The progress in sequencing of complete genomes highlights the growing need to understand the structural principles underlying the folding and function of proteins. In FY00, we have focused on three major aspects: (1) Ab initio folding of peptides: Based on extensive computer simulations at full atomic detail and including solvent, we have successfully studied the reversible folding of small alanine and glycine based peptides into alpha-helices. This allowed us to identify the energetics, time scales, and mechanisms of the initial phases of helix formation as a critical step in protein folding. Our results also shed new light on a recent experimental controversy, supporting laser temperature jump experiments, but disagreeing with stopped-flow circular dichroism measurements. (2) Protein dynamics and identification of essential modes: One of the key steps leading from protein structure to function is the identification of the essential dynamics, associated for instance with substrate access and release, or with catalytic activity. From an analysis of the time evolution of protein conformations in molecular simulations, we developed a new estimate of the number of degrees of freedom that are relevant in a particular time regime. (3) Ligand binding and hydrophobic effects. One of the main objectives of computational structural biology is the design and optimization of drug molecules. We are developing a hydrophobic force field that allows us to map regions at the protein surface with strong hydrophobic interaction centers to bind ligands. Preliminary results for an inhibitor of the HIV-1 gp41 fusion peptide show excellent agreement with a combinatorially optimized ligand, and with explicit, but computationally demanding molecular simulations.

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Intramural Research (Z01)
Project #
1Z01DK029033-01
Application #
6420988
Study Section
(LCP)
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
2000
Total Cost
Indirect Cost
Name
U.S. National Inst Diabetes/Digst/Kidney
Department
Type
DUNS #
City
State
Country
United States
Zip Code
Rosta, Edina; Buchete, Nicolae-Viorel; Hummer, Gerhard (2009) Thermostat artifacts in replica exchange molecular dynamics simulations. J Chem Theory Comput 5:1393-1399
Best, Robert B; Hummer, Gerhard (2009) Biochemistry. Unfolding the secrets of calmodulin. Science 323:593-4
Kim, Young C; Tang, Chun; Clore, G Marius et al. (2008) Replica exchange simulations of transient encounter complexes in protein-protein association. Proc Natl Acad Sci U S A 105:12855-60
Best, Robert B; Buchete, Nicolae-Viorel; Hummer, Gerhard (2008) Are current molecular dynamics force fields too helical? Biophys J 95:L07-9
Buchete, Nicolae-Viorel; Hummer, Gerhard (2008) Peptide folding kinetics from replica exchange molecular dynamics. Phys Rev E Stat Nonlin Soft Matter Phys 77:030902
Buchete, Nicolae-Viorel; Hummer, Gerhard (2008) Coarse master equations for peptide folding dynamics. J Phys Chem B 112:6057-69
Kim, Young C; Hummer, Gerhard (2008) Coarse-grained models for simulations of multiprotein complexes: application to ubiquitin binding. J Mol Biol 375:1416-33
Canagarajah, Bertram J; Hummer, Gerhard; Prinz, William A et al. (2008) Dynamics of cholesterol exchange in the oxysterol binding protein family. J Mol Biol 378:737-48
Tikhonova, Irina G; Best, Robert B; Engel, Stanislav et al. (2008) Atomistic insights into rhodopsin activation from a dynamic model. J Am Chem Soc 130:10141-9
Turjanski, Adrian Gustavo; Gutkind, J Silvio; Best, Robert B et al. (2008) Binding-induced folding of a natively unstructured transcription factor. PLoS Comput Biol 4:e1000060

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