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Physico-chemical characteristics of engineered nanomaterials are known to be important in determining the impact on organisms but effects are equally dependent upon the characteristics of the organism exposed. Species sensitivity may vary by orders of magnitude, which could be due to differences in the type or magnitude of the biochemical response, exposure or uptake of nanomaterials. Synthesizing conclusions across studies and species is difficult as multiple species are not often included in a study, and differences in batches of nanomaterials, the exposure duration and media across experiments confound comparisons. Here three model species, Danio rerio, Daphnia magna and Chironomus riparius, that differ in sensitivity to lithium cobalt oxide nanosheets are found to differ in immune-response, iron–sulfur protein and central nervous system pathways, among others. Nanomaterial uptake and dissolution does not fully explain cross-species differences. This comparison provides insight into how biomolecular responses across species relate to the varying sensitivity to nanomaterials. 

Growing evidence across organisms points to altered energy metabolism as an adverse outcome of metal oxide nanomaterial toxicity, with a mechanism of toxicity potentially related to the redox chemistry of processes involved in energy production. Despite this evidence, the significance of this mechanism has gone unrecognized in nanotoxicology due to the field’s focus on oxidative stress as a universal—but non-specific—nanotoxicity mechanism. To further explore metabolic impacts, we determined LCO’s effects on these pathways in the model organism Daphnia magna through global gene expression analysis using RNA-Seq and untargeted metabolomics by direct-injection mass spectrometry. Our results show a sublethal 1 mg/L 48 h exposure of D. magna to LCO nanosheets causes significant impacts on metabolic pathways versus untreated controls, while exposure to ions released over 48 hr does not. Specifically, transcriptomic analysis using DAVID indicated significant enrichment (Benjamini-adjusted p ≤0.0.5) in LCO-exposed animals for changes in pathways involved in the cellular response to starvation (25 genes), mitochondrial function (70 genes), ATP-binding (70 genes), oxidative phosphorylation (53 genes), NADH dehydrogenase activity (12 genes), and protein biosynthesis (40 genes). Metabolomic analysis using MetaboAnalyst indicated significant enrichment (gamma-adjusted p < 0.1) for changes in amino acid metabolism (19 metabolites) and starch, sucrose, and galactose metabolism (7 metabolites). Overlap of significantly impacted pathways by RNA-Seq and metabolomics suggests amino acid breakdown and increased sugar import for energy production. Results indicate that LCO-exposed Daphnia are responding to energy starvation by altering metabolic pathways, both at the gene expression and metabolite level. These results support altered energy production as a sensitive nanotoxicity adverse outcome for LCO exposure and suggest negative impacts on energy metabolism as an important avenue for future studies of nanotoxicity, including for other biological systems and for metal oxide nanomaterials more broadly. 

Lithium intercalation compounds, such as the complex metal oxide, lithium nickel manganese cobalt oxide (LiNi x Mn y Co 1−x−y O 2 , herein referred to as NMC), have demonstrated their utility as energy storage materials. In response to recent concerns about the global supply of cobalt, industrially synthesized NMCs are shifting toward using NMC compositions with enriched nickel content. However, nickel is one of the more toxic components of NMC materials, meriting investigation of the toxicity of these materials on environmentally relevant organisms. Herein, the toxicity of both nanoscale and microscale Ni-enriched NMCs to the bacterium, Shewanella oneidensis MR-1, and the zooplankton, Daphnia magna , was assessed. Unexpectedly, for the bacteria, all NMC materials exhibited similar toxicity when used at equal surface area-based doses, despite the different nickel content in each. Material dissolution to toxic species, namely nickel and cobalt ions, was therefore modelled using a combined density functional theory and thermodynamics approach, which showed an increase in material stability due to the Ni-enriched material containing nickel with an oxidation state >2. The increased stability of this material means that similar dissolution is expected between Ni-enriched NMC and equistoichiometric NMC, which is what was found in experiments. For S. oneidensis , the toxicity of the released ions recapitulated toxicity of NMC nanoparticles. For D. magna , nickel enrichment increased the observed toxicity of NMC, but this toxicity was not due to ion release. Association of the NMC was observed with both S. oneidensis and D. magna. This work demonstrates that for organisms where the major mode of toxicity is based on ion release, including more nickel in NMC does not impact toxicity due to increased particle stability; however, for organisms where the core composition dictates the toxicity, including more nickel in the redesign strategy may lead to greater toxicity due to nanoparticle-specific impacts on the organism.