Grouping of histone deacetylase inhibitors and other toxicants disturbing neural crest migration by transcriptional profiling
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Functional assays, such as the "migration inhibition of neural crest cells" (MINC) developmental toxicity test, can identify toxicants without requiring knowledge on their mode of action (MoA). Here, we were interested, whether (i) inhibition of migration by structurally diverse toxicants resulted in a unified signature of transcriptional changes; (ii) whether statistically-identified transcript patterns would inform on compound grouping even though individual genes were little regulated, and (iii) whether analysis of a small group of biologically-relevant transcripts would allow the grouping of compounds according to their MoA. We analyzed transcripts of 35 'migration genes' after treatment with 16 migration-inhibiting toxicants. Clustering, principal component analysis and correlation analyses of the data showed that mechanistically related compounds (e.g. histone deacetylase inhibitors (HDACi), PCBs) triggered similar transcriptional changes, but groups of structurally diverse toxicants largely differed in their transcriptional effects. Linear discriminant analysis (LDA) confirmed the specific clustering of HDACi across multiple separate experiments. Similarity of the signatures of the HDACi trichostatin A and suberoylanilide hydroxamic acid to the one of valproic acid (VPA), suggested that the latter compound acts as HDACi when impairing neural crest migration. In conclusion, the data suggest that (i) a given functional effect (e.g. inhibition of migration) can be associated with highly diverse signatures of transcript changes; (ii) statistically significant grouping of mechanistically-related compounds can be achieved on the basis of few genes with small regulations. Thus, incorporation of mechanistic markers in functional in vitro tests may support read-across procedures, also for structurally un-related compounds.
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DRESER, Nadine, Bastian ZIMMER, Christian DIETZ, Elena SÜGIS, Giorgia PALLOCCA, Johanna NYFFELER, Johannes MEISIG, Nils BLÜTHGEN, Michael R. BERTHOLD, Tanja WALDMANN, Marcel LEIST, 2015. Grouping of histone deacetylase inhibitors and other toxicants disturbing neural crest migration by transcriptional profiling. In: NeuroToxicology. 2015, 50, pp. 56-70. ISSN 0161-813X. eISSN 1872-9711. Available under: doi: 10.1016/j.neuro.2015.07.008BibTex
@article{Dreser2015Group-32362,
year={2015},
doi={10.1016/j.neuro.2015.07.008},
title={Grouping of histone deacetylase inhibitors and other toxicants disturbing neural crest migration by transcriptional profiling},
volume={50},
issn={0161-813X},
journal={NeuroToxicology},
pages={56--70},
author={Dreser, Nadine and Zimmer, Bastian and Dietz, Christian and Sügis, Elena and Pallocca, Giorgia and Nyffeler, Johanna and Meisig, Johannes and Blüthgen, Nils and Berthold, Michael R. and Waldmann, Tanja and Leist, Marcel}
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<dcterms:abstract xml:lang="eng">Functional assays, such as the "migration inhibition of neural crest cells" (MINC) developmental toxicity test, can identify toxicants without requiring knowledge on their mode of action (MoA). Here, we were interested, whether (i) inhibition of migration by structurally diverse toxicants resulted in a unified signature of transcriptional changes; (ii) whether statistically-identified transcript patterns would inform on compound grouping even though individual genes were little regulated, and (iii) whether analysis of a small group of biologically-relevant transcripts would allow the grouping of compounds according to their MoA. We analyzed transcripts of 35 'migration genes' after treatment with 16 migration-inhibiting toxicants. Clustering, principal component analysis and correlation analyses of the data showed that mechanistically related compounds (e.g. histone deacetylase inhibitors (HDACi), PCBs) triggered similar transcriptional changes, but groups of structurally diverse toxicants largely differed in their transcriptional effects. Linear discriminant analysis (LDA) confirmed the specific clustering of HDACi across multiple separate experiments. Similarity of the signatures of the HDACi trichostatin A and suberoylanilide hydroxamic acid to the one of valproic acid (VPA), suggested that the latter compound acts as HDACi when impairing neural crest migration. In conclusion, the data suggest that (i) a given functional effect (e.g. inhibition of migration) can be associated with highly diverse signatures of transcript changes; (ii) statistically significant grouping of mechanistically-related compounds can be achieved on the basis of few genes with small regulations. Thus, incorporation of mechanistic markers in functional in vitro tests may support read-across procedures, also for structurally un-related compounds.</dcterms:abstract>
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