Abstract

It is the goal of this research to provide a definitive molecular description, by experimental and theoretical techniques, of calcium and magnesium ion binding to prothrombin (human and bovine), its Fragment 1 and appropriate fragment peptides in various states of decarboxylation. Metal binding to prothrombin is thought to be primarily a gamma-carboxyglutamic acid (Gla) event; these aminoacids are prominently displayed along the N- terminus of prothrombin and several other coagulation proteins. We shall (a) conduct a series of condition-consistent metal binding measurements by the technique of equilibrium dialysis, (b) develop a dialysis technique for utilizing the short half-life isotope Mg-28, (c) investigate the Ca2+ ion-selective electrode as a sensitive device for determining low and high concentrations of Ca2+ in the presence and absence of magnesium. In the theoretical studies we will (a) use molecular mechanics and molecular dynamics techniques to find local and global energy minima, respectively, of the 18-23 loop and related Gla containing peptides in the presence and absence of Ca2+ and Mg2+. (b) Use the same techniques as (a) augmented by semiempirical techniques to compute binding of Gla (or malonate) and arginine to (guanidinium) of possible stabilizing salt bridge structures thought to be present in prothrombin. (c) Use distance geometry techniques and the techniques in (a) to interpret experimental 2D- NMR experiments performed on peptides derived or synthesized from the N-terminus regions of Fragment 1 by R.G. Hiskey's group. The theoretical calculations should ultimately provide a good estimate of the metal bound structure of prothrombin. Addendum Further, we will a) investigate the determination of Mg2+ binding with electrodes, b) continue to develop a statistical technique which promises to find the critical number of ligands to effect a biophysical response, c) perform quantum chemical calculations on beta hydroxy aspartic acid models, important in the negative feedback loop of coagulation, d) determine the binding free energy for Ca2+ and Mg2+ to Gla containing models.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL027995-07
Application #
3339416
Study Section
Hematology Subcommittee 2 (HEM)
Project Start
1988-04-01
Project End
1993-03-31
Budget Start
1991-04-01
Budget End
1992-03-31
Support Year
7
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Type
Schools of Arts and Sciences
DUNS #
078861598
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Chen, Z; Blandl, T; Prorok, M et al. (1998) Conformational changes in conantokin-G induced upon binding of calcium and magnesium as revealed by NMR structural analysis. J Biol Chem 273:16248-58
Li, L; Darden, T A; Freedman, S J et al. (1997) Refinement of the NMR solution structure of the gamma-carboxyglutamic acid domain of coagulation factor IX using molecular dynamics simulation with initial Ca2+ positions determined by a genetic algorithm. Biochemistry 36:2132-8
Cabaniss, S; Deerfield 2nd, D W; Monroe, D M et al. (1995) Is Ca(II) ion binding to prothrombin fragment 1 intrinsically cooperative, or is the cooperative binding accounted for by self-association? Blood Coagul Fibrinolysis 6:464-73
Li, L; Darden, T; Foley, C et al. (1995) Homology modeling and molecular dynamics simulation of human prothrombin fragment 1. Protein Sci 4:2341-8
Deerfield 2nd, D W; Pedersen, L G (1995) The first solvation shell of magnesium and calcium ions in a model nucleic acid environment: an ab initio study. J Biomol Struct Dyn 13:167-80
Deerfield 2nd, D W; Fox, D J; Head-Gordon, M et al. (1995) The first solvation shell of magnesium ion in a model protein environment with formate, water, and X-NH3, H2S, imidazole, formaldehyde, and chloride as ligands: an Ab initio study. Proteins 21:244-55
Frech, M; Darden, T A; Pedersen, L G et al. (1994) Role of glutamine-61 in the hydrolysis of GTP by p21H-ras: an experimental and theoretical study. Biochemistry 33:3237-44
York, D M; Darden, T A; Pedersen, L G et al. (1993) Molecular dynamics simulation of HIV-1 protease in a crystalline environment and in solution. Biochemistry 32:1443-53
York, D M; Darden, T A; Pedersen, L G et al. (1993) Molecular modeling studies suggest that zinc ions inhibit HIV-1 protease by binding at catalytic aspartates. Environ Health Perspect 101:246-50
Foley, C K; Pedersen, L G; Charifson, P S et al. (1992) Simulation of the solution structure of the H-ras p21-GTP complex. Biochemistry 31:4951-9

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