Abstract

The primary goal of the proposed research is a detailed understanding of the relationships between structure and energy that determine the structure and functions of proteins. A major focus will be the development and application methods for the study of problems such as protein folding and protein stability and the prediction of binding free energies of substrates to proteins. In most applications, relative free energies in solution will be obtained by combining gas phase molecular mechanics calculation with the evaluation of solvation free energies. Electrostatic contributions to solvation are obtained from numerical solutions to the Poisson-Boltzmann (PB) equation. Non-polar contributions are calculated from free energy/surface area relationships. The methodological emphasis will involve the development of algorithms which yield rapid and accurate numerical solutions to the PB equation. The goal is to reach the point where a solvation free energy calculation on a molecule is as fast as a gas phase energy evaluation in molecular mechanics program. This will make it possible to include solvent directly in conformational search procedures, energy minimization and molecular dynamics. Preliminary estimates suggest that a combination of multigriding and adaptive gridding techniques make this a reasonable goal. Methods involving surface charges will also be developed to calculate forces on atoms directly from PB calculations. Proposed research on protein folding will focus on three areas. l) A recently developed method to calculate the pH dependence of protein stability will be used to study acid denaturation. The stability of the compact """"""""molten globule"""""""" states formed under acidic conditions will be considered in this context. 2) The factors that determine secondary structure stability, including individual amino acid propensities, will be elucidated with calculations of relative conformational energies. 3) A method to distinguish stable from unstable protein conformations will be developed. Calculations will be carried out of the relative binding energies of different inhibitors to the HIV protease. Studies will be made of compounds for which both structural and thermodynamic data are available. Similar studies will also be carried out on the binding of peptides to class I MHC proteins. High resolution structures are currently available for the binding of different peptides to the same class I protein and binding affinities have also been measured. An attempt will be made to understand the energetic principles and structural rules involved in antigen recognition. The health relatedness of the proposed research is in the general principles about protein structure and function that are being developed. In addition the results of the research will be applicable to structure- based drug design in general, with specific applications to the design of HIV protease inhibitors and to the design of antiviral drugs that act on MHC proteins.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37GM030518-16
Application #
2021905
Study Section
Molecular and Cellular Biophysics Study Section (BBCA)
Project Start
1981-09-01
Project End
1999-11-30
Budget Start
1996-12-01
Budget End
1997-11-30
Support Year
16
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Biochemistry
Type
Schools of Medicine
DUNS #
167204994
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Hirabayashi, Yusuke; Kwon, Seok-Kyu; Paek, Hunki et al. (2017) ER-mitochondria tethering by PDZD8 regulates Ca2+ dynamics in mammalian neurons. Science 358:623-630
Hwang, Howook; Dey, Fabian; Petrey, Donald et al. (2017) Structure-based prediction of ligand-protein interactions on a genome-wide scale. Proc Natl Acad Sci U S A 114:13685-13690
Sheng, Ren; Jung, Da-Jung; Silkov, Antonina et al. (2016) Lipids Regulate Lck Protein Activity through Their Interactions with the Lck Src Homology 2 Domain. J Biol Chem 291:17639-50
Hwang, Howook; Petrey, Donald; Honig, Barry (2016) A hybrid method for protein-protein interface prediction. Protein Sci 25:159-65
Ma, Lijiang; Bayram, Yavuz; McLaughlin, Heather M et al. (2016) De novo missense variants in PPP1CB are associated with intellectual disability and congenital heart disease. Hum Genet 135:1399-1409
Park, Mi-Jeong; Sheng, Ren; Silkov, Antonina et al. (2016) SH2 Domains Serve as Lipid-Binding Modules for pTyr-Signaling Proteins. Mol Cell 62:7-20
Westphalen, C Benedikt; Takemoto, Yoshihiro; Tanaka, Takayuki et al. (2016) Dclk1 Defines Quiescent Pancreatic Progenitors that Promote Injury-Induced Regeneration and Tumorigenesis. Cell Stem Cell 18:441-55
Garzón, José Ignacio; Deng, Lei; Murray, Diana et al. (2016) A computational interactome and functional annotation for the human proteome. Elife 5:
Wang, Donglai; Kon, Ning; Lasso, Gorka et al. (2016) Acetylation-regulated interaction between p53 and SET reveals a widespread regulatory mode. Nature 538:118-122
Shang, Linshan; Henderson, Lindsay B; Cho, Megan T et al. (2016) De novo missense variants in PPP2R5D are associated with intellectual disability, macrocephaly, hypotonia, and autism. Neurogenetics 17:43-9

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