Mechanistic and structural studies are proposed on the 8alpha-S-cysteinyl FAD-containing enzymes: monoamine oxidase B (MAO B) and monoamine oxidase A (MAO A). Human MAO B and MAO A expressed in yeast will be purified and characterized, and compared with the physical and chemical properties of human placental MAO A and bovine liver MAO B. A systematic investigation of ring substituent effects on the binding and rate of CH bond cleavage of benzylamine substrates will be extended from current work on bovine MAO B to recombinant human MAO A and MAO B. Ring-substituent effects on phenethylamine substrate analogs on the binding and rate of CH bond cleavage will also be investigated with MAO A and MAO B and the results compared with the benzylamine data to provide detailed information on steric effects on catalysis.Investigations into whether tunneling contributes to the hydrogen transfer step in MAO B and MAO A will be done in collaboration with Dr. J. Klinman, U. Calif., Berkeley. Evidence for the catalytic involvement and identity of an amino acid radical which may function in hydrogen atom abstraction will be sought in MAO A and MAO B using ESR and ENDOR of native and isotopically labeled enzymes. The oxidation/reduction potentials for the OX/SQ and SQ/HQ couples of the covalent flavin coenzymes in MAO B and in MAO A will be determined using spectrocoulometry. The results of these studies should provide new insights into the catalytic mechanisms of MAO A and of MAO B and provide a basis for the development of specific inhibitors for each enzyme which are of neuropharmacological importance as targets for drug therapy. Anti- depressants used clinically are MAO A inhibitors while the clinical use of MAO B inhibitors is to potentiate L-Dopa therapy of patients with Parkinson's Disease.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM029433-11A1
Application #
3277026
Study Section
Physical Biochemistry Study Section (PB)
Project Start
1982-07-01
Project End
1997-07-31
Budget Start
1993-08-01
Budget End
1994-07-31
Support Year
11
Fiscal Year
1993
Total Cost
Indirect Cost
Name
Emory University
Department
Type
Schools of Medicine
DUNS #
042250712
City
Atlanta
State
GA
Country
United States
Zip Code
30322
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Orru, R; Aldeco, M; Edmondson, D E (2013) Do MAO A and MAO B utilize the same mechanism for the C-H bond cleavage step in catalysis? Evidence suggesting differing mechanisms. J Neural Transm (Vienna) 120:847-51
Milczek, Erika M; Binda, Claudia; Rovida, Stefano et al. (2011) The 'gating' residues Ile199 and Tyr326 in human monoamine oxidase B function in substrate and inhibitor recognition. FEBS J 278:4860-9
Wang, Jin; Edmondson, Dale E (2011) Topological probes of monoamine oxidases A and B in rat liver mitochondria: inhibition by TEMPO-substituted pargyline analogues and inactivation by proteolysis. Biochemistry 50:2499-505
Binda, Claudia; Mattevi, Andrea; Edmondson, Dale E (2011) Structural properties of human monoamine oxidases A and B. Int Rev Neurobiol 100:1-11
Binda, Claudia; Aldeco, Milagros; Geldenhuys, Werner J et al. (2011) Molecular Insights into Human Monoamine Oxidase B Inhibition by the Glitazone Anti-Diabetes Drugs. ACS Med Chem Lett 3:39-42
MacMillar, Susanna; Edmondson, Dale E; Matsson, Olle (2011) Nitrogen kinetic isotope effects for the monoamine oxidase B-catalyzed oxidation of benzylamine and (1,1-(2)H2)benzylamine: nitrogen rehybridization and CH bond cleavage are not concerted. J Am Chem Soc 133:12319-21
Nucci, Nathaniel V; Pometun, Maxim S; Wand, A Joshua (2011) Mapping the hydration dynamics of ubiquitin. J Am Chem Soc 133:12326-9
Binda, Claudia; Milczek, Erika M; Bonivento, Daniele et al. (2011) Lights and shadows on monoamine oxidase inhibition in neuroprotective pharmacological therapies. Curr Top Med Chem 11:2788-96

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