首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Genetic toxicity assessment: employing the best science for human safety evaluation part III: the comet assay as an alternative to in vitro clastogenicity tests for early drug candidate selection.
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Genetic toxicity assessment: employing the best science for human safety evaluation part III: the comet assay as an alternative to in vitro clastogenicity tests for early drug candidate selection.

机译:遗传毒性评估:采用人类安全性评估的最佳科学方法,第三部分:彗星测定法可替代体外裂解法,用于早期候选药物的选择。

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摘要

Early screening of drug candidates for genotoxicity typically includes an analysis for mutagenicity in bacteria and for clastogenicity in cultured mammalian cells. In addition, in recent years, an early assessment of photogenotoxicity potential has become increasingly important. Also, for screening purposes, expert computer systems can be used to identify structural alerts. In cases where structural alerts are identified, mutagenicity testing limited to bacteria can be conducted. The sequence of computer-aided analysis and limited testing using bacteria allows for screening a comparatively large number of drug candidates. In contrast, considerably more resources, in terms of supplies, technical time, and the amount of a test substance needed, are required when screening for clastogenic activity in mammalian cells. In addition, the relatively large percentage of false positive results for rodent carcinogenicity associated with clastogenicity assays is of considerable concern. As a consequence, mammaliancell-based alternatives to clastogenicity assays are needed for early screening of mammalian genotoxicity. The comet assay is a relatively fast, simple, and sensitive technique for the analysis of DNA damage in mammalian cells. This assay seems especially useful for screening purposes because false positives associated with excessive toxicity appear to occur less frequently, only relatively small amounts of a test compound are needed, and certain steps of the test procedure can be automated. Therefore, the in vitro comet assay is proposed as an alternative to cytogenetic assays in early genotoxicity/photogenotoxicity screening of drug candidates.
机译:对具有遗传毒性的候选药物进行早期筛选通常包括对细菌的致突变性和培养的哺乳动物细胞的致裂性进行分析。另外,近年来,对光遗传毒性潜力的早期评估变得越来越重要。同样,出于筛选目的,可以使用专家计算机系统来识别结构警报。在确定结构警报的情况下,可以进行仅限于细菌的致突变性测试。使用细菌进行计算机辅助分析和有限测试的顺序可以筛选出相对大量的候选药物。相反,在筛选哺乳动物细胞中的致胶裂活性时,需要大量的资源,包括供应,技术时间和所需测试物质的数量。另外,与杀灭力试验相关的啮齿动物致癌性假阳性结果的相对较大的百分比是相当令人关注的。因此,为早期筛查哺乳动物的遗传毒性,需要用基于哺乳动物细胞的方法代替裂解性测定法。彗星测定法是一种相对快速,简单且灵敏的技术,用于分析哺乳动物细胞中的DNA损伤。该测定法似乎对于筛选目的特别有用,因为与过度毒性相关的假阳性似乎不那么频繁地发生,仅需要相对少量的测试化合物,并且测试程序的某些步骤可以自动化。因此,在候选药物的早期遗传毒性/光遗传毒性筛选中,提出了体外彗星试验作为细胞遗传学试验的替代方法。

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