In vivo genotoxicity testing strategies: Report from the 8th International Workshop on Genotoxicity Testing (IWGT).

IF 2.3 4区 医学 Q3 ENVIRONMENTAL SCIENCES Environmental and Molecular Mutagenesis Pub Date : 2023-11-09 DOI:10.1002/em.22578
Carol Beevers, Yoshifumi Uno, Krista Meurer, Shuichi Hamada, Kiyohiro Hashimoto, David Kirkland, Matthew J LeBaron, Frank Le Curieux, Ludovic Le Hegarat, Hans-Joerg Martus, Kenichi Masumura, Wakako Ohyama, Daniel J Roberts, Marie Vasquez, James Whitwell, Kristine L Witt
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引用次数: 1

Abstract

The in vivo working group (WG) considered three topics: acceptable maximum doses for negative erythrocyte micronucleus (MN) tests, validation status of MN assays in non-hematopoietic tissues, and nuisance factors in the comet assay. The WG reached agreement on many issues, including: negative erythrocyte MN studies should be acceptable if dosing is conducted to Organisation for Economic Co-operation and Development (OECD) test guideline (TG) 474 recommendations and if sufficient bone marrow exposure is demonstrated; consensus on the evidence required to demonstrate "sufficient" exposure was not reached. The liver MN test using six-week-old rats is sufficiently validated to develop an OECD TG, but the impact of animal age warrants additional study. Ki-67 is a reliable marker for cellular proliferation in hepatocytes. The gastrointestinal tract MN test is useful for detecting poorly absorbed or rapidly degraded aneugens, and for genotoxic metabolites formed in the colon. Although current validation data are insufficient to support the development of an OECD TG, the methodologies are sufficient to consider as an appendix to OECD TG474. Comparison of comet assay results to laboratory historical control data (HCD) should not be used in data evaluation, unless the HCD distribution is demonstrated to be stable and the predominant source of HCD variation is due to animal, not study, factors. No universally acceptable negative control limit for any tissue was identified. Methodological differences in comet studies can result in variable data interpretations; more data are required before best practice recommendations can be made. Hedgehogs alone are unreliable indicators of cytotoxicity and additional investigations into cytotoxicity markers are required.

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体内基因毒性测试策略:第八届国际基因毒性测试研讨会报告。
体内工作组审议了三个主题:红细胞微核阴性试验的可接受最大剂量;非造血组织中MN测定的验证状态;彗星试验中的干扰因素。工作组在许多问题上达成了一致,包括:如果按照经合组织测试指南(TG)474的建议给药,并且证明有足够的骨髓暴露,则红细胞MN阴性研究应是可接受的;对于证明“充分”暴露所需的证据没有达成共识。使用六周大鼠进行的肝脏MN测试已充分验证,可以产生OECD TG,但动物年龄的影响值得进一步研究。Ki-67是肝细胞增殖的可靠标志物。胃肠道MN测试可用于检测吸收不良或快速降解的非整倍体,以及结肠中形成的遗传毒性代谢物。尽管目前的验证数据不足以支持经合组织TG474的制定,但这些方法足以作为经合组织TG473的附录。彗星试验结果与实验室历史对照数据(HCD)的比较不应用于数据评估,除非HCD分布被证明是稳定的,并且HCD变化的主要来源是动物因素,而不是研究因素。没有发现任何组织的普遍可接受的阴性对照限值。彗星研究的方法差异可能导致数据解释的变化;在提出最佳实践建议之前,还需要更多的数据。单独的刺猬是不可靠的细胞毒性指标,需要对细胞毒性标志物进行额外的研究。这篇文章受版权保护。保留所有权利。
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来源期刊
CiteScore
5.40
自引率
10.70%
发文量
52
审稿时长
12-24 weeks
期刊介绍: Environmental and Molecular Mutagenesis publishes original research manuscripts, reviews and commentaries on topics related to six general areas, with an emphasis on subject matter most suited for the readership of EMM as outlined below. The journal is intended for investigators in fields such as molecular biology, biochemistry, microbiology, genetics and epigenetics, genomics and epigenomics, cancer research, neurobiology, heritable mutation, radiation biology, toxicology, and molecular & environmental epidemiology.
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Investigation of mutagenicity of styrene in tumor target and non-target tissues of transgenic Big Blue® mice. Issue Information AOP report: Development of an adverse outcome pathway for deposition of energy leading to abnormal vascular remodeling Issue Information Absence of genotoxicity following pulmonary exposure to metal oxides of copper, tin, aluminum, zinc, and titanium in mice
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