Blood-Related Toxicity after Traumatic Brain Injury: Potential Targets for Neuroprotection

Emergency visits, hospitalizations, and deaths due to traumatic brain injury (TBI) have increased significantly over the past few decades. While the primary early brain trauma is highly deleterious to the brain, the secondary injury post-TBI is postulated to significantly impact mortality. The prese...

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Published inMolecular neurobiology Vol. 57; no. 1; pp. 159 - 178
Main Authors Robicsek, Steven A., Bhattacharya, Ayon, Rabai, Ferenc, Shukla, Krunal, Doré, Sylvain
Format Journal Article
LanguageEnglish
Published New York Springer US 01.01.2020
Springer Nature B.V
Subjects
Biomedical and Life Sciences
Biomedicine
Blood
Cell Biology
Cell death
Edema
Ferritin
Haptoglobin
Heme
Hemin
Hemoglobin
Hemopexin
Immune clearance
Immune response
Inflammation
Lipid peroxidation
Metabolites
Morbidity
Mortality
Neurobiology
Neurology
Neuroprotection
Neurosciences
Oxidants
Oxygenase
Pain perception
Reactive oxygen species
Therapeutic applications
Toxicity
Traumatic brain injury
Hemopexin
CD163
Iron
CD36
LRP1
Ferritin
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Summary:Emergency visits, hospitalizations, and deaths due to traumatic brain injury (TBI) have increased significantly over the past few decades. While the primary early brain trauma is highly deleterious to the brain, the secondary injury post-TBI is postulated to significantly impact mortality. The presence of blood, particularly hemoglobin, and its breakdown products and key binding proteins and receptors modulating their clearance may contribute significantly to toxicity. Heme, hemin, and iron, for example, cause membrane lipid peroxidation, generate reactive oxygen species, and sensitize cells to noxious stimuli resulting in edema, cell death, and increased morbidity and mortality. A wide range of other mechanisms such as the immune system play pivotal roles in mediating secondary injury. Effective scavenging of all of these pro-oxidant and pro-inflammatory metabolites as well as controlling maladaptive immune responses is essential for limiting toxicity and secondary injury. Hemoglobin metabolism is mediated by key molecules such as haptoglobin, heme oxygenase, hemopexin, and ferritin. Genetic variability and dysfunction affecting these pathways (e.g., haptoglobin and heme oxygenase expression) have been implicated in the difference in susceptibility of individual patients to toxicity and may be target pathways for potential therapeutic interventions in TBI. Ongoing collaborative efforts are required to decipher the complexities of blood-related toxicity in TBI with an overarching goal of providing effective treatment options to all patients with TBI.
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ISSN:0893-7648
1559-1182
1559-1182
DOI:10.1007/s12035-019-01766-8