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Screening for angiogenic inhibitors in zebrafish to evaluate apredictive model for developmental vascular toxicity

机译:筛选斑马鱼中的血管生成抑制剂以评估发育性血管毒性的预测模型

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摘要

Chemically-induced vascular toxicity during embryonic development may cause a wide range of adverse effects. To identify putative vascular disrupting chemicals (pVDCs), a predictive pVDC signature was constructed from 124 U.S. EPA ToxCast high-throughput screening (HTS) assays and used to rank 1060 chemicals for their potential to disrupt vascular development. Thirty-seven compounds were selected for targeted testing in transgenic Tg(kdrl:EGFP) and Tg(fli1:EGFP) zebrafish embryos to identify chemicals that impair developmental angiogenesis. We hypothesized that zebrafish angiogenesis toxicity data would correlate with human cell-based and cell-free in vitro HTS ToxCast data. Univariate statistical associations used to filter HTS data based on correlations with zebrafish angiogenic inhibition in vivo revealed 132 total significant associations, 33 of which were already captured in the pVDC signature, and 689 non-significant assay associations. Correlated assays were enriched in cytokine and extracellular matrix pathways. Taken together, the findings indicate the utility of zebrafish assays to evaluate an HTS-based predictive toxicity signature and also provide an experimental basis for expansion of the pVDC signature with novel HTS assays.
机译:胚胎发育过程中化学诱导的血管毒性可能引起广泛的不良影响。为了识别推定的血管破坏化学物质(pVDC),根据124种美国EPA ToxCast高通量筛选(HTS)分析方法构建了预测性pVDC信号,并使用1060种化学物质对它们破坏血管发育的潜力进行了排名。选择了37种化合物在转基因Tg(kdrl:EGFP)和Tg(fli1:EGFP)斑马鱼胚胎中进行靶向测试,以鉴定会损害发育性血管生成的化学物质。我们假设斑马鱼血管生成毒性数据将与基于人类细胞和无细胞的体外HTS ToxCast数据相关。基于与体内斑马鱼血管生成抑制的相关性来过滤HTS数据的单变量统计关联揭示了132个共有的显着关联,其中33个已经捕获在pVDC签名中,还有689个非重要的分析关联。相关测定富含细胞因子和细胞外基质途径。综上所述,这些发现表明斑马鱼测定法可用于评估基于HTS的预测毒性标记,并且还为利用新型HTS测定法扩展pVDC标记提供了实验基础。

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