H202 AND OXY-RADICAL STRESS IN CATECHOLAMINE NEURONS
Project Number5R01NS023017-07
Contact PI/Project LeaderCOHEN, GERALD
Awardee OrganizationMOUNT SINAI SCHOOL OF MEDICINE OF CUNY
Description
Abstract Text
The goals are to assess the production, reactions, and detoxification
pathways of hydrogen peroxide and oxy-radicals within the nervous system.
Experiments will concentrate on catecholamine neurons, which provide an
arry of drug-mediated tools that facilitate manipulations in vitro and in
vivo, and anatomical tools that permit the visualization of these neurons
where they exist intermingled with other cell types. For example,
catecholamine levels can be lowered (e.g., alpha-methyl-p-tyrosine) or
raised (e.g., L-dopa), and monoamine neurons can be visualized under the
fluorescence microscope or by electron microscopy. A major tool will be
the investigation of neurotoxins that appear to operate via the formation
of hydrogen peroxide and oxy-radicals. Organotypic cultures of nervous
system will studied; experiments with animals are also planned. We are
particularly interested in the role that monoamine oxidase may play as a
primary generator of hydrogen peroxide within monoamine neurons. Hydrogen
peroxide, in turn, serves as precursor of the highly-reactive hydroxyl
radical.
The immediate research goals are the amplification of experiments that are
already under way. These include: 1) the study of the neurotoxin, MPTP;
2) histochemical evaluation of intracellular levels of GSH (reduced
glutathione) as an index of oxidative stress; and 3) development of
technology to detect the hydroxyl radical within catecholamine neurons.
The long range goals are 1) to apply the new methodology to study other
neurotoxins or other procedures that appear to produce an oxidative stress
in the nervous system (e.g., hyperbaric oxygenation, ischemia, reperfusion
stress) and 2) to evaluate other aspects of GSH metabolism that can provide
an index of oxidative stress (study of GSSG, mixed disulfides, and GSH
adducts with catecholamines). These studies will help to define the role
of peroxides and oxy-radicals in damage to the nervous system.
Public Health Relevance Statement
Data not available.
NIH Spending Category
No NIH Spending Category available.
Project Terms
MAO inhibitorsPongidaecatecholaminesdetoxificationelectron microscopyfluorescence microscopygas chromatography mass spectrometryglutathionehigh performance liquid chromatographyhydrogen peroxidehydroxyl groupimmunochemistrylaboratory ratneuronsneurotoxinsorgan cultureoxidative stressreperfusionsuperoxides
National Institute of Neurological Disorders and Stroke
CFDA Code
DUNS Number
UEI
Project Start Date
01-December-1985
Project End Date
30-November-1993
Budget Start Date
01-December-1991
Budget End Date
30-November-1993
Project Funding Information for 1992
Total Funding
$242,034
Direct Costs
$150,552
Indirect Costs
$91,482
Year
Funding IC
FY Total Cost by IC
1992
National Institute of Neurological Disorders and Stroke
$242,034
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 5R01NS023017-07
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No Publications available for 5R01NS023017-07
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