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地乐酚在人胎盘中的胎盘转运和代谢。

Transplacental transfer and metabolism of diuron in human placenta.

机构信息

Faculty of Health Sciences, School of Pharmacy/Toxicology, University of Eastern Finland, P.O. BOX 1627, FI-70211, Kuopio, Finland.

Faculty of Health Sciences, School of Pharmacy/Toxicology, University of Eastern Finland, P.O. BOX 1627, FI-70211, Kuopio, Finland.

出版信息

Toxicol Lett. 2018 Oct 1;295:307-313. doi: 10.1016/j.toxlet.2018.07.012. Epub 2018 Jul 20.

Abstract

Diuron is a broad-spectrum phenylurea derived herbicide which is commonly used across the globe. Diuron is toxic to the reproductive system of animals and carcinogenic to rat urothelium, and recently found to be genotoxic in human cells. In in vivo, it is metabolized predominately into 3-(3,4-dichlorophenyl)-1-methyl urea (DCPMU) in humans and 3-(3, 4-dichlorophenyl)urea (DCPU) in animals. Information on diuron toxicokinetics and related toxicity in human placenta is absent. We have investigated the toxicokinetics of diuron in ex vivo human placental perfusion and in in vitro human placental microsomes and human trophoblastic cancer cells (BeWo). Diuron crossed human placenta readily in placental perfusion. Furthermore, diuron was metabolized into DCPMU in perfused placenta and in in vitro incubations using microsomes from placentas of smokers. In incubations with placental microsomes from non-smokers, and in BeWo cells, metabolism to DCPMU was detected but only with the highest used diuron concentration (100 μM). Diuron metabolism was inhibited upon addition of α-naphthoflavone, a CYP1A1 inhibitor, underscoring the role of CYP1A1 in the metabolism. In conclusion, it is evident that diuron crosses human placenta and diuron can be metabolized in the placenta to a toxic metabolite via CYP1A1. This implicates in vivo fetal exposure to diuron if pregnant women are exposed to diuron, which may result in fetotoxicity.

摘要

敌草隆是一种广泛使用的苯脲类除草剂,在全球范围内都有使用。敌草隆对动物的生殖系统有毒性,对大鼠尿路上皮有致癌性,最近还被发现对人类细胞具有遗传毒性。在体内,它主要在人类中代谢为 3-(3,4-二氯苯基)-1-甲基脲(DCPMU),在动物中代谢为 3-(3,4-二氯苯基)脲(DCPU)。关于敌草隆在人胎盘内的毒代动力学和相关毒性的信息尚不清楚。我们已经研究了敌草隆在离体人胎盘灌注和体外人胎盘微粒体和人滋养层癌细胞(BeWo)中的毒代动力学。敌草隆在胎盘灌注中很容易穿过人胎盘。此外,在灌注胎盘和使用来自吸烟者胎盘的微粒体进行的体外孵育中,敌草隆代谢为 DCPMU。在用来自不吸烟者的胎盘微粒体和 BeWo 细胞进行的孵育中,检测到代谢为 DCPMU,但仅在使用的最高敌草隆浓度(100 μM)下。加入 CYP1A1 抑制剂α-萘黄酮后,敌草隆的代谢被抑制,这突显了 CYP1A1 在代谢中的作用。总之,很明显敌草隆穿过人胎盘,并且敌草隆可以在胎盘内通过 CYP1A1 代谢为有毒代谢物。这意味着如果孕妇接触敌草隆,胎儿会接触到敌草隆,如果接触到胎儿,可能会导致胎儿毒性。

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