Oxidative Bioactivation of
            <i>S</i>
            -Alkyl Phosphorothiolate Pesticides: Stereospecificity of Profenofos Insecticide Activation

Wing, Keith D.; Glickman, Andrew H.; Casida, John E.

doi:10.1126/science.6849116

Cited by 91 publications

(54 citation statements)

References 12 publications

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“…Methamidophos, however, contrary to other S-alkylphosphorothiolates, is not activated to more potent AChE inhibitors by mouse liver microsomes (Wing et al 1982) or by hen liver microsomes (our unpublished results).…”

Section: Discussionmentioning

confidence: 69%

Interaction of methamidophos with hen and human acetylcholinesterase and neuropathy target esterase

et al. 1991

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Methamidophos causes acute cholinergic toxicity in several species, including man, and organophosphate-induced delayed polyneuropathy which has been reported in man but not in the hen. Acetylcholinesterase (AChE) and neuropathy target esterase (NTE) are thought to be the molecular targets of acute and delayed toxicity, respectively. The rate constants of inhibition (ka) and reactivation (k + 3) of human and hen brain AChE and NTE by methamidophos resolved optical isomers are here reported. NTE inhibition was progressive and irreversible. Human and hen NTE ka (M-1.m-1) for D-(+) methamidophos was 88 and 59, respectively, and for L-(-) methamidophos 3.2 and 3.0, respectively. AChE spontaneously reactivates after inhibition. D-(+) methamidophos 10(-3).ka (M-1.m-1) for human and hen AChE was 0.24 and 0.13; 10(3).k+3 (m-1) was 0.83 and 0.69, respectively. L-(-) Methamidophos 10(-3).ka (M-1.m-1) for human and hen AChE was 5.7 and 2.8, whereas 10(3).k+3 (m-1) was 6.50 and 1.52, respectively. L-(-)-Inhibited AChE reactivated to about 60% for human and 30% for hen enzymes, respectively. D-(+)-Inhibited AChE reactivated to about 10-20% for both species. Maximal reactivation occurred within 4-6 h when a plateau was reached. The larger and faster reactivation of human AChE inhibited in vitro by L-(-) methamidophos suggests that a corresponding effect might be possible in vivo and therefore explain, in part, the relatively higher susceptibility of man to delayed polyneuropathy induced by racemic methamidophos which occurs, however, with doses always causing severe cholinergic toxicity.

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Section: Discussionmentioning

confidence: 69%

Interaction of methamidophos with hen and human acetylcholinesterase and neuropathy target esterase

et al. 1991

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“…This is due to the preferential sulfoxidation of (−)-profenofos in vivo, resulting in a metabolite that is up to 34 times more inhibitory to AChE Fosthiazate pk1 > pk2 > pk4 > pk3 CD and LPD Daphnia magna Acute toxicity; in vitro inhibition of electric eel acetylcholinesterase not stereoselective; has 4 stereoisomers due to presence of P and C chiral centers; stereoisomers identified based on elution order on Chiralpak ® AD column [35] Chloramidophos pk3 > pk2 > pk1 > pk4 CD Daphnia magna Acute toxicity; has 4 stereoisomers due to presence of P and C chiral centers; stereoisomers identified based on elution order on Chiralpak ® AD column [36] a CD: circular dichroism detector; LPD: laser polarimeter detector. [67]. The same study also showed the preferential detoxification of (+)-profenofos.…”

Section: Enantioselective Insecticidal Activitymentioning

confidence: 61%

“…Like profenofos, methamidophos also contains a sulfur substituent to the chiral P in its structure, and may be subject to similar bioactivation processes as previously described here for profenofos [5,67] (Fig. 1).…”

Section: Enantioselective Non-target Toxicitymentioning

confidence: 75%

Chirality of organophosphorus pesticides: Analysis and toxicity

Nillos

Gan

Schlenk

2010

Journal of Chromatography B

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“…Esterases responsible for detoxification of temephos in this study may be inhibited by DEF with or without induction by BZT. Many phosphorothiolates, including DEF, can be converted to highly potent esterase inhibitors by P450 catalysis (Hur et al, 1992;Wing et al, 1983). If this is the case, BZT may induce P450s that carry out oxidative bioactivation of DEF.…”

Section: Discussionmentioning

confidence: 97%

Induction of microsomal cytochrome P450s by tire‐leachate compounds, habitat components of Aedes albopictus mosquito larvae

Suwanchaichinda

Brattsten

2002

Arch Insect Biochem Physiol

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Benzothiazole (BZT) and its derivatives are the major leachate compounds of automobile tires, the principal breeding habitat of Aedes albopictus, particularly in the United States. Effects of the compounds on insecticide toxicity, and activities and expression of microsomal cytochrome P450s (P450s) in the mosquito larvae were examined. Mosquito larvae were more tolerant to carbaryl, rotenone, and temephos when they were pre-exposed to tire-leachate compounds, particularly BZT. There was no change in toxicity from the aldrin treatment by BZT. The effect of BZT was reversed when a P450 inhibitor, piperonyl butoxide, was applied in admixture with the insecticides. Microsomes from BZT-treated larvae had increased peroxidation activity of tetramethylbenzidine. This correlated with increased intensity of SDS-PAGE protein bands corresponding to molecular weights of 59 and 62 kD, which were detected as heme-containing proteins, a characteristic of P450s. The results suggest that BZT induces P450s, which detoxify insecticides and thus cause insecticide tolerance in the mosquito larvae. Arch.

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Oxidative Bioactivation of S -Alkyl Phosphorothiolate Pesticides: Stereospecificity of Profenofos Insecticide Activation

Cited by 91 publications

References 12 publications

Interaction of methamidophos with hen and human acetylcholinesterase and neuropathy target esterase

Interaction of methamidophos with hen and human acetylcholinesterase and neuropathy target esterase

Chirality of organophosphorus pesticides: Analysis and toxicity

Induction of microsomal cytochrome P450s by tire‐leachate compounds, habitat components of Aedes albopictus mosquito larvae

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