Information-Driven, Ensemble Flexible Peptide Docking Using HADDOCK
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Publication date
2017
Editors
Schueler-Furman, Ora
London, Nir
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Supervisors
Document Type
Part of book
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Abstract
Modeling protein-peptide interactions remains a significant challenge for docking programs due to the inherent highly flexible nature of peptides, which often adopt different conformations whether in their free or bound forms. We present here a protocol consisting of a hybrid approach, combining the most frequently found peptide conformations in complexes with representative conformations taken from molecular dynamics simulations of the free peptide. This approach intends to broaden the range of conformations sampled during docking. The resulting ensemble of conformations is used as a starting point for information-driven flexible docking with HADDOCK. We demonstrate the performance of this protocol on six cases of increasing difficulty, taken from a protein-peptide benchmark set. In each case, we use knowledge of the binding site on the receptor to drive the docking process. In the majority of cases where MD conformations are added to the starting ensemble for docking, we observe an improvement in the quality of the resulting models.
Keywords
Protein-peptide docking, Flexibility, Information-driven docking, Ensemble docking, HADDOCK, Molecular dynamics simulations, Taverne
Citation
Geng, C, Narasimhan, S, Garcia Lopes Maia Rodrigues, J & Bonvin, A M J J 2017, Information-Driven, Ensemble Flexible Peptide Docking Using HADDOCK. in O Schueler-Furman & N London (eds), Modeling Peptide-Protein Interactions : Methods and Protocols. vol. 1561, Methods in Molecular Biology, vol. 1561, Springer, New York, pp. 109-138. https://doi.org/10.1007/978-1-4939-6798-8_8