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Structural Characterization of Protein-Protein Complexes by Integrating Computational Docking with Small-angle Scattering Data
Authors:Carles Pons,Marco D&rsquo  Abramo,Dmitri I. Svergun,Pau Bernadó  ,Juan Ferná  ndez-Recio
Affiliation:
  • 1 Life Sciences Department, Barcelona Supercomputing Center (BSC), C/ Jordi Girona 29, Barcelona 08034, Spain
  • 2 Computational Bioinformatics, National Institute of Bioinformatics (INB), C/ Jordi Girona 29, Barcelona 08034, Spain
  • 3 Joint IRB-BSC Program on Computational Biology, Institute for Research in Biomedicine, Parc Científic de Barcelona, C/ Baldiri Reixach 10, Barcelona 08028, Spain
  • 4 Department of Biochemistry and Molecular Biology, University of Barcelona, Avda. Diagonal 645, Barcelona 08028, Spain
  • 5 European Molecular Biology Laboratory, Hamburg Outstation, Notkestrasse 85, D-22603 Hamburg, Germany
  • 6 Institute for Research in Biomedicine, Parc Científic de Barcelona, C/ Baldiri Reixach 10, Barcelona 08028, Spain
  • Abstract:X-ray crystallography and NMR can provide detailed structural information of protein-protein complexes, but technical problems make their application challenging in the high-throughput regime. Other methods such as small-angle X-ray scattering (SAXS) are more promising for large-scale application, but at the cost of lower resolution, which is a problem that can be solved by complementing SAXS data with theoretical simulations. Here, we propose a novel strategy that combines SAXS data and accurate protein-protein docking simulations. The approach has been benchmarked on a large pool of known structures with synthetic SAXS data, and on three experimental examples. The combined approach (pyDockSAXS) provided a significantly better success rate (43% for the top 10 predictions) than either of the two methods alone. Further analysis of the influence of different docking parameters made it possible to increase the success rates for specific cases, and to define guidelines for improving the data-driven protein-protein docking protocols.
    Keywords:SAS, small-angle scattering   SAXS, small-angle X-ray scattering   SANS, small-angle neutron scattering   RDC, residual dipolar coupling   NMA, normal mode analysis   EM, electron microscopy
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