Acute and delayed neuroinflammatory response following experimental penetrating ballistic brain injury in the rat
Open Access
- 2 July 2007
- journal article
- research article
- Published by Springer Nature in Journal of Neuroinflammation
- Vol. 4 (1) , 17
- https://doi.org/10.1186/1742-2094-4-17
Abstract
Background: Neuroinflammation following acute brain trauma is considered to play a prominent role in both the pathological and reconstructive response of the brain to injury. Here we characterize and contrast both an acute and delayed phase of inflammation following experimental penetrating ballistic brain injury (PBBI) in rats out to 7 days post-injury. Methods: Quantitative real time PCR (QRT-PCR) was used to evaluate changes in inflammatory gene expression from the brain tissue of rats exposed to a unilateral frontal PBBI. Brain histopathology was assessed using hematoxylin and eosin (H&E), silver staining, and immunoreactivity for astrocytes (GFAP), microglia (OX-18) and the inflammatory proteins IL-1β and ICAM-1. Results: Time course analysis of gene expression levels using QRT-PCR indicated a peak increase during the acute phase of the injury between 3–6 h for the cytokines TNF-α (8–11 fold), IL-1β (11–13 fold), and IL-6 (40–74 fold) as well as the cellular adhesion molecules VCAM (2–3 fold), ICAM-1 (7–15 fold), and E-selectin (11–13 fold). Consistent with the upregulation of pro-inflammatory genes, peripheral blood cell infiltration was a prominent post-injury event with peak levels of infiltrating neutrophils (24 h) and macrophages (72 h) observed throughout the core lesion. In regions of the forebrain immediately surrounding the lesion, strong immunoreactivity for activated astrocytes (GFAP) was observed as early as 6 h post-injury followed by prominent microglial reactivity (OX-18) at 72 h and resolution of both cell types in cortical brain regions by day 7. Delayed thalamic inflammation (remote from the primary lesion) was also observed as indicated by both microglial and astrocyte reactivity (72 h to 7 days) concomitant with the presence of fiber degeneration (silver staining). Conclusion: In summary, PBBI induces both an acute and delayed neuroinflammatory response occurring in distinct brain regions, which may provide useful diagnostic information for the treatment of this type of brain injury.Keywords
This publication has 45 references indexed in Scilit:
- Purinergic receptors modulate MAP kinases and transcription factors that control microglial inflammatory gene expressionNeurochemistry International, 2006
- Pathophysiological roles of extracellular nucleotides in glial cells: differential expression of purinergic receptors in resting and activated microgliaBrain Research Reviews, 2005
- Astrocytic swelling in cerebral ischemia as a possible cause of injury and target for therapyGlia, 2005
- Astrocyte activation and reactive gliosisGlia, 2005
- Delayed Treatment of Ischemia/Reperfusion Brain InjuryStroke, 2004
- Proteasome Inhibitor PS519 Reduces Infarction and Attenuates Leukocyte Infiltration in a Rat Model of Focal Cerebral IschemiaStroke, 2000
- Drug-Induced Neuroprotection From Global Ischemia Is Associated With Prevention of Persistent but Not Transient Activation of Nuclear Factor-κB in RatsStroke, 1998
- Determination of S-100 and glial fibrillary acidic protein concentrations in cerebrospinal fluid after brain infarction.Stroke, 1991
- Thalamic atrophy following cerebral infarction in the territory of the middle cerebral artery.Stroke, 1991
- Neural damage in the rat thalamus after cortical infarcts.Stroke, 1990