4.7 Article

Coupling Environmental Whole Mixture Toxicity Screening with Unbiased RNA-Seq Reveals Site-Specific Biological Responses in Zebrafish

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TOXICS
卷 11, 期 3, 页码 -

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MDPI
DOI: 10.3390/toxics11030201

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passive sampling; Danio rerio; polycyclic aromatic hydrocarbons; mixtures; developmental; transcriptomics

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Passive sampling device (PSD) with developmental toxicity assays in zebrafish can effectively detect the whole mixture toxicity of bioavailable non-polar organics in environmental sites. By incorporating RNA-Seq, this study investigated the toxicity of PSD extracts from two locations in Portland Harbor Superfund Site on zebrafish embryos. The results showed that RM 6.5W had higher concentrations of PAHs and exhibited higher toxicity, while the gene expression profiles were similar between the two extracts.
Passive sampling device (PSD) extracts paired with developmental toxicity assays in Danio Rerio (zebrafish) are excellent sensors for whole mixture toxicity associated with the bioavailable non-polar organics at environmental sites. We expand this concept by incorporating RNA-Seq in 48-h post fertilization zebrafish statically exposed to PSD extracts from two Portland Harbor Superfund Site locations: river mile 6.5W (RM 6.5W) and river mile 7W (RM 7W). RM 6.5W contained higher concentrations of polycyclic aromatic hydrocarbons (PAHs), but the diagnostic ratios of both extracts indicated similar PAH sourcing and composition. Developmental screens determined RM 6.5W to be more toxic with the most sensitive endpoint being a wavy notochord malformation. Differential gene expression from exposure to both extracts was largely parallel, although more pronounced for RM 6.5W. When compared to the gene expression associated with individual chemical exposures, PSD extracts produced some gene signatures parallel to PAHs but were more closely matched by oxygenated-PAHs. Additionally, differential expression, reminiscent of the wavy notochord phenotype, was not accounted for by either class of chemical, indicating the potential of other contaminants driving mixture toxicity. These techniques offer a compelling method for non-targeted hazard characterization of whole mixtures in an in vivo vertebrate system without requiring complete chemical characterization.

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