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鉴定抑制人类神经嵴细胞迁移的潜在发育毒物特有的转录组特征和生物标志物。

Identification of transcriptome signatures and biomarkers specific for potential developmental toxicants inhibiting human neural crest cell migration.

作者信息

Pallocca Giorgia, Grinberg Marianna, Henry Margit, Frickey Tancred, Hengstler Jan G, Waldmann Tanja, Sachinidis Agapios, Rahnenführer Jörg, Leist Marcel

机构信息

Department of In Vitro Toxicology and Biomedicine, University of Konstanz, Box 657, 78457, Constance, Germany.

Department of Statistics, TU Dortmund University, 44139, Dortmund, Germany.

出版信息

Arch Toxicol. 2016 Jan;90(1):159-80. doi: 10.1007/s00204-015-1658-7. Epub 2015 Dec 26.

DOI:10.1007/s00204-015-1658-7
PMID:26705709
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4710658/
Abstract

The in vitro test battery of the European research consortium ESNATS ('novel stem cell-based test systems') has been used to screen for potential human developmental toxicants. As part of this effort, the migration of neural crest (MINC) assay has been used to evaluate chemical effects on neural crest function. It identified some drug-like compounds in addition to known environmental toxicants. The hits included the HSP90 inhibitor geldanamycin, the chemotherapeutic arsenic trioxide, the flame-retardant PBDE-99, the pesticide triadimefon and the histone deacetylase inhibitors valproic acid and trichostatin A. Transcriptome changes triggered by these substances in human neural crest cells were recorded and analysed here to answer three questions: (1) can toxicants be individually identified based on their transcript profile; (2) how can the toxicity pattern reflected by transcript changes be compacted/dimensionality-reduced for practical regulatory use; (3) how can a reduced set of biomarkers be selected for large-scale follow-up? Transcript profiling allowed clear separation of different toxicants and the identification of toxicant types in a blinded test study. We also developed a diagrammatic system to visualize and compare toxicity patterns of a group of chemicals by giving a quantitative overview of altered superordinate biological processes (e.g. activation of KEGG pathways or overrepresentation of gene ontology terms). The transcript data were mined for potential markers of toxicity, and 39 transcripts were selected to either indicate general developmental toxicity or distinguish compounds with different modes-of-action in read-across. In summary, we found inclusion of transcriptome data to largely increase the information from the MINC phenotypic test.

摘要

欧洲研究联盟ESNATS(“基于新型干细胞的测试系统”)的体外测试组合已用于筛选潜在的人类发育毒物。作为这项工作的一部分,神经嵴迁移(MINC)试验已用于评估化学物质对神经嵴功能的影响。除了已知的环境毒物外,它还鉴定出了一些类药物化合物。筛选出的物质包括热休克蛋白90抑制剂格尔德霉素、化疗药物三氧化二砷、阻燃剂多溴二苯醚-99、农药三唑酮以及组蛋白脱乙酰酶抑制剂丙戊酸和曲古抑菌素A。在此记录并分析了这些物质在人神经嵴细胞中引发的转录组变化,以回答三个问题:(1)能否根据毒物的转录谱单独识别它们;(2)如何将转录变化所反映的毒性模式进行压缩/降维以用于实际监管;(3)如何选择一组简化的生物标志物用于大规模后续研究?转录谱分析能够在一项盲法测试研究中清晰区分不同的毒物并识别毒物类型。我们还开发了一个图表系统,通过对改变的上级生物过程(如KEGG通路的激活或基因本体术语的过度表达)进行定量概述,来可视化和比较一组化学物质的毒性模式。对转录数据进行挖掘以寻找潜在的毒性标志物,选择了39个转录本来指示一般发育毒性或在类推中区分具有不同作用模式的化合物。总之,我们发现纳入转录组数据在很大程度上增加了来自MINC表型测试的信息。

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