Abstract

Structural flexibility plays an important role in protein function and is essential for the protein-protein and protein-ligand recognition mechanisms known as induced- and selected-fit. Surface loops, which typically participate in such processes, can prevail in flexibility states ranging from a random coil to a well defined structure, where a loop resides in a single wide microstate (WM), defined by local structural fluctuations. A loop can also exhibit intermediate flexibility, where several WMs are populated significantly in thermodynamic equilibrium. To date structure determination of large loops is still an unsolved problem in homology studies. None of the existing approaches has addressed the problem of loop flexibility in a systematic way. A statistical mechanics methodology for treating flexibility was developed recently by us and applied successfully to predict the solution structures and populations of cyclic peptides in DMSO. In this project it will be extended to protein loops in water. This methodology consists of (1) a novel optimization of atomic solvation parameters (ASPs), (2) an extensive conformational search using our local torsional deformations (LTD) method for identifying the most stable WMs, and (3) simulating these WMs by Monte Carlo and calculating their free energies (hence populations) with our local states (LS) method. The loop energy is defined by a force field and a solvation term which depends on the ASPs. The optimized ASPs are those for which the global energy minimum structure of the loop becomes the loop's X-ray structure. This procedure differs from the common derivation of ASPs, which is based on the free energy of transfer of small molecules from the gas phase to water. We have already optimized ASPs for a loop of ribonuclease A based on the OPLS and AMBER force fields. Exceptionally good results obtained with AMBER. The transferability of the ASPS will be tested by studying hypervariable loops of antibodies and other known loop structures. Problems addressed by CASP5 will be attacked as well. We shall concentrate on the intermediate flexibility of loops participating in enzyme binding, catalysis, and recognition processes that are important in rational drug design. To be able to treat long loops, the efficiency of the LTD and LS methods will be enhanced. Our unique tools are applicable to a wide range of problems in structural biology, such as protein engineering, docking, and threading.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM061916-04
Application #
6636511
Study Section
Molecular and Cellular Biophysics Study Section (BBCA)
Program Officer
Wehrle, Janna P
Project Start
2001-05-01
Project End
2005-04-30
Budget Start
2003-05-01
Budget End
2005-04-30
Support Year
4
Fiscal Year
2003
Total Cost
$186,354
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Genetics
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

White, Ronald P; Meirovitch, Hagai (2006) Minimalist explicit solvation models for surface loops in proteins. J Chem Theory Comput 2:1135-1151
Szarecka, Agnieszka; Meirovitch, Hagai (2006) Optimization of the GB/SA solvation model for predicting the structure of surface loops in proteins. J Phys Chem B 110:2869-80
White, Ronald P; Meirovitch, Hagai (2006) Free volume hypothetical scanning molecular dynamics method for the absolute free energy of liquids. J Chem Phys 124:204108
Cheluvaraja, Srinath; Meirovitch, Hagai (2005) Calculation of the entropy and free energy from monte carlo simulations of a peptide stretched by an external force. J Phys Chem B 109:21963-70
White, Ronald P; Meirovitch, Hagai (2005) Calculation of the entropy of random coil polymers with the hypothetical scanning Monte Carlo method. J Chem Phys 123:214908
Cheluvaraja, Srinath; Meirovitch, Hagai (2005) Calculation of the entropy and free energy by the hypothetical scanning Monte Carlo method: application to peptides. J Chem Phys 122:54903
White, Ronald P; Funt, Jason; Meirovitch, Hagai (2005) Calculation of the Entropy of Lattice Polymer Models from Monte Carlo Trajectories. Chem Phys Lett 410:430-435
Ozkan, S Banu; Meirovitch, Hagai (2004) Conformational search of peptides and proteins: Monte Carlo minimization with an adaptive bias method applied to the heptapeptide deltorphin. J Comput Chem 25:565-72
White, Ronald P; Meirovitch, Hagai (2004) Lower and upper bounds for the absolute free energy by the hypothetical scanning Monte Carlo method: application to liquid argon and water. J Chem Phys 121:10889-904
Cheluvaraja, Srinath; Meirovitch, Hagai (2004) Simulation method for calculating the entropy and free energy of peptides and proteins. Proc Natl Acad Sci U S A 101:9241-6

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