Interactive toxicity effect of combined exposure to hematite and amorphous silicon dioxide nanoparticles in human A549 cell line.

The study on the health effects of combined exposure to various contaminants has been recommended by many authors. The objective of the present study was to examine the effects of the co-exposure to hematite and amorphous silicon dioxide (A-SiO2) nanoparticles on the human lung A549 cell line. The A549 cell line was exposed to 10, 50, 100, and 250 µg/ml concentrations of hematite and A-SiO2 nanoparticles both independently and in combination. Their toxicity in both circumstances was investigated by MTT, intracellular reactive oxygen species, cell glutathione content, and mitochondrial membrane potential tests, and the type of interaction was investigated by statistical analysis using Statistical Package for Social Sciences (SPSS, v. 21). Results showed that the independent exposure to either hematite or A-SiO2 compared with the control group produced more toxic effects on the A549 cell line. The toxicity of combined exposure of the nanoparticles was lower compared with independent exposure, and antagonistic interactive effects were detected. The findings of this study could be useful in clarifying the present debate on the health effects of combined exposure of hematite and A-SiO2 nanoparticles. Because of the complexities of combined exposures, further studies of this kind are recommended.

Investigation of the effect of magnetite iron oxide particles size on cytotoxicity in A549 cell line.

INTRODUCTION: Magnetite as iron oxide is widely used in various industries, in the pharmaceutical industry in particular where it is used for its magnetic properties. The environmental and occupational exposure to airborne nanoparticles and microparticles of iron oxide compounds have been reported. Since authors have reported contradictory results, the objective of this study was to investigate the effect of particles' size in their toxicities. METHODS: The human cell line A549 was exposed with magnetite iron oxide in two size categories of micro (≥5 µm) and nano (<100 nm), with four concentrations of 10, 50, 100, and 250 µg/ml at two time periods of 24 and 72 h. The cell viability, reactive oxygen species (ROS), changes in mitochondrial membrane potential, and incidence of apoptosis were studied. RESULTS: Nano and micro magnetite particles demonstrated diverse toxicity effects on the A549 cell line at the 24- and 72-h exposure periods; however, the effects produced were time- and concentration-dependent. Nano magnetite particles produced greater cellular toxicities in forms of decreased viabilities at concentration exposures greater than 50 µg/ml (p < 0.05), along with increased ROS (p < 0.05), decreased cellular membrane potential (p < 0.05), and reduced rate of apoptosis (p < 0.05). DISCUSSION: The results of this study demonstrated that magnetite iron in nano-range sizes had a greater absorbability for the A549 cell line compared to micro sizes, and at the same time, nanoparticles were more toxic than microparticles, demonstrating higher production of ROS and decreased viabilities. Considering the greater toxicity of nanoparticles of magnetite iron in this study, thorough precautionary control measures must be taken before they can be used in various industries.

The effect of single and combined exposures to magnetite and polymorphous silicon dioxide nanoparticles on the human A549 cell line: in vitro study.

The increasing trend of nanoparticle usage in science and technology has led to significant human exposure. Occupational exposure to iron oxides and silica dust has been reported in mining, manufacturing, construction, and pharmaceutical operations. The combined toxicological effects of nanoparticles and simultaneous exposure to other compounds have given rise to a new concern. Hence, the objective of this study was to investigate the toxicological effects of magnetite and polymorphous silicon dioxide nanoparticles in single and combined exposures. The polymorphous silicon dioxide nanoparticles were obtained from the milled quartz particles under 100 nm in diameter. The milled particles were purified through chloric and nitric acid wash processes. The toxic effects of the magnetite nanoparticles were investigated independently and in combination with quartz using the A549 cell line for durations of 24 and 72 h, and using diverse concentrations of 10, 50, 100, and 250 µg/mL. MTT, ROS, mitochondrial membrane potential, and cell glutathione content assays were used to evaluate the amount of cell damage in this study. The statistical significance level in one-way ANOVA and independent t test was considered to be at the 5% confidence level. The size and purity of polymorphous silicon dioxide nanoparticles were measured by TEM and ICP-OES analysis, respectively. The particles' diameters were under 100 nm and demonstrated a purity of higher than 99%. The toxicity results of this study showed a dependency on concentration and exposure duration in reducing the cell viability, cellular glutathione content, and mitochondrial membrane potential, as well as increasing the ROS generation in single and combined exposures with magnetite and polymorphous silicon dioxide nanoparticles. The toxic effects of combined exposure to these nanoparticles were less than the single exposures, and statistically significant antagonistic interactions were detected. Combined exposure to polymorphous silicon dioxide and magnetite nanoparticles, in comparison with their single exposures, could affect health in an antagonistic manner. Since this study has been the first of its kind, further studies investigating the health effects of single and combined exposures to these compounds are needed to verify our findings. Generally, studies such as this one could contribute to the field of combined toxicity effects.