Enhanced sampling and overfitting analyses in structural refinement of nucleic acids into electron microscopy maps.

Academic Article

Abstract

  • Flexible fitting computational algorithms are often useful to interpret low-resolution maps of many macromolecular complexes generated by electron microscopy (EM) imaging. One such atomistic simulation technique is molecular dynamics flexible fitting (MDFF), which has been widely applied to generate structural models of large ribonucleoprotein assemblies such as the ribosome. We have previously shown that MDFF simulations of globular proteins are sensitive to the resolution of the target EM map and the strength of restraints used to preserve the secondary structure elements during fitting (Vashisth, H.; et al. Structure 2012, 20, 1453-1462). In this work, we aim to systematically examine the quality of structural models of various nucleic acids obtained via MDFF by varying the map resolution and the strength of structural restraints. We also demonstrate how an enhanced conformational sampling technique for proteins, temperature-accelerated molecular dynamics (TAMD), can be combined with MDFF for the structural refinement of nucleic acids in EM maps. Finally, we also demonstrate application of TAMD-assisted MDFF (TAMDFF) on a RNA/protein complex and suggest that TAMDFF is a viable strategy for enhanced conformational fitting in target maps of ribonucleoprotein complexes.
  • Authors

  • Vashisth, Harish
  • Skiniotis, Georgios
  • Brooks, Charles L
  • Status

    Publication Date

  • April 11, 2013
  • Keywords

  • Algorithms
  • Cryoelectron Microscopy
  • Molecular Dynamics Simulation
  • Nucleic Acid Conformation
  • Nucleic Acids
  • Protein Structure, Secondary
  • Ribonucleoproteins
  • Digital Object Identifier (doi)

    Start Page

  • 3738
  • End Page

  • 3746
  • Volume

  • 117
  • Issue

  • 14