In vitro reactivation potency of some acetylcholinesterase reactivators against sarin- and cyclosarin-induced inhibitions

Kuča, Kamil; Cabal, Jiřı́; Jun, Daniel; Kassa, Jiřı́; Bartošová, Lucie; Kunešová, Gabriela

doi:10.1002/jat.1065

Cited by 18 publications

(14 citation statements)

References 19 publications

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“…The results confirm that the position of hydroxyiminomethyl groups influences the reactivation potency [30 -33]. In this case, compounds bearing oxime groups in positions 3-4 (6, 9, 12) and 3-3 (14,17,20) were almost ineffective, compounds with oxime groups in positions 2-3 (7, 10), 2-4 (8, 11), 2-2 (16, 19) and 4-4 (15,18,21) showed satisfactory reactivation ability against paraoxon-inhibited AChE. Another important factor for reactivation potency is the structure of the connecting chain as was discussed previously [14 -16].…”

Section: Resultssupporting

confidence: 69%

“…Moreover, each position of oxime on the pyridinium ring is able to reactivate another type of inhibitor. While position four is more suitable for tabun or pesticide-inhibited AChE, position two is effective against sarin, soman or VXinhibited AChE [19][20][21]. Position three has usually low efficacy due to the dissociation constant at the pH of human blood [19].…”

Section: Introductionmentioning

confidence: 99%

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Synthesis of a novel series of non-symmetrical bispyridinium compounds bearing a xylene linker and evaluation of their reactivation activity against tabun and paraoxon-inhibited acetylcholinesterase

Musílek

Holas

Kuča³

et al. 2007

Journal of Enzyme Inhibition and Medicinal Chemistry

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Section: Resultssupporting

confidence: 69%

Section: Introductionmentioning

confidence: 99%

Synthesis of a novel series of non-symmetrical bispyridinium compounds bearing a xylene linker and evaluation of their reactivation activity against tabun and paraoxon-inhibited acetylcholinesterase

Musílek

Holas

Kuča³

et al. 2007

Journal of Enzyme Inhibition and Medicinal Chemistry

Self Cite

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“…This is due to the fact that the oxime group of both newly synthesized oximes is situated in position 4. The oxime HI-6 having an oxime group in position 2 generally showed markedly higher reactivating and therapeutic efficacy against cyclosarin than other commonly used oximes (6,8,9), although the differences between the neuroprotective efficacy of the oxime HI-6 and other oximes studied are not as high in this study.…”

Section: Discussioncontrasting

confidence: 37%

“…On the other hand, the number of aldoxime groups is not so important. The oxime HI-6 has only one oxime group but it is significantly more efficacious to reactivate cyclosarin-inhibited AChE than bispyridinium oximes with two aldoxime groups, such as obidoxime, methoxime or trimedoxime (6,9). The chain linking the two quaternary nitrogens in bispyridinium oximes exerts a great influence on the reactivating and therapeutic efficacy, although this part of the oxime reactivator molecule does not play any role in the dephosphorylation process.…”

Section: Discussionmentioning

confidence: 99%

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

Kassa

Karasová

Tesarova

et al. 2008

Acta Med. (Hradec Kralove, Czech Repub.)

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Summary: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.

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“…Even the oxime HI-6 that is considered to be the best reactivator of cyclosarin-inhibited AChE (6,9,10,20,21) is not satisfactorily effective oxime for the elimination of cyclosarin-induced neurotoxic signs and symptoms due to low penetration through BBB and low reactivating efficacy in the CNS (6,22). On the other hand, it is known that the oximes may also attentuate nerve agent-induced brain insult via different mechanisms other than AChE reactivation (35).…”

Section: Discussionmentioning

confidence: 99%

A Comparison of the Neuroprotective Efficacy of Individual Oximes (Hi-6, Trimedoxime, K203) and Their Mixtures (Hi-6 + Trimedoxime, Hi-6 + K203) in Cyclosarin-Poisoned Rats

Kassa¹,

Karasová²

2011

Mil. Med. Sci. Lett.

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SummaryThe ability of three oximes (HI-6, trimedoxime, K203) to reduce cyclosarin-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. Cyclosarin-induced neurotoxicity and the neuroprotective effects of HI-6, trimedoxime or K203 alone and HI-6 combined with trimedoxime or K203 in rats poisoned with cyclosarin at a sublethal dose (80 µg/kg i.m.; 70% of LD 50 value) were monitored by the functional observational battery at 24 hours and 7 days following cyclosarin challenge. The results indicate that all types of antidotal treatment are able to survive cyclosarin-poisoned rats 7 days following cyclosarin poisoning while one non-treated cyclosarin-poisoned rats died within 24 hours following cyclosarin challenge. All three oximes alone as well as both oxime mixtures combined with atropine were able to slightly decrease cyclosarin-induced neurotoxicity in the case of sublethal poisoning but they did not eliminate all cyclosarin-induced acute neurotoxic signs and symptoms. Their ability to reduce cyclosarininduced acute neurotoxicity 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 antidotal treatment of acute cyclosarin poisoning compared to the individual oximes.

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In vitro reactivation potency of some acetylcholinesterase reactivators against sarin- and cyclosarin-induced inhibitions

Cited by 18 publications

References 19 publications

Synthesis of a novel series of non-symmetrical bispyridinium compounds bearing a xylene linker and evaluation of their reactivation activity against tabun and paraoxon-inhibited acetylcholinesterase

Synthesis of a novel series of non-symmetrical bispyridinium compounds bearing a xylene linker and evaluation of their reactivation activity against tabun and paraoxon-inhibited acetylcholinesterase

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

A Comparison of the Neuroprotective Efficacy of Individual Oximes (Hi-6, Trimedoxime, K203) and Their Mixtures (Hi-6 + Trimedoxime, Hi-6 + K203) in Cyclosarin-Poisoned Rats

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