Your search keyword '"Jiří Kassa"' showing total 86 results

1. A Comparison of the Neuroprotective and Reactivating Efficacy of a Novel Bispyridinium Oxime K870 with Commonly Used Pralidoxime and the Oxime HI-6 in Tabun-Poisoned Rat

Author

Jiří Kassa, Jana Hatlapatková, Jana Žďárová Karasová, Vendula Hepnarová, Filip Caisberger, and Jaroslav Pejchal

Subjects

Medicine

Abstract

Aim: The comparison of neuroprotective and central reactivating effects of the oxime K870 in combination with atropine with the efficacy of standard antidotal treatment in tabun-poisoned rats. Methods: The neuroprotective effects of antidotal treatment were determined in rats poisoned with tabun at a sublethal dose using a functional observational battery 2 h and 24 h after tabun administration, the tabun-induced brain damage was investigated by the histopathological evaluation and central reactivating effects of oximes was evaluated by the determination of acetylcholinesterase activity in the brain using a standard spectrophotometric method. Results: The central reactivating efficacy of a newly developed oxime K870 roughly corresponds to the central reactivating efficacy of pralidoxime while the ability of the oxime HI-6 to reactivate tabun-inhibited acetylcholinesterase in the brain was negligible. The ability of the oxime K870 to decrease tabun-induced acute neurotoxicity was slightly higher than that of pralidoxime and similar to the oxime HI-6. These results roughly correspond to the histopathological evaluation of tabun-induced brain damage. Conclusion: The newly synthesized oxime K870 is not a suitable replacement for commonly used oximes in the antidotal treatment of acute tabun poisonings because its neuroprotective efficacy is only slightly higher or similar compared to studied currently used oximes.

Published

2021

2. Dose Dependent Prophylactic Efficacy of 6-Chlorotacrine in Soman-Poisoned Mice

Author

Jiří Kassa and Jan Korábečný

Subjects

soman, 6-chlorotacrine, atropine, HI‑6, pharmacological pretreatment, mice, Medicine

Abstract

Aim: The influence of the dose on the ability of promising newly prepared reversible inhibitor of acetylcholinesterase (6-chlorotacrine) to increase the resistance of mice against soman and the efficacy of antidotal treatment of soman-poisoned mice was evaluated. Methods: The evaluation of the effect of pharmacological pretreatment is based on the identification of changes of soman-induced toxicity that was evaluated by the assessment of its LD50 value and its 95% confidence limit using probit-logarithmical analysis of death occurring within 24 hrs after administration of soman. Results: The dose of 6-chlorotacrine significantly influences the prophylactic efficacy of 6-chlorotacrine. Its highest dose was only able to significantly protect mice against acute toxicity of soman and increase the efficacy of antidotal treatment (atropine in combination with the oxime HI-6) of soman-poisoned mice. In addition, the highest dose of 6-chlorotacrine was significantly more effective to protect mice from soman poisoning than its lowest dose. Conclusion: These findings demonstrate the important influence of the dose of 6-chlorotacine on its prophylactic efficacy in the case of pharmacological pretreatment of soman poisoning in mice.

Published

2018

3. The Evaluation of Benefit of Newly Prepared Reversible Inhibitors of Acetylcholinesterase and Commonly Used Pyridostigmine as Pharmacological Pretreatment of Soman-Poisoned Mice

Author

Jiří Kassa, Jan Korábečný, and Eugenie Nepovimová

Subjects

soman, reversible inhibitors of acetylcholinesterase, antidotes, pharmacological pretreatment, mice, Medicine

Abstract

Aim: The ability of four newly prepared reversible inhibitors of acetylcholinesterase (6-chlorotacrine, 7-phenoxytacrine, compounds 1 and 2) and currently used carbamate pyridostigmine to increase the resistance of mice against soman and the efficacy of antidotal treatment of soman-poisoned mice was evaluated. Methods: The evaluation of the effect of pharmacological pretreatment is based on the identification of changes of soman-induced toxicity that was evaluated by the assessment of its LD50 value and its 95% confidence limit using probitlogarithmical analysis of death occurring within 24 h after administration of soman. Results: 6-chlorotacrine was only able to markedly protect mice against acute toxicity of soman. In addition, the pharmacological pretreatment with 6-chlorotacrine or compound 2 was able to increase the efficacy of antidotal treatment (the oxime HI-6 in combination with atropine) of soman-poisoned mice. The other newly prepared reversible inhibitors of acetylcholinesterase (7-phenoxytacrine, compound 1) as well as commonly used pyridostigmine did not influence the efficacy of antidotal treatment. Conclusion: These findings demonstrate that pharmacological pretreatment of somanpoisoned mice can be promising and useful in the case of administration of 6-chlorotacrine and partly compound 2.

Published

2017

4. The Evaluation of the Potency of Newly Developed Oximes (K727, K733) and Trimedoxime to Counteract Acute Neurotoxic Effects of Tabun in Rats

Author

Jiří Kassa, Jana Hatlapatková, and Jana Žďárová Karasová

Subjects

Tabun, Neurotoxicity, Functional observational battery, Oximes, Rats, Medicine

Abstract

Aim: The ability of two newly developed oximes (K727, K733) to reduce tabun-induced acute neurotoxic signs and symptoms was evaluated and compared with currently available trimedoxime in rats. Methods: The neuroprotective effects of the oximes studied combined with atropine on Wistar rats poisoned with tabun at a lethal dose (380 μg/kg i.m.; 90% of LD50 value) were evaluated. Tabun-induced neurotoxicity was monitored by the functional observational battery consisting of 38 measurements of sensory, motor and autonomic nervous functions at 2 hours following tabun challenge. Results: All tested oximes combined with atropine enable tabun-poisoned rats to survive till the end of experiment. Both newly developed oximes (K727, K733) combined with atropine were able to decrease tabun-induced neurotoxicity in the case of lethal poisoning although they did not eliminate all tabun-induced acute neurotoxic signs and symptoms. Conclusion: The ability of both novel bispyridinium oximes to decrease tabun-induced acute neurotoxicity was slightly lower than that of trimedoxime. Therefore, the newly developed oximes are not suitable for the replacement of commonly used oximes such as trimedoxime in the treatment of acute tabun poisonings.

Published

2016

5. Natural Detoxification Capacity to Inactivate Nerve Agents Sarin and VX in the Rat Blood

Author

Jiří Bajgar, Jiří Cabal, Jiří Kassa, and Michal Pavlík

Subjects

Sarin, VX, Detoxification, Rat, Blood, Cholinesterases, Medicine

Abstract

Background: The method of continual determination of the rat blood cholinesterase activity was developed to study the changes of the blood cholinesterases following different intervetions. Aims: The aim of this study is registration of cholinesterase activity in the rat blood and its changes to demonstrate detoxification capacity of rats to inactivate sarin or VX in vivo. Methods: The groups of female rats were premedicated (ketamine and xylazine) and cannulated to a. femoralis. Continual blood sampling (0.02 ml/min) and monitoring of the circulating blood cholinesterase activity were performed. Normal activity was monitored 1–2 min and then the nerve agent was administered i.m. (2× LD50). Using different time intervals of the leg compression and relaxation following the agent injection, cholinesterase activity was monitored and according to the inhibition obtained, detoxification capacity was assessed. Results: Administration of sarin to the leg, then 1 and 5 min compression and 20 min later relaxation showed that further inhibition in the blood was not observed. On the other hand, VX was able to inhibit blood cholinesterases after this intervention. Conclusions: The results demonstrated that sarin can be naturally detoxified on the contrary to VX. Described method can be used as model for other studies dealing with changes of cholinesterases in the blood following different factors.

Published

2016

6. The Ability of Oxime Mixtures to Increase the Reactivating and Therapeutic Efficacy of Antidotal Treatment of Cyclosarin Poisoning in Rats and Mice

Author

Jiří Kassa, Jana Zdarová Karasová, Růžena Pavlíková, Filip Caisberger, and Jiří Bajgar

Subjects

Acetylcholinesterase, Cyclosarin, HI‑6, Trimedoxime, K203, Mice, Medicine

Abstract

The reactivating and therapeutic efficacy of two combinations of oximes (HI‑6 + trimedoxime and HI‑6 + K203) was compared with the effectiveness of antidotal treatment involving single oxime (HI‑6, trimedoxime, K203) using in vivo methods. In vivo determined percentage of reactivation of cyclosarin‑inhibited blood and tissue acetylcholinesterase in poisoned rats showed that the reactivating efficacy of both combinations of oximes is slightly higher than the reactivating efficacy of the most effective individual oxime in blood, diaphragm as well as in brain. Moreover, both combinations of oximes were found to be slightly more efficacious in the reduction of acute lethal toxic effects in cyclosarin‑poisoned mice than the antidotal treatment involving single oxime. Based on the obtained data, we can conclude that the antidotal treatment involving chosen combinations of oximes brings a beneficial effect for its ability to counteract the acute poisoning with cyclosarin.

Published

2012

7. A Comparison of the Potency of Newly Developed Oximes (K347, K628) and Currently Available Oximes (Obidoxime, HI-6) to Counteract Acute Neurotoxic Effects of Tabun in Rats

Author

Jiří Kassa, Jana Žďárová Karasová, Sandra Tesařová, Kamil Musílek, and Kamil Kuča

Subjects

Tabun, Functional observational battery, K347, K628, Obidoxime, HI‑6, Medicine

Abstract

The ability of newly developed oximes (K347, K628) to reduce tabun-induced acute neurotoxic signs and symptoms was compared with currently available oximes (obidoxime, HI-6) using a functional observational battery. The neuroprotective effects of the oximes studied (K347, K628, obidoxime, HI-6) combined with atropine on rats poisoned with tabun at a sublethal dose (220 μg/kg i.m.; 80 % of LD50 value) were evaluated. Tabun-induced neurotoxicity was monitored by a functional observational battery and automatic measurement of motor activity at 24 hours following tabun challenge. The results indicate that all tested oximes combined with atropine enable tabun-poisoned rats to survive 24 hours following tabun challenge. Both newly developed oximes (K347, K628) combined with atropine are able to decrease tabun-induced neurotoxicity in the case of sublethal poisonings but they do not eliminate all tabun-induced acute neurotoxic signs and symptoms. Their ability to decrease the tabun-induced acute neurotoxicity is higher than that of the oxime HI-6 and it is slightly slower than the neuroprotective efficacy of obidoxime. As the neuroprotective potency of both newly developed oximes (K347, K628) is not as high as the potency of obidoxime, they are not a suitable replacement for obidoxime for the treatment of acute tabun poisonings.

Published

2010

8. A Comparison of the Neuroprotective Efficacy of Newly Developed Oximes (K156, K203) and Currently Available Oximes (Obidoxime, HI-6) in Cyclosarin-poisoned Rats

Author

Jiří Kassa, Jana Žďárová Karasová, Sandra Tesařová, Kamil Kuča, and Kamil Musílek

Subjects

Cyclosarin, K156, K203, Obidoxime, HI‑6, Funtional observational battery, Medicine

Abstract

The neuroprotective effects of newly developed oximes (K156, K203) and currently available oximes (obidoxime, HI-6) in combination with atropine in rats poisoned with cyclosarin were studied. The cyclosarin-induced neurotoxicity was monitored using a functional observational battery 24 hours after cyclosarin challenge. The results indicate that a newly developed oxime K156 is able to counteract slightly cyclosarin-induced neurotoxicity while another newly developed oxime K203 is completely ineffective in reducing cyclosarin-induced neurotoxic signs and symptoms. The neuroprotective efficacy of K156 is comparable with commonly used obidoxime and oxime HI-6. Thus, none of the newly developed oximes achieves better neuroprotective efficacy than both commonly used oximes. They are therefore not suitable replacements for antidotal treatment of acute poisonings with cyclosarin.

Published

2008

9. Comparison of Effects of Different Antidotes on Tabun-Induced Cognitive Impairment in Rats Using Water Maze

Author

Gabriela Kunešová and Jiří Kassa

Subjects

Tabun, Water maze, Cognitive function, Atropine, Obidoxime, Trimedoxime, Medicine

Abstract

In the past, scientists focused on the development of antidotes (mainly anticholinergics in combination with reactivators of inhibited acetylcholinesterase – oximes) to increase the number of surviving nerve agent-intoxicated individuals. Recently, they are interested in antidotes able not only to protect nerve agent-poisoned men from lethal toxic effects but also to improve their life quality by improvement of their central cognitive functions. In our study, the water maze was used to measure spatial working learning and memory in the case of tabun-induced cognitive impairment in albino Wistar rats. Antidotal treatment consisted of atropine alone or a combination of atropine with an oxime (obidoxime, trimedoxime or oxime HI-6). Our results suggest that atropine alone is not sufficient as a treatment for saving cognitive functions impaired by tabun. On the other hand, the addition of oxime to atropine contributes to improvement of cognitive performance in tabun-poisoned rats regardless of type of oxime.

Published

2006

10. A Comparison of the Potency of the Oxime HLö-7 and Currently Used Oximes (HI-6, Pralidoxime, Obidoxime) to Reactivate Nerve Agent-Inhibited Rat Brain Acetylcholinesterase by in vitro Methods

Author

Kamil Kuča, Jiří Cabal, Jiří Kassa, Daniel Jun, and Martina Hrabinová

Subjects

Sarin, Cyclosarin, Tabun, VX, Obidoxime, Pralidoxime, Medicine

Abstract

1. The efficacy of the oxime HLö-7 and currently used oximes (pralidoxime, obidoxime, HI-6) to reactivate acetylcholinesterase inhibited by various nerve agents (sarin, tabun, cyclosarin, VX) was tested by in vitro methods. 2. Both H oximes (HLö-7, HI-6) were found to be more efficacious reactivators of sarin and VX-inhibited acetylcholinesterase than pralidoxime and obidoxime. On the other hand, their potency to reactivate tabun-inhibited acetylcholinesterase is very low and does not reach the reactivating efficacy of obidoxime. In the case of cyclosarin, the oxime HI-6 was only found to be able to sufficiently reactivate cyclosarin-inhibited acetylcholinesterase in vitro. 3. Thus, the oxime HLö-7 does not seem to be more efficacious reactivator of nerve agent-inhibited acetylcholinesterase than HI-6 according to in vitro evaluation of their reactivation potency and, therefore, it is not more suitable to be introduced for antidotal treatment of nerve agent-exposed people than HI-6.

Published

2005

11. The Influence of the Time of Antidotal Treatment Administration on the Potency of Newly Developed Oximes to Counteract Acute Toxic Effects of Tabun in Mice

Author

Jiří Kassa

Subjects

Tabun, K027, K048, Oximes, Acute toxicity, Mice, Medicine

Abstract

1. The influence of the time of administration of antidotal treatment consisting of anticholinergic drug (atropine) and newly developed oxime (K027 or K048) on its effectiveness to eliminate tabun-induced lethal toxic effects was studied in mice. 2. The therapeutic efficacy of antidotal treatment of tabun-induced acute poisoning depends on the time of its administration regardless of the choice of the oxime. 3. Our results show that both oximes studied (K027, K048) are able to sufficiently eliminate lethal effects of tabun. Nevertheless, their efficacy significantly decreases when they were administered 5 min after tabun poisoning. 4. The findings support the hypothesis that both newly developed oximes appear to be suitable oximes to counteract acute toxicity of tabun although their ability to eliminate lethal toxic effects of tabun significantly decreases with prolonged time interval between tabun challenge and antidotal treatment administration.

Published

2005

12. The Influence of the Time of Antidotal Treatment Administration on Its Effectiveness Against Tabun-Induced Poisoning in Mice

Author

Jiří Kassa

Subjects

Tabun, Pralidoxime, Obidoxime, HI-6, Trimedoxime, Acute toxicity, Medicine

Abstract

Summary: 1. The influence of the time of administration of antidotal treatment consisting of anticholinergic drug (atropine) and oxime (pralidoxime, obidoxime, HI-6 or trimedoxime) on its effectiveness to eliminate tabun-induced lethal effects was studied in mice. 2. The therapeutic efficacy of antidotal treatment of tabun-induced acute poisoning depends on the time of its administration when obidoxime or the oxime HI-6 was used as an acetylcholinesterase reactivator. 3. Pralidoxime is practically ineffective to eliminate acute toxic effects of tabun regardless of the time of its administration. 4. Our results show that trimedoxime seems to be the most effective to eliminate lethal effects of tabun. In addition, its efficacy does not decrease when it is administered 5 min after tabun poisoning. 5. The findings support the hypothesis that trimedoxime appears to be the most suitable oxime to counteract acute toxicity of tabun because of its ability to eliminate lethal effects of tabun when it is injected 5 min after tabun challenge on the contrary to other oximes tested.

Published

2004

13. Assessment of the Therapeutic and Anticonvulsive Efficacy of a Drug Combination Consisting of Trihexyphenidyle and HI-6 in Soman-Poisoned Rats

Author

Jiří Kassa and Ivan Samnaliev

Subjects

Soman, Atropine, Trihexyphenidyle, HI-6, Acute toxicity, Convulsions, Medicine

Abstract

1. The influence of two anticholinergic drugs (atropine, trihexyphenidyle) on the effectiveness of antidotal treatment to eliminate soman-induced lethal effects and convulsions was studied in rats. 2. The oxime HI-6 when combined with centrally acting anticholinergic drug trihexyphenidyle seems to be more efficacious in the elimination of acute toxic effects of soman than its combination with atropine. 3. The findings support the hypothesis that the choice of the anticholinergic drug is important for the effectiveness of antidotal mixture in the case of antidotal treatment of soman-induced acute poisoning.

Published

2004

14. Anticholinergic Drugs – Functional Antidotes for the Treatment of Tabun Intoxication

Author

Gabriela Krejčová and Jiří Kassa

Subjects

Nerve agents, Tabun, Atropine, Benactyzine, Biperiden, Scopolamine, Medicine

Abstract

Summary: 1. To study the influence of antidotes on tabun-induced neurotoxicity, the rats were injected intramuscularly with organophosphate tabun (LD50). The efficacy of choice antidotal treatment consisting of acetylcholinesterase reactivator obidoxime and one of four anticholinergic drugs (atropine, benactyzine, biperiden, scopolamine) was compared. 2. Testing of tabun-induced neurotoxicity progress was carried out using the method Functional observational battery. The experimental animals as well as controls were observed at 24 hours and 7 days following tabun or saline administration. 3. The results were compared to the condition of animals without anticholinergic drug (oxime alone) and control rats that received physiological solution instead of tabun and treatment. Antidotal treatment involving centrally acting anticholinergic drugs (benactyzine, biperiden, scopolamine) showed significantly higher neuroprotective efficacy compared to antidotal treatment containing atropine.

Published

2004

15. A Comparison of the Neuroprotective Efficacy of Pharmacological Pretreatment and Antidotal Treatment in Soman-Poisoned Rats

Author

Jiří Kassa, Gabriela Krejčová, and Ivan Samnaliev

Subjects

Soman, Functional observational battery, Motor activity, PANPAL, Pyridostigmine, Biperiden, Medicine

Abstract

1. To study the influence of pharmacological pretreatment (PANPAL or pyridostigmine combined with biperiden) and antidotal treatment (the oxime HI-6 plus atropine) on soman-induced neurotoxicity, male albino rats were poisoned with a lethal dose of soman (54 (g/kg i.m.; 100% of LD50 value) and observed at 24 hours and 7 days following soman challenge. The neurotoxicity of soman was evaluated using a Functional observational battery and an automatic measurement of motor activity. 2. Pharmacological pretreatment as well as antidotal treatment were able to eliminate some of soman-induced neurotoxic effects observed at 24 hours following soman poisoning. The combination of pharmacological pretreatment (PANPAL or pyridostigmine combined with biperiden) and antidotal treatment was found to be more effective in the elimination of soman-induced neurotoxicity in rats at 24 hours following soman challenge in comparison with the administration of pharmacological pretreatment or antidotal treatment alone. To compare both pharmacological pretreatments, the combination of pyridostigmine with biperiden seems to be more efficacious to eliminate soman-induced signs of neurotoxicity than PANPAL. 3. At 7 days following soman poisoning, the combination of pharmacological pretreatment involving pyridostigmine and biperiden with antidotal treatment was only able to completely eliminate somaninduced neurotoxic signs. 4. Thus, our findings confirm that the combination of pharmacological pretreatment and antidotal treatment is able not only to protect the experimental animals from the lethal effects of soman but also to eliminate most soman-induced signs of neurotoxicity in poisoned rats. The pharmacological pretreatment containing pyridostigmine and biperiden appears to be more efficacious to eliminate soman-induced neurotoxic sings than PANPAL.

Published

2003

16. The Impairment of Spatial Memory Following Low-Level Sarin Inhalation Exposure and Antidotal Treatment in Rats

Author

Jiří Kassa, Gabriela Krejčová, and Josef Vachek

Subjects

Sarin, Low-level inhalation exposure, Spatial memory, Rat, Antidotal treatment, Medicine

Abstract

1. To study the influence of antidotes on low-level sarin-induced impairment of cognitive functions, the rats were exposed to three various low concentrations of sarin (LEVEL 1–3) for 60 minutes in the inhalation chamber. In addition, one group of rats was exposed to LEVEL 2 of sarin repeatedly. 2. Testing of cognitive functions was carried out using the Y-maze evaluating learning and spatial memory. The correct averse behavior of sarin-exposed rats in the Y-maze was tested several times within four weeks following sarin inhalation exposure and antidotal treatment to look for any cognitive impairments. 3. The results were compared to the Y-maze performance of sarin-exposed rats without antidotal treatment and control rats exposed to pure air instead of sarin with or without antidotal treatment. While antidotal treatment was able to eliminate a short-term deficiency in the Y-maze performance in rats exposed to the LEVEL 1 of sarin, a significant decrease in the Y-maze performance in rats exposed to sarin at the LEVEL 2 and 3 was only shortened. Sarin-induced spatial memory impairments in rats exposed repeatedly to sarin at the LEVEL 2 was also shortened when rats were treated following each sarin inhalation exposure. 4. The findings confirm that antidotes currently used for nerve agent poisonings are beneficial for the treatment of rats singly or repeatedly exposed to non-convulsive symptomatic or even clinically asymptomatic concentrations of sarin.

Published

2002

17. The Influence of Anticholinergic Drug and Oxime Selection on the Effectiveness of Antidotal Treatment Against Tabun-Induced Poisoning in Mice

Author

Jiří Kassa

Subjects

Tabun, Oximes, Anticholinergic drugs, Acute toxicity, Mice, Medicine

Abstract

1. The influence of oximes (pralidoxime, obidoxime, HI-6) and anticholinergic drugs (atropine, benactyzine, biperiden, scopolamine) on the effectiveness of antidotal treatment to eliminate tabun-induced lethal effects was studied in mice. 2. Obidoxime seems to be the most efficacious oxime for the elimination of tabun-induced lethal effects in mice, although the difference in the efficacy of obidoxime and HI-6 is not significant when they are combined with atropine. 3. Obidoxime and HI-6 when combined with centrally acting anticholinergic drugs (benactyzine, biperiden and scopolamine) seem to be more efficacious in the elimination of toxic effects of the lethal dose of tabun than their combination with atropine. 4. The findings support the hypothesis that the choice of acetylcholinesterase reactivators as well as the anticholinergic drug selection are important for the effectiveness of antidotal mixture in the case of antidotal treatment of tabun-induced acute poisoning.

Published

2002

18. The Influence of Oxime Selection on the Efficacy of Antidotal Treatment of Soman-Poisoned Rats

Author

Jiří Kassa and Josef Fusek

Subjects

Soman, Atropine, HI-6, Obidoxime, Pralidoxime, Rat, Medicine

Abstract

1. The influence of some acetylcholinesterase reactivators (HI-6, obidoxime, pralidoxime) on the efficacy of antidotal treatment to eliminate soman-induced disturbance of respiration and circulation and to protect experimental animals poisoned with supralethal dose of soman (1.5 × LD50) was investigated in a rat model with on-line monitoring of respiratory and circulatory parameters. 2. Obidoxime or pralidoxime in combination with atropine were insufficient to enable soman-poisoned rats to survive for 2 hours when given 1 minute after the administration of soman. 3. On the other hand, the ability of the oxime HI-6 in combination with atropine to prevent soman-induced alteration of respiration and circulation was significantly higher. Some rats treated with HI-6 in combination with atropine were fully protected against the lethal toxic effects of soman within 2 hours following soman administration. 4. Our findings confirm that the oxime HI-6 seems to be a much more suitable and efficacious acetylcholinesterase reactivator for the antidotal treatment of severe acute soman-induced poisoning than currently used obidoxime or pralidoxime.

Published

2002

19. Effect of Atropine and the Oxime HI-6 on Low-Level Sarin-Induced Alteration of Performance of Rats in a T-Maze

Author

Gabriela Krejčová, Jiří Kassa, and Josef Vachek

Subjects

Sarin, Atropine, Oxime HI-6, Spatial memory, Multiple T-maze, Rat, Medicine

Abstract

1. To study the influence of antidotes on low-level sarin-induced alteration of cognitive functions, male albino Wistar rats were exposed to three various low concentrations of sarin for 60 minutes in the inhalation chamber. One minute following sarin exposure, the rats were i.m. treated with the oxime HI-6 in combination with atropine. Control rats were treated with antidotes as experimental rats but exposed to the pure air instead of sarin. Cognitive functions of the rats were tested using a T-maze where spatial memory and spatial orientation were evaluated. The performance of sarin-exposed and treated rats in the T-maze was tested several times within six weeks (single exposure) or five weeks (repeated exposure) following inhalation exposure to evaluate cognitive impairments. 2. In the case of single exposure to sarin, no statistically significant differencies between the performances of the control and the experimental groups in the alteration of spatial memory and spatial orientation were observed. The repeated exposure of treated rats to clinically asymptomatic dose of sarin (LEVEL 2) did not change the effect of low-level sarin exposure on spatial memory of the experimental rats compared to the single exposure to the same dose of sarin. 3. The decrease in the T-maze performance of the control rats was caused by the impairments of rat’s mobility due to the features of a solution of antidotes.

Published

2002

20. Long Term Effects of Low-Level Sarin Inhalation Exposure on the Spatial Memory of Rats in a T-Maze

Author

Jiří Kassa, Marie Koupilová, and Josef Vachek

Subjects

Sarin, Low-level inhalation exposure, Spatial memory, T-maze, Rat, Medicine

Abstract

To study the influence of low-level sarin exposure on cognitive functions, male albino Wistar rats were exposed to three various low concentrations of sarin (LEVEL 1–3) for 60 minutes in the inhalation chamber. Testing of cognitive functions was carried out using the T-maze evaluating learning and spatial memory. The behavior of sarin-exposed rats in the T-maze was tested several times within five weeks following sarin inhalation exposure to look for any cognitive impairments. The alteration of cognition was evaluated by using a method studying memory elicitation in response to appetitive motivation in a multiple T-maze. 2. Statistically significant, short-term deficiency in the T-maze performance was observed in rats exposed to symptomatic (LEVEL 3) as well as clinically asymptomatic concentration (LEVEL 2) of sarin. The repeated exposure of rats to clinically asymptomatic dose of sarin (LEVEL 2R) did not change the effect of lowlevel sarin exposure on spatial memory compared to the single exposure to the same dose of sarin. 3. Thus, sarin is able to influence the cognitive functions (e.g. spatial memory) even at low doses that do not cause clinically manifested intoxication following the inhalation exposure. Nevetheless, the alteration of spatial memory lasts for a short time only, in contrast with the severe sarin poisoning.

Published

2001

21. The Long Term Influence of Low-Level Sarin Exposure on Behavioral and Neurophysiological Functions in Rats

Author

Jiří Kassa, Marie Koupilová, Josef Herink, and Josef Vachek

Subjects

Sarin, Low level inhalation exposure, Long term effects, FOB, Excitability, Rat, Medicine

Abstract

1. Long term effects of low doses of highly toxic organophosphorus agent sarin on behavioral and neurophysiological functions were studied in rats exposed to sarin by inhalation. The toxic effects of sarin were monitored using a functional observational battery (FOB), an automatic measurement of motor activity and a test of excitability of central nervous system at 3, 6 and 12 months following sarin exposure. 2. The results indicate that sarin at symptomatic as well as asymptomatic doses (level 2 and 3) is able to induce some neurotoxic effects (a decrease in activity and mobility, an alteration of gait, an increase in stereotyped behavior) including an increase in the excitability of central nervous system (an increase in convulsive activity following the administration of pentamethylenetetrazole) in rats at 3 months following inhalation exposure. Some sings of increased excitability were also observed in sarin-exposed rats following 6 or 12 months (an increase in exploratory activity, body temperature and a hindlimb grip strength at 6 months following exposure to sarin at asymptomatic doses, an increase in tail-pinch response at 12 months following exposure to sarin at symptomatic doses). 3. Therefore, nerve agents such as sarin seem to be harmful not only at high, clinically symptomatic doses but also at low, clinically asymptomatic doses because of long term manifestation of alteration of neurophysiological functions in sarin-exposed rats without disruption of cholinergic nervous system.

Published

2001

22. Long Term Alteration of Immune Functions Following Low Level Exposure to Sarin in Rats

Author

Jiří Kassa, Zuzana Kročová, and Josef Vachek

Subjects

Sarin, Low level inhalation exposure, Immunotoxicity, Rat, Medicine

Abstract

1. Long term alteration of immune functions caused by low doses of nerve agent sarin were studied in rats exposed to sarin by inhalation. The alteration of immune functions by sarin was monitored by using two methods (the evaluation of in vitro spontaneous as well as stimulated proliferation of spleen cells and in vitro bactericidal activity of peritoneal macrophages) at 3, 6 and 12 months following sarin exposure. 2. The results indicate that not only symptomatic but also asymptomatic dose of sarin is able to alter some immune functions at six and twelve months following exposure to sarin. 3. Thus, not only organophosphorus insecticides but also nerve agents such as sarin can be potentially immunotoxic even at very low doses that do not cause clinically manifested intoxication following the inhalation exposure. The ability of sarin at low doses to alter immune functions seems to be really long term (up to 12 months following the exposure).

Published

2000

23. The Long Term Changes in Liver DNA and Total Protein Contents Following Low Level Sarin Exposure in Rats

Author

Jiří Kassa, František Skopec, and Josef Vachek

Subjects

Sarin, Low level inhalation exposure, DNA, Protein, Liver, Rat, Medicine

Abstract

1. The changes in contents of DNA and total protein in the liver of the rats exposed to low level sarin by inhalation at 3, 6 and 12 months following the exposure were studied. The influence of sarin on the DNA and protein metabolism in liver was determinated by the measurements of incorporation of tritiated thymidine into DNA, the concentration of DNA and total protein. 2. Our results show that not only symptomatic level 3 but also asymptomatic levels 1 and 2 of sarin are able to significantly decrease the incorporation of radiolabelled thymidine without changing total concentrations of DNA as well as protein at three months following sarin exposure. On the other hand, the significant decrease in total contents of DNA and protein in liver without the changes in the incorporation of tritiated thymidine was determined in liver six months following sarin exposure. Practically no significant changes in the metabolism of DNA and protein were observed at 12 months following sarin exposure. 3. Thus, not only clinically manifested intoxication but also low-level, asymptomatic exposure to nerve agents such as sarin is able to influence the metabolism of nucleic acids as well as proteins even several months following the exposure.

Published

2000

24. Neuroprotective Effects of Antidotes in Soman-Poisoned Rats

Author

Jiří Kassa and Marie Koupilová

Subjects

Neurotoxicity, Soman, Behavioral screening, Obidoxime, Atropine, Rat, Medicine

Abstract

1. The neuroprotective effects of antidotes (atropine, obidoxime/atropine mixture, HI-6/atropine mixture) on rats poisoned with soman at a sublethal dose (48 μg/kg i.m.; 60% of LD50 value) were studied. The neurotoxicity was monitored using a functional observational battery (FOB) and an automatic measurement of motor activity. The neurotoxicity of soman was monitored at 24h and 7d following soman poisoning. 2. The results indicate that atropine alone and the oxime HI-6 in combination with atropine seem to be effective antidotal treatment for the elimination of soman-induced neurotoxicity in the case of sublethal poisonings. 3. On the other hand, the combination of obidoxime with atropine appears to be practically ineffective in diminishing neurotoxic soman-induced symptoms. 4. Dealing with neuroprotective effects of antidotes, the oxime HI-6 in combination with atropine seems to be more suitable antidotal mixture than obidoxime in combination with atropine even in the case of sublethal poisoning with nerve agents.

Published

1999

25. The Influence of Anticholinergic Drug Selection on the Effectiveness of Oximes Against Soman-Induced Supralethal Poisoning in Mice

Author

Jiří Kassa

Subjects

Soman, Oximes, Anticholinergic drugs, Acute toxicity, Mice, Medicine

Abstract

1. The influence of anticholinergic drugs (atropine, benactyzine, biperiden) on the efficacy of monopyridinium and bispyridinium oximes (HI-6, BI-6, obidoxime, pralidoxime, methoxime) on soman-induced supralethal poisoning was studied in mice. 2. While methoxime combined with benactyzine or biperiden seems to be more efficacious in the elimination of toxic effects of supralethal dose of soman than its combination with atropine, the efficacy of the other oximes studied against soman-induced toxic effects is not significantly influenced by the anticholinergic drug selection. 3. On the other hand, there are big differences in the effectiveness of oximes tested as to their ability to eliminate toxic effects of soman at supralethal doses. 4. The findings support the fact that the choice of acetylcholinesterase reactivator is more important than the anticholinergic drug selection for the effectivenes of antidotal mixture in the case of prophylactic administration of antidotes.

Published

2001

26. A Comparison of the Efficacy of New Monopyridinium Oximes with the Oxime HI-6 Against Mevinphos in Mice

Author

Jiří Kassa and Jiří Bielavský

Subjects

Mevinphos, Monopyridinium oximes, HI-6, Benactyzine, LD50, Mouse, Medicine

Abstract

1. The therapeutic efficacy of three new monopyridinium oximes (2,4-PAEtM, 2,5-PAEtM, 2,5-PAAM) and the bispyridinium oxime HI-6 was evaluated in combination with benactyzine against acute poisoning with the organophosphorus insecticide mevinphos in mice. 2. When mice were treated two min after mevinphos poisoning, no significant differences in the therapeutic effectiveness of tested oximes were observed. They increased the 24h LD50 values of mevinphos about three times in comparison with non-treated intoxicated animals. 3. On the other hand, there were significant differences in their therapeutic efficacy when they were administered 30 sec following mevinphos challenge. The monopyridinium oxime 2,5-PAEtM seems to be the most efficacious against mevinphos toxicity. 4. Use of new monopyridinium oxime 2,5-PAEtM appears to be the improvement in the antidotal treatment of poisoning with organophosphorus insecticide mevinphos in comparison with HI-6.

Published

1999

27. A Comparison of the Therapeutic Efficacy of Conventional and Modern Oximes Against Supralethal Doses of Highly Toxic Organophosphates in Mice

Author

Jiří Kassa

Subjects

Soman, Sarin, Cyclosin, Pralidoxime, Obidoxime, Methoxime, Medicine

Abstract

1. The therapeutic efficacy of various oximes (pralidoxime, obidoxime, methoxime, HI-6, HLö-7, BI-6) against supralethal nerve agent poisoning (soman, sarin, cyclosin) in mice was tested. 2. New oxime BI-6, synthesized in our laboratory, is significantly more efficacious than conventional oximes but a little less efficacious than other H-oximes (HI- 6, HLö-7). 3. H-oximes (HI-6, HLö-7) seem to be the most efficacious reactivators of nerve agent-inhibited acetylcholinesterase for antidotal treatment of supralethal nerve agent poisoning in mice.

Published

1998

28. Changes of Cholinesterase Activity in the Erythrocytes, Plasma, Diaphragm, Liver and Various Parts of the Brain in the Rabbit Following Transfusion of Erythrocytes with Soman Inhibited Acetylcholinesterase

Author

Jiří Kassa, Jiří Bajgar, and Josef Fusek

Subjects

Soman, Acetycholinesterase, Butyrylcholinesterase, Blood-transfusion, Rabbit, Medicine

Abstract

1. The changes of cholinesterase activity in rabbit blood, peripheral tissues and the central nervous system following transfusion of erythrocytes with soman inhibited acetylcholinesterase were demonstrated. 2. After incubation with soman for 0.5 or 24 h, erythrocytes without acetylcholinesterase activity were injected to intact rabbits and cholinesterase activity in the erythrocytes, plasma, diaphragm, liver and various parts of the brain were evaluated 24 h following blood-transfusion. 3. When erythrocytes were incubated with soman for 24 h, no changes of cholinesterase activity in the rabbit following blood-transfusion were observed with an exception of erythrocyte acetylcholinesterase. 4. When erythrocytes were incubated with soman for 0.5 h, a significant decrease in cholinesterase activity in the erythrocytes, plasma, diaphragm and liver following blood-transfusion was found. These data show that soman is able to release from erythrocytes and inhibit cholinesterase activities not only in vitro but also in vivo although the significant inhibition of cholinesterase activities by soman was only observed in the peripheral compartment.

Published

1997

29. A Comparison of the Neuroprotective and Reactivating Efficacy of a Novel Bispyridinium Oxime K870 with Commonly Used Pralidoxime and the Oxime HI-6 in Tabun-Poisoned Rats

Author

Jaroslav Pejchal, Jiří Kassa, Filip Caisberger, Vendula Hepnarova, Jana Žďárová Karasová, and Jana Hatlapatková

Subjects

Cholinesterase Reactivators, Pralidoxime, Antidotes, Pyridinium Compounds, Brain damage, Pharmacology, Neuroprotection, Poisons, chemistry.chemical_compound, Oximes, medicine, Animals, Chemical Warfare Agents, Rats, Wistar, Tabun, Pralidoxime Compounds, Neurotoxicity, General Medicine, medicine.disease, Oxime, Acetylcholinesterase, Organophosphates, Rats, Atropine, chemistry, Medicine, Cholinesterase Inhibitors, medicine.symptom, medicine.drug

Abstract

Aim: The comparison of neuroprotective and central reactivating effects of the oxime K870 in combination with atropine with the efficacy of standard antidotal treatment in tabun-poisoned rats. Methods: The neuroprotective effects of antidotal treatment were determined in rats poisoned with tabun at a sublethal dose using a functional observational battery 2 h and 24 h after tabun administration, the tabun-induced brain damage was investigated by the histopathological evaluation and central reactivating effects of oximes was evaluated by the determination of acetylcholinesterase activity in the brain using a standard spectrophotometric method. Results: The central reactivating efficacy of a newly developed oxime K870 roughly corresponds to the central reactivating efficacy of pralidoxime while the ability of the oxime HI-6 to reactivate tabun-inhibited acetylcholinesterase in the brain was negligible. The ability of the oxime K870 to decrease tabun-induced acute neurotoxicity was slightly higher than that of pralidoxime and similar to the oxime HI-6. These results roughly correspond to the histopathological evaluation of tabun-induced brain damage. Conclusion: The newly synthesized oxime K870 is not a suitable replacement for commonly used oximes in the antidotal treatment of acute tabun poisonings because its neuroprotective efficacy is only slightly higher or similar compared to studied currently used oximes.

Published

2021

30. Evaluation of soman-induced extracranial histopathology in the context of clinical biochemistry, mitotic and apoptotic activity and morphometric analysis

Author

Jiří Kassa, Jana Hatlapatková, Jan Misik, and Jaroslav Pejchal

Subjects

0301 basic medicine, medicine.medical_specialty, Pathology, Necrosis, Health, Toxicology and Mutagenesis, Biomedical Engineering, Context (language use), Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, chemistry.chemical_compound, Hyperaemia, Artificial Intelligence, Edema, Soman, medicine, Large intestine, General Pharmacology, Toxicology and Pharmaceutics, General Immunology and Microbiology, General Neuroscience, General Medicine, Small intestine, 030104 developmental biology, medicine.anatomical_structure, chemistry, Histopathology, medicine.symptom, General Agricultural and Biological Sciences

Abstract

We aimed this study to evaluate histopathology of heart, lung, liver, kidney, small and large intestine in the context of clinical biochemistry, mitotic (intestine only) and apoptotic activity and morphometric analysis (intestine and lung only). Male Wistar rats were poisoned by soman ( i.m. , 52 μg kg −1 ; 70% LD 50 ). Samples were taken 1, 3 and 7 days following soman exposure. Biochemistry was evaluated in blood. Hematoxylin-eosin staining, Mallory's PTAH method, immunohistochemical detection of activated-caspase-3, TUNEL, and morphometric computer analysis were performed. We found increased AST and CK in blood, areas ranging from acute myolysis and necrosis to areas undergoing resolution in heart, a biphasic response consisting of hyperaemia, edema and bleeding leading to decreased airiness (day 1) and delayed inflammatory response with increased apoptosis (day 7) in lung, lymphangiectasis in small intestine (day 1) and subepithelial edema in large intestine (day 3) after soman intoxication. In intestine, mitotic activity decreased in crypts 1 and 7 days after the intoxication. Apoptotic activity decreased in the superficial compartment on the day 1, whereas it increased in the same compartment 3 days after the poisoning. Soman intoxication at the sublethal dose induced significant biochemical changes in blood and histopathological changes in heart, lung and intestine.

Published

2017

31. Comparison of the neuroprotective effects of a novel bispyridinium oxime KR-22934 with the oxime K203 and obidoxime in tabun-poisoned male rats

Author

Kamil Musilek, Kamil Kuca, Jiří Kassa, Jana Žďárová Karasová, and Young-Sik Jung

Subjects

Obidoxime, General Immunology and Microbiology, Chemistry, General Neuroscience, Health, Toxicology and Mutagenesis, Biomedical Engineering, Neurotoxicity, General Medicine, Pharmacology, medicine.disease, Oxime, Median lethal dose, Neuroprotection, General Biochemistry, Genetics and Molecular Biology, Atropine, chemistry.chemical_compound, Artificial Intelligence, Anesthesia, medicine, Potency, General Pharmacology, Toxicology and Pharmaceutics, General Agricultural and Biological Sciences, medicine.drug, Tabun

Abstract

Summary The neuroprotective effects of a novel oxime KR-22934, the oxime K203 and obidoxime in combination with atropine in rats poisoned with tabun at a sublethal dose (200 μg/kg i.m.; 80% LD 50 ) were studied. The tabun-induced neurotoxicity was monitored at 24 h following tabun challenge using a functional observational battery and an automatic measurement of motor activity. The results indicate that all tabun-poisoned rats treated with oximes in combination with atropine were able to survive within 24 h following tabun poisoning. One tabun-poisoned rat without antidotal treatment died within 24 h. The oximes KR-22934 and K203 combined with atropine showed a similar potency to decrease tabun-induced neurotoxicity at 24 h after tabun administration while the neuroprotective efficacy of obidoxime was slightly higher. However, no oxime was able to eliminate tabun-induced neurotoxicity completely. When atropine was administered alone, negligible neuroprotective efficacy was observed. Based on the results, a novel oxime KR-22934 did not bring any improvement of the neuroprotective efficacy of antidotal treatment of acute tabun poisonings.

Published

2014

32. Entry of oxime K027 into the different parts of rat brain: Comparison with obidoxime and oxime HI-6

Author

Jiří Kassa, Filip Zemek, Kamil Kuca, and Jana Žďárová Karasová

Subjects

Obidoxime, Aché, Stereochemistry, Health, Toxicology and Mutagenesis, Central nervous system, Biomedical Engineering, Brain tissue, Pharmacology, General Biochemistry, Genetics and Molecular Biology, chemistry.chemical_compound, Artificial Intelligence, medicine, General Pharmacology, Toxicology and Pharmaceutics, Volume concentration, General Immunology and Microbiology, General Neuroscience, General Medicine, Oxime, Rat brain, Acetylcholinesterase, language.human_language, medicine.anatomical_structure, chemistry, language, General Agricultural and Biological Sciences, medicine.drug

Abstract

Acetylcholinesterase reactivators (oximes) are highly hydrophilic compounds. This factor is considered to limit their distribution through the human body, especially into the central nervous system. However, some results contradict this hypothesis and confirm low concentrations of oximes inside the CNS. This study aims to verify oxime penetration through the blood–brain barrier, and into different brain regions. It has been confirmed that oximes can penetrate the BBB after therapeutic dose administration (0.73%, 0.69%, and 0.52% corresponding to obidoxime, HI-6, and new oxime K027). Although the whole brain level of K027 seems to be lower compared with other oximes we have to keep in mind that these numbers represent only a percentage of the concentration found in plasma. So, for more adequate comparison it is essential to have a look at the actual concentration of oximes in the wet brain tissue: 106.6 ± 19.87 ng/g (K027), 49.88 ± 10.21 ng/g (obidoxime) and 86.51 ± 42.37 ng/g (HI-6), where concentration of K027 was one order of magnitude higher than obidoxime and HI-6. In spite of the fact that the distribution of oximes into the CNS is minimal and concentrations differ from section to section, reasonable reactivation should still occur.

Published

2014

33. Therapeutic efficacy of a novel bispyridinium oxime K203 and commonly used oximes (HI-6, obidoxime, trimedoxime, methoxime) in soman-poisoned male rats and mice

Author

Jiří Kassa, Jana Žd'árová Karasová, and Markéta Krejčiová

Subjects

Obidoxime, General Immunology and Microbiology, General Neuroscience, Health, Toxicology and Mutagenesis, Biomedical Engineering, General Medicine, Pharmacology, Oxime, Acetylcholinesterase, General Biochemistry, Genetics and Molecular Biology, Acute toxicity, chemistry.chemical_compound, chemistry, Artificial Intelligence, In vivo, Soman, medicine, Potency, Trimedoxime, General Pharmacology, Toxicology and Pharmaceutics, General Agricultural and Biological Sciences, medicine.drug

Abstract

The potency of a novel oxime K203 in reactivating soman-inhibited acetylcholinesterase and reducing acute toxicity of soman was compared with commonly used oximes (HI-6, obidoxime, trimedoxime, methoxime) using in vivo methods. The study determining percentage of reactivation of soman-inhibited blood and tissue acetylcholinesterase in rats showed that the potency of the oxime K203 to reactivate soman-inhibited acetycholinesterase in the peripheral compartment is slightly higher than obidoxime and trimedoxime, especially in the diaphragm, slightly lower than methoxime and markedly lower compared to the oxime HI-6. The reactivating efficacy of the oximes studied in the peripheral compartment roughly corresponds to their potency to reduce acute toxicity of soman in mice. Based on the obtained data, we can conclude that the oxime K203 is not suitable for the replacement of the oxime HI-6 for the antidotal treatment of acute soman poisoning due to its relatively low potency to counteract acute toxicity of soman.

Published

2013

34. FROM THE RESEARCH OF CHOLINESTERASE REACTIVATORS TO THE EFFECTIVE THERAPY OF ORGANOPHOSPHATE/NERVE AGENT POISONING

Author

Jiri Bajgar and Jiří Kassa

Subjects

Emergency Medical Services, Chemical Warfare Agents, Sarin, biology, business.industry, Veterinary (miscellaneous), Cholinesterase Reactivators, Organophosphate, Public Health, Environmental and Occupational Health, Pharmacology, chemistry.chemical_compound, Immunology and Microbiology (miscellaneous), chemistry, Emergency Medicine, medicine, biology.protein, business, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Nerve agent, medicine.drug, Cholinesterase

Abstract

Nerve agents belong to the most toxic organophosphates (OP) in the group of cholinesterase inhibitors. They can be used as chemical warfare agents and, they can be (and were) misused by terrorists, as happened in Matsumoto city (1994) and Tokyo subway (1995). Sarin was used in these cases. Medical protection against their effect (i.e. antidotal treatment) is of prime importance (Bajgar 2004, 2012; Marrs et al. 1996). Moreover, poisoning with OP is commonly reported internationally (Eyer 2003). Therefore, the development of more effective antidotes against intoxication with nerve agents/OP is still necessary.

Published

2012

35. Soman and VX: different effect on cellular signalling

Author

Zuzana Šinkorová, Klara Kubelkova, Jiří Kassa, Jan Österreicher, Jaroslav Pejchal, Lenka Zárybnická, Kamil Kuca, and Aleš Tichý

Subjects

General Immunology and Microbiology, biology, Enterocyte, Chemistry, General Neuroscience, Health, Toxicology and Mutagenesis, Biomedical Engineering, Computer image, General Medicine, Pharmacology, CREB, Median lethal dose, General Biochemistry, Genetics and Molecular Biology, chemistry.chemical_compound, medicine.anatomical_structure, Artificial Intelligence, Anesthesia, Toxicity, Soman, medicine, biology.protein, General Pharmacology, Toxicology and Pharmaceutics, General Agricultural and Biological Sciences, Transcription factor, Calcium signaling

Abstract

Summary The purpose of our study was to examine the early expression of p21 and activated transcription factors ATF-2, CREB, Elk-1, p53 after soman and VX poisoning, to throw light on the pathogenetic mechanism of nerve agent-induced non-specific effects. Male Wistar rats were i.m. poisoned by soman (60 μg.kg −1 ‐ 70% LD 50 ) or VX (8 μg.kg −1 ‐ 70% LD 50 ). Samples were taken 4, 24, and 72 hours after poisoning, immunohistochemically stained and phospho-ATF-2 Thr-69/71 , phospho-CREB Ser-133 , phospho-Elk-1 Ser-383 , phospho-p53 Ser-15 , and protein p21 expressions were measured using computer Image analysis in apical and cryptal enterocytes of the colon transversum. After soman poisoning, we observed an increased phospho-CREB in cryptal enterocytes 4, 24, and 72 h after poisoning, while apical enterocytes expressed increased phospho-CREB only 72 h after intoxication. Phospho-Elk-1 significantly dropped 4 and 24 h after soman poisoning in the cryptal compartment. Activation of ATF-2 and p53 and expression of p21 were not changed 4, 24, and 72 h after soman poisoning. VX poisoning did not change any of measured parameters. Soman and VX showed a different effect on cellular signalling. Soman seems to cause additional effects, which are not related to the basic mechanism of nerve agent-induced toxicity and which temporarily suppress promitotic pathways of proliferating cells and persist in cells during the differentiation process.

Published

2012

36. A comparison of the reactivating and therapeutic efficacy of the newly developed bispyridinium oxime K203 with currently available oximes, in sarin poisoned rats and mice

Author

Jana Žd'árová Karasová, Jiří Bajgar, Vendula Sepsova, and Jiří Kassa

Subjects

Obidoxime, Sarin, General Immunology and Microbiology, General Neuroscience, Health, Toxicology and Mutagenesis, Biomedical Engineering, General Medicine, Pharmacology, Oxime, Acetylcholinesterase, General Biochemistry, Genetics and Molecular Biology, Acute toxicity, chemistry.chemical_compound, chemistry, Artificial Intelligence, In vivo, medicine, Potency, Organic chemistry, Trimedoxime, General Pharmacology, Toxicology and Pharmaceutics, General Agricultural and Biological Sciences, medicine.drug

Abstract

This study compares the abilities of the newly developed bispyridinium oxime K203 with currently available oximes (HI-6, obidoxime, and trimedoxime) in the reactivation of sarin-inhibited acetylcholinesterase and the reduction of the acute toxicity of sarin. The percentage of reactivation of sarin-inhibited rat blood and tissue acetylcholinesterase was determined in vivo and it was shown that the potency of bispyridinium oxime K203 to reactivate sarin-inhibited acetylcholinesterase roughly corresponds to the relatively low reactivating efficacy of obidoxime and trimedoxime except in the diaphragm where K203 was not effective. On the other hand, the oxime HI-6 was found to be a very efficient reactivator of sarin-inhibited acetylcholinesterase in the peripheral as well as central compartment. The oxime HI-6 was able to reduce the acute toxicity of sarin by more than four times, but the other oximes studied, including K203, decreased the acute toxicity of sarin by less than three times. Based on these results, we can conclude that the reactivating and therapeutic efficacy of the oxime K203 is significantly lower compared to the oxime HI-6 and, therefore, it is not a suitable replacement for the oxime HI-6 in the antidotal treatment of acute sarin poisoning.

Published

2011

37. Evaluation of the neuroprotective efficacy of individual oxime (HI-6) and oxime mixtures (HI-6 + trimedoxime, HI-6 + K203) in tabun-poisoned rats

Author

Sandra Tesařová, Jana Žďárová Karasová, and Jiří Kassa

Subjects

General Immunology and Microbiology, business.industry, General Neuroscience, Health, Toxicology and Mutagenesis, Biomedical Engineering, Neurotoxicity, Signs and symptoms, General Medicine, Pharmacology, Oxime, medicine.disease, Neuroprotection, General Biochemistry, Genetics and Molecular Biology, Atropine, chemistry.chemical_compound, chemistry, Artificial Intelligence, medicine, Trimedoxime, General Pharmacology, Toxicology and Pharmaceutics, General Agricultural and Biological Sciences, business, medicine.drug, Tabun

Abstract

The ability of the oxime HI-6 to reduce tabun-induced acute neurotoxic signs and symptoms was compared with the neuroprotective efficacy of two combinations of oximes (HI-6 + trimedoxime, HI-6 + K203) using a functional observational battery. Tabun-induced neurotoxicity and the neuroprotective effects of HI-6 alone, and HI-6 combined with trimedoxime or K203, in rats poisoned with tabun at a sublethal dose (200 μg/kg i.m.; 80% of LD50 value), were monitored by the functional observational battery at 24 hours following tabun challenge. The results indicate that both oxime mixtures tested, combined with atropine are able to allow tabun-poisoned rats to survive for 24 hours following tabun challenge, while one non-treated tabun poisoned rat and one tabun-poisoned rat treated with the oxime HI-6 alone combined with atropine, died within 24 hours following tabun challenge. The oxime HI-6 alone, as well as both oxime mixtures combined with atropine, were able to decrease tabun-induced neurotoxicity in the case of sublethal poisonings, but they did not eliminate all tabun-induced acute neurotoxic signs and symptoms. Their ability to reduce tabun-induced acute neurotoxcicity was almost the same, regardless of type of antidotal treatment. Thus, the tested combinations of oximes were not able to increase the neuroprotective effectiveness of the antidotal treatment of acute tabun poisonings compared to the individual oxime.

Published

2009

38. Inhibition of blood cholinesterases by nerve agents in vitro

Author

Jiří Kassa, Josef Fusek, Vaclav Blaha, Jiří Bajgar, Daniel Jun, Kamil Kuca, Jiří Cabal, and Jana Žďárová Karasová

Subjects

Sarin, General Immunology and Microbiology, biology, Chemistry, General Neuroscience, Health, Toxicology and Mutagenesis, Biomedical Engineering, General Medicine, Pharmacology, Rat blood, General Biochemistry, Genetics and Molecular Biology, In vitro, chemistry.chemical_compound, Artificial Intelligence, In vivo, Soman, medicine, biology.protein, General Pharmacology, Toxicology and Pharmaceutics, General Agricultural and Biological Sciences, Blood stream, Nerve agent, medicine.drug, Cholinesterase

Abstract

The bimolecular rate constants (ka) of inhibition were determined for cholinesterase in rat blood in vivo and three nerve agents in vitro. They were in the range of 105-106 M.min -1 with the highest value for VX (ka = 8.92 × 106), the next highest for soman (ka = 3.22 × 106) and the lowest for sarin (ka = 0.39 × 106), respectively. The inhibition rate is the same in vitro and in vivo; when the real inhibition in vivo and in vitro is compared, it is possible to assess the concentration of the nerve agent present in the blood stream. When administered intramuscularly it is about 70% of the dose administered.

Published

2009

39. Toxic Effects of Sarin in Rats at Three Months Following Single or Repeated Low-Level Inhalation Exposure

Author

Koupilová M, Jiří Kassa, Herink J, Miloš Tichý, Miroslav Pecka, Zuzana Krocova, and Jiří Bajgar

Subjects

Pharmacology, Inhalation exposure, Sarin, chemistry.chemical_compound, chemistry, Inhalation, business.industry, Health, Toxicology and Mutagenesis, Toxicity, Medicine, Toxicology, business

Published

2008

40. A Comparison of the Potency of the Oxime HLö-7 and Currently Used Oximes (HI-6, Pralidoxime, Obidoxime) to Reactivate Nerve Agent-Inhibited Rat Brain Acetylcholinesterase by in vitro Methods

Author

Jiří Kassa, Daniel Jun, Martina Hrabinova, J. Cabal, and Kamil Kuca

Subjects

Male, Obidoxime, Cholinesterase Reactivators, Sarin, Obidoxime Chloride, 050402 sociology, Pralidoxime, Antidotes, lcsh:Medicine, Cyclosarin, Pyridinium Compounds, In Vitro Techniques, Pharmacology, VX, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, 0504 sociology, Oximes, medicine, Animals, Chemical Warfare Agents, Rats, Wistar, Tabun, Nerve agent, 030203 arthritis & rheumatology, Pralidoxime Compounds, Chemistry, lcsh:R, 05 social sciences, Brain, General Medicine, Oxime, Acetylcholinesterase, Rats, Cholinesterase Inhibitors, medicine.drug

Abstract

1. The efficacy of the oxime HLö-7 and currently used oximes (pralidoxime, obidoxime, HI-6) to reactivate acetylcholinesterase inhibited by various nerve agents (sarin, tabun, cyclosarin, VX) was tested by in vitro methods. 2. Both H oximes (HLö-7, HI-6) were found to be more efficacious reactivators of sarin and VX-inhibited acetylcholinesterase than pralidoxime and obidoxime. On the other hand, their potency to reactivate tabun-inhibited acetylcholinesterase is very low and does not reach the reactivating efficacy of obidoxime. In the case of cyclosarin, the oxime HI-6 was only found to be able to sufficiently reactivate cyclosarin-inhibited acetylcholinesterase in vitro. 3. Thus, the oxime HLö-7 does not seem to be more efficacious reactivator of nerve agent-inhibited acetylcholinesterase than HI-6 according to in vitro evaluation of their reactivation potency and, therefore, it is not more suitable to be introduced for antidotal treatment of nerve agent-exposed people than HI-6.

Published

2005

41. Five oximes (K-27, K-33, K-48, BI-6 and methoxime) in comparison with pralidoxime:in vitro reactivation of red blood cell acetylcholinesterase inhibitied by paraoxon

Author

Jiří Kassa, Georg Petroianu, Kamil Kuca, and Kholoud Arafat

Subjects

Male, Obidoxime, Cholinesterase Reactivators, Erythrocytes, Pralidoxime, Stereochemistry, In Vitro Techniques, Toxicology, Paraoxon, Inhibitory Concentration 50, chemistry.chemical_compound, Oximes, medicine, Humans, Cholinesterase, Chromatography, biology, Chemistry, Organophosphate, Oxime, Acetylcholinesterase, biology.protein, Female, Cholinesterase Inhibitors, medicine.drug

Abstract

Oximes are cholinesterase reactivators of use in poisoning with organophosphorus compounds. Pralidoxime (PRX) is used clinically as an adjunct to atropine in such exposure. Clinical experience with PRX (and other oximes) is, however, disappointing and routine use has been questioned. In addition it is known that oximes are not equally effective against all existing organophosphorus compounds. There is a clear demand for ‘broad spectrum’ cholinesterase reactivators with a higher efficacy than PRX. Over the years new reactivators of cholinesterase of potential clinical utility have been developed. Their chemical structures were derived from those of existing esterase reactivators, especially pralidoxime, obidoxime and HI-6. The purpose of the study was to quantify in vitro the extent of oxime (pralidoxime, K-27, K-33, K-48, methoxime and BI-6) conferred protection, using paraoxon as an inhibitor. Paraoxon (POX), the active metabolite of parathion (O,O-diethyl-O-p-nitro-phenyl phosphorothioate) is a non-neuropathic organophosphate. Red blood cell (RBC) acetylcholinesterase (AChE) activities in whole blood were measured photometrically in the presence of different POX concentrations and the IC50 was calculated. Determinations were repeated in the presence of increasing oxime concentrations. The IC50 of POX increases with the oxime concentration in a linear manner. The calculated IC50 values were plotted against the oxime concentrations to obtain an IC50 shift curve. The slope of the shift curve (tg α) was used to quantify the magnitude of the protective effect (nm IC50 increase per µm reactivator). Based on our determinations the new K series of reactivators is far superior to pralidoxime, methoxime and BI-6, K-27 being the outstanding compound with a tg α value of 3.7 (nm IC50 increase per µm reactivator) which is ≈ 13 times the reactivator ability of PRX. In general there is an (expected) inverse relationship between the binding constant K and the slope of the IC50 shift curve (tg α) for all oximes examined. K-27 (the most protective substance judging by the tg α) has the lowest K value (highest affinity). In vivo testing of the new oximes as an organophosphate protective agent is necessary. Copyright © 2005 John Wiley & Sons, Ltd.

Published

2005

42. A comparison of protective and anticonvulsive efficacy of two prophylactic mixtures in soman-poisoned rats

Author

Ivan Samnaliev and Jiří Kassa

Subjects

General Immunology and Microbiology, business.industry, General Neuroscience, Health, Toxicology and Mutagenesis, Biomedical Engineering, General Medicine, Pharmacology, General Biochemistry, Genetics and Molecular Biology, chemistry.chemical_compound, chemistry, Artificial Intelligence, Soman, Medicine, General Pharmacology, Toxicology and Pharmaceutics, General Agricultural and Biological Sciences, business

Published

2004

43. Oximes-induced reactivation of rat brain acetylcholinesterase inhibited by VX agent

Author

Jiří Kassa and Kamil Kuca

Subjects

Male, 0301 basic medicine, Obidoxime, Cholinesterase Reactivators, Aché, Stereochemistry, Health, Toxicology and Mutagenesis, In Vitro Techniques, Toxicology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Oximes, medicine, Animals, Potency, Rats, Wistar, chemistry.chemical_classification, 030102 biochemistry & molecular biology, Brain, Organothiophosphorus Compounds, General Medicine, Oxime, Acetylcholinesterase, In vitro, language.human_language, Rats, Enzyme, chemistry, 030220 oncology & carcinogenesis, language, Cholinesterase Inhibitors, Pyridinium, medicine.drug

Abstract

A comparison of one mono- and seven bisquaternary acetylcholinesterase (AChE) reactivators of acetylcholinesterase inhibited by VX agent was performed. As a source of the acetylcholinesterase, a rat brain homogenate was taken. There were significant differences in reactivation potency of all tested oximes. The oxime TO205 seems to be the most efficacious followed by TO046, HI-6, HS-6, K027, obidoxime, MMC and 2-PAM. In addition, the results of this study showed that the reactivation potency of the tested reactivators depends on many factors-such as the number of pyridinium rings, the number of oxime groups and their position, as well as the length and the shape of linkage bridge between two pyridinium rings.

Published

2004

44. The Influence of Single or Repeated Low-Level Sarin Exposure on Immune Functions of Inbred BALB/c Mice

Author

Zuzana Krocova, Jiří Kassa, Valeria Sheshko, I. Kasalova, Lucie Ševelová, and Věra Neubauerová

Subjects

Sarin, Phagocyte, T-Lymphocytes, Spleen, Toxicology, BALB/c, Mice, chemistry.chemical_compound, Immune system, Antigens, CD, Administration, Inhalation, medicine, Animals, Chemical Warfare Agents, Nerve agent, Pharmacology, Inhalation exposure, Immunity, Cellular, Mice, Inbred BALB C, biology, General Medicine, biology.organism_classification, medicine.anatomical_structure, chemistry, Immunology, Female, Cholinesterase Inhibitors, CD8, medicine.drug

Abstract

To study the influence of single or repeated low-level sarin inhalation exposure on immune functions, inbred BALB/c mice were exposed to low clinically asymptomatic concentrations of sarin for 60 min. in the inhalation chamber. The evaluation of immune functions was carried out using phenotyping of CD3 (T-lymphocytes), CD4 (helper T-lymphocytes), CD8 (cytotoxic T-lymphocytes) and CD19 (B-lymphocytes) in the lungs, blood and spleen, lymphoproliferation of spleen cells stimulated in vitro by various mitogens (concanavalin A, lipopolysaccharides), phagocyte activity of peritoneal and alveolar macrophages, production of N-oxides by peritoneal macrophages and the measurement of the natural killer cell activity at one week after sarin exposure. The results were compared to the values obtained from control mice exposed to pure air instead of sarin. The results indicate that an asymptomatic dose of sarin is able to alter the reaction of the immune system at one week after exposure to sarin. While the number of CD3 cells in lung was significantly decreased, a slight increase in CD19 cells was observed especially in the lungs after a single sarin inhalation exposure. Lymphoproliferation was significantly decreased regardless of the mitogen and sarin concentration used and the number of low-level sarin exposures. The ability of peritoneal and alveolar macrophages to phagocyte the microbes was also decreased regardless of the number of low-level sarin exposures. The production of N-oxides by peritoneal macrophages was decreased following a single low-level sarin exposure but increased following repeated low-level sarin inhalation exposure. Nevertheless, the changes in the production of N-oxides that reflects a bactericidal activity of peritoneal macrophages was not significant. The natural killer cell activity was significantly higher in the case of inhalation exposure of mice to low concentration of sarin regardless of the number of exposures. Thus, not only organophosphorous insecticides but also nerve agents such as sarin are able to alter immune functions following a single inhalation exposure even at a dose that does not cause clinically manifested intoxication. Generally, the repeated exposure to low concentrations of sarin does not increase the alteration of immune functions compared to the single low-level sarin exposure with the exception of phagocyte activity of alveolar macrophages and natural killer cell activity.

Published

2004

45. The Influence of Sarin on Various Physiological Functions in Rats Following Single or Repeated Low-Level Inhalation Exposure

Author

Herink J, Gabriela Krejčová, F. Skopec, Jiří Kassa, Jiří Bajgar, Miloš Tichý, Miroslav Pecka, and Lucie Ševelová

Subjects

DNA Replication, Male, Nervous system, Sarin, Erythrocytes, Time Factors, Health, Toxicology and Mutagenesis, Central nervous system, Clinical Chemistry Tests, Pharmacology, Toxicology, chemistry.chemical_compound, Administration, Inhalation, medicine, Animals, Nervous System Physiological Phenomena, Chemical Warfare Agents, Nerve agent, Inhalation exposure, Inhalation Exposure, Hematologic Tests, Behavior, Animal, Dose-Response Relationship, Drug, DNA synthesis, Inhalation, Chemistry, Rats, Specific Pathogen-Free Organisms, medicine.anatomical_structure, Liver, Cholinergic, Cholinesterase Inhibitors, medicine.drug

Abstract

Long-term effects of low doses of highly toxic organophosphorus agent sarin on various hematological and biochemical markers and physiological functions were studied in rats exposed to sarin by inhalation. The results indicate that low-level sarin-exposed rats show long-term increase in studied markers of stress and decrease in synthesis of DNA de novo without the disturbance of the functions of cholinergic nervous system. Moreover, sarin at low doses is able to induce some neurotoxic effects including an increase in the excitability of central nervous system in rats at 3 mo following inhalation exposure. Relatively long-term spatial discrimination impairments in rats exposed to low-level sarin was demonstrated too. Therefore, nerve agents such as sarin seem to be harmful not only at high, clinically symptomatic doses but also at low doses without acute clinical manifestation of overstimulation of cholinergic nervous system because of long-term manifestation of alteration of neurophysiological and neurobehavioral functions in sarin-exposed rats.

Published

2004

46. A Comparison of the Ability of a New Bispyridinium Oxime—1-(4-hydroxyiminomethylpyridinium)-4-(4-carbamoylpyridinium)butane Dibromide and Currently used Oximes to Reactivate Nerve Agent-inhibited Rat Brain Acetylcholinesterase byIn VitroMethods

Author

Jiří Kassa and Kamil Kuca

Subjects

Male, Obidoxime, Cholinesterase Reactivators, Sarin, Pralidoxime, Population, Cyclosarin, Pyridinium Compounds, In Vitro Techniques, Pharmacology, Nervous System, chemistry.chemical_compound, Oximes, Drug Discovery, medicine, Animals, Rats, Wistar, education, Tabun, Nerve agent, education.field_of_study, Dose-Response Relationship, Drug, Molecular Structure, Brain, General Medicine, Oxime, Rats, Enzyme Activation, chemistry, Acetylcholinesterase, Cholinesterase Inhibitors, medicine.drug

Abstract

The efficacy of a new bispyridinium oxime 1-(4-hydroxyiminomethylpyridinium)-4-(4-carbamoylpyridinium)butane dibromide, called K048, and currently used oximes (pralidoxime, obidoxime, the oxime HI-6) to reactivate acetylcholinesterase inhibited by various nerve agents (sarin, tabun, cyclosarin, VX) was tested by in vitro methods. The new oxime K048 was found to be a more efficacious reactivator of nerve agent-inhibited acetylcholinesterase than pralidoxime (in the case of VX, tabun and cyclosarin), obidoxime (cyclosarin and tabun) and HI-6 (tabun) but it did not reach the efficacy of currently used oximes for the reactivation of acetylcholinesterase inhibited by sarin. Thus, the oxime K048 seems to be a relatively efficacious broad spectrum acetylcholinesterase reactivator and, therefore, it could be useful for the treatment of a nerve agent-exposed population if information about detection of the type of nerve agent is not available.

Published

2003

47. Neuroprotective Effects of Currently Used Antidotes in Tabun-Poisoned Rats

Author

Jiří Kassa and Gabriela Krejèová

Subjects

Pharmacology, Obidoxime, Pralidoxime, Health, Toxicology and Mutagenesis, Lethal dose, Neurotoxicity, Toxicology, medicine.disease, Acetylcholinesterase, chemistry.chemical_compound, Atropine, chemistry, Anesthesia, Soman, medicine, Tabun, medicine.drug

Abstract

The neuroprotective effects of antidotes (atropine, pralidoxime/atropine, obidoxime/atropine and HI-6/atropine mixtures) on rats poisoned with tabun at a lethal dose (220 μg/kg intramuscularly; 100% of LD50 value) were studied. The tabun-induced neurotoxicity was monitored using a functional observational battery and an automatic measurement of motor activity. The neurotoxicity of tabun was monitored at 24 hr and 7 days after tabun challenge. The results indicate that atropine alone is not able to protect the rats from the lethal effects of tabun. Three non-treated tabun-poisoned rats and one tabun-poisoned rat treated with atropine alone died within 24 hr. On the other hand, atropine combined with all tested oximes allows all tabun-poisoned rats to survive at least 7 days following tabun challenge. Obidoxime combined with atropine seems to be the most effective antidotal treatment for the elimination of tabun-induced neurotoxicity in the case of lethal poisoning among tested antidotal mixtures. The antidotal mixture consisting of atropine and HI-6 is significantly less effective than the combination of atropine with obidoxime in the elimination of tabun-induced neurotoxicity in rats at 24 hr following tabun challenge. Pralidoxime in combination with atropine appears to be practically ineffective to decrease tabun-induced neurotoxicity at 24 hours as well as 7 days following tabun poisoning. Due to its neuroprotective effects, obidoxime seems to be the most effective and most suitable oxime for the antidotal treatment of acute tabun exposure among currently used oximes. Thus, the replacement of obidoxime by a more effective acetylcholinesterase reactivator for soman poisoning, the oxime HI-6, can to a small extent diminish the neuroprotective efficacy of antidotal treatment in the case of acute tabun poisonings.

Published

2003

48. A Comparison of the Neuroprotective Efficacy of Pharmacological Pretreatment and Antidotal Treatment in Soman-Poisoned Rats

Author

Ivan Samnaliev, Jiří Kassa, and Gabriela Krejčová

Subjects

Atropine, Male, Cholinesterase Reactivators, 050402 sociology, Premedication, Antidotes, Soman, lcsh:Medicine, Pyridinium Compounds, Pharmacology, Functional observational battery, Neuroprotection, Motor activity, Biperiden, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, 0504 sociology, Oximes, medicine, Animals, Chemical Warfare Agents, Rats, Wistar, Pyridostigmine, 030203 arthritis & rheumatology, business.industry, 05 social sciences, Lethal dose, lcsh:R, Neurotoxicity, General Medicine, medicine.disease, Rats, Trihexyphenidyl, Drug Combinations, Neuroprotective Agents, chemistry, Benactyzine, PANPAL, Drug Therapy, Combination, Cholinesterase Inhibitors, business, medicine.drug, Pyridostigmine Bromide

Abstract

1. To study the influence of pharmacological pretreatment (PANPAL or pyridostigmine combined with biperiden) and antidotal treatment (the oxime HI-6 plus atropine) on soman-induced neurotoxicity, male albino rats were poisoned with a lethal dose of soman (54 (g/kg i.m.; 100% of LD50 value) and observed at 24 hours and 7 days following soman challenge. The neurotoxicity of soman was evaluated using a Functional observational battery and an automatic measurement of motor activity. 2. Pharmacological pretreatment as well as antidotal treatment were able to eliminate some of soman-induced neurotoxic effects observed at 24 hours following soman poisoning. The combination of pharmacological pretreatment (PANPAL or pyridostigmine combined with biperiden) and antidotal treatment was found to be more effective in the elimination of soman-induced neurotoxicity in rats at 24 hours following soman challenge in comparison with the administration of pharmacological pretreatment or antidotal treatment alone. To compare both pharmacological pretreatments, the combination of pyridostigmine with biperiden seems to be more efficacious to eliminate soman-induced signs of neurotoxicity than PANPAL. 3. At 7 days following soman poisoning, the combination of pharmacological pretreatment involving pyridostigmine and biperiden with antidotal treatment was only able to completely eliminate somaninduced neurotoxic signs. 4. Thus, our findings confirm that the combination of pharmacological pretreatment and antidotal treatment is able not only to protect the experimental animals from the lethal effects of soman but also to eliminate most soman-induced signs of neurotoxicity in poisoned rats. The pharmacological pretreatment containing pyridostigmine and biperiden appears to be more efficacious to eliminate soman-induced neurotoxic sings than PANPAL.

Published

2003

49. The influence of low-level sarin inhalation exposure on spatial memory in rats

Author

Jiří Kassa, Josef Vachek, and Koupilová M

Subjects

Male, medicine.medical_specialty, Sarin, Clinical Biochemistry, Toxicology, Biochemistry, Asymptomatic, Behavioral Neuroscience, chemistry.chemical_compound, Memory, Internal medicine, Administration, Inhalation, medicine, Animals, Memory disorder, Maze Learning, Biological Psychiatry, Volume concentration, Pharmacology, Inhalation exposure, Inhalation, business.industry, Cognitive disorder, medicine.disease, Rats, Endocrinology, chemistry, Anesthesia, Toxicity, Cholinesterase Inhibitors, medicine.symptom, business

Abstract

To study the influence of low-level sarin exposure on cognitive functions, the rats were exposed to three various low concentrations of sarin (Levels 1-3) for 60 min in the inhalation chamber. In addition, one group of rats was exposed to Level 2 of sarin repeatedly. Testing of cognitive functions was carried out using the Y-maze evaluating learning and spatial memory. The correct averse behavior of sarin-exposed rats in the Y-maze was tested several times within 6 weeks following sarin inhalation exposure to look for any cognitive impairments. The results were compared to the Y-maze performance of control rats exposed to pure air instead of sarin. While a subtle and short-term deficiency in the Y-maze performance was observed in rats exposed to the Levels 1 and 2 of sarin, the exposure to the Level 3 of sarin caused a significant decrease in the Y-maze performance for a relatively long time. Similar sarin-induced spatial memory impairments were demonstrated in rats exposed repeatedly to the Level 2. A decrease in the Y-maze performance was observed until the end of the third week following the last exposure to sarin. Thus, our findings confirm that both nonconvulsive symptomatic and clinically asymptomatic concentrations of sarin can cause relatively long-term memory impairments in sarin-poisoned rats when the rats are exposed to clinically asymptomatic sarin concentration repeatedly.

Published

2001

50. Long Term Effects of Low-Level Sarin Inhalation Exposure on the Spatial Memory of Rats in a T-Maze

Author

Josef Vachek, Koupilová M, and Jiří Kassa

Subjects

Sarin, 050402 sociology, lcsh:Medicine, Asymptomatic, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Spatial memory, 0504 sociology, medicine, Volume concentration, Cholinesterase, 030203 arthritis & rheumatology, Inhalation exposure, Single exposure, biology, 05 social sciences, lcsh:R, Cognition, General Medicine, Low-level inhalation exposure, T-maze, chemistry, Anesthesia, biology.protein, Rat, medicine.symptom, Psychology

Abstract

To study the influence of low-level sarin exposure on cognitive functions, male albino Wistar rats were exposed to three various low concentrations of sarin (LEVEL 1–3) for 60 minutes in the inhalation chamber. Testing of cognitive functions was carried out using the T-maze evaluating learning and spatial memory. The behavior of sarin-exposed rats in the T-maze was tested several times within five weeks following sarin inhalation exposure to look for any cognitive impairments. The alteration of cognition was evaluated by using a method studying memory elicitation in response to appetitive motivation in a multiple T-maze. 2. Statistically significant, short-term deficiency in the T-maze performance was observed in rats exposed to symptomatic (LEVEL 3) as well as clinically asymptomatic concentration (LEVEL 2) of sarin. The repeated exposure of rats to clinically asymptomatic dose of sarin (LEVEL 2R) did not change the effect of lowlevel sarin exposure on spatial memory compared to the single exposure to the same dose of sarin. 3. Thus, sarin is able to influence the cognitive functions (e.g. spatial memory) even at low doses that do not cause clinically manifested intoxication following the inhalation exposure. Nevetheless, the alteration of spatial memory lasts for a short time only, in contrast with the severe sarin poisoning.

Published

2001