| HOME | HELP | FEEDBACK | SUBSCRIPTIONS | ARCHIVE | SEARCH | TABLE OF CONTENTS |
Biophys J, September 2001, p. 1275-1284, Vol. 81, No. 3
Structural Biology and Modeling, Bristol-Myers Squibb Pharmaceutical Research Institute, Princeton, New Jersey 08543 USA
Simulation studies have been performed to evaluate the
utility of site-directed spin labeling for determining the structures of protein-ligand complexes, given a known protein structure. Two
protein-ligand complexes were used as model systems for these studies:
a 1.9-Å-resolution x-ray structure of a dihydrofolate reductase mutant
complexed with methotrexate, and a 1.5-Å-resolution x-ray structure of
the V-Src tyrosine kinase SH2 domain complexed with a five-residue
phosphopeptide. Nitroxide spin labels were modeled at five
dihydrofolate reductase residue positions and at four SH2 domain
residue positions. For both systems, after energy minimization,
conformational ensembles of the spin-labeled residues were generated by
simulated annealing while holding the remainder of the protein-ligand
complex fixed. Effective distances, simulating those that could be
obtained from 1H-NMR relaxation measurements, were
calculated between ligand protons and the spin labels. These were
converted to restraints with several different levels of precision.
Restrained simulated annealing calculations were then performed with
the aim of reproducing target ligand-binding modes. The effects of
incorporating a few supplementary short-range (
5.0 Å) distance
restraints were also examined. For the dihydrofolate
reductase-methotrexate complex, the ligand-binding mode was reproduced
reasonably well using relatively tight spin-label restraints, but
methotrexate was poorly localized using loose spin-label restraints.
Short-range and spin-label restraints proved to be complementary. For
the SH2 domain-phosphopeptide complex without the short-range
restraints, the peptide did not localize to the correct depth in the
binding groove; nevertheless, the orientation and internal conformation
of the peptide was reproduced moderately well. Use of the spin-label
restraints in conjunction with the short-range restraints resulted in
relatively well defined structural ensembles. These results indicate
that restraints derived from site-directed spin labeling can contribute
significantly to defining the orientations and conformations of bound
ligands. Accurate ligand localization appears to require either a few
supplementary short-range distance restraints, or relatively tight
spin-label restraints, with at least one spin label positioned so that
some of the restraints draw the ligand into the binding pocket in the latter case.
Biophys J, September 2001, p. 1275-1284, Vol. 81, No. 3
© 2001 by the Biophysical Society 0006-3495/01/09/1275/10 $2.00
This article has been cited by other articles:
 |
|
 |
|
  S. C. DeSensi, D. P. Rangel, A. H. Beth, T. P. Lybrand, and E. J. Hustedt Simulation of Nitroxide Electron Paramagnetic Resonance Spectra from Brownian Trajectories and Molecular Dynamics Simulations Biophys. J., May 15, 2008; 94(10): 3798 - 3809. [Abstract] [Full Text] [PDF]
|
|
| HOME | HELP | FEEDBACK | SUBSCRIPTIONS | ARCHIVE | SEARCH | TABLE OF CONTENTS |
