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Neonicotinoid Metabolism: Compounds, Substituents, Pathways, Enzymes, Organisms, and Relevance

机译:新烟碱代谢:化合物,取代基,途径,酶,生物和相关性

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Neonicotinoids are one of the three principal insecticide chemotypes. The seven major commercial neonicotinoids are readily biodegraded by metabolic attack at their N-heterocyclylmethyl moiety, heterocyclic or acyclic spacer, and N-nitroimine, nitromethylene, or N-cyanoimine tip. Phase 1 metabolism is largely dependent on microsomal CYP4S0 isozymes with situ selectivity in hydroxylation, desaturation, dealkylation, sulfoxidation, and nitro reduction. Cytosolic aldehyde oxidase is a nitroreductase for some neonicotinoids. Phase II metabolism involves methylation, acetylation, and formation of glucurpnide, glucoside, amino acid, and sulfate- and glutathione-derived conjugates. Some neonicotinoids act as proinsecticides with metabolism to more potent nicotinic agonists. Pest resistance is more commonly due to synergist-reversible CYP4S0 detoxification than to nAChR mutants or variants. Metabolites in some cases contribute to mammalian hepatotoxicity and carcinogenesis and in others to enhanced plant vigor and stress shields. These relationships explain much of neonicotinoid comparative toxicology and provide the basis for continued and improved safety and effectiveness of this chemotype.
机译:新烟碱是三种主要杀虫剂化学型之一。七种主要的商业类烟碱在它们的N-杂环基甲基部分,杂环或无环间隔基团以及N-硝基亚胺,硝基亚甲基或N-氰基亚胺末端易受代谢攻击而被生物降解。 1期代谢在很大程度上取决于微粒体CYP4SO同工酶,在羟基化,去饱和,脱烷基,硫氧化和硝基还原中具有原位选择性。胞质醛氧化酶是某些新烟碱类的硝基还原酶。 II期代谢涉及甲基化,乙酰化以及葡糖苷,葡糖苷,氨基酸以及硫酸盐和谷胱甘肽衍生的结合物的形成。一些新烟碱类药物可作为杀虫剂,具有对更有效的烟碱激动剂代谢的作用。与nAChR突变体或变体相比,害虫抗性更常见是由于增效剂可逆的CYP4S0解毒作用。在某些情况下,代谢物会导致哺乳动物的肝毒性和致癌作用,而在另一些情况下,则会增强植物的活力和抵御压力。这些关系解释了新烟碱类药物的比较毒理学,并为该化学型的持续和改进的安全性和有效性提供了基础。

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