Biochemical basis of selective disease controlling activity of mepanipyrim

Miura, Ichiro; Maeno, Shinichiro

doi:10.1584/jpestics.g06-27

Cited by 2 publications

(2 citation statements)

References 17 publications

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“…Several analogues (e.g., cyprodinil and Pyrimethanil) are also in agricultural use. Their mode of action is (a) inhibition of specific amino acid biosynthesis and/or (b) inhibition of protein sequestration ,, . The major mode of action of mepanipyrim is proposed to be the inhibition of pathogenicity-related protein secretion .…”

Section: Introductionmentioning

confidence: 99%

“…Their mode of action is (a) inhibition of specific amino acid biosynthesis and/or (b) inhibition of protein sequestration ,, . The major mode of action of mepanipyrim is proposed to be the inhibition of pathogenicity-related protein secretion . Mepanipyrim is quite a safe compound (acute oral LD 50 > 5000 mg kg −1 , rat) suggesting the least harmful effects on human or animal health, and several toxicological studies were reported − , .…”

Section: Introductionmentioning

confidence: 99%

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Metabolism of a Fungicide Mepanipyrim by Soil Fungus Cunninghamella elegans ATCC36112

Zhu

Keum

Yang

et al. 2010

J. Agric. Food Chem.

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Mepanipyrim is a fungicide against several plant pathogens. However, no metabolic details have been established in fungi, which is the most important biomass in the natural environment. Cunninghamella elegans is a well-known fungal species with its strong resemblance to the mammalian xenobiotic metabolism. In this study, the detailed metabolic pathways of mepanipyrim were investigated with C. elegans. Approximately 87% of mepanipyrim was removed within 12 h with concomitant accumulation of nine metabolites. Structures of the metabolites were fully or tentatively identified with GC-MS and (1)H NMR. To determine the possible role of representative oxidative enzymes, piperonyl butoxide and methimazole were treated, and the kinetic responses of mepanipyrim and its metabolites were measured. Dose-dependent inhibition of metabolism was observed with piperonyl butoxide, while methimazole also inhibited the metabolism less effectively. The results indicate the possible involvement of cytochrome P450 and flavin-dependent monooxygenase in mepanipyrim metabolism. Comprehensive metabolic pathways can be deduced from the detailed analysis of metabolite profiles in control and inhibitor assays.

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