Abstract
Molecular docking is the most commonly used technique in the modern drug discovery process where computational approaches involving docking algorithms are used to dock small molecules into macromolecular target structures. Over the recent years several evaluation studies have been reported by independent scientists comparing the performance of the docking programs by using default 'black box' protocols supplied by the software companies. Such studies have to be considered carefully as the docking programs can be tweaked towards optimum performance by selecting the parameters suitable for the target of interest. In this study we address the problem of selecting an appropriate docking and scoring function combination (88 docking algorithm-scoring functions) for substrate specificity predictions for feruloyl esterases, an industrially relevant enzyme family. We also propose the 'Key Interaction Score System' (KISS), a more biochemically meaningful measure for evaluation of docking programs based on pose prediction accuracy.
Original language | English |
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Journal | Scientific Reports |
Volume | 2 |
ISSN | 2045-2322 |
DOIs | |
Publication status | Published - 2012 |
Keywords
- MULTIDISCIPLINARY
- PROTEIN-STRUCTURE PREDICTION
- VIRTUAL SCREENING ACCURACY
- SCORING FUNCTIONS
- I-TASSER
- POSE PREDICTION
- DRUG DISCOVERY
- TOOLS
- ALGORITHMS
- ENRICHMENT
- RECEPTORS