Improved linking of motifs to their TFs using domain information

Nina Baumgarten; Florian Schmidt; Marcel H Schulz

doi:10.1093/bioinformatics/btz855

Improved linking of motifs to their TFs using domain information

Bioinformatics. 2020 Mar 1;36(6):1655-1662. doi: 10.1093/bioinformatics/btz855.

Authors

Nina Baumgarten^{1

2}, Florian Schmidt^{3

4}, Marcel H Schulz^{1

2

3

4}

Affiliations

¹ Institute for Cardiovascular Regeneration, Goethe University, Frankfurt am Main 60590, Germany.
² German Center for Cardiovascular Regeneration, Partner Site Rhein-Main, Frankfurt am Main 60590, Germany.
³ High-throughput Genomics & Systems Biology, Cluster of Excellence MMCI, Saarland University.
⁴ Research Group Computational Biology, Max Planck Institute for Informatics, Saarland Informatics Campus, Saarbrücken 66123, Germany.

Abstract

Motivation: A central aim of molecular biology is to identify mechanisms of transcriptional regulation. Transcription factors (TFs), which are DNA-binding proteins, are highly involved in these processes, thus a crucial information is to know where TFs interact with DNA and to be aware of the TFs' DNA-binding motifs. For that reason, computational tools exist that link DNA-binding motifs to TFs either without sequence information or based on TF-associated sequences, e.g. identified via a chromatin immunoprecipitation followed by sequencing (ChIP-seq) experiment.In this paper, we present MASSIF, a novel method to improve the performance of existing tools that link motifs to TFs relying on TF-associated sequences. MASSIF is based on the idea that a DNA-binding motif, which is correctly linked to a TF, should be assigned to a DNA-binding domain (DBD) similar to that of the mapped TF. Because DNA-binding motifs are in general not linked to DBDs, it is not possible to compare the DBD of a TF and the motif directly. Instead we created a DBD collection, which consist of TFs with a known DBD and an associated motif. This collection enables us to evaluate how likely it is that a linked motif and a TF of interest are associated to the same DBD. We named this similarity measure domain score, and represent it as a P-value. We developed two different ways to improve the performance of existing tools that link motifs to TFs based on TF-associated sequences: (i) using meta-analysis to combine P-values from one or several of these tools with the P-value of the domain score and (ii) filter unlikely motifs based on the domain score.

Results: We demonstrate the functionality of MASSIF on several human ChIP-seq datasets, using either motifs from the HOCOMOCO database or de novo identified ones as input motifs. In addition, we show that both variants of our method improve the performance of tools that link motifs to TFs based on TF-associated sequences significantly independent of the considered DBD type.

Availability and implementation: MASSIF is freely available online at https://github.com/SchulzLab/MASSIF.

Supplementary information: Supplementary data are available at Bioinformatics online.

Publication types

Meta-Analysis
Research Support, Non-U.S. Gov't

MeSH terms

Binding Sites
Chromatin Immunoprecipitation
Computational Biology
DNA-Binding Proteins*
Nucleotide Motifs
Protein Binding
Sequence Analysis, DNA
Transcription Factors*

Substances

DNA-Binding Proteins
Transcription Factors