Abstract

Fourier correlation techniques are very efficient for docking bound (i.e., co-crystallized) protein conformations using measures of surface complementarity as the target function. However, when docking unbound (i.e., independently crystallized) conformations, the method yields an enormous number of false positives (i.e., conformations with good score but large RMSD). The major goal of this proposal is to add post-processing steps to the Fourier docking algorithm in order to remove all false positives. Post-processing will include a rigid-body filter to reduce the number of candidate structures, a flexible filter that eliminates all far-from-native conformations (with RMSDs over 10 A), and a flexible docking algorithm to refine the remaining few. The filtering and refinement steps utilize the changing contributions that electrostatics, desolvation, and molecular mechanics exhibit at the different stages of both protein-protein association and docking. The rigid body analysis is based on the mapping of electrostatic and desolvation interactions between proteins in encounter complexes; i.e., before extensive surface contacts are established. These interactions are much less sensitive to structural perturbations than the measures of surface complementarity, and provide a useful scoring function. However, due to the differences in side chain conformations between bound and unbound states, within the framework of the rigid body analysis, the discrimination is not perfect, and cannot eliminate all false positives. Inclusion of molecular mechanics and accounting for flexibility yield dramatic improvement. In particular, after extensive molecular mechanics minimization of the structures, the sum of van der Waals, electrostatic, and solvation/entropic energy terms, not only discriminates the near-native conformations from decoys in all systems studied, but also provides a relatively good ranking of near-native structures. These preliminary results support the central hypothesis that all false positives can be removed while retaining and improving the good docked conformations. The efficiency of the entire docking algorithm is further increased by pre-processing steps that either attempt to improve the conformations of surface side chains, or introduce a nonuniform Gaussian blurring in order to avoid spurious overlaps. An automatic procedure combining Fourier docking programs with the post- and pre-processing steps will provide a powerful research tool in applications that currently cannot be addressed by computational methods.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM061867-03
Application #
6525948
Study Section
Molecular and Cellular Biophysics Study Section (BBCA)
Program Officer
Wehrle, Janna P
Project Start
2000-09-01
Project End
2003-08-31
Budget Start
2002-09-01
Budget End
2003-08-31
Support Year
3
Fiscal Year
2002
Total Cost
$212,949
Indirect Cost

  Institution

Name
Boston University
Department
Engineering (All Types)
Type
Schools of Engineering
DUNS #
042250712
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Zarbafian, Shahrooz; Moghadasi, Mohammad; Roshandelpoor, Athar et al. (2018) Protein docking refinement by convex underestimation in the low-dimensional subspace of encounter complexes. Sci Rep 8:5896
Yueh, Christine; Hall, David R; Xia, Bing et al. (2017) ClusPro-DC: Dimer Classification by the Cluspro Server for Protein-Protein Docking. J Mol Biol 429:372-381
Kozakov, Dima; Hall, David R; Xia, Bing et al. (2017) The ClusPro web server for protein-protein docking. Nat Protoc 12:255-278
Bohnuud, Tanggis; Luo, Lingqi; Wodak, Shoshana J et al. (2017) A benchmark testing ground for integrating homology modeling and protein docking. Proteins 85:10-16
Vajda, Sandor; Yueh, Christine; Beglov, Dmitri et al. (2017) New additions to the ClusPro server motivated by CAPRI. Proteins 85:435-444
Im, Wonpil; Liang, Jie; Olson, Arthur et al. (2016) Challenges in structural approaches to cell modeling. J Mol Biol 428:2943-64
Lensink, Marc F; Velankar, Sameer; Kryshtafovych, Andriy et al. (2016) Prediction of homoprotein and heteroprotein complexes by protein docking and template-based modeling: A CASP-CAPRI experiment. Proteins 84 Suppl 1:323-48
Mamonov, Artem B; Moghadasi, Mohammad; Mirzaei, Hanieh et al. (2016) Focused grid-based resampling for protein docking and mapping. J Comput Chem 37:961-70
Xia, Bing; Vajda, Sandor; Kozakov, Dima (2016) Accounting for pairwise distance restraints in FFT-based protein-protein docking. Bioinformatics 32:3342-3344
Padhorny, Dzmitry; Kazennov, Andrey; Zerbe, Brandon S et al. (2016) Protein-protein docking by fast generalized Fourier transforms on 5D rotational manifolds. Proc Natl Acad Sci U S A 113:E4286-93

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