Acute minocycline treatment mitigates the symptoms of mild blast-induced traumatic brain injury

Erzsebet Kovesdi; Alaa Kamnaksh; Daniel Wingo; Farid Ahmed; Neil E. Grunberg; Joseph B. Long; Christine E. Kasper; Denes V. Agoston

doi:10.3389/fneur.2012.00111

Acute minocycline treatment mitigates the symptoms of mild blast-induced traumatic brain injury

Erzsebet Kovesdi, Alaa Kamnaksh, Daniel Wingo, Farid Ahmed, Neil E. Grunberg, Joseph B. Long, Christine E. Kasper, Denes V. Agoston^*

^*Corresponding author for this work

Anatomy, Physiology, and Genetics

Research output: Contribution to journal › Article › peer-review

131 Scopus citations

Abstract

Mild traumatic brain injury (mTBI) represents a significant challenge for the civilian and military health care systems due to its high prevalence and overall complexity. Our earlier works showed evidence of neuroinflammation, a late onset of neurobehavioral changes, and lasting memory impairment in a rat model of mild blast-inducedTBI (mbTBI).The aim of our present study was to determine whether acute treatment with the non-steroidal antiinflammatory drug minocycline (Minocin®) can mitigate the neurobehavioral abnormalities associated with mbTBI, Furthermore, we aimed to assess the effects of the treatment on select inflammatory, vascular, neuronal, and glial markers in sera and in brain regions associated with anxiety and memory (amygdala, prefrontal cortex, ventral, and dorsal hippocampus) following the termination (51 days post-injury) of the experiment. Four hours after a single exposure to mild blast overpressure or sham conditions, we treated animals with a daily dose of minocycline (50 mg/kg) or physiological saline (vehicle) for four consecutive days. At 8 and 45 days post-injury, we tested animals for locomotion, anxiety, and spatial memory. Injured animals exhibited significantly impaired memory and increased anxiety especially at the later testing time point. Conversely, injured and minocycline treated rats' performance was practically identical to control (sham) animals in the open field, elevated plus maze, and Barnes maze. Protein analyses of sera and brain regions showed significantly elevated levels of all of the measured biomarkers (except VEGF) in injured and untreated rats. Importantly, minocycline treatment normalized serum and tissue levels of the majority of the selected inflammatory, vascular, neuronal, and glial markers. In summary, acute minocycline treatment appears to prevent the development of neurobehavioral abnormalities likely through mitigating the molecular pathologies of the injury in an experimental model of mbTBI.

Original language	English
Article number	Article 111
Journal	Frontiers in Neurology
Volume	JUL
DOIs	https://doi.org/10.3389/fneur.2012.00111
State	Published - 2012

Keywords

Anti-inflammatory
Neurobehavior
Proteomics
Tbi
Treatment

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10.3389/fneur.2012.00111

Cite this

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title = "Acute minocycline treatment mitigates the symptoms of mild blast-induced traumatic brain injury",

abstract = "Mild traumatic brain injury (mTBI) represents a significant challenge for the civilian and military health care systems due to its high prevalence and overall complexity. Our earlier works showed evidence of neuroinflammation, a late onset of neurobehavioral changes, and lasting memory impairment in a rat model of mild blast-inducedTBI (mbTBI).The aim of our present study was to determine whether acute treatment with the non-steroidal antiinflammatory drug minocycline (Minocin{\textregistered}) can mitigate the neurobehavioral abnormalities associated with mbTBI, Furthermore, we aimed to assess the effects of the treatment on select inflammatory, vascular, neuronal, and glial markers in sera and in brain regions associated with anxiety and memory (amygdala, prefrontal cortex, ventral, and dorsal hippocampus) following the termination (51 days post-injury) of the experiment. Four hours after a single exposure to mild blast overpressure or sham conditions, we treated animals with a daily dose of minocycline (50 mg/kg) or physiological saline (vehicle) for four consecutive days. At 8 and 45 days post-injury, we tested animals for locomotion, anxiety, and spatial memory. Injured animals exhibited significantly impaired memory and increased anxiety especially at the later testing time point. Conversely, injured and minocycline treated rats' performance was practically identical to control (sham) animals in the open field, elevated plus maze, and Barnes maze. Protein analyses of sera and brain regions showed significantly elevated levels of all of the measured biomarkers (except VEGF) in injured and untreated rats. Importantly, minocycline treatment normalized serum and tissue levels of the majority of the selected inflammatory, vascular, neuronal, and glial markers. In summary, acute minocycline treatment appears to prevent the development of neurobehavioral abnormalities likely through mitigating the molecular pathologies of the injury in an experimental model of mbTBI.",

keywords = "Anti-inflammatory, Neurobehavior, Proteomics, Tbi, Treatment",

author = "Erzsebet Kovesdi and Alaa Kamnaksh and Daniel Wingo and Farid Ahmed and Grunberg, {Neil E.} and Long, {Joseph B.} and Kasper, {Christine E.} and Agoston, {Denes V.}",

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T1 - Acute minocycline treatment mitigates the symptoms of mild blast-induced traumatic brain injury

AU - Kovesdi, Erzsebet

AU - Kamnaksh, Alaa

AU - Wingo, Daniel

AU - Ahmed, Farid

AU - Grunberg, Neil E.

AU - Long, Joseph B.

AU - Kasper, Christine E.

AU - Agoston, Denes V.

PY - 2012

Y1 - 2012

N2 - Mild traumatic brain injury (mTBI) represents a significant challenge for the civilian and military health care systems due to its high prevalence and overall complexity. Our earlier works showed evidence of neuroinflammation, a late onset of neurobehavioral changes, and lasting memory impairment in a rat model of mild blast-inducedTBI (mbTBI).The aim of our present study was to determine whether acute treatment with the non-steroidal antiinflammatory drug minocycline (Minocin®) can mitigate the neurobehavioral abnormalities associated with mbTBI, Furthermore, we aimed to assess the effects of the treatment on select inflammatory, vascular, neuronal, and glial markers in sera and in brain regions associated with anxiety and memory (amygdala, prefrontal cortex, ventral, and dorsal hippocampus) following the termination (51 days post-injury) of the experiment. Four hours after a single exposure to mild blast overpressure or sham conditions, we treated animals with a daily dose of minocycline (50 mg/kg) or physiological saline (vehicle) for four consecutive days. At 8 and 45 days post-injury, we tested animals for locomotion, anxiety, and spatial memory. Injured animals exhibited significantly impaired memory and increased anxiety especially at the later testing time point. Conversely, injured and minocycline treated rats' performance was practically identical to control (sham) animals in the open field, elevated plus maze, and Barnes maze. Protein analyses of sera and brain regions showed significantly elevated levels of all of the measured biomarkers (except VEGF) in injured and untreated rats. Importantly, minocycline treatment normalized serum and tissue levels of the majority of the selected inflammatory, vascular, neuronal, and glial markers. In summary, acute minocycline treatment appears to prevent the development of neurobehavioral abnormalities likely through mitigating the molecular pathologies of the injury in an experimental model of mbTBI.

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