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Effect of metoclopramide and ranitidine on the inhibition of human AChE by VX in vitro

✍ Scribed by A. Bartling; H. Thiermann; L. Szinicz; F. Worek


Publisher
John Wiley and Sons
Year
2005
Tongue
English
Weight
111 KB
Volume
25
Category
Article
ISSN
0260-437X

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✦ Synopsis


The repeated misuse of highly toxic organophosphorus-type (OP) chemical warfare agents ('nerve agents') emphasizes the necessity for the development of effective medical countermeasures. The standard treatment with atropine and acetylcholinesterase (AChE) reactivators ('oximes') is considered to be ineffective with certain nerve agents due to low oxime efficacy. Therefore, pretreatment with carbamate-type compounds, e.g. pyridostigmine, was recommended to improve antidotal efficacy. Recently, the clinically used reversible AChE inhibitors metoclopramide (MCP) and ranitidine (RAN) were shown to exhibit some protective effect against the OP pesticide paraoxon in vitro and in vivo. The present study was undertaken to investigate a potential protective effect of MCP and RAN against inhibition of human AChE by the nerve agent VX (O-ethyl S-[2-(diisopropylamino)ethyl)methylphosphonothioate). Hemoglobin-free human erythrocyte membranes were incubated with various, human relevant MCP (0.5-2 µ µ µ µ µM) and RAN (0.5-5 µ µ µ µ µM) concentrations starting 1 min before addition of VX (1-40 nM). Both compounds failed to increase VX IC 50 values. In addition, human AChE was incubated with higher than human relevant therapeutic concentrations of MCP (1 µ µ µ µ µM-1 mM) and RAN (1 µ µ µ µ µM-2.0 mM) and inhibited by 40 nM VX. At concentrations higher than 100 µ µ µ µ µM MCP and RAN caused a concentration dependent increase of residual AChE activity 15 min after addition of VX. These data indicate that MCP and RAN may be ineffective in protecting human AChE against inhibition by the nerve agent VX at human relevant doses.


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