利用灵敏的、与 OECD 一致的设计,解决历来不一致的艾姆斯试验阴性/啮齿动物致癌性阳性 N-亚硝胺问题。

IF 2.5 4区 医学 Q3 GENETICS & HEREDITY
Mutagenesis Pub Date : 2024-11-01 DOI:10.1093/mutage/geae027
Dean N Thomas, John W Wills, Mark Burman, Abbie N Williams, Danielle S G Harte, Ruby A Buckley, Mike W Urquhart, Anne-Sophie Bretonnet, Benjamin Jeffries, Angela T White, James S Harvey, Jonathan R Howe, Anthony M Lynch
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引用次数: 0

摘要

体外细菌逆向突变(Ames)试验对于评估药物杂质的诱变性至关重要。对于 N-亚硝胺(NAs),历史数据表明,对于该化学类别的某些成员,阿姆斯试验的结果与其相关的啮齿动物致癌性结果并不相关。这导致监管机构不再认为仅通过经合组织(OECD)认可的阿姆斯试验(标准或增强)得出的阴性结果足以评估药物产品中作为杂质存在的 NAs 的潜在致癌风险。因此,需要进行大量的后续体内试验,以确定NA杂质的潜在致突变性和遗传毒性致癌性(即超出ICH M7指南对非NA杂质的规定)。我们之前已经证明,烷基亚硝胺的诱变性可以通过适当设计的、与 OECD 一致的埃姆斯试验进行检测,并确定了对检测灵敏度贡献最大的条件。这种经合组织调整的埃姆斯试验设计用于评估七种亚硝胺,即(甲基(新戊基)亚硝胺、N-甲基-N-亚硝基-2-丙胺、N-亚硝基二异丙基胺、双(2-甲氧基乙基)亚硝基胺、N-亚硝基-N-甲基-4-氟苯胺、二亚硝基乙胺丁醇、(R,R)-和一亚硝基咖啡碱),这些物质在以往的阿姆斯试验中呈阴性,但在啮齿动物致癌性研究中呈阳性。在经合组织(OECD)统一的阿姆斯试验中,所有七种 NA 都被证明具有诱变性,因此在阿姆斯试验与啮齿动物致癌性的相关性方面,这些化合物不应再被视为不一致(假阴性)。这些结果证实了 OECD 阿姆斯试验在检测 NA 诱变性方面的灵敏度,并进一步证明了它在 ICH M7 框架中的重要地位,该框架用于评估药品中的诱变杂质,以限制潜在的致癌风险。此外,我们还提供了 1-环戊基-4-亚硝基哌嗪的数据,表明它可以作为合适的阳性对照,进一步提高阿姆斯检测法对 NA 类化学物质灵敏度的信心。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Resolution of Historically Discordant Ames Test Negative / Rodent Carcinogenicity Positive N-nitrosamines using a Sensitive, OECD-aligned Design.

The in vitro Bacterial Reverse Mutation (Ames) Test is crucial for evaluating the mutagenicity of pharmaceutical impurities. For N-nitrosamines (NAs) historical data indicated that for certain members of this chemical class the outcomes of the Ames Test did not correlate with their associated rodent carcinogenicity outcomes. This has resulted in negative outcomes in an OECD aligned Ames Test alone (standard or enhanced) no longer being considered sufficient by regulatory authorities to assess potential carcinogenic risk of NAs if present as impurities in drug products. Consequently, extensive follow-up in vivo testing can be required to characterise the potential mutagenicity and genotoxic carcinogenicity of NA impurities (i.e., beyond that defined in the ICH M7 guideline for non-NA impurities). We previously demonstrated that the mutagenicity of alkyl-nitrosamines can be detected by the appropriately designed, OECD aligned Ames Test and identified those conditions that contributed most to assay sensitivity. This OECD aligned Ames Test design was used to assess seven NAs, i.e. (methyl(neopentyl)nitrosamine, N-methyl-N-nitroso-2-propanamine, N-nitrosodiisopropylamine, bis(2-methoxyethyl)nitrosoamine, N-nitroso-N-methyl-4-fluoroaniline, dinitrosoethambutol, (R,R)- and mononitrosocaffeidine) that were reported to be negative in historical Ames Tests but positive in rodent carcinogenicity studies. All seven of the NAs were demonstrated to be mutagenic in the OECD aligned Ames test and therefore these compounds should no longer be considered as discordant (false negatives) with respect to the correlation of the Ames Test and rodent carcinogenicity. These results confirm the sensitivity of the OECD aligned Ames Test for the detection of NA mutagenicity and provides further support of its pivotal placement within the ICH M7 framework for the assessment of mutagenic impurities in pharmaceuticals to limit potential carcinogenic risk. In addition, we present data for 1-cyclopentyl-4-nitrosopiperazine, that indicates it could serve as a suitable positive control to provide further confidence in the sensitivity of the Ames Test for the NA chemical class.

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来源期刊
Mutagenesis
Mutagenesis 生物-毒理学
CiteScore
5.90
自引率
3.70%
发文量
22
审稿时长
6-12 weeks
期刊介绍: Mutagenesis is an international multi-disciplinary journal designed to bring together research aimed at the identification, characterization and elucidation of the mechanisms of action of physical, chemical and biological agents capable of producing genetic change in living organisms and the study of the consequences of such changes.
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