Development of status epilepticus, sustained calcium elevations and neuronal injury in a rat survival model of lethal paraoxon intoxication

Deshpande, Laxmikant S.; Carter, Dawn S.; Phillips, Kristin F.; Blair, Robert E.; DeLorenzo, Robert J.

doi:10.1016/j.neuro.2014.04.006

Cited by 49 publications

(84 citation statements)

References 39 publications

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“…If toxicity developed, antidotal therapy was initiated with SC atropine (2 mg/kg in 0.40-0.45 ml) and SC pralidoxime (25 mg/kg in 0.20-0.30 ml) and repeated as needed. Doses chosen were the same used in other studies of OP intoxication [20] and also replicated those used in our prior study [6]. Twenty-four hours later, the rats that received DFP were then randomized to the DFPnaltrexone group to receive SC naltrexone (5 mg/kg/day in 0.2-0.3 ml; N=9) for 12 weeks, or the DFP-saline group to receive an equal volume of SC saline for the same time period (N=8).…”

Section: Methodsmentioning

confidence: 99%

Chronic Treatment with Naltrexone Prevents Memory Retention Deficits in Rats Poisoned with the Sarin Analog Diisopropylfluorophosphate (DFP) and Treated with Atropine and Pralidoxime

2015

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Humans and rats poisoned with sarin develop chronic neurological disabilities that are not prevented with standardized antidotal therapy. We hypothesized that rats poisoned with the sarin analogue diisopropylfluorophosphate (DFP) and resuscitated with atropine and pralidoxime would have long-term memory deficits that were preventable with naltrexone treatment. Long Evans rats (250-275 g) were randomized to: DFP (N=8): single subcutaneous (SC) injection of DFP (5 mg/kg). Treatment (N=9): DFP (5 mg/kg) followed by chronic naltrexone (5 mg/kg/day × 12 weeks). Control (N= 12): single SC injection of isopropyl alcohol, (DFP vehicle) followed by chronic naltrexone (5 mg/kg/day). If toxicity developed after injection, antidotal therapy was initiated with atropine (2 mg/kg) and pralidoxime (25 mg/kg) and repeated as needed. After 12 weeks, rats underwent testing for place learning (acquisition) across 5 days of training using the Morris Water Maze. On day 6 a memory retention test was performed. Statistical analysis was performed using IBM SPSS Statistics. Rats receiving DFP rapidly developed toxicity requiring antidotal rescue. No differences in acquisition were seen between the DFP vs. DFP+naltrexone rats. During memory testing, DFP-poisoned rats spent significantly less time (29.4±2.11 versus 38.5±2.5 s, p<0.05) and traveled less distance (267±24.6 versus 370±27.5 cm, p<0.05) in the target quadrant compared to the treatment group. Treatment rats performed as well as control rats (p>0.05) on the test for memory retention. Poisoning with DFP induced impaired memory retention. Deficits were not prevented by acute rescue with atropine and pralidoxime. Chronic naltrexone treatment led to preserved memory after DFP poisoning.

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Section: Methodsmentioning

confidence: 99%

Chronic Treatment with Naltrexone Prevents Memory Retention Deficits in Rats Poisoned with the Sarin Analog Diisopropylfluorophosphate (DFP) and Treated with Atropine and Pralidoxime

2015

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“…In animal models of epilepsy, patterns of dysregulated Ca 21 dynamics have been well established (McNamara et al, 2006;Deshpande et al, 2010Deshpande et al, , 2014Chen, 2012). Aberrant Ca 21 dynamics have been proposed to be a major, if not essential, contributor to seizure induction and pathophysiology (McNamara et al, 2006;Chen, 2012).…”

Section: Introductionmentioning

confidence: 99%

Rapid Throughput Analysis Demonstrates that Chemicals with Distinct Seizurogenic Mechanisms Differentially Alter Ca²⁺ Dynamics in Networks Formed by Hippocampal Neurons in Culture

et al. 2015

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Primary cultured hippocampal neurons (HN) form functional networks displaying synchronous Ca 21 oscillations (SCOs) whose patterns influence plasticity. Whether chemicals with distinct seizurogenic mechanisms differentially alter SCO patterns was investigated using mouse HN loaded with the Ca 21 indicator fluo-4-AM. Intracellular Ca 21 dynamics were recorded from 96 wells simultaneously in real-time using fluorescent imaging plate reader.

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“…By optimizing the standard three-drug regimen of atropine, pralidoxime chloride (2-PAM), and diazepam we were able to achieve a significantly higher survival rates. We also observed multi-focal neuronal injury and protracted hippocampal Ca 2+ elevations following severe DFP and POX exposures (Deshpande et al, 2010, Deshpande et al, 2014). Given the critical role of Ca 2+ signaling in neuronal plasticity, these severe OP induced alterations in Ca 2+ dynamics could underlie some of the long-term plasticity changes associated with OP and nerve agent toxicity (Filbert et al, 2005).…”

Section: Introductionmentioning

confidence: 66%

“…We have recently reported the development of a rat survival model of severe OP intoxication using POX and DFP (Deshpande et al, 2010, Deshpande et al, 2014). The mortality, behavioral manifestations, and electroencephalogram profile for DFP and POX-induced cholinergic crisis were identical to those reported for human OP and nerve agent exposures.…”

Section: Introductionmentioning

confidence: 99%

Chronic behavioral and cognitive deficits in a rat survival model of paraoxon toxicity

et al. 2014

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Organophosphate (OP) compounds, including paraoxon (POX), are similar to nerve agents such as sarin. There is a growing concern that OP agents could be weaponized to cause mass civilian causalities. We have developed a rodent survival model of POX toxicity that is being used to evaluate chronic morbidity and to screen for medical countermeasures against severe OP exposure. It is well known that the survivors of nerve gas and chronic OP exposure exhibit neurobehavioral deficits such as mood changes, depression, and memory impairments. In this study we investigated whether animals surviving severe POX exposure exhibited long-term neurological impairments. POX exposure produced overt signs of cholinergic toxicity. Rats were rescued using an optimized atropine, 2-PAM and diazepam therapy. Surviving rats were studied using established behavioral assays for identifying symptoms of depression and memory impairment 3-months after POX exposure. In the forced swim test, POX rats exhibited increased immobility time indicative of a despair-like state. In the sucrose preference test, POX rats consumed significantly less sucrose water indicating anhedonia-like condition. POX rats also displayed increased anxiety as characterized by significantly lower performance in the open arm of the elevated plus maze. Further, when tested with a novel object recognition paradigm, POX rats exhibited a negative discrimination ratio indicative of impaired recognition memory. The results indicate that this model of survival from severe POX exposure can be employed to study some of the molecular bases for OP-induced chronic behavioral and cognitive comorbidities and develop therapies for their treatment.

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Development of status epilepticus, sustained calcium elevations and neuronal injury in a rat survival model of lethal paraoxon intoxication

Cited by 49 publications

References 39 publications

Chronic Treatment with Naltrexone Prevents Memory Retention Deficits in Rats Poisoned with the Sarin Analog Diisopropylfluorophosphate (DFP) and Treated with Atropine and Pralidoxime

Chronic Treatment with Naltrexone Prevents Memory Retention Deficits in Rats Poisoned with the Sarin Analog Diisopropylfluorophosphate (DFP) and Treated with Atropine and Pralidoxime

Rapid Throughput Analysis Demonstrates that Chemicals with Distinct Seizurogenic Mechanisms Differentially Alter Ca²⁺ Dynamics in Networks Formed by Hippocampal Neurons in Culture

Chronic behavioral and cognitive deficits in a rat survival model of paraoxon toxicity

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Development of status epilepticus, sustained calcium elevations and neuronal injury in a rat survival model of lethal paraoxon intoxication

Cited by 49 publications

References 39 publications

Chronic Treatment with Naltrexone Prevents Memory Retention Deficits in Rats Poisoned with the Sarin Analog Diisopropylfluorophosphate (DFP) and Treated with Atropine and Pralidoxime

Chronic Treatment with Naltrexone Prevents Memory Retention Deficits in Rats Poisoned with the Sarin Analog Diisopropylfluorophosphate (DFP) and Treated with Atropine and Pralidoxime

Rapid Throughput Analysis Demonstrates that Chemicals with Distinct Seizurogenic Mechanisms Differentially Alter Ca2+ Dynamics in Networks Formed by Hippocampal Neurons in Culture

Chronic behavioral and cognitive deficits in a rat survival model of paraoxon toxicity

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Rapid Throughput Analysis Demonstrates that Chemicals with Distinct Seizurogenic Mechanisms Differentially Alter Ca²⁺ Dynamics in Networks Formed by Hippocampal Neurons in Culture