Phil-Je Kim

Potential Toxicity of Differential Functionalized Multiwalled Carbon Nanotubes (MWCNT) in Human Cell Line (BEAS2B) and Caenorhabditis elegans

The aim of this study was to evaluate in vitro (human bronchial epithelial cells, BEAS2B cells) and in vivo (the nematode Caenorhabditis elegans, C. elegans) toxicity outcomes following exposure to pristine as well as surface-functionalized multiwalled carbon nanotubes (MWCNT) following hydroxylation-oxygenation (O+), amination (NH2), or carboxylation (COOH) of the carbon nanotubes (CNT). Cell viability and proliferation were measured by Ez-Cytox, trypan blue exclusion, and colony formation assays. The genotoxic potential of the MWCNT was determined by using the alkaline comet assay. In addition, survival and reproduction were used as endpoints for detection of toxicity of MWCNT in C. elegans. The carboxylated (COOH)-MWCNT was found most toxic as evidenced by cytotoxic and genotoxic among all tested compounds. The order of sensitivity was COOH > O+ > NH2 > pristine. There were almost no marked changes in survival following exposure of C. elegans to MWCNT. It is of interest that only pristine MWCNT exerted significant reduction in reproductive capacity of C. elegans. Surface functionalization significantly influenced the bioactivity of MWCNT, which displayed species as well as target-organ specificity. The mechanisms underlying these specific modes of nano-biological interactions need to be elucidated.

Ecotoxicity of bare and coated silver nanoparticles in the aquatic midge, Chironomus riparius

Although sediment is generally considered to be the major sink for nanomaterials in aquatic environments, few studies have addressed the ecotoxicity of nanomaterials in the presence of sediment. In the present study, the ecotoxicity of silver nanoparticles (AgNPs) with a range of organic coatings was examined in a freshwater sediment-dwelling organism, Chironomus riparius, using acute and chronic ecotoxicity endpoints, including molecular indicators. The toxicity of AgNPs coated with different organic materials, such as polyvinylpyrrolidone, gum arabic, and citrate, to C. riparius was compared with that of bare-AgNPs and AgNO3 (ionic silver). Total silver concentration was also measured to monitor the behavior of the AgNPs in water and sediment and to determine how ion dissolution affects the toxicity of all AgNPs. The coated- and bare-AgNPs caused DNA damage and oxidative stress-related gene expression. In addition, the bare-AgNPs and AgNO3 had a significant effect on development and reproduction. The surface coatings generally mitigated the toxicity of AgNPs to C. riparius, which can be explained by the reduced number of ions released from coated-AgNPs. Citrate-AgNPs caused the most significant alteration at the molecular level, but this did not translate to higher-level effects. Finally, comparing previously conducted studies on AgNP-induced gene expression without sediments, the authors show that the presence of sediment appears to mitigate the toxicity of AgNPs.

Toxic Effects of Alumina Nanoparticles in Rat Cerebrums and Kidneys

Objectives: Alumina nanoparticles (, Al-NPs) are used for various purposes, including as coating agents and paint additives. Their potential toxicity has raised concern for human health. This study focuses on exploring the toxic effects on the brain and kidneys caused by Al-NPs exposure in rats. Methods: The animals were orally administered Al-NPs at 10, 50 and 100 mg/kg body weight for 28 days following OECD TG 407. To determine the targeted toxicity of Al-NPs, histopathological examination and gene expression analysis were conducted on the rats. Results: The Al-NPs treatment induced kidney tubular dilatation. In the rat cerebrums, the expression levels of 126 genes experienced two-fold or greater increases in response to Al-NPs, including other genes encoding proteins involved in cell differentiation, transcription and signal transduction. In the rat kidneys, the expression levels of 152 genes also showed two-fold or greater increases in response to Al-NPs, including other genes encoding proteins involved in apoptosis, transcription and signal transduction. Conclusion: These results suggest that exposure to Al-NPs influences cellular signal pathways of kidney and cerebrum, and it can be a toxic indicators of nanometrials.