Abstract

This is a competitive renewal application for a Research Scientist Award (RSA). The overall objectives of this project are to further study the structure, function and the regulation of monoamine oxidase (MAO) A and B. MAO is an important enzyme in catecholamine metabolism. Abnormal levels of MAO activity have been shown in a number of mental disorders. These objectives will be accomplished using human MAO A, MAO B, cDNAs and human MAO A and B genomic clones isolated in this laboratory.
The specific aims of this five-year RSA application are described below: (I) To further investigate the structure and function of MAO A and B: The amino acids and domains responsible for MAO A and B substrate and inhibitor specificities will be identified by site-directed mutagenesis and chimeric enzymes constructed among MAO A, MAO B and trout MAO (trout MAO exhibits nonclassical inhibitor sensitivities). These mutants will be expressed in yeast. The kinetic parameters for substrates (Km) and inhibitors (Ki) will be determined. The regions responsible for mitochondrial targeting will be identified by using a series of C- terminal deletions and chimeric mutants. The kinetic parameter (Km, Ki) determination and Western blot will be performed on purified mitochondria to demonstrate if the MAO A or B protein is targeted to mitochondria. (II) To further investigate the mechanisms of regulation of MAO A and B gene expression: A new gene upstream of MAO A core promoter will be cloned and characterized. A novel repressor which down regulates MAO B promoter activity will be isolated by screening an expression library and by affinity column chromatography. Cell-specific elements (enhancers and silencers) and transcription factors for MAO A and B gene expression will be identified by transient expression assay, combined with mutations, deletions, gel retardation and DNaseI footprinting assays. The mechanisms of hormone stimulation of MAO A and B will be investigated. Further, the regulation of MAO A expression by the concentration and DNA binding efficiency of Sp1 in cells will be studied. Whether the increased MAO B catalytic activity in aged human brains and Alzheimer's patients is related to altered promoter sequences and/or the concentrations of transcription factors will be examined. These studies will provide most fundamental knowledge on the regulation of MAO A and B gene expression. The new knowledge may ultimately lead to a novel approach for designing specific MAO inhibitors which modulate MAO activity at the gene level, and may be used for patients with mental disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Scientist Award (K05)
Project #
5K05MH000796-10
Application #
2674334
Study Section
Neuropharmacology and Neurochemistry Review Committee (NPNC)
Project Start
1989-04-01
Project End
2000-04-30
Budget Start
1998-05-01
Budget End
2000-04-30
Support Year
10
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Southern California
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
041544081
City
Los Angeles
State
CA
Country
United States
Zip Code
90089

  Publications

Holschneider, D P; Scremin, O U; Chialvo, D R et al. (2002) Heart rate dynamics in monoamine oxidase-A- and -B-deficient mice. Am J Physiol Heart Circ Physiol 282:H1751-9
Holschneider, D P; Scremin, O U; Roos, K P et al. (2002) Increased baroreceptor response in mice deficient in monoamine oxidase A and B. Am J Physiol Heart Circ Physiol 282:H964-72
Geha, R M; Rebrin, I; Chen, K et al. (2001) Substrate and inhibitor specificities for human monoamine oxidase A and B are influenced by a single amino acid. J Biol Chem 276:9877-82
Hauptmann, N; Shih, J C (2001) 2-Naphthylamine, a compound found in cigarette smoke, decreases both monoamine oxidase A and B catalytic activity. Life Sci 68:1231-41
Wong, W K; Chen, K; Shih, J C (2001) Regulation of human monoamine oxidase B gene by Sp1 and Sp3. Mol Pharmacol 59:852-9
Rebrin, I; Geha, R M; Chen, K et al. (2001) Effects of carboxyl-terminal truncations on the activity and solubility of human monoamine oxidase B. J Biol Chem 276:29499-506
Fornai, F; Giorgi, F S; Gesi, M et al. (2001) Biochemical effects of the monoamine neurotoxins DSP-4 and MDMA in specific brain regions of MAO-B-deficient mice. Synapse 39:213-21
Holschneider, D P; Chen, K; Seif, I et al. (2001) Biochemical, behavioral, physiologic, and neurodevelopmental changes in mice deficient in monoamine oxidase A or B. Brain Res Bull 56:453-62
Geha, R M; Chen, K; Shih, J C (2000) Phe(208) and Ile(199) in human monoamine oxidase A and B do not determine substrate and inhibitor specificities as in rat. J Neurochem 75:1304-9
Holschneider, D P; Shih, J C (2000) Genotype to phenotype: challenges and opportunities. Int J Dev Neurosci 18:615-8

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