Grouping of UVCB substances with new approach methodologies (NAMs) data.

IF 5.8
ALTEX Pub Date : 2021-01-01 Epub Date: 2020-10-09 DOI:10.14573/altex.2006262
John S House, Fabian A Grimm, William D Klaren, Abigail Dalzell, Srikeerthana Kuchi, Shu-Dong Zhang, Klaus Lenz, Peter J Boogaard, Hans B Ketelslegers, Timothy W Gant, Fred A Wright, Ivan Rusyn
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引用次数: 17

Abstract

One of the most challenging areas in regulatory science is assessment of the substances known as UVCB (unknown or variable composition, complex reaction products and biological materials). Because the inherent complexity and variability of UVCBs present considerable challenges for establishing sufficient substance similarity based on chemical characteristics or other data, we hypothesized that new approach methodologies (NAMs), including in vitro test-derived biological activity signatures to characterize substance similarity, could be used to support grouping of UVCBs. We tested 141 petroleum substances as representative UVCBs in a compendium of 15 human cell types representing a variety of tissues. Petroleum substances were assayed in dilution series to derive point of departure estimates for each cell type and phenotype. Extensive quality control measures were taken to ensure that only high-confidence in vitro data were used to determine whether current groupings of these petroleum substances, based largely on the manufacturing process and physico-chemical properties, are justifiable. We found that bioactivity data-based groupings of petroleum substances were generally consistent with the manufacturing class-based categories. We also showed that these data, especially bioactivity from human induced pluripotent stem cell (iPSC)-derived and primary cells, can be used to rank substances in a manner highly concordant with their expected in vivo hazard potential based on their chemical compositional profile. Overall, this study demonstrates that NAMs can be used to inform groupings of UVCBs, to assist in identification of repre­sentative substances in each group for testing when needed, and to fill data gaps by read-across.

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用新方法方法(NAMs)数据对UVCB物质进行分组。
监管科学中最具挑战性的领域之一是评估被称为UVCB(未知或可变成分,复杂反应产物和生物材料)的物质。由于uvcb固有的复杂性和可变性为基于化学特性或其他数据建立足够的物质相似性提出了相当大的挑战,我们假设新的方法方法(NAMs),包括体外测试衍生的生物活性特征来表征物质相似性,可以用来支持uvcb的分组。我们在代表各种组织的15种人类细胞类型的纲要中测试了141种石油物质作为代表uvcb。石油物质在稀释系列中进行分析,以得出每种细胞类型和表型的起始点估计。采取了广泛的质量控制措施,以确保仅使用高可信度的体外数据来确定这些石油物质的当前分组是否合理,这些分组主要基于制造过程和物理化学性质。我们发现基于生物活性数据的石油物质分类与基于制造类的分类基本一致。我们还表明,这些数据,特别是来自人类诱导多能干细胞(iPSC)衍生细胞和原代细胞的生物活性,可用于根据其化学成分特征,以高度一致的方式对物质进行排序。总体而言,本研究表明,NAMs可用于通知uvcb分组,在需要时协助识别每组中的代表性物质进行测试,并通过读取来填补数据空白。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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