Traumatic brain injury‐induced excitotoxicity assessed in a controlled cortical impact model

AM Palmer, DW Marion, ML Botscheller… - Journal of …, 1993 - Wiley Online Library
AM Palmer, DW Marion, ML Botscheller, PE Swedlow, SD Styren, ST DeKosky
Journal of neurochemistry, 1993Wiley Online Library
Using a controlled cortical impact model of traumatic brain injury (TBI) coupled with tissue
microdialysis, interstitial concentrations of aspartate and glutamate (together with serine and
glutamine) were assessed in rat frontal cortex. Histological analysis indicated that the
severity of injury following severe TBI (depth of deformation= 3.5 mm) was approximately
twice that occurring following moderate TBI (depth of deformation= 1.5 mm). Both groups
demonstrated significant postinjury maximal increases in excitatory amino acid (EAA) …
Abstract
Using a controlled cortical impact model of traumatic brain injury (TBI) coupled with tissue microdialysis, interstitial concentrations of aspartate and glutamate (together with serine and glutamine) were assessed in rat frontal cortex. Histological analysis indicated that the severity of injury following severe TBI (depth of deformation = 3.5 mm) was approximately twice that occurring following moderate TBI (depth of deformation = 1.5 mm). Both groups demonstrated significant postinjury maximal increases in excitatory amino acid (EAA) concentration, which were proportional to the severity of injury. The mean ± SEM fold increase in dialysate concentrations of aspartate was 38 ± 13 (n = 5) for moderate TBI and 74 ± 12 (n = 5) for severe TBI. Fold increases in glutamate concentrations were 81 ± 26 and 144 ± 23 for moderate and severe TBI, respectively. Although these increases normalized within 20–30 min following moderate TBI, concentrations of aspartate and glutamate took >60 min to normalize after severe TBI. Changes in levels of nontransmitter amino acids were much smaller. Fold increases for serine concentrations were 4.6 ± 0.6 and 7.6 ± 1.7 in moderate and severe TBI, respectively; glutamine concentrations had similar small fold increases (2.6 ± 0.2 and 4.1 ± 0.6, respectively). Calculation of interstitial concentrations following severe TBI indicated that aspartate and glutamate maximally increased to 123 ± 20 and 414 ± 66 μM, respectively. To determine the extent to which such tissue concentrations of EAAs could contribute to the injury seen in TBI, the EAA receptor agonists N‐methyl‐d‐ aspartate and α‐amino‐3‐hydroxy‐5‐methyl‐4‐isoxazolepropionic acid were slowly injected into rat cortex. Remarkably similar histological injuries were produced by this procedure, supporting the notion that TBI is an excitotoxic injury.
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