Abstract

There is compelling evidence that excessive activation of receptors for the excitatory amino acids glutamate and aspartate leads to at least a portion of the neuronal damage seen with brain hypoxia and ischemia (H/I). The experiments in this project will examine certain specific questions related to excitatory amino acid receptors and the pathophysiology and therapy of cerebral H/I in the newborn. First, we will determine the developmental profile of excitotoxic neuronal injury, concentrating specifically on the N-methyl-D-aspartate (NMDA) receptor at different pre- and post-natal ages. We expect that NMDA toxicity is not constant through development and that there may be windows of extreme sensitivity. We will utilize the NMDA agonist cysteine, which freely crosses the placenta and replicates the neurotoxicity of NMDA. We also wish to extend preliminary observations that overactivation of NMDA receptors can cause brain hemorrhage in young animals, suggesting another link between excitotoxicity and neonatal brain damage. Second, we will examine the developmental profile of NMDA antagonist neurotoxicity. Many neurobiologists believe that these drugs may protect the brain from H/I, but are concerned that they also harbor toxic potential. We have preliminary evidence that they are relatively nontoxic in young animals and want to determine the therapeutic window for these drugs more accurately. If we verify the safety of this class of drugs in the newborn, the may have widespread therapeutic use in early treatment of H/I. Third, using new calcium-sensitive fluorescent dyes, we plan to examine the role of excitatory amino acid receptors in controlling the rise in ionized intracellular calcium, and presumably neuronal injury, in hypoxic human brain slices obtained from focal cortical resections. These will be the first experiments to directly test the hypothesis that overactivation of excitatory amino acid receptors plays a role in the pathophysiology of human H/I brain injury.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Exploratory Grants (P20)
Project #
5P20NS032568-02
Application #
3761164
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
2
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Type
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Schechtman, Kenneth B; Gray, Diana L; Baty, Jack D et al. (2002) Decision-making for termination of pregnancies with fetal anomalies: analysis of 53,000 pregnancies. Obstet Gynecol 99:216-22
Almli, C R; Ball, R H; Wheeler, M E (2001) Human fetal and neonatal movement patterns: Gender differences and fetal-to-neonatal continuity. Dev Psychobiol 38:252-73
Werth, J L; Deshmukh, M; Cocabo, J et al. (2000) Reversible physiological alterations in sympathetic neurons deprived of NGF but protected from apoptosis by caspase inhibition or Bax deletion. Exp Neurol 161:203-11
Rothman, S M (1999) Mutations of the mitochondrial genome: clinical overview and possible pathophysiology of cell damage. Biochem Soc Symp 66:111-22
Powers, W J; Rosenbaum, J L; Dence, C S et al. (1998) Cerebral glucose transport and metabolism in preterm human infants. J Cereb Blood Flow Metab 18:632-8
Neil, J J; Shiran, S I; McKinstry, R C et al. (1998) Normal brain in human newborns: apparent diffusion coefficient and diffusion anisotropy measured by using diffusion tensor MR imaging. Radiology 209:57-66
Werth, J L; Park, T S; Silbergeld, D L et al. (1998) Excitotoxic swelling occurs in oxygen and glucose deprived human cortical slices. Brain Res 782:248-54
Handran, S D; Werth, J L; DeVivo, D C et al. (1997) Mitochondrial morphology and intracellular calcium homeostasis in cytochrome oxidase-deficient human fibroblasts. Neurobiol Dis 3:287-98
Hamvas, A; Nogee, L M; Mallory Jr, G B et al. (1997) Lung transplantation for treatment of infants with surfactant protein B deficiency. J Pediatr 130:231-9
Hyrc, K; Handran, S D; Rothman, S M et al. (1997) Ionized intracellular calcium concentration predicts excitotoxic neuronal death: observations with low-affinity fluorescent calcium indicators. J Neurosci 17:6669-77

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