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Transgenic rat models for mutagenesis and carcinogenesis

机译:转基因大鼠致突变和致癌模型

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摘要

Rats are a standard experimental animal for cancer bioassay and toxicological research for chemicals. Although the genetic analyses were behind mice, rats have been more frequently used for toxicological research than mice. This is partly because they live longer than mice and induce a wider variety of tumors, which are morphologically similar to those in humans. The body mass is larger than mice, which enables to take samples from organs for studies on pharmacokinetics or toxicokinetics. In addition, there are a number of chemicals that exhibit marked species differences in the carcinogenicity. These compounds are carcinogenic in rats but not in mice. Such examples are aflatoxin B1 and tamoxifen, both are carcinogenic to humans. Therefore, negative mutagenic/carcinogenic responses in mice do not guarantee that the chemical is not mutagenic/carcinogenic to rats or perhaps to humans. To facilitate research on in vivo mutagenesis and carcinogenesis, several transgenic rat models have been established. In general, the transgenic rats for mutagenesis are treated with chemicals longer than transgenic mice for more exact examination of the relationship between mutagenesis and carcinogenesis. Transgenic rat models for carcinogenesis are engineered mostly to understand mechanisms underlying chemical carcinogenesis. Here, we review papers dealing with the transgenic rat models for mutagenesis and carcinogenesis, and discuss the future perspective.
机译:大鼠是用于癌症生物测定和化学毒理学研究的标准实验动物。尽管遗传分析落后于小鼠,但大鼠比小鼠更常用于毒理学研究。部分原因是它们的寿命比小鼠长,并且会诱发多种肿瘤,这些肿瘤的形态与人类相似。体重大于小鼠,因此可以从器官中取样进行药代动力学或毒代动力学研究。另外,许多化学物质在致癌性方面表现出明显的物种差异。这些化合物对大鼠有致癌作用,但对小鼠却没有。这样的例子是黄曲霉毒素B1和他莫昔芬,两者均对人类致癌。因此,小鼠的诱变/致癌反应阴性不能保证该化学物质不会对大鼠或人类造成诱变/致癌。为了促进体内诱变和致癌作用的研究,已经建立了几种转基因大鼠模型。通常,用于诱变的转基因大鼠的化学处理时间长于转基因小鼠,以更精确地检查诱变与癌变之间的关系。转基因大鼠致癌模型主要用于了解化学致癌机制。在这里,我们审查有关诱变和致癌转基因大鼠模型的论文,并讨论未来的前景。

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