Abstract

The central event after traumatic brain injury (TI) is the transient, or ongoing impairment of electrophysiological function, manifest as coma, """"""""concussion"""""""" or neurological deficit. Persistent reduction in the Resting Membrane Potential, and consequent failure to adequately re-polarize neuronal and axonal membranes, are the most likely mechanisms for eliciting these effects. This application revolves around the central hypothesis that mitochondrial dysfunction and reduced ionic pumping, leading bioenergetic failure, is the major limiting factor, determining neuronal and axonal recovery after TBI. In this application, we build upon our previous studies, demonstrating massive excitatory neurotransmitter release after TBI, leading to calcium influx. This in turn damages mitochondria, neurofilaments, and second-messenger mediated ion channels, among many other events. These issues will be explored in the clinic and laboratory settings. Specifically, in rat TBI models, we will use immunohistochemistry, molecular biology, electrophysiology, and behavioral testing to validate the hypothesis that calcium-mediated damage to inhibitory GABA Cl channels exacerbates neuronal damage, and thus worsens outcomes, and that GABA agonists improve outcome. We will directly measure cytochrome oxidase activity, to show that mitochondria are functionally impaired after TBI, and we will posit that specific blockade of the Mitochondria Transition Pore (MPT) with Cyclosporin A, will prevent these changes, and improve outcome. In severely head injured patients, simultaneous microdialysis, and a new coaxial depth electrode, together with a tissue oxygen/CO2/pH sensor system, will be placed in the same brain region to test the effect of increased oxygen tension, and Cyclosporin A under the interplay of neurochemical and neurophysiological events. We will use AVDO2, AVD lactate, and AVD glucose to assess global therapy effects, and relate them to CBF and MRI parameters. Finally, we will use MRI water mapping, Diffusion Weighted Imaging, and CBF mapping, to show that the brain swelling, which almost always follows TBI is due to cytotoxic edema. These methods will also test the hypothesis that Cyclosporin A will ameliorate cytotoxic edema, and that N Acetyl Aspartate spectroscopy will constitute a """"""""surrogate marker"""""""" for mitochondrialy, and neuronal damage in human TBI. Thus, these novel techniques, through a tightly integrated set of laboratory and clinical studies, will yield new mechanistic insights, and specifically evaluate Cyclosporin A and several other putative new therapies in TBI.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Specialized Center (P50)
Project #
5P50NS012587-25
Application #
6393283
Study Section
National Institute of Neurological Disorders and Stroke Initial Review Group (NSD)
Program Officer
Michel, Mary E
Project Start
1979-04-01
Project End
2005-08-31
Budget Start
2001-09-01
Budget End
2002-08-31
Support Year
25
Fiscal Year
2001
Total Cost
$1,260,320
Indirect Cost

  Institution

Name
Virginia Commonwealth University
Department
Neurosurgery
Type
Schools of Medicine
DUNS #
City
Richmond
State
VA
Country
United States
Zip Code
23298

  Publications

Kleindienst, Andrea; Dunbar, Jana G; Glisson, Renee et al. (2013) The role of vasopressin V1A receptors in cytotoxic brain edema formation following brain injury. Acta Neurochir (Wien) 155:151-64
Brophy, Gretchen M; Mazzeo, Anna Teresa; Brar, Satjit et al. (2013) Exposure of cyclosporin A in whole blood, cerebral spinal fluid, and brain extracellular fluid dialysate in adults with traumatic brain injury. J Neurotrauma 30:1484-9
Prieto, Ruth; Tavazzi, Barbara; Taya, Keisuke et al. (2011) Brain energy depletion in a rodent model of diffuse traumatic brain injury is not prevented with administration of sodium lactate. Brain Res 1404:39-49
Fazzina, Giovanna; Amorini, Angela M; Marmarou, Christina R et al. (2010) The protein kinase C activator phorbol myristate acetate decreases brain edema by aquaporin 4 downregulation after middle cerebral artery occlusion in the rat. J Neurotrauma 27:453-61
Mazzeo, Anna Teresa; Brophy, Gretchen M; Gilman, Charlotte B et al. (2009) Safety and tolerability of cyclosporin a in severe traumatic brain injury patients: results from a prospective randomized trial. J Neurotrauma 26:2195-206
Fabricius, Martin; Fuhr, Susanne; Willumsen, Lisette et al. (2008) Association of seizures with cortical spreading depression and peri-infarct depolarisations in the acutely injured human brain. Clin Neurophysiol 119:1973-84
Mazzeo, Anna Teresa; Alves, Oscar Luis; Gilman, Charlotte B et al. (2008) Brain metabolic and hemodynamic effects of cyclosporin A after human severe traumatic brain injury: a microdialysis study. Acta Neurochir (Wien) 150:1019-31;discussion 1031
Lu, J; Marmarou, A; Choi, S et al. (2005) Mortality from traumatic brain injury. Acta Neurochir Suppl 95:281-5
Tavazzi, Barbara; Signoretti, Stefano; Lazzarino, Giuseppe et al. (2005) Cerebral oxidative stress and depression of energy metabolism correlate with severity of diffuse brain injury in rats. Neurosurgery 56:582-9; discussion 582-9
Signoretti, Stefano; Marmarou, Anthony; Tavazzi, Barbara et al. (2004) The protective effect of cyclosporin A upon N-acetylaspartate and mitochondrial dysfunction following experimental diffuse traumatic brain injury. J Neurotrauma 21:1154-67

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