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化学致癌物作用模式的分类框架及实用指南。

A classification framework and practical guidance for establishing a mode of action for chemical carcinogens.

作者信息

Butterworth Byron E

机构信息

Butterworth Consulting, 4820 Regalwood Dr., Raleigh, NC 27613, USA.

出版信息

Regul Toxicol Pharmacol. 2006 Jun;45(1):9-23. doi: 10.1016/j.yrtph.2006.01.011. Epub 2006 Mar 10.

Abstract

The recently released U.S. Environmental Protection Agency (U.S. EPA) Supplemental Guidance for Assessing Risk from Early Life Exposure to Carcinogens (SGAC) provides guidance to account for potential increased early life susceptibility to carcinogens that are acting via a mutagenic mode of action. While determination of the mode of carcinogenic action is central to the SGAC procedures and other regulatory risk assessments, little guidance is given as to the approaches, criteria, and nature of the evidence required to define a mutagenic mode of action. The purpose of this paper is to provide a framework along with practical guidance for the process of assigning a mode of action. Strengths, weaknesses, reliability, and choice of a test battery are discussed for select bacterial, cell culture, whole animal and human cell assays. Common confounding factors of induced pathology, cytolethality, and regenerative cell proliferation in rodent cancer bioassays are discussed along with approaches to account for these effects in assigning a mode of action and in risk assessments. Specific examples are given to illustrate the complexity in generating a data set sufficient to move from the default regulatory position of assuming a genotoxic mode of action to actually assigning a nongenotoxic mode of action. A two-part framework is proposed for assigning a mode of action. First, a weight of evidence approach is used to assess mutagenic potential based on results of genetic toxicology test systems. Second, a descriptor is assigned to classify the degree to which mutagenic activity likely played a role in the mode of action of tumor formation. This option provides a more realistic way of describing the mode of action instead of being bound by the strict genotoxic vs. nongenotoxic choices.

摘要

美国环境保护局(U.S. EPA)最近发布的《评估生命早期接触致癌物风险的补充指南》(SGAC)为考虑生命早期对通过诱变作用方式起作用的致癌物潜在易感性增加提供了指导。虽然致癌作用方式的确定是SGAC程序和其他监管风险评估的核心,但对于定义诱变作用方式所需证据的方法、标准和性质,几乎没有给出指导。本文的目的是为确定作用方式的过程提供一个框架以及实用指南。针对选定的细菌、细胞培养、全动物和人类细胞试验,讨论了测试组合的优点、缺点、可靠性和选择。讨论了啮齿动物癌症生物测定中诱导病理学、细胞致死性和再生细胞增殖的常见混杂因素,以及在确定作用方式和风险评估中考虑这些影响的方法。给出了具体例子来说明生成足以从假定遗传毒性作用方式的默认监管立场转向实际确定非遗传毒性作用方式的数据集的复杂性。提出了一个用于确定作用方式的两部分框架。首先,基于遗传毒理学测试系统的结果,采用证据权重法评估诱变潜力。其次,指定一个描述符来分类诱变活性在肿瘤形成作用方式中可能发挥作用的程度。这种选择提供了一种更现实的描述作用方式的方法,而不是受严格的遗传毒性与非遗传毒性选择的限制。

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