4.6 Article

Interspecies differences in cytochrome P450-mediated metabolism of neonicotinoids among cats, dogs, rats, and humans

COMPARATIVE BIOCHEMISTRY AND PHYSIOLOGY C-TOXICOLOGY & PHARMACOLOGY (2021)

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Journal

COMPARATIVE BIOCHEMISTRY AND PHYSIOLOGY C-TOXICOLOGY & PHARMACOLOGY
Volume 239, Issue -, Pages -

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.cbpc.2020.108898

Keywords

Neonicotinoids; Cytochrome P450; Species variations; In vitro microsomal assay

Categories

Biochemistry & Molecular Biology Endocrinology & Metabolism Toxicology Zoology

Funding

  1. Ministry of Education, Culture, Sports, Science, and Technology of Japan [16H0177906, 18K1984708, 18KK028708, JPMXS0420100620, 17K2003807, 18H0413208, 17KK0009]
  2. foundation of JSPS Bilateral Open Partnership Joint Research Projects [JPJSBP120209902]
  3. Environment Research and Technology Development Fund of the Environmental Restoration and Conservation Agency of Japan [SII1/3-2, 4RF-1802/18949907]
  4. Soroptimist Japan Foundation
  5. Nakajima Foundation
  6. Sumitomo Foundation
  7. Nihon Seimei Foundation
  8. Act Beyond Trust
  9. Japan Prize Foundation
  10. Triodos Foundation
  11. JST/JICA
  12. SATREPS (Science and Technology Research Partnership for Sustainable Development) [JPMJSA1501]
  13. Hokkaido University School of Veterinary Medicine Wise/Leading Travel and Subsistence grant

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The study revealed differences in metabolites of neonicotinoids and CYP activities among common pet species, humans, and rats. The results showed that the CYP-mediated neonicotinoid metabolism varied depending on species and each neonicotinoid. Further studies should focus on identifying the differences in hepatic metabolism of neonicotinoids in these species using recombinant CYP enzymes.
Neonicotinoid insecticides are used for agricultural and non-agricultural purposes worldwide. Pets are directly exposed to neonicotinoids in veterinary products and through environmental contamination. Cytochrome P450 (CYP) is among the most significant xenobiotic metabolizing enzymes that oxidizes several chemicals, including neonicotinoids. However, CYP activities and metabolite compositions of neonicotinoid metabolites are unknown in most domesticated pet species. Our objectives were to reveal the differences in metabolites of neonicotinoids (imidacloprid, clothianidin, and acetamiprid) and CYP activities among common pet species (cats and dogs), humans, and rats. The results indicated that the CYP-mediated neonicotinoid metabolism was different depending on species and each neonicotinoid. Among these four species, the kinetics of imidacloprid metabolism indicated that rats have the highest rate of oxidation of imidacloprid to 4OH-imidacloprid, while the greatest enzyme kinetics of imidacloprid metabolism to 5OH-imidacloprid were found in rats and humans. Clothianidin was rapidly metabolized to 1-methyl-3-nitroguanidine and dm-clothianidin in rats, but cats and humans showed the lowest formation of dm-clothianidin. CYP activities in metabolism of acetamiprid to dm-acetamiprid and N-acetyl-acetamiprid were determined to be significantly higher in humans compared to other species. However, further studies should be targeted at identifying the differences in hepatic metabolism of neonicotinoids in these species using recombinant CYP enzymes.

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