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通过比较除草剂双唑草腈的致毒代谢物的动力学和动态学,研究其在人和啮齿动物中的比较肝毒性。

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

作者信息

Matsunaga Kohei, Fukunaga Satoki, Abe Jun, Takeuchi Hayato, Kitamoto Sachiko, Tomigahara Yoshitaka

机构信息

Environmental Health Science Laboratory, Sumitomo Chemical Co., Ltd., 3-1-98 Kasugade-Naka, Konohana-ku, Osaka 554-8558, Japan.

出版信息

J Pestic Sci. 2021 Nov 20;46(4):333-341. doi: 10.1584/jpestics.D21-026.

Abstract

A new herbicide, epyrifenacil (S-3100), inhibits protoporphyrinogen oxidase (PPO) in plants. Repeated administration of epyrifenacil in laboratory animals led to some toxicological changes related to PPO inhibition, , hepatotoxicity caused by porphyrin accumulation and anemia caused by the inhibition of heme biosynthesis. studies revealed that an ester-cleaved metabolite, S-3100-CA, is predominant in mammals, exhibits PPO-inhibitory activity, and thus is the cause of epyrifenacil-induced toxicity. To assess the human risk, the effects of species differences on the dynamics (PPO inhibition) and kinetics (liver uptake) of epyrifenacil were evaluated separately. The results of assays revealed an approximately tenfold weaker inhibition of PPO by S-3100-CA in humans than in rodents and six- to thirteen-fold less hepatic uptake of S-3100-CA in humans than in mice. Finally, it was suggested that humans are less sensitive to the toxicity of epyrifenacil than are rodents, although further mechanistic research is highly anticipated.

摘要

一种新型除草剂——环丙酰草胺(S - 3100)可抑制植物中的原卟啉原氧化酶(PPO)。在实验动物中反复施用环丙酰草胺会导致一些与PPO抑制相关的毒理学变化,即卟啉积累引起的肝毒性以及血红素生物合成抑制导致的贫血。研究表明,一种酯裂解代谢产物S - 3100 - CA在哺乳动物中占主导地位,具有PPO抑制活性,因此是环丙酰草胺诱导毒性的原因。为评估人类风险,分别评估了物种差异对环丙酰草胺动力学(PPO抑制)和动力学(肝脏摄取)的影响。检测结果显示,S - 3100 - CA对人类PPO的抑制作用比对啮齿动物弱约十倍,且人类肝脏对S - 3100 - CA的摄取比对小鼠少六至十三倍。最后,研究表明人类对环丙酰草胺毒性的敏感性低于啮齿动物,不过仍迫切期待进一步的机制研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/495c/8640676/c9e6e51ee02c/jps-46-4-D21-026-figure01.jpg

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