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Literature DB >> 30363160

Lack of human relevance for procymidone's developmental toxicity attributable to species difference in its kinetics and metabolism.

Yoshitaka Tomigahara¹, Hirokazu Tarui¹, Masayoshi Matsui¹, Motohiro Kurosawa¹, Satoshi Kawamura¹, Naohiko Isobe¹.

Abstract

The agricultural fungicide procymidone can cause external genitalia abnormalities in rats but not monkeys or rabbits. To investigate the relevance of developmental findings in rats to humans, we conducted in vitro plasma protein binding studies, in vitro metabolism (biotransformation) studies using liver S9 fractions and hepatocytes, and in vivo metabolism and excretion studies using chimeric mice with humanized hepatocytes. On the basis of these results, we concluded that the metabolic and excretion profiles of procymidone in humans are similar to those in monkeys and rabbits but differ from those in rats. From the findings of this and previous studies, we judge the developmental toxicity potential of procymidone to be very low in humans.

Entities: Chemical Disease Species

Keywords: biotransformation; chimeric mouse; developmental toxicity; human relevance; procymidone; species differences

Year: 2018 PMID： 30363160 PMCID： PMC6140727 DOI： 10.1584/jpestics.D17-085

Source DB: PubMed Journal: J Pestic Sci ISSN： 1348-589X Impact factor: 1.519

12 in total

1. Determination of the hepatocellularity number for human, dog, rabbit, rat and mouse livers from protein concentration measurements.

Authors: Anna-Karin Sohlenius-Sternbeck
Journal: Toxicol In Vitro Date: 2006-06-29 Impact factor: 3.500

2. Comparative hepatotoxicity of a herbicide, epyrifenacil, in humans and rodents by comparing the dynamics and kinetics of its causal metabolite.

Authors: Kohei Matsunaga; Satoki Fukunaga; Jun Abe; Hayato Takeuchi; Sachiko Kitamoto; Yoshitaka Tomigahara
Journal: J Pestic Sci Date: 2021-11-20 Impact factor: 2.529

2 in total

Lack of human relevance for procymidone's developmental toxicity attributable to species difference in its kinetics and metabolism.

1. Determination of the hepatocellularity number for human, dog, rabbit, rat and mouse livers from protein concentration measurements.

2. Normal organ weights in men: part II-the brain, lungs, liver, spleen, and kidneys.

3. In vivo drug metabolism model for human cytochrome P450 enzyme using chimeric mice with humanized liver.

4. Normal Organ Weights in Women: Part II-The Brain, Lungs, Liver, Spleen, and Kidneys.

5. Expression of human phase II enzymes in chimeric mice with humanized liver.

6. Expression of human cytochromes P450 in chimeric mice with humanized liver.

7. The affinity of procymidone to androgen receptor in rats and mice.

8. Metabolism of procymidone derivatives in female rats.

Review 9. Application of chimeric mice with humanized liver for predictive ADME.

10. Change trends of organ weight background data in sprague dawley rats at different ages.

1. Researches on the evaluation of pesticide safety in humans using a pharmacokinetic approach.

2. Comparative hepatotoxicity of a herbicide, epyrifenacil, in humans and rodents by comparing the dynamics and kinetics of its causal metabolite.