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91种化学物质的转基因啮齿动物突变与体内彗星试验反应的比较。

A comparison of transgenic rodent mutation and in vivo comet assay responses for 91 chemicals.

作者信息

Kirkland David, Levy Dan D, LeBaron Matthew J, Aardema Marilyn J, Beevers Carol, Bhalli Javed, Douglas George R, Escobar Patricia A, Farabaugh Christopher S, Guerard Melanie, Johnson George E, Kulkarni Rohan, Le Curieux Frank, Long Alexandra S, Lott Jasmin, Lovell David P, Luijten Mirjam, Marchetti Francesco, Nicolette John J, Pfuhler Stefan, Roberts Daniel J, Stankowski Leon F, Thybaud Veronique, Weiner Sandy K, Williams Andrew, Witt Kristine L, Young Robert

机构信息

Kirkland Consulting, PO Box 79, Tadcaster LS24 0AS, UK.

US Food and Drug Administration Center for Food Safety and Applied Nutrition, College Park, MD, USA.

出版信息

Mutat Res Genet Toxicol Environ Mutagen. 2019 Mar;839:21-35. doi: 10.1016/j.mrgentox.2019.01.007. Epub 2019 Jan 18.

Abstract

A database of 91 chemicals with published data from both transgenic rodent mutation (TGR) and rodent comet assays has been compiled. The objective was to compare the sensitivity of the two assays for detecting genotoxicity. Critical aspects of study design and results were tabulated for each dataset. There were fewer datasets from rats than mice, particularly for the TGR assay, and therefore, results from both species were combined for further analysis. TGR and comet responses were compared in liver and bone marrow (the most commonly studied tissues), and in stomach and colon evaluated either separately or in combination with other GI tract segments. Overall positive, negative, or equivocal test results were assessed for each chemical across the tissues examined in the TGR and comet assays using two approaches: 1) overall calls based on weight of evidence (WoE) and expert judgement, and 2) curation of the data based on a priori acceptability criteria prior to deriving final tissue specific calls. Since the database contains a high prevalence of positive results, overall agreement between the assays was determined using statistics adjusted for prevalence (using AC1 and PABAK). These coefficients showed fair or moderate to good agreement for liver and the GI tract (predominantly stomach and colon data) using WoE, reduced agreement for stomach and colon evaluated separately using data curation, and poor or no agreement for bone marrow using both the WoE and data curation approaches. Confidence in these results is higher for liver than for the other tissues, for which there were less data. Our analysis finds that comet and TGR generally identify the same compounds (mainly potent mutagens) as genotoxic in liver, stomach and colon, but not in bone marrow. However, the current database content precluded drawing assay concordance conclusions for weak mutagens and non-DNA reactive chemicals.

摘要

已编制了一个包含91种化学物质的数据库,这些化学物质均有来自转基因啮齿动物突变试验(TGR)和啮齿动物彗星试验的已发表数据。目的是比较这两种试验检测遗传毒性的敏感性。针对每个数据集,将研究设计和结果的关键方面制成表格。大鼠的数据集比小鼠少,尤其是在TGR试验中,因此,将两个物种的结果合并进行进一步分析。在肝脏和骨髓(最常研究的组织)以及单独评估或与其他胃肠道段联合评估的胃和结肠中比较了TGR和彗星试验的反应。使用两种方法评估了每种化学物质在TGR和彗星试验中所检查组织中的总体阳性、阴性或不确定试验结果:1)基于证据权重(WoE)和专家判断的总体判定,以及2)在得出最终组织特异性判定之前,根据先验可接受标准对数据进行整理。由于该数据库中阳性结果的比例很高,因此使用针对患病率进行调整的统计方法(使用AC1和PABAK)来确定试验之间的总体一致性。这些系数显示,使用WoE时,肝脏和胃肠道(主要是胃和结肠数据)的一致性为中等或良好,使用数据整理方法单独评估胃和结肠时一致性降低,使用WoE和数据整理方法时骨髓的一致性较差或无一致性。对于肝脏,对这些结果的信心高于其他组织,因为其他组织的数据较少。我们的分析发现,彗星试验和TGR试验通常能识别出在肝脏、胃和结肠中具有遗传毒性的相同化合物(主要是强效诱变剂),但在骨髓中则不然。然而,当前数据库的内容排除了对弱诱变剂和非DNA反应性化学物质得出试验一致性结论的可能性。

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