Literature DB >> 15720138

Identification of aldehyde oxidase as the neonicotinoid nitroreductase.

Ryan A Dick1, David B Kanne, John E Casida.   

Abstract

Imidacloprid (IMI), the prototypical neonicotinoid insecticide, is used worldwide for crop protection and flea control on pets. It is both oxidatively metabolized by cytochrome P450 enzymes and reduced at the nitroguanidine moiety by a previously unidentified cytosolic "neonicotinoid nitroreductase", the subject of this investigation. Two major metabolites are detected on incubation of IMI with rabbit liver cytosol: the nitrosoguanidine (IMI-NO) and the aminoguanidine (IMI-NH2). Three lines of evidence identify the molybdo-flavoenzyme aldehyde oxidase (AOX, EC 1.2.3.1) as the neonicotinoid nitroreductase. First, classical AOX electron donor substrates (benzaldehyde, 2-hydroxypyrimidine, and N-methylnicotinamide) dramatically increase the rate of formation of IMI metabolites. Allopurinol and diquat are also effective electron donors, while NADPH and xanthine are not. Second, AOX inhibitors (potassium cyanide, menadione, and promethazine) inhibit metabolite formation when N-methylnicotinamide is utilized as an electron donor. Without the addition of an electron donor, rabbit liver cytosol reduces IMI only to IMI-NO at a slow rate. This reduction is also inhibited by potassium cyanide, menadione, and promethazine, as well as by additional AOX inhibitors, cimetidine and chlorpromazine. Finally, IMI nitroreduction by AOX is sensitive to an aerobic atmosphere, but to a much lesser extent than cytochrome P450 2D6. Large species differences are observed in the IMI nitroreductive activity of liver cytosol. While rabbit and monkey (Cynomolgus) give the highest levels of total metabolite formation, human, mouse, cow, and rat also metabolize IMI rapidly. In contrast, dog, cat, and chicken liver cytosols do not reduce IMI at appreciable rates. AOX, as a neonicotinoid nitroreductase, may limit the persistence of IMI, and possibly other neonicotinoids, in mammals.

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Year:  2005        PMID: 15720138     DOI: 10.1021/tx049737i

Source DB:  PubMed          Journal:  Chem Res Toxicol        ISSN: 0893-228X            Impact factor:   3.739


  8 in total

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Journal:  Comp Biochem Physiol C Toxicol Pharmacol       Date:  2018-02-03       Impact factor: 3.228

Review 2.  A review of antiviral drugs and other compounds with activity against feline herpesvirus type 1.

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3.  Enzymes and inhibitors in neonicotinoid insecticide metabolism.

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Journal:  J Agric Food Chem       Date:  2009-06-10       Impact factor: 5.279

4.  Enzyme Kinetics, Pharmacokinetics, and Inhibition of Aldehyde Oxidase.

Authors:  Erickson M Paragas; Kanika Choughule; Jeffrey P Jones; John T Barr
Journal:  Methods Mol Biol       Date:  2021

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6.  Association of Gallbladder Mucocele Histologic Diagnosis with Selected Drug Use in Dogs: A Matched Case-Control Study.

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Review 7.  An Overview on the Effect of Neonicotinoid Insecticides on Mammalian Cholinergic Functions through the Activation of Neuronal Nicotinic Acetylcholine Receptors.

Authors:  Jean-Noël Houchat; Alison Cartereau; Anaïs Le Mauff; Emiliane Taillebois; Steeve H Thany
Journal:  Int J Environ Res Public Health       Date:  2020-05-06       Impact factor: 3.390

8.  Acute effects of the imidacloprid metabolite desnitro-imidacloprid on human nACh receptors relevant for neuronal signaling.

Authors:  Udo Kraushaar; Marcel Leist; Dominik Loser; Karin Grillberger; Maria G Hinojosa; Jonathan Blum; Yves Haufe; Timm Danker; Ylva Johansson; Clemens Möller; Annette Nicke; Susanne H Bennekou; Iain Gardner; Caroline Bauch; Paul Walker; Anna Forsby; Gerhard F Ecker
Journal:  Arch Toxicol       Date:  2021-10-10       Impact factor: 5.153

  8 in total

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