Saturday, 13 July 2013

SLiMSuite at the OMICS Group 3rd International Conference on Proteomics & Bioinformatics

If anyone is attending the OMICS Group 3rd International Conference on Proteomics & Bioinformatics this week then be sure to say hello. I am speaking on the last day in the “Computational Biology” track.. (Never the best time to talk at a conference as there is limited time for follow up but at least it is before lunch!)

SLiM Pickings: mining structural and sequence data for the prediction of short linear protein interaction motifs

Short Linear Motifs (SLiMs) are short functional protein sequences that act as ligands to mediate transient protein-protein interactions (PPI) in critical biological pathways and signaling networks. SLiMs are short (3-15aa), generally tolerate considerable sequence variation and typically have fewer than five residues critical for function. These features result in a degree of evolutionary plasticity not seen in domains and SLiMs often add new functions to proteins by convergent evolution. They also present a challenge for computational identification, making it difficult to differentiate biological signal from stochastic patterns. Despite this, discovering new SLiMs is of great interest due to their potential as therapeutic targets.

In recent years, we have made great progress in SLiM discovery, particularly through development of the SLiMSuite package of bioinformatics tools. SLiMs generally occur in structurally disordered regions of proteins and exhibit evolutionary conservation relative to other disordered residues. SLiMFinder uses this knowledge and exploits patterns of convergent evolution to predict novel, over-represented motifs within a statistical framework with high specificity. Applying this approach to a comprehensive set of human PPI data has highlighted interactome complexity and quality as the next challenges for SLiM prediction. Our latest development, QSLiMFinder (“Query” SLiMFinder) tackles some of these issues by incorporating specific interaction data to restrict the motif search space, which improves both the sensitivity and biological relevance of predictions. We are now using QSLiMFinder to combine structurally defined domain-motif interactions with large-scale PPI data to perform large-scale de novo SLiM prediction.

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