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Abstract
The study determined the effect of intravenous administration of acutely toxic or sub-lethal doses of Na-oleate-coated Fe3O4 (OC-Fe3O4) nanoparticles (NPs) on liver structure and function in Wistar rats, compared to titanium dioxide (TiO2) NPs and saline-injected controls. The acute study, using a modified OECD 425 progressive dosing procedure, found LD50 values of 59.22 and 36.42 mg/kg for TiO2 and OC-Fe3O4 NPs, respectively. In the sub-lethal study, rats were either injected with saline (negative controls), a sub-lethal reference (0.592 mg/kgTiO2 NPs, equal to 1% of LD50 on a body weight basis) or OC-Fe3O4 NPs in doses equivalent to 0.1, 1 or 10% of the LD50, respectively (corresponding to 0.0364, 0.364 and 3.64 mg Fe3O4/kg body weight). Animals were sampled 24 h, 1, 2 and 4 weeks post-injection for adverse effects. Mitochondrial respiration was significantly increased 2 weeks after injection of 10% OC-Fe3O4 NPs compared to controls, but the effect was transient. Cholesterol and triacylglycerol concentrations in the liver tissue did not increase in any treatment. There were some disturbances to antioxidant enzymes after OC-Fe3O4 NPs treatment in the livers of animals 1 week post-exposure; with the most sensitive changes occurring in glutathione peroxidase (GPx) and glutathione S-transferase (GST) activities. Lipidosis and mild necrosis with changes in sinusoid space were also observed in histological sections of the liver. Overall, these data suggest that the liver likely retains functional integrity with acute and sub-lethal doses of OC-Fe3O4 NPs, albeit with some stimulation of redox defences and evidence of some tissue injury.
Acknowledgements
Analyses of size distribution and pH of both types of NPs were done in University of Venice (by equipment NICOMP 370, submicron particle sizer, Nicomp International, Inc., New York, NY, USA). Michael Hockings and Lewis Young are thanked for their help in preparing the liver sections at Plymouth University. The authors acknowledge the support of the European Commission 7th Framework Programme for the NanoTEST project (Health-2007-1.3-4, Contract no: 201335). The work was also supported by EC FP7 QualityNano [INFRA-2010-1.131], Contract no: 214547-2, and EC FP7 NANoREG, [NMP.2012.1.3-3], Contract no: 310584.
Declaration of interest
The authors report no conflicts of interest. The authors alone are responsible for the content and writing of the paper.