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小鼠多器官碱性单细胞凝胶电泳试验:对国际癌症研究机构(IARC)和美国国家毒理学计划(NTP)评估的30种芳香胺的检测结果

The alkaline single cell gel electrophoresis assay with mouse multiple organs: results with 30 aromatic amines evaluated by the IARC and U.S. NTP.

作者信息

Sasaki Y F, Fujikawa K, Ishida K, Kawamura N, Nishikawa Y, Ohta S, Satoh M, Madarame H, Ueno S, Susa N, Matsusaka N, Tsuda S

机构信息

Laboratory of Genotoxicity, Faculty of Chemical and Biological Engineering, Hachinohe National College of Technology, Tamonoki Uwanotai 16-1, Hachinohe, Aomori 039-11, Japan.

出版信息

Mutat Res. 1999 Mar 15;440(1):1-18. doi: 10.1016/s1383-5718(99)00006-6.

Abstract

The genotoxicity of 30 aromatic amines selected from IARC (International Agency for Research on Cancer) groups 1, 2A, 2B and 3 and from the U.S. NTP (National Toxicology Program) carcinogenicity database were evaluated using the alkaline single cell gel electrophoresis (SCG) (Comet) assay in mouse organs. We treated groups of four mice once orally at the maximum tolerated dose (MTD) and sampled stomach, colon, liver, kidney, bladder, lung, brain, and bone marrow 3, 8 and 24 h after treatment. For the 20 aromatic amines that are rodent carcinogens, the assay was positive in at least one organ, suggesting a high predictive ability for the assay. For most of the SCG-positive aromatic amines, the organs exhibiting increased levels of DNA damage were not necessarily the target organs for carcinogenicity. It was rare, in contrast, for the target organs not to show DNA damage. Organ-specific genotoxicity, therefore, is necessary but not sufficient for the prediction of organ-specific carcinogenicity. For the 10 non-carcinogenic aromatic amines (eight were Ames test-positive and two were Ames test-negative), the assay was negative in all organs studied. In the safety evaluation of chemicals, it is important to demonstrate that Ames test-positive agents are not genotoxic in vivo. Chemical carcinogens can be classified as genotoxic (Ames test-positive) and putative non-genotoxic (Ames test-negative) carcinogens. The alkaline SCG assay, which detects DNA lesions, is not suitable for identifying non-genotoxic carcinogens. The present SCG study revealed a high positive response ratio for rodent genotoxic carcinogens and a high negative response ratio for rodent genotoxic non-carcinogens. These results suggest that the alkaline SCG assay can be usefully used to evaluate the in vivo genotoxicity of chemicals in multiple organs, providing for a good assessment of potential carcinogenicity.

摘要

使用碱性单细胞凝胶电泳(SCG)(彗星试验)对从国际癌症研究机构(IARC)第1、2A、2B和3组以及美国国家毒理学计划(NTP)致癌性数据库中选取的30种芳香胺在小鼠器官中的遗传毒性进行了评估。我们以最大耐受剂量(MTD)对每组4只小鼠进行一次口服给药,并在给药后3、8和24小时采集胃、结肠、肝脏、肾脏、膀胱、肺、脑和骨髓样本。对于20种啮齿动物致癌物芳香胺,该试验在至少一个器官中呈阳性,表明该试验具有较高的预测能力。对于大多数SCG阳性芳香胺,显示DNA损伤水平升高的器官不一定是致癌作用的靶器官。相比之下,靶器官不显示DNA损伤的情况很少见。因此,器官特异性遗传毒性对于预测器官特异性致癌性是必要的,但不是充分的。对于10种非致癌性芳香胺(8种Ames试验阳性,2种Ames试验阴性),该试验在所有研究器官中均为阴性。在化学品的安全性评估中,证明Ames试验阳性的试剂在体内无遗传毒性很重要。化学致癌物可分为遗传毒性(Ames试验阳性)和推定非遗传毒性(Ames试验阴性)致癌物。检测DNA损伤的碱性SCG试验不适用于鉴定非遗传毒性致癌物。目前的SCG研究显示,啮齿动物遗传毒性致癌物的阳性反应率较高,啮齿动物遗传毒性非致癌物的阴性反应率较高。这些结果表明,碱性SCG试验可有效地用于评估化学品在多个器官中的体内遗传毒性,从而对潜在致癌性进行良好评估。

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