首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Evaluation of dichloroacetic acid for carcinogenicity in genetically modified Tg.AC hemizygous and p53 haploinsufficient mice.
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Evaluation of dichloroacetic acid for carcinogenicity in genetically modified Tg.AC hemizygous and p53 haploinsufficient mice.

机译:在转基因的Tg.AC半合子和p53单倍体不足小鼠中评估二氯乙酸的致癌性。

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There has been considerable interest in the use of genetically modified mice for detecting potential environmental carcinogens. For this reason, the National Toxicology Program has been evaluating Tg.AC hemizygous and p53 haploinsufficient mice as models to detect potential carcinogens. It was reasoned that these mouse models might also prove more effective than standard rodent models in evaluating the numerous disinfection byproducts that are found in low concentrations in drinking water. Dichloroacetic acid (DCA) is one of the most frequently found disinfection byproducts and DCA has been consistently shown to cause hepatocellular tumors in rats and mice in standard rodent studies. Tg.AC hemizygous and p53 haploinsufficient mice were exposed in the drinking water to DCA for up to 41 weeks. In a second study Tg.AC mice were subjected to dermal DCA exposure for up to 39 weeks. Increased incidences and severity of cytoplasmic vacuolization of hepatocytes were seen in the p53 mice, but there was no evidence of carcinogenic activity at exposures of up to 2000 mg/l in the drinking water. Increased incidences and severity of cytoplasmic vacuolization of hepatocytes were seen in the drinking water study with Tg.AC mice and a modest non-dose-related increase in pulmonary adenomas was observed in males exposed to 1000 mg/l in the drinking water. Dermal exposure up to 500 mg/kg for 39 weeks resulted in increased dermal papillomas at the site of application in Tg.AC mice. No significant increase in papillomas under the same study conditions was seen in the 26-week study. For DCA under these study conditions, the p53 and Tg.AC mice appear less sensitive to hepatocarcinogenesis than standard rodent models. These results suggest caution for the use of Tg.AC and p53 mice to screen unknown chemicals in drinking water for potential carcinogenicity.
机译:使用基因修饰的小鼠来检测潜在的环境致癌物已引起相当大的兴趣。因此,美国国家毒理学计划一直在评估Tg.AC半合子小鼠和p53单倍体不足小鼠作为检测潜在致癌物的模型。有理由认为,这些小鼠模型在评估饮用水中低浓度下发现的多种消毒副产物方面也可能比标准啮齿动物模型更有效。二氯乙酸(DCA)是最常见的消毒副产物之一,在标准啮齿动物研究中,DCA一直被证明可引起大鼠和小鼠的肝细胞肿瘤。 Tg.AC半合子和p53单倍体不足的小鼠在饮用水中暴露于DCA长达41周。在第二项研究中,Tg.AC小鼠经历了皮肤DCA暴露长达39周。在p53小鼠中发现肝细胞胞浆空泡的发生率和严重性增加,但是在饮用水中暴露量高达2000 mg / l时,没有致癌活性的证据。在Tg.AC小鼠的饮用水研究中发现肝细胞胞浆空泡的发生率和严重性增加,并且在饮用水中暴露于1000 mg / l的雄性中,肺腺瘤出现了与剂量无关的适度增加。在Tg.AC小鼠中,皮肤暴露至500 mg / kg达39周导致真皮乳头状瘤发生部位增加。在为期26周的研究中,在相同的研究条件下,乳头状瘤没有明显增加。对于这些研究条件下的DCA,p53和Tg.AC小鼠对肝癌发生的敏感性似乎不如标准啮齿动物模型。这些结果表明,谨慎使用Tg.AC和p53小鼠筛查饮用水中未知的化学物质是否具有潜在的致癌性。

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