OXIMES OF αω‐DIQUATERNARY ALKANE SALTS AS ANTIDOTES TO ORGANOPHOSPHATE ANTICHOLINESTERASES

Abstract

Sixteen compounds of the general structure {HON: CH.C₃H₄N⁺.[CH₂]_n.R⁺}2Br⁻ have been synthesized in which the position of the oxime group in the pyridine ring, the second charged group R⁺ and the number of methylene groups between the charged atoms have been varied. The rate at which these compounds reactivate Cholinesterase inhibited by ethyl pyrophosphate has been studied and a number have been found which are more active than 2-hydroxyiminomethyl-N-methylpyridinium methanesulphonate. Since considerable variation in structure was found among those compounds which are better reactivators than the latter, the concept that 2-hydroxyiminomethyl-N-methylpyridinium salts are unique in their ability to fit the surface of the inhibited enzyme is no longer tenable. The reactivating power of these oximes correlated well with their ability, when given in conjunction with atropine, to save the lives of mice poisoned by ethyl pyrophosphate. The most effective compounds, NN′-trimethylenebis-(4-hydroxyiminomethylpyridinium bromide) and NN′-hexamethylenebis(2-hydroxyiminomethylpyridinium bromide), contained a further oxime group in R⁺, but the second oxime group was not essential for high activity. These new oximes were also superior in saving the lives of mice poisoned with sarin (isopropyl methylphosphonofluoridate), but the improvement was not as dramatic as when the mice were poisoned with ethyl pyrophosphate. The toxicity of the compounds varied with both n and R⁺ and was unrelated to the therapeutic potency.