Abstract

Three fundamental aspects of cytochrome c function that have general implications for many other proteins will be studied: (1) Regulation of cytochrome c conformational dynamics and midpoint reduction potential by pH. At alkaline pH, the Met80 ligand to the heme iron is replaced by either Lys79 or Lys73 to produce two alkaline conformational states. Electrochemical, stopped-flow, and NMR analysis of these two conformational isomers will be undertaken through analysis of the Lys79Ala and Lys73Ala variants to assess their structural and functional properties. Related studies will consider (a) the conformational dynamics of mutations at Phe82 that have previously been shown to lower the PKa for the conformational equilibrium, (b) the conformational and functional consequences of replacing residues 79 and 73 with alternative """"""""alkaline ligands,"""""""" and (c) the identity of the conformationally-linked titratable group that deprotonates prior to loss of the Met80 ligand. (2) Interaction and reaction of cytochrome c with other heme proteins. (a) The interaction of cytochrome c with cytochrome b5 will be studied through application of a novel NMR technique for identification of surface Lys residues involved in complex formation, through detailed electrostatics modelling of potentiometric titrations of the cytochrome c-cytochrome b5 complex and by rapid kinetics techniques. (b) The cytochrome c-cytochrome c peroxidase complex will be characterized by potentiometric titrations and rapid kinetics techniques that will include use of critically selected mutants of the peroxidase predicted to disrupt each of the two binding sites for the cytochrome. These results will also be simulated by electrostatics modelling calculations. (c) The complex formed by human erythrocyte cytochrome b5 and human hemoglobin and its subunits will be analyzed by potentiometric titrations. Parallel studies will assess the influence of complex formation on the spectroscopic and ligand binding characteristics of hemoglobin. (3) The role of electron donor structure on kinetics of intramolecular electron transfer kinetics. Synthetic flavocytochromes produced by a combination of site-directed mutagenesis and chemical modification will be used to study the effect of electron donor structure on intramolecular electron transfer kinetics by comparison with published results obtained with analogous cytochrome derivatives in which ruthenium complexes serve as the electron donor.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM033804-11
Application #
2177150
Study Section
Physical Biochemistry Study Section (PB)
Project Start
1985-09-20
Project End
1997-08-31
Budget Start
1995-09-01
Budget End
1996-08-31
Support Year
11
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of British Columbia
Department
Type
DUNS #
800772162
City
Vancouver
State
BC
Country
Canada
Zip Code
V6 1-Z3

  Publications

Pollock, W B; Rosell, F I; Twitchett, M B et al. (1998) Bacterial expression of a mitochondrial cytochrome c. Trimethylation of lys72 in yeast iso-1-cytochrome c and the alkaline conformational transition. Biochemistry 37:6124-31
Moore, G R; Cox, M C; Crowe, D et al. (1998) N epsilon,N epsilon-dimethyl-lysine cytochrome c as an NMR probe for lysine involvement in protein-protein complex formation. Biochem J 332 ( Pt 2):439-49
McGee, W A; Rosell, F I; Liggins, J R et al. (1996) Thermodynamic cycles as probes of structure in unfolded proteins. Biochemistry 35:1995-2007
Rafferty, S P; Guillemette, J G; Berghuis, A M et al. (1996) Mechanistic and structural contributions of critical surface and internal residues to cytochrome c electron transfer reactivity. Biochemistry 35:10784-92
Mauk, A G; Mauk, M R; Moore, G R et al. (1995) Experimental and theoretical analysis of the interaction between cytochrome c and cytochrome b5. J Bioenerg Biomembr 27:311-30
Mauk, M R; Ferrer, J C; Mauk, A G (1994) Proton linkage in formation of the cytochrome c-cytochrome c peroxidase complex: electrostatic properties of the high- and low-affinity cytochrome binding sites on the peroxidase. Biochemistry 33:12609-14
Guillemette, J G; Barker, P D; Eltis, L D et al. (1994) Analysis of the bimolecular reduction of ferricytochrome c by ferrocytochrome b5 through mutagenesis and molecular modelling. Biochimie 76:592-604
Hildebrandt, P; Vanhecke, F; Buse, G et al. (1993) Resonance Raman study of the interactions between cytochrome c variants and cytochrome c oxidase. Biochemistry 32:10912-22
Davies, A M; Guillemette, J G; Smith, M et al. (1993) Redesign of the interior hydrophilic region of mitochondrial cytochrome c by site-directed mutagenesis. Biochemistry 32:5431-5
Hildebrandt, P; Vanhecke, F; Heibel, G et al. (1993) Structural changes in cytochrome c upon hydrogen-deuterium exchange. Biochemistry 32:14158-64

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