS). In silico methods have been developed to search for CRMs by determining the combination of TFBS that are statistically overrepresented in a certain geneset. Most of these methods solve this combinatorial problem by relying on computational intensive optimization methods. As a result their usage is limited to finding CRMs in small datasets (containing a few genes only) and using binding sites for a restricted number of transcription factors (TFs) out of which the optimal module will be selected. Results We present an itemset mining based strategy for computationally detecting cis-regulatory modules (CRMs) in a set of genes. We tested our method by applying it on a large benchmark data set, derived from a ChIP-Chip analysis and compared its performance with other well known cis-regulatory module detection tools. Conclusion We show that by exploiting the computational efficiency of an itemset mining approach and combining it with a well-designed statistical scoring scheme, we were able to prioritize the biologically valid CRMs in a large set of coregulated genes using binding sites for a large number of potential TFs as input.