Atomic-level accuracy in simulations of large protein crystals.
AUTOR(ES)
York, D M
RESUMO
Proper treatment of long-range Coulombic forces presents a major obstacle to providing realistic molecular dynamics simulations of macromolecules. Traditional approximations made to lessen computational cost ultimately lead to unrealistic behavior. The particle mesh Ewald method accommodates long-range Coulombic forces accurately and efficiently by use of fast Fourier transform techniques. We report a 1-ns simulation of bovine pancreatic trypsin inhibitor in a crystal unit cell using the particle mesh Ewald methodology. We find an rms backbone deviation from the x-ray structure (0.33 A) that is lower than that observed between bovine pancreatic trypsin inhibitor in different crystal forms and much lower than those of previous simulations. These results bridge the gap between structures obtained from molecular simulation and those from experiment.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=44677Documentos Relacionados
- Atomic-level observation of macromolecular crowding effects: Escape of a protein from the GroEL cage
- Simulations of nucleation and early growth stages of protein crystals.
- Preparation of large monodomain phospholipid bilayer smectic liquid crystals.
- Significance of bound water to local chain conformations in protein crystals.
- Laboratory handling of crystals.
