Abstract

Predicting folded protein structure from the primary amino acid sequence remains one of the great unsolved problems in biochemistry. In turn, an understanding of the molecular dynamics of folded proteins is imperative for understanding their biological function. In recent years it has become clear that protein structure, folding patterns and dynamics all depend upon the interplay among a number of subtle interactions. To understand this interplay, biochemists must develop a deeper physical insights into these various interactions. A recent major advance towards understanding the forces that control protein structure is the discovery of short alanine-based peptides, 16-mers and 17-mers, that form stable alpha-helices in aqueous solution. These helices exhibit a thermal unfolding transition between 0 degrees C and 60 degrees C. They are constructed from naturally-occurring amino acids and, therefore, serve as excellent models of helical structures in natural proteins. These helices further serve as a testing ground for theories of protein molecular dynamics. We propose to greatly advance the understanding of these peptides by using Electron Spin Resonance (ESR) to study spin labeled peptide analogs. Using such techniques, our lab is the first to have demonstrated an ability to experimentally measure local position dependent peptide dynamics and these measurements are now providing a reference point for computer molecular dynamics studies. In past work we have shown that helical peptides can be spin labeled with a minimal perturbation of their alpha-helix -> coil equilibrium. We have further shown that the dynamic details extracted from a combination of ESR experiments and Circular Dichroism (CD) experiments can be used to provide a detailed description of peptide dynamics throughout the folding process. Our research plan is to now combine our ESR technology with peptide design technology and systematically probe the physical aspects that control helix formation, stability and local motions. The chief goals of the proposed research are: 1) Determine a mobility profile along the alpha-helix backbone;2) Localize the influence of helix-breaking residues; 3) Detect the interactions among large residue side chains that are located close to each other on the helix surface; 4) Determine the actual winding geometry of these helical peptides to distinguish 3(10) helix from alpha-helix.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM046870-03
Application #
2184358
Study Section
Physical Biochemistry Study Section (PB)
Project Start
1992-08-01
Project End
1995-07-31
Budget Start
1994-08-01
Budget End
1995-07-31
Support Year
3
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
University of California Santa Cruz
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
City
Santa Cruz
State
CA
Country
United States
Zip Code
95064

  Publications

Aronoff-Spencer, E; Burns, C S; Avdievich, N I et al. (2000) Identification of the Cu2+ binding sites in the N-terminal domain of the prion protein by EPR and CD spectroscopy. Biochemistry 39:13760-71
Monaco, V; Formaggio, F; Crisma, M et al. (1999) Orientation and immersion depth of a helical lipopeptaibol in membranes using TOAC as an ESR probe. Biopolymers 50:239-53
Bennati, M; Gerfen, G J; Martinez, G V et al. (1999) Nitroxide side-chain dynamics in a spin-labeled helix-forming peptide revealed by high-frequency (139.5-GHz) EPR spectroscopy. J Magn Reson 139:281-6
Bolin, K A; Anderson, D J; Trulson, J A et al. (1999) NMR structure of a minimized human agouti related protein prepared by total chemical synthesis. FEBS Lett 451:125-31
Trulson, J A; Millhauser, G L (1999) The effect of mutations on peptide models of the DNA binding helix of p53: evidence for a correlation between structure and tumorigenesis. Biopolymers 49:215-24
Martinez, G V; Millhauser, G L (1998) A neural network approach to the rapid computation of rotational correlation times from slow motional ESR spectra. J Magn Reson 134:124-30
Lundberg, K M; Stenland, C J; Cohen, F E et al. (1997) Kinetics and mechanism of amyloid formation by the prion protein H1 peptide as determined by time-dependent ESR. Chem Biol 4:345-55
Severcan, F; Stenland, C; Millhauser, G (1997) ESR studies of pig citrate synthase. Biochem Soc Trans 25:380S
Millhauser, G L; Stenland, C J; Hanson, P et al. (1997) Estimating the relative populations of 3(10)-helix and alpha-helix in Ala-rich peptides: a hydrogen exchange and high field NMR study. J Mol Biol 267:963-74
Millhauser, G L; Stenland, C J; Bolin, K A et al. (1996) Local helix content in an alanine-rich peptide as determined by the complete set of 3JHN alpha coupling constants. J Biomol NMR 7:331-4

Showing the most recent 10 out of 17 publications