4.5 Article

A novel paradigm for assessing efficacies of potential antidotes against neurotoxins in mice

期刊

TOXICOLOGY LETTERS
卷 175, 期 1-3, 页码 111-117

出版社

ELSEVIER IRELAND LTD
DOI: 10.1016/j.toxlet.2007.10.001

关键词

cyanide; animal model; recovery; righting reflex; oral efficacy

资金

  1. NINDS NIH HHS [1U01NS058087-01, U01 NS058087-01, U01 NS058087] Funding Source: Medline

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Historically, antidotal potencies of cyanide antagonists were measured as increases in the experimental LD50 for cyanide elicited by the antidotes. This required the use of high doses of cyanide following pre-treatment with the putative antidote. Since IACUC guidelines at our institutions strongly discourage LD50 determinations: we developed a new test paradigm that allowed for maximal survival of cyanide-treated animals with greatly reduced numbers of animals. Symptoms of cyanide toxicity include disruption of neuromuscular coordination, i.e., the righting reflex. Therefore, to establish a dose-response curve, the times required for recovery of this righting reflex with increasing doses of cyanide were measured. A cyanide dose that disrupted this righting reflex for approximately I It with minimal deaths was then selected. Using this paradigm, the current cyanide antidotes, viz., nitrite plus thiosultate and hydroxocobalamin, as well as some potential cyanide antidotes that we developed, were evaluated pre- and postcyanide. This allowed, for the first time, the assessment of the post-cyanide effectiveness of the current antidotes against cyanide poisoning in a live animal. In addition, some prototype compounds were found to exhibit antidotal efficacy not only when injected i.p. following cyanide, but also when administered orally 30 min before cyanide. Pre-cyanide oral efficacy suggests that such compounds have the potential of being administered prophylactically before exposure to cyanide. This new test paradigm was found to be a powerful tool for assessing the efficacies of some novel antidotes against cyanide and should be equally applicable for evaluating putative antidotes for other neurotoxins. Published by Elsevier Ireland Ltd.

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