Using Restraints in EROS-Dock Improves Model Quality in Pairwise and Multicomponent Protein Docking - INRIA - Institut National de Recherche en Informatique et en Automatique Accéder directement au contenu
Article Dans Une Revue Proteins - Structure, Function and Bioinformatics Année : 2020

Using Restraints in EROS-Dock Improves Model Quality in Pairwise and Multicomponent Protein Docking

Résumé

Protein docking algorithms aim to predict the 3D structure of a protein complex from the structures of its separated components. In the past, most docking algorithms focused on docking pairs of proteins to form dimeric complexes. However, attention is now turning towards the more difficult problem of using docking methods to predict the structures of multi-component complexes. In both cases, however, the constituent proteins often change conformation upon complex formation, and this can cause many algorithms to fail to detect near-native binding orientations due to the high number of atomic steric clashes in the list of candidate solutions. An increasingly popular way to retain more near-native orientations is to define one or more restraints that serve to modulate or override the effect of steric clashes. Here, we present an updated version of our “EROS-DOCK” docking algorithm which has been extended to dock arbitrary dimeric and trimeric complexes, and to allow the user to define residue-residue or atom-atom interaction restraints. Our results show that using even just one residue-residue restraint in each interaction interface is sufficient to increase the number of cases with acceptable solutions within the top 10 from 51 to 121 out of 173 pairwise docking cases, and to successfully dock 8 out of 11 trimeric complexes.
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Dates et versions

hal-02930827 , version 1 (04-09-2020)

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Maria Elisa Ruiz Echartea, David Ritchie, Isaure Chauvot de Beauchêne. Using Restraints in EROS-Dock Improves Model Quality in Pairwise and Multicomponent Protein Docking. Proteins - Structure, Function and Bioinformatics, 2020, 88 (8), pp.1121-1128. ⟨10.1002/prot.25959⟩. ⟨hal-02930827⟩
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