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Influence of Experimental End Point on the Therapeutic Efficacy of Essential and Additional Antidotes in Organophosphorus Nerve Agent-Intoxicated Mice

J. Kassa, CM. Timperley, M. Bird, AC. Green, JEH. Tattersall

Kassa, Jiri
Autor Kassa, Jiri ORCID Department of Toxicology and Military Pharmacy, Faculty of Military Health Sciences, University of Defence, 60200 Brno, Czech Republic
Timperley, Christopher M
Autor Timperley, Christopher M Chemical, Biological and Radiological Division, Defence Science and Technology Laboratory (DSTL), Salisbury SP4 0JQ, UK
Bird, Mike
Autor Bird, Mike Chemical, Biological and Radiological Division, Defence Science and Technology Laboratory (DSTL), Salisbury SP4 0JQ, UK
Green, A Christopher
Autor Green, A Christopher Chemical, Biological and Radiological Division, Defence Science and Technology Laboratory (DSTL), Salisbury SP4 0JQ, UK
Tattersall, John E H
Autor Tattersall, John E H Chemical, Biological and Radiological Division, Defence Science and Technology Laboratory (DSTL), Salisbury SP4 0JQ, UK

Toxics. 2022 ; 10 (4) : . [pub] 20220415

ISSN 2305-6304
Medvik
Zdroj

Jazyk angličtina Země Švýcarsko

Typ dokumentu časopisecké články

Perzistentní odkaz https://www.medvik.cz/link/bmc22017368

Grantová podpora
Long-term organization development plan - Medical Aspects of Weapons of Mass Destruction Ministry of Defence

Online Plný text

NLK Directory of Open Access Journals od 2013
PubMed Central od 2015
Europe PubMed Central od 2015
ProQuest Central od 2013-01-01
Open Access Digital Library od 2013-01-01
ROAD: Directory of Open Access Scholarly Resources od 2013

PubMed 35448453
DOI 10.3390/toxics10040192
Knihovny.cz E-zdroje

Publikační typ
časopisecké články MeSH

The therapeutic efficacy of treatments for acute intoxication with highly toxic organophosphorus compounds, called nerve agents, usually involves determination of LD50 values 24 h after nerve agent challenge without and with a single administration of the treatment. Herein, the LD50 values of four nerve agents (sarin, soman, tabun and cyclosarin) for non-treated and treated intoxication were investigated in mice for experimental end points of 6 and 24 h. The LD50 values of the nerve agents were evaluated by probit-logarithmical analysis of deaths within 6 and 24 h of i.m. challenge of the nerve agent at five different doses, using six mice per dose. The efficiency of atropine alone or atropine in combination with an oxime was practically the same at 6 and 24 h. The therapeutic efficacy of the higher dose of the antinicotinic compound MB327 was slightly higher at the 6 h end point compared to the 24 h end point for soman and tabun intoxication. A higher dose of MB327 increased the therapeutic efficacy of atropine alone for sarin, soman and tabun intoxication, and that of the standard antidotal treatment (atropine and oxime) for sarin and tabun intoxication. The therapeutic efficacy of MB327 was lower than the oxime-based antidotal treatment. To compare the 6 and 24 h end points, the influence of the experimental end point was not observed, with the exception of the higher dose of MB327. In addition, only a negligible beneficial impact of the compound MB327 was observed. Nevertheless, antinicotinics may offer an additional avenue for countering poisoning by nerve agents that are difficult to treat, and synthetic and biological studies towards the development of such novel drugs based on the core bispyridinium structure or other molecular scaffolds should continue.

Chemical Biological and Radiological Division Defence Science and Technology Laboratory Salisbury SP4 0JQ UK

Department of Toxicology and Military Pharmacy Faculty of Military Health Sciences University of Defence 60200 Brno Czech Republic

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