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My research interests stem from a fascination with the molecular basis of evolutionary change and how we can harness genetic sequence patterns to make useful predictions about biological systems. I started my academic career as a geneticist, modelling how transposable elements may be selectively retained and spread through a clonal population of bacteria. After my PhD, I moved into full-time bioinformatics, with a focus on protein sequence analysis. As a postdoc in Dublin, I developed a bioinformatics (sequence analysis) method for the rational design of biologically active short peptides. The biological activity of these short peptides got me interested in short protein-protein interaction motifs, which have been the subsequent focus of my research. During my second postdoc, I coined the term "Short Linear Motif" (SLiM) for a specific type of protein interaction motif and was instrumental in developing SLiMDisc and SLiMFinder, two of the first algorithms for successfully predicting SLiMs from protein sequences. These and other algorithms are now available in the SLiMSuite bioinformatics package and online webservers.
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crossref(2023)
bioRxiv (Cold Spring Harbor Laboratory) (2023)
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