Off to a good start? Review of the predictivity of reactivity methods modelling the molecular initiating event of skin sensitization.

IF 4.5 2区 医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL Altex-Alternatives To Animal Experimentation Pub Date : 2023-01-01 Epub Date: 2023-06-12 DOI:10.14573/altex.2212201
Nathalie Alépée, Fleur Tourneix, Akanksha Singh, Nadège Ade, Sébastien Grégoire
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Abstract

The assessment of skin sensitizing properties of chemicals has moved away from animal methods to new approach methodologies (NAM), guided by qualitative mechanistic understanding operationalized in an adverse outcome pathway (AOP). As with any AOP, the molecular initiating event (MIE) of covalent binding of a chemical to skin proteins is particularly important. This MIE has been modelled by several test methods by measuring the reaction of a test chemical with model peptides in chemico. To better understand the similarities and differences, a data repository with publicly available data for the direct peptide reactivity assay (DPRA), amino acid derivative reactivity assay (ADRA) and kinetic DPRA (kDPRA), as well as the peroxidase peptide reactivity assay (PPRA) was assembled. The repository comprises 260 chemicals with animal and human reference data, data on four relevant physicochemical properties, and between 161 to 242 test chemical results per test method. First, an overview of the experimental conditions of the four test methods was compiled allowing to readily compare them. Second, data analyses demonstrated that the test methods’ predictivity was consistently reduced for poorly watersoluble chemicals and that the DPRA and ADRA can be used interchangeably. It also revealed new categorization thresholds for the DPRA and ADRA that are potentially relevant for strategic uses. In summary, a detailed assessment of reactivity test methods is provided, highlighting their potential and limitations. The results presented are intended to stimulate scientific discussion around test methods modelling the MIE of the skin sensitization AOP.

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有一个良好的开端吗?皮肤致敏分子启动事件建模反应性方法的预测性综述。
化学品皮肤致敏特性的评估已从动物方法转向新的方法(NAM),以在不良结果途径(AOP)中操作的定性机制理解为指导。与任何AOP一样,化学物质与皮肤蛋白共价结合的分子起始事件(MIE)尤为重要。这种MIE已经通过几种测试方法建模,通过测量测试化学品与chemico中的模型肽的反应。为了更好地理解相似性和差异性,组装了一个数据库,其中包含直接肽反应性测定(DPRA)、氨基酸衍生物反应性分析(ADRA)和动力学DPRA(kDPRA)以及过氧化物酶肽反应性试验(PPRA)的公开数据。该储存库包括260种化学品,包括动物和人类参考数据、四种相关物理化学性质的数据,以及每种测试方法161至242个测试化学结果。首先,对四种测试方法的实验条件进行了概述,以便进行比较。其次,数据分析表明,对于水溶性差的化学品,测试方法的预测性一直在降低,DPRA和ADRA可以互换使用。它还揭示了DPRA和ADRA的新分类阈值,这些阈值可能与战略用途相关。总之,提供了反应性试验方法的详细评估,强调了其潜力和局限性。所提供的结果旨在激发围绕皮肤致敏AOP的MIE建模测试方法的科学讨论。
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来源期刊
Altex-Alternatives To Animal Experimentation
Altex-Alternatives To Animal Experimentation MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
7.70
自引率
8.90%
发文量
89
审稿时长
2 months
期刊介绍: ALTEX publishes original articles, short communications, reviews, as well as news and comments and meeting reports. Manuscripts submitted to ALTEX are evaluated by two expert reviewers. The evaluation takes into account the scientific merit of a manuscript and its contribution to animal welfare and the 3R principle.
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