Abstract

The proposed research involves a comprehensive investigation of the relationship of structure to function in monomeric sarcosine oxidase (MSOX), a prototypical member of a superfamily of amine-oxidizing enzymes that contain covalently bound derivatives of the vitamin riboflavin. MSOX is an important catabolic enzyme commonly found in soil bacteria and widely used in the clinical evaluation of renal function. The MSOX superfamily contains several biomedically significant human enzymes, including sarcosine dehydrogenase, an enzyme defective in sarcosinemic patients and monoamine oxidase, a drug target in the treatment of Parkinson's disease and depression. The overall goal of these studies is to gain a deeper understanding of the mechanism of flavoenzyme catalysis, the molecular basis for enzyme specificity and the modulation of the inherent chemical reactivity of flavins by the protein environment. We will determine the crystal structure for various MSOX-substrate complexes in studies that build on our success in obtaining a preliminary 2.0 A resolution structure for the E-S complex with L-proline. Amine oxidation generally requires an unprotonated amino group but the substrates for MSOX are amino acids that exist in solution at neutral pH as unreactive zwitterions. We will evaluate the proposal that substrates are activated for oxidation by MSOX via a mechanism that involves a substantial decrease in the pKa of the enzyme-bound versus the free amino acid. The mechanism of substrate oxidation will be investigated in studies involving a mechanism-based inhibitor, alternate substrates, deuterium isotope effects, stereochemical analysis, mutagenesis and molecular dynamic simulations. We will probe the role of the covalent flavin linkage in reconstitution and structural studies with a MSOX apoprotein preparation containing a mutation that allows noncovalent flavin binding but blocks covalent attachment. The mechanism of covalent flavin attachment will be characterized in in vitro flavinylation studies with wild type apoenzyme or appropriate mutants. These studies represent a multidisciplinary approach, involving a combination of biochemical, structural and modeling efforts. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM031704-25
Application #
7158563
Study Section
Special Emphasis Panel (ZRG1-SSS-B (01))
Program Officer
Ikeda, Richard A
Project Start
1995-09-03
Project End
2008-12-31
Budget Start
2007-01-01
Budget End
2008-12-31
Support Year
25
Fiscal Year
2007
Total Cost
$348,928
Indirect Cost

  Institution

Name
Drexel University
Department
Biochemistry
Type
Schools of Medicine
DUNS #
002604817
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Kommoju, Phaneeswara-Rao; Chen, Zhi-wei; Bruckner, Robert C et al. (2011) Probing oxygen activation sites in two flavoprotein oxidases using chloride as an oxygen surrogate. Biochemistry 50:5521-34
Bruckner, Robert C; Winans, Jennifer; Jorns, Marilyn Schuman (2011) Pleiotropic impact of a single lysine mutation on biosynthesis of and catalysis by N-methyltryptophan oxidase. Biochemistry 50:4949-62
Jorns, Marilyn Schuman; Chen, Zhi-Wei; Mathews, F Scott (2010) Structural characterization of mutations at the oxygen activation site in monomeric sarcosine oxidase . Biochemistry 49:3631-9
Zhao, Guohua; Bruckner, Robert C; Jorns, Marilyn Schuman (2008) Identification of the oxygen activation site in monomeric sarcosine oxidase: role of Lys265 in catalysis. Biochemistry 47:9124-35
Hassan-Abdallah, Alshaimaa; Zhao, Guohua; Chen, Zhi-wei et al. (2008) Arginine 49 is a bifunctional residue important in catalysis and biosynthesis of monomeric sarcosine oxidase: a context-sensitive model for the electrostatic impact of arginine to lysine mutations. Biochemistry 47:2913-22
Hassan-Abdallah, Alshaimaa; Zhao, Guohua; Jorns, Marilyn Schuman (2008) Covalent flavinylation of monomeric sarcosine oxidase: identification of a residue essential for holoenzyme biosynthesis. Biochemistry 47:1136-43
Zhao, Gouhua; Jorns, Marilyn Schuman (2006) Spectral and kinetic characterization of the michaelis charge transfer complex in monomeric sarcosine oxidase. Biochemistry 45:5985-92
Chen, Zhi-wei; Hassan-Abdulah, Alshaimaa; Zhao, Gouhua et al. (2006) Heterotetrameric sarcosine oxidase: structure of a diflavin metalloenzyme at 1.85 A resolution. J Mol Biol 360:1000-18
Hassan-Abdallah, Alshaimaa; Zhao, Guohua; Jorns, Marilyn Schuman (2006) Role of the covalent flavin linkage in monomeric sarcosine oxidase. Biochemistry 45:9454-62
Hynson, Robert M G; Mathews, F Scott; Schuman Jorns, Marilyn (2006) Identification of a stable flavin-thiolate adduct in heterotetrameric sarcosine oxidase. J Mol Biol 362:656-63

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