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44种化学物质的啮齿动物致癌性预测:结果

Prediction of rodent carcinogenicity for 44 chemicals: results.

作者信息

Ashby J, Tennant R W

机构信息

Zeneca Central Toxicology Laboratory, Alderley Park, Macclesfield, Cheshire, UK.

出版信息

Mutagenesis. 1994 Jan;9(1):7-15. doi: 10.1093/mutage/9.1.7.

Abstract

Methods by which rodent carcinogenicity can be predicted have been prospectively validated for 40 chemicals evaluated for carcinogenicity by the US National Toxicology Program. It is concluded that a chemical of unknown carcinogenicity can be predicted to be in one of three possible categories--probably carcinogenic, probably non-carcinogenic or of uncertain activity. The last category is unlikely to contain genotoxic trans-species and/or multiple-site carcinogens. The component parameters of such predictions are one or more of several aspects of chemical structure, genotoxicity and rodent toxicity. Each of these parameters requires refinement but all are developed to the point that they can be integrated to make assessment of possible carcinogenicity. Carcinogenicity tends to be overpredicted by this integrated technique, each part of which has already been simulated by computer modelling. Improvements in predictive methodology will flow from three assumptions: (i) that emphasis must be placed equally on the properties of the test chemical and the responses it elicits in tissues for which carcinogenicity is to be predicted, (ii) that the integration of different predictive technique is preferable to the exclusive use of a single technique, and (iii) that the general predictivity of any technique or combination of techniques appears to be limited to < or = 80%, imposed by inadequate knowledge, and uncertainties in the experimental evaluation and classification of carcinogenic responses for diverse chemicals. This last statement does not preclude the attainment of higher accuracy within a congeneric series of chemicals. Foreknowledge of the likely outcome of a rodent carcinogenicity bioassay is now possible and will contribute to the focusing of animal testing resources.

摘要

对于美国国家毒理学计划评估致癌性的40种化学物质,预测啮齿动物致癌性的方法已得到前瞻性验证。得出的结论是,一种未知致癌性的化学物质可被预测为处于三种可能类别之一——可能致癌、可能不致癌或活性不确定。最后一类不太可能包含遗传毒性跨物种和/或多部位致癌物。此类预测的组成参数是化学结构、遗传毒性和啮齿动物毒性等几个方面中的一个或多个。这些参数中的每一个都需要完善,但都已发展到可以整合起来以评估可能的致癌性的程度。通过这种综合技术往往会过度预测致癌性,其中每个部分都已通过计算机建模进行了模拟。预测方法的改进将源于三个假设:(i)必须同等重视受试化学物质的特性及其在要预测致癌性的组织中引发的反应,(ii)不同预测技术的整合优于单独使用单一技术,以及(iii)由于知识不足以及对各种化学物质致癌反应的实验评估和分类存在不确定性,任何技术或技术组合的一般预测性似乎都限于≤80%。最后这一说法并不排除在同类化学物质系列中获得更高的准确性。现在有可能预先知道啮齿动物致癌性生物测定的可能结果,这将有助于集中动物试验资源。

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