Transcriptomics of Traumatic Brain Injury: Gene Expression and Molecular Pathways of Different Grades of Insult in a Rat Organotypic Hippocampal Culture Model
Transcriptomics of Traumatic Brain Injury: Gene Expression and Molecular Pathways of Different Grades of Insult in a Rat Organotypic Hippocampal Culture Model
Traumatic brain injury (TBI) is the one of the most common forms of head trauma, and it remains a leading cause of death and disability. It is known that the initial mechanical axonal injury triggers a complex cascade of neuroinflammatory and metabolic events, the understanding of which is essential for clinical, translational, and pharmacological research. These can occur even in mild TBI, and are associated with several post-concussion manifestations, including transiently heightened vulnerability to a second insult. Recent studies have challenged the tenet that ischemia is the ultimate modality of tissue damage following TBI, as metabolic dysfunction can develop in the presence of normal perfusion and before intracranial hypertension. In order to elucidate the cellular and molecular changes occurring in TBI as a direct result of neuronal injury and in the absence of ischemic damage, we performed a microarray analysis of expressed genes and molecular interaction pathways for different levels of severity of trauma using an in-vitro model. A stretch injury, equivalent to human diffuse axonal injury, was delivered to rat organotypic hippocampal slice cultures, and mRNA levels following a 10% (mild) and 50% (severe) stretch were compared with controls at 24 h. More genes were differentially expressed following 10% stretch than 50% stretch, indicating the early activation of complex cellular mechanisms. The data revealed remarkable differential gene expression following mTBI, even in the absence of cell damage. Pathway analysis revealed that molecular interactions in both levels of injury were similar, with IL-1beta playing a central role. Additional pathways of neurodegeneration involving RhoA (ras homolog gene family, member A) were found in 50% stretch.
349-359
Di Pietro, Valentina
52a26fb6-7579-4cdc-aee6-26cb6e9ff175
Amin, Daven
330dd55d-7d4f-44e0-902c-8b9f3e1dbba1
Pernagallo, Salvatore
513cfbf4-68d8-4b82-9411-15171fd5197a
Lazzarino, Giuseppe
2344efe0-43bc-4781-9f72-451f3d7f407d
Tavazzi, Barbara
22416dea-27d4-496d-8104-803bc0b0f13c
Vagnozzi, Roberto
3c1c46f7-9a64-459e-82cd-50cf9ee73a2e
Pringle, Ashley
6339ed95-c491-43a8-b2fb-2384466dc80d
Belli, Antonio
33707b7b-b004-4245-aead-98a8e1e2b2e2
19 February 2010
Di Pietro, Valentina
52a26fb6-7579-4cdc-aee6-26cb6e9ff175
Amin, Daven
330dd55d-7d4f-44e0-902c-8b9f3e1dbba1
Pernagallo, Salvatore
513cfbf4-68d8-4b82-9411-15171fd5197a
Lazzarino, Giuseppe
2344efe0-43bc-4781-9f72-451f3d7f407d
Tavazzi, Barbara
22416dea-27d4-496d-8104-803bc0b0f13c
Vagnozzi, Roberto
3c1c46f7-9a64-459e-82cd-50cf9ee73a2e
Pringle, Ashley
6339ed95-c491-43a8-b2fb-2384466dc80d
Belli, Antonio
33707b7b-b004-4245-aead-98a8e1e2b2e2
Di Pietro, Valentina, Amin, Daven, Pernagallo, Salvatore, Lazzarino, Giuseppe, Tavazzi, Barbara, Vagnozzi, Roberto, Pringle, Ashley and Belli, Antonio
(2010)
Transcriptomics of Traumatic Brain Injury: Gene Expression and Molecular Pathways of Different Grades of Insult in a Rat Organotypic Hippocampal Culture Model.
Journal of Neurotrauma, 27 (2), .
(doi:10.1089/neu.2009.1095).
Abstract
Traumatic brain injury (TBI) is the one of the most common forms of head trauma, and it remains a leading cause of death and disability. It is known that the initial mechanical axonal injury triggers a complex cascade of neuroinflammatory and metabolic events, the understanding of which is essential for clinical, translational, and pharmacological research. These can occur even in mild TBI, and are associated with several post-concussion manifestations, including transiently heightened vulnerability to a second insult. Recent studies have challenged the tenet that ischemia is the ultimate modality of tissue damage following TBI, as metabolic dysfunction can develop in the presence of normal perfusion and before intracranial hypertension. In order to elucidate the cellular and molecular changes occurring in TBI as a direct result of neuronal injury and in the absence of ischemic damage, we performed a microarray analysis of expressed genes and molecular interaction pathways for different levels of severity of trauma using an in-vitro model. A stretch injury, equivalent to human diffuse axonal injury, was delivered to rat organotypic hippocampal slice cultures, and mRNA levels following a 10% (mild) and 50% (severe) stretch were compared with controls at 24 h. More genes were differentially expressed following 10% stretch than 50% stretch, indicating the early activation of complex cellular mechanisms. The data revealed remarkable differential gene expression following mTBI, even in the absence of cell damage. Pathway analysis revealed that molecular interactions in both levels of injury were similar, with IL-1beta playing a central role. Additional pathways of neurodegeneration involving RhoA (ras homolog gene family, member A) were found in 50% stretch.
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Published date: 19 February 2010
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Local EPrints ID: 73600
URI: http://eprints.soton.ac.uk/id/eprint/73600
ISSN: 0897-7151
PURE UUID: fee0eff3-77e0-46b1-8810-51022e3c94b9
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Date deposited: 09 Mar 2010
Last modified: 14 Mar 2024 02:38
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Author:
Valentina Di Pietro
Author:
Daven Amin
Author:
Salvatore Pernagallo
Author:
Giuseppe Lazzarino
Author:
Barbara Tavazzi
Author:
Roberto Vagnozzi
Author:
Antonio Belli
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