A pharmacological analysis of the neuroprotective efficacy of the brain- and cell-permeable calpain inhibitor MDL-28170 in the mouse controlled cortical impact traumatic brain injury model

The cytoskeletal and neuronal protective effects of early treatment with the blood-brain barrier- and cell-permeable calpain inhibitor MDL-28170 was examined in the controlled cortical impact (CCI) traumatic brain injury (TBI) model in male CF-1 mice. This was preceded by a dose-response and pharmac...

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Veröffentlicht in:	Journal of neurotrauma 2010-12, Vol.27 (12), p.2233-2243
Hauptverfasser:	Thompson, Stephanie N, Carrico, Kimberly M, Mustafa, Ayman G, Bains, Mona, Hall, Edward D
Format:	Artikel
Sprache:	eng
Schlagworte:	Analysis of Variance Animals Blood-Brain Barrier - drug effects Blood-Brain Barrier - metabolism Blood-Brain Barrier - pathology Blotting, Western Brain Brain damage Brain Injuries - drug therapy Brain Injuries - pathology Calpain Calpain - antagonists & inhibitors Cells Cerebral Cortex - drug effects Cerebral Cortex - injuries Cerebral Cortex - metabolism Cerebral Cortex - pathology Cyclosporine Dipeptides - pharmacology Dipeptides - therapeutic use Dosage and administration Dose-Response Relationship, Drug Hippocampus - drug effects Hippocampus - metabolism Hippocampus - pathology Inhibitor drugs Injuries Male Membrane proteins Mice Nerve Degeneration - drug therapy Nerve Degeneration - metabolism Nerve Degeneration - pathology Neurodegeneration Neurons Neurons - drug effects Neurons - metabolism Neurons - pathology Original Properties Rodents Spectrin - metabolism
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container_title	Journal of neurotrauma
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creator	Thompson, Stephanie N Carrico, Kimberly M Mustafa, Ayman G Bains, Mona Hall, Edward D
description	The cytoskeletal and neuronal protective effects of early treatment with the blood-brain barrier- and cell-permeable calpain inhibitor MDL-28170 was examined in the controlled cortical impact (CCI) traumatic brain injury (TBI) model in male CF-1 mice. This was preceded by a dose-response and pharmacodynamic evaluation of IV or IP doses of MDL-28170 with regard to ex vivo inhibition of calpain 2 activity in harvested brain homogenates. From these data, we tested the effects of an optimized MDL-28170 dosing regimen on calpain-mediated degradation of the neuronal cytoskeletal protein α-spectrin in cortical or hippocampal tissue of mice 24 h after CCI-TBI (1.0 mm depth, 3.5 m/sec velocity). With treatment initiated at 15 min post-TBI, α-spectrin degradation was significantly reduced by 40% in hippocampus and 44% in cortex. This effect was still observed with a 1-h but not a 3-h post-TBI delay. The cytoskeletal protection is most likely taking place in neurons surrounding the area of mainly necrotic degeneration, since MDL-28170 did not reduce hemispheric lesion volume as measured by the aminocupric silver staining method. This lack of effect on lesion volume has been seen with other calpain inhibitors, which suggests that pharmacological calpain inhibition by itself, while able to reduce axonal injury, may not be able to produce a measurable reduction in lesion volume. This is in contrast to certain other neuroprotective mechanistic approaches such as the mitochondrial protectant cyclosporine A, which produces at least a partial decrease in lesion volume in the same model. Accordingly, the combination of a calpain inhibitor with a compound such as cyclosporine A may be needed to achieve the optimal degree of post-TBI neuroprotection.
doi_str_mv	10.1089/neu.2010.1474
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This lack of effect on lesion volume has been seen with other calpain inhibitors, which suggests that pharmacological calpain inhibition by itself, while able to reduce axonal injury, may not be able to produce a measurable reduction in lesion volume. This is in contrast to certain other neuroprotective mechanistic approaches such as the mitochondrial protectant cyclosporine A, which produces at least a partial decrease in lesion volume in the same model. 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This was preceded by a dose-response and pharmacodynamic evaluation of IV or IP doses of MDL-28170 with regard to ex vivo inhibition of calpain 2 activity in harvested brain homogenates. From these data, we tested the effects of an optimized MDL-28170 dosing regimen on calpain-mediated degradation of the neuronal cytoskeletal protein α-spectrin in cortical or hippocampal tissue of mice 24 h after CCI-TBI (1.0 mm depth, 3.5 m/sec velocity). With treatment initiated at 15 min post-TBI, α-spectrin degradation was significantly reduced by 40% in hippocampus and 44% in cortex. This effect was still observed with a 1-h but not a 3-h post-TBI delay. The cytoskeletal protection is most likely taking place in neurons surrounding the area of mainly necrotic degeneration, since MDL-28170 did not reduce hemispheric lesion volume as measured by the aminocupric silver staining method. This lack of effect on lesion volume has been seen with other calpain inhibitors, which suggests that pharmacological calpain inhibition by itself, while able to reduce axonal injury, may not be able to produce a measurable reduction in lesion volume. This is in contrast to certain other neuroprotective mechanistic approaches such as the mitochondrial protectant cyclosporine A, which produces at least a partial decrease in lesion volume in the same model. Accordingly, the combination of a calpain inhibitor with a compound such as cyclosporine A may be needed to achieve the optimal degree of post-TBI neuroprotection.</description><subject>Analysis of Variance</subject><subject>Animals</subject><subject>Blood-Brain Barrier - drug effects</subject><subject>Blood-Brain Barrier - metabolism</subject><subject>Blood-Brain Barrier - pathology</subject><subject>Blotting, Western</subject><subject>Brain</subject><subject>Brain damage</subject><subject>Brain Injuries - drug therapy</subject><subject>Brain Injuries - pathology</subject><subject>Calpain</subject><subject>Calpain - antagonists & inhibitors</subject><subject>Cells</subject><subject>Cerebral Cortex - drug effects</subject><subject>Cerebral Cortex - injuries</subject><subject>Cerebral Cortex - metabolism</subject><subject>Cerebral Cortex - pathology</subject><subject>Cyclosporine</subject><subject>Dipeptides - pharmacology</subject><subject>Dipeptides - therapeutic use</subject><subject>Dosage and administration</subject><subject>Dose-Response Relationship, Drug</subject><subject>Hippocampus - 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This was preceded by a dose-response and pharmacodynamic evaluation of IV or IP doses of MDL-28170 with regard to ex vivo inhibition of calpain 2 activity in harvested brain homogenates. From these data, we tested the effects of an optimized MDL-28170 dosing regimen on calpain-mediated degradation of the neuronal cytoskeletal protein α-spectrin in cortical or hippocampal tissue of mice 24 h after CCI-TBI (1.0 mm depth, 3.5 m/sec velocity). With treatment initiated at 15 min post-TBI, α-spectrin degradation was significantly reduced by 40% in hippocampus and 44% in cortex. This effect was still observed with a 1-h but not a 3-h post-TBI delay. The cytoskeletal protection is most likely taking place in neurons surrounding the area of mainly necrotic degeneration, since MDL-28170 did not reduce hemispheric lesion volume as measured by the aminocupric silver staining method. This lack of effect on lesion volume has been seen with other calpain inhibitors, which suggests that pharmacological calpain inhibition by itself, while able to reduce axonal injury, may not be able to produce a measurable reduction in lesion volume. This is in contrast to certain other neuroprotective mechanistic approaches such as the mitochondrial protectant cyclosporine A, which produces at least a partial decrease in lesion volume in the same model. Accordingly, the combination of a calpain inhibitor with a compound such as cyclosporine A may be needed to achieve the optimal degree of post-TBI neuroprotection.</abstract><cop>United States</cop><pub>Mary Ann Liebert, Inc</pub><pmid>20874056</pmid><doi>10.1089/neu.2010.1474</doi><tpages>11</tpages><oa>free_for_read</oa></addata></record>
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subjects	Analysis of Variance Animals Blood-Brain Barrier - drug effects Blood-Brain Barrier - metabolism Blood-Brain Barrier - pathology Blotting, Western Brain Brain damage Brain Injuries - drug therapy Brain Injuries - pathology Calpain Calpain - antagonists & inhibitors Cells Cerebral Cortex - drug effects Cerebral Cortex - injuries Cerebral Cortex - metabolism Cerebral Cortex - pathology Cyclosporine Dipeptides - pharmacology Dipeptides - therapeutic use Dosage and administration Dose-Response Relationship, Drug Hippocampus - drug effects Hippocampus - metabolism Hippocampus - pathology Inhibitor drugs Injuries Male Membrane proteins Mice Nerve Degeneration - drug therapy Nerve Degeneration - metabolism Nerve Degeneration - pathology Neurodegeneration Neurons Neurons - drug effects Neurons - metabolism Neurons - pathology Original Properties Rodents Spectrin - metabolism
title	A pharmacological analysis of the neuroprotective efficacy of the brain- and cell-permeable calpain inhibitor MDL-28170 in the mouse controlled cortical impact traumatic brain injury model
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