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Journal article

Subacute oral toxicity investigation of selenium nanoparticles and selenite in rats

From

National Food Institute, Technical University of Denmark1

Research group for Nano-Bio Science, National Food Institute, Technical University of Denmark2

Research Group for Risk Benefit, National Food Institute, Technical University of Denmark3

Research Group for Analytical Food Chemistry, National Food Institute, Technical University of Denmark4

Danish Hydraulic Institute5

Selenium (Se) nanoparticles have been proposed as food supplements. However, the particle formulation may exert unexpected toxicity. The aim was therefore to compare toxicity of low doses of Se nanoparticles and the dissolved, ionized Se species selenite. Female rats were dosed orally for 28 d with either: 0.05, 0.5, or 4 mg Se/kg body weight (bw)/day as 20 nm Se nanoparticles or 0.05 or 0.5 mg Se/kg bw/day as sodium selenite.

Male rats were dosed 4 mg Se/kg bw/day as Se nanoparticles. Body weight and clinical appearance were recorded throughout the experiment. At necropsy, blood samples were taken for hematological and clinical chemistry analyses; organ weights were recorded. At the high-dose of Se nanoparticles, overt toxicity occurred and the female animals had to be euthanized prematurely, whereas the male animals were reduced in dose.

At all doses of Se nanoparticles and at 0.5 mg Se/kg bw/day as selenite, a lower body weight gain as compared to vehicle occurred. Relative liver weight was increased for both Se formulations at 0.5 mg Se/kg bw/day. Creatinine clearance and urinary pH were affected in some Se dosed groups. There were no effects among dosed groups on brain neurotransmitters or on hematological parameters compared with controls.

There were no histological changes in the livers of animals exposed to Se nanoparticles or to selenite. Based on effects on body weight and liver weight, selenium nanoparticles and ionic Se exerted similar toxicity. This suggests that a nanoparticle-specific toxicity of Se did not occur.

Language: English
Publisher: Taylor & Francis
Year: 2019
Pages: 76-83
ISSN: 15256014 and 01480545
Types: Journal article
DOI: 10.1080/01480545.2018.1491589
ORCIDs: Hadrup, Niels , Löschner, Katrin , Mandrup Egebjerg, Karen , Ravn-Haren, Gitte and Frandsen, Henrik Lauritz

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