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首页> 外文期刊>Food and Chemical Toxicology: An International Journal Published for the British Industrial Biological Research >Involvement of constitutive androstane receptor in liver hypertrophy and liver tumor development induced by triazole fungicides
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Involvement of constitutive androstane receptor in liver hypertrophy and liver tumor development induced by triazole fungicides

机译:本构雄甾烷受体参与三唑类杀菌剂诱导的肝肥大和肝肿瘤的发展

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摘要

We clarified the involvement of constitutive androstane receptor (CAR) in triazole-induced liver hypertrophy and tumorigenesis using CAR-knockout (CARKO) mice. Seven-week-old male CARKO and wild-type (WT) mice were treated with 200 ppm cyproconazole (Cypro), 1500 ppm tebuconazole (Teb), or 200 ppm fluconazole (Flu) in the diet for 27 weeks after initiation by diethylnitrosamine (DEN). At weeks 4 (without DEN) and 13 (with DEN), WT mice in all treatment groups and CARKO mice in Teb group revealed liver hypertrophy with mainly Cyp2b10 and following Cyp3al1 inductions in the liver. Teb also induced Cyp4a10 in both genotypes. Cypro induced slight and duration-dependent liver hypertrophy in CARKO mice. At week 27, Cypro and Teb significantly increased eosinophilic altered foci and/or adenomas in WT mice. These proliferating lesions were clearly reduced in CARKO mice administered both compounds. The eosinophilic adenomas caused by Flu decreased in CARKO mice. The present study indicates that CAR is the main mediator of liver hypertrophy induced by Cypro and Flu, but not Teb. In contrast CAR played a crucial role in liver tumor development induced by all three triazoles. (C) 2015 Elsevier Ltd. All rights reserved.
机译:我们阐明了组成型雄烷受体(CAR)参与三唑诱导的肝脏肥大和使用CAR基因敲除(CARKO)小鼠的肿瘤发生。七周大的雄性CARKO和野生型(WT)小鼠在饮食中用200 ppm环丙康唑(Cypro),1500 ppm戊唑醇(Teb)或200 ppm氟康唑(Flu)在二乙基亚硝胺( DEN)。在第4周(无DEN)和第13周(有DEN),所有治疗组的WT小鼠和Teb组的CARKO小鼠均显示肝脏肥大,主要为Cyp2b10,随后在肝脏中诱导Cyp3al1。 Teb还可以诱导两种基因型的Cyp4a10。 Cypro诱发了CARKO小鼠轻度和持续时间依赖性的肝脏肥大。在第27周时,Cypro和Teb显着增加了WT小鼠嗜酸性改变的病灶和/或腺瘤。在给予两种化合物的CARKO小鼠中,这些增生性病变均明显减少。由流感引起的嗜酸性腺瘤在CARKO小鼠中减少。本研究表明,CAR是Cypro和Flu诱导的肝肥大的主要介质,而不是Teb。相反,CAR在所有三种三唑诱导的肝肿瘤发展中起着至关重要的作用。 (C)2015 Elsevier Ltd.保留所有权利。

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