Abstract

Cardiac arrest and stroke are two of the leading causes of mortality. An estimated 1.25 million people suffer heart attacks annually and nearly 500,000 of these die. 500,000 individuals will have strokes and roughly 30% of these will die. In both instances, many of the survivors will be severely and permanently disabled as a result of injury to their central nervous systems. To date there have been no clinically effective pharmacologic tools for amelioration of brain damage arising from a stroke or cardiac arrest. Ischemia results in a massive release of the excitotoxic amino acids, glutamate and aspartate, into the extracellular environmental of the brain, precipitating an influx of calcium into cells. Intracellular calcium in turn activates various calcium-dependent enzymes, including nucleases, proteases and phospholipases, resulting in a chain of events, including lipolysis, during ischemia, and free fatty acid metabolism and generation of superoxide radicals during reperfusion. Free radicals can initiate a chain reaction of lipid peroxidation, with extensive destruction of plasma and mitochondrial membranes and failure of cellular homeostasis and metabolism. To reduce the neurologic morbidity associated with resuscitation int cardiac arrest or stroke, it will be necessary to understand the molecular mechanisms underlying reperfusion injury with delayed neuronal death. A rat four vessel occlusion (o) model of cerebral ischemia/reperfusion will be used to assess the degree of o injury as revealed by the rate of glutamate, aspartate, gamma-aminobutyric acid, adenosine and inosine efflux into the interstitial spaces of the rat cerebral cortex. The role of phospholipases in the release of these substances will be assessed with the use of specific inhibitors of these enzymes, and of the protein kinases which activate phospholipase. Further evidence of phospholipase activation will be sought by applying these enzymes directly onto the cerebral cortex and measuring amino acid and purine release. An involvement of free radicals in amino acid and purine efflux during ischemia/reperfusion will be assessed by preventing free radical action with inhibitors of the enzymes responsible for their formation or by the artificial generation of free radicals in the cerebral cortex. A chronic rat 4VO model will be used to evaluate the ability of phospholipase inhibitors to prevent ischemia/reperfusion injuries, manifested as neurological disabilities and hippocampal CA1 pyramidal cell injury. Overall, these experiments should provide definitive evidence on the molecular mechanisms responsible for neuronal injury and death,a with significant implications for the development of novel therapeutic approaches to the prevention and treatment of ischemia/reperfusion induced brain damage.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS026912-07A1
Application #
2266195
Study Section
Neurology B Subcommittee 2 (NEUB)
Project Start
1988-12-01
Project End
1999-04-30
Budget Start
1995-07-15
Budget End
1996-04-30
Support Year
7
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Wayne State University
Department
Physiology
Type
Schools of Medicine
DUNS #
City
Detroit
State
MI
Country
United States
Zip Code
48202

  Publications

Phillis, John W; O'Regan, Michael H (2003) Studies on taurine efflux from the rat cerebral cortex during exposure to hyposmotic, high K+ and ouabain-containing aCSF. Adv Exp Med Biol 526:433-44
Phillis, John W; O'Regan, Michael H (2002) Energy utilization in the ischemic/reperfused brain. Int Rev Neurobiol 51:377-414
Phillis, J W; Ren, J; O'Regan, M H (2001) Studies on the effects of lactate transport inhibition, pyruvate, glucose and glutamine on amino acid, lactate and glucose release from the ischemic rat cerebral cortex. J Neurochem 76:247-57
Guyot, L L; Diaz, F G; O'Regan, M H et al. (2001) Real-time measurement of glutamate release from the ischemic penumbra of the rat cerebral cortex using a focal middle cerebral artery occlusion model. Neurosci Lett 299:37-40
Guyot, L L; Diaz, F G; O'Regan, M H et al. (2001) The effect of streptozotocin-induced diabetes on the release of excitotoxic and other amino acids from the ischemic rat cerebral cortex. Neurosurgery 48:385-90; discussion 390-1
Estevez, A Y; Song, D; Phillis, J W et al. (2000) Effects of the anion channel blocker DIDS on ouabain- and high K(+)-induced release of amino acids from the rat cerebral cortex. Brain Res Bull 52:45-50
Guyot, L L; Diaz, F G; O'Regan, M H et al. (2000) Topical glucose and accumulation of excitotoxic and other amino acids in ischemic cerebral cortex. Horm Metab Res 32:9-Jun
Phillis, J W; Ren, J; O'Regan, M H (2000) Transporter reversal as a mechanism of glutamate release from the ischemic rat cerebral cortex: studies with DL-threo-beta-benzyloxyaspartate. Brain Res 868:105-12
Guyot, L L; Diaz, F G; O'Regan, M H et al. (2000) Topical insulin and accumulation of excitotoxic and other amino acids in ischemic rat cerebral cortex. Proc Soc Exp Biol Med 224:28-31
Guyot, L L; Diaz, F G; O'Regan, M H et al. (2000) The effect of intravenous insulin on accumulation of excitotoxic and other amino acids in the ischemic rat cerebral cortex. Neurosci Lett 288:61-5

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