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首页> 外文期刊>Toxicology and Applied Pharmacology >Induction of glutathione S-transferase placental form positive foci in liver and epithelial hyperplasia in urinary bladder, but no tumor development in male Fischer 344 rats treated with monomethylarsonic acid for 104 weeks.
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Induction of glutathione S-transferase placental form positive foci in liver and epithelial hyperplasia in urinary bladder, but no tumor development in male Fischer 344 rats treated with monomethylarsonic acid for 104 weeks.

机译:谷胱甘肽S-转移酶胎盘的诱导在肝脏和膀胱上皮增生中形成阳性灶,但在用单甲基ar磺酸处理104周的雄性Fischer 344大鼠中无肿瘤发展。

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摘要

The carcinogenicity of monomethylarsonic acid (MMA(V)), a major metabolite of inorganic arsenics in human and experimental animals, was investigated in male Fischer 344 rats. A total of 129 rats at 10 weeks of age were randomly divided into three groups and received drinking water containing MMA(V) at doses of 0 (Control), 50, and 200 ppm ad libitum for 104 weeks. No significant differences were found between the control and the MMA(V)-treated groups regarding clinical signs, mortality, hematological, and serum biochemistry findings. Quantitative analysis of glutathione S-transferase placental form (GST-P) positive foci in liver revealed a significant increase of numbers and areas in the 200 ppm MMA(V)-treated group. In the urinary bladder MMA(V) induced simple hyperplasia and significantly elevated the proliferating cell nuclear antigen (PCNA)-positive index in the urothelium. A variety of tumors developed in rats of all groups, including the controls, but all were histologically similar to those known to occur spontaneously in F344 rats and there were no significant differences among the groups. Thus, it could be concluded that, under the present experimental conditions, MMA(V) induced lesions in the liver and urinary bladder, but did not cause tumor development in male F344 rats even after 2 years exposure.
机译:在雄性Fischer 344大鼠中研究了单甲基ar磺酸(MMA(V))是人体和实验动物中无机砷的主要代谢产物的致癌性。将总共​​129只10周龄的大鼠随机分为三组,并随机接受0(对照组),50和200 ppm剂量的含MMA(V)的饮用水,持续104周。在对照组和MMA(V)治疗组之间,在临床体征,死亡率,血液学和血清生物化学方面没有发现显着差异。肝脏中谷胱甘肽S-转移酶胎盘形式(GST-P)阳性灶的定量分析显示,在200 ppm MMA(V)治疗组中,数目和面积显着增加。在膀胱中,MMA(V)引起简单的增生,并显着提高了上皮细胞中增殖细胞核抗原(PCNA)阳性指数。各组大鼠(包括对照组)均出现了多种肿瘤,但其组织学与已知在F344大鼠中自发发生的肿瘤相似,各组之间无显着差异。因此,可以得出结论,在当前的实验条件下,MMA(V)诱导了肝脏和膀胱的损伤,但是即使暴露2年后,它也不会引起雄性F344大鼠的肿瘤发展。

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