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斑马鱼化学筛选中观察到的生物活性的暴露变化的系统评估

Systematic Assessment of Exposure Variations on Observed Bioactivity in Zebrafish Chemical Screening.

作者信息

Wilson Lindsay B, Truong Lisa, Simonich Michael T, Tanguay Robyn L

机构信息

Department of Environmental and Molecular Toxicology and the Sinnhuber Aquatic Research Laboratory, Oregon State University, Corvallis, OR 97333, USA.

出版信息

Toxics. 2020 Oct 14;8(4):87. doi: 10.3390/toxics8040087.

Abstract

The embryonic zebrafish is a powerful tool for high-throughput screening of chemicals. While this model has significant potential for use in safety assessments and chemical prioritization, a lack of exposure protocol harmonized across laboratories has limited full model adoption. To assess the potential that exposure protocols alter chemical bioactivity, we screened a set of eight chemicals and one 2D nanomaterial across four different regimens: (1) the current Tanguay laboratory's standard protocol of dechorionated embryos and static exposure in darkness; (2) exposure with chorion intact; (3) exposure under a 14 h light: 10 h dark cycle; and (4) exposure with daily chemical renewal. The latter three regimens altered the concentrations, resulting in bioactivity of the test agents compared to that observed with the Tanguay laboratory's standard regimen, though not directionally the same for each chemical. The results of this study indicate that with the exception for the 2D nanomaterial, the screening design did not change the conclusion regarding chemical bioactivity, just the nominal concentrations producing the observed activity. Since the goal of tier one chemical screening often is to differentiate active from non-active chemicals, researchers could consider the trade-offs regarding cost, labor, and sensitivity in their study design without altering hit rates. Taken further, these results suggest that it is reasonably feasible to reach agreement on a standardized exposure regiment, which will promote data sharing without sacrificing data content.

摘要

斑马鱼胚胎是用于化学品高通量筛选的强大工具。虽然该模型在安全评估和化学品优先级排序方面具有巨大潜力,但各实验室缺乏统一的暴露方案限制了该模型的全面应用。为了评估暴露方案对化学品生物活性的影响,我们在四种不同方案下筛选了一组八种化学品和一种二维纳米材料:(1)坦圭实验室目前的标准方案,即去除卵膜的胚胎在黑暗中进行静态暴露;(2)卵膜完整时的暴露;(3)在14小时光照:10小时黑暗周期下的暴露;(4)每天更换化学品的暴露。与坦圭实验室的标准方案相比,后三种方案改变了浓度,导致受试物的生物活性发生变化,不过每种化学品的变化方向并不相同。本研究结果表明,除二维纳米材料外,筛选设计并未改变关于化学品生物活性的结论,只是改变了产生观察到的活性的名义浓度。由于一级化学品筛选的目标通常是区分活性化学品和非活性化学品,研究人员在研究设计中可以考虑成本、人力和灵敏度之间的权衡,而不会改变命中率。进一步来看,这些结果表明就标准化暴露方案达成一致是合理可行的,这将促进数据共享而不牺牲数据内容。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/14db/7712973/de85d0d138c2/toxics-08-00087-g001.jpg

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