首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Application of Benchmark Concentration (BMC) Analysis on Zebrafish Data: A New Perspective for Quantifying Toxicity in Alternative Animal Models
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Application of Benchmark Concentration (BMC) Analysis on Zebrafish Data: A New Perspective for Quantifying Toxicity in Alternative Animal Models

机译:基准浓度(BMC)分析在斑马鱼数据中的应用:替代动物模型中量化毒性的新视角

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Over the past decade, the zebrafish is increasingly being used as a model to screen for chemical-mediated toxicities including developmental toxicity (DT) and neurotoxicity (NT). One of the major challenges is lack of harmonization in data analysis approaches, thereby posing difficulty in comparing findings across laboratories. To address this, we sought to establish a unified data analysis strategy for both DT and NT data, by adopting the benchmark concentration (BMC) analysis. There are two critical aspects in the BMC analysis: having a toxicity endpoint amenable for BMC and selecting a proper benchmark response (BMR) for the endpoint. For the former, in addition to the typical endpoints in NT assay (eg, hyper/hypo- response quantified by distance moved), we also used endpoints that assess the differences in movement patterns between chemical-treated embryos and control embryos. For the latter, we standardized the selection of BMR, which is analogous to minimum activity threshold, based on intrinsic response variations in the endpoint. When comparing our BMC results with a traditionally used LOAEL method (lowest-observed-adverse-effect level), we found high active compound concordance (100% for DT vs 74% for NT); generally, the BMC was more sensitive than LOAEL (no. of BMC more sensitive/no. of concordant active compounds, 43/50 for DT vs 16/26 for NT). Using the BMC with standardized toxicity endpoints and an appropriate BMR, we may now have a unified data-analysis approach to comparing results across different zebrafish datasets, for a better understanding of strengths and challenges when using the zebrafish as a screening tool.
机译:在过去十年中,斑马鱼越来越多地被用作筛选化学介导的毒性,包括发育毒性(DT)和神经毒性(NT)的模型。其中一个主要挑战是在数据分析方法中缺乏协调,从而在比较实验室跨越表演时难以摆脱困难。为了解决这个问题,我们试图通过采用基准集中度(BMC)分析来建立DT和NT数据的统一数据分析策略。 BMC分析中存在两个关键方面:具有用于BMC的毒性终点,并为端点选择适当的基准响应(BMR)。对于前者,除了NT测定中的典型终点(例如,通过距离量化的超级/次次响应)之外,我们还使用终点,该端点评估化学处理的胚胎和对照胚胎之间的运动模式的差异。对于后者,我们标准化了BMR的选择,这些BMR类似于最小活动阈值,基于端点中的内在响应变化。在将我们的BMC结果与传统使用的LoAEL方法(最低观察到的 - 不良效果水平)进行比较时,我们发现高活性复合协调(对于NT的DT 74%100%);通常,BMC比LOAEL更敏感(BMC更敏感/否。交叉活性化合物,43/50用于NT的DT 16/26)。使用BMC具有标准化的毒性端点和适当的BMR,我们现在可以进行统一的数据分析方法来比较不同斑马鱼数据集的结果,以便在使用斑马鱼作为筛选工具时更好地了解优势和挑战。

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