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HERO ID
1761955
Reference Type
Journal Article
Title
Genotoxicity of Aluminum Oxide (Al1O3) Nanoparticle in Mammalian Cell Lines
Author(s)
Kim, YJ; Choi, HanS; Song, MiK; Youk, DaY; Kim, JiHee; Ryu, JaeC
Year
2009
Is Peer Reviewed?
1
Journal
Molecular & Cellular Toxicology
ISSN:
1738-642X
EISSN:
2092-8467
Volume
5
Issue
2
Page Numbers
172-178
Web of Science Id
WOS:000267509300012
Abstract
Nanoparticles are small-scale substances (<100 nm) with
unique properties, complex exposure and health risk implications. Aluminum oxide (Al2O3)
nanoparticles (NP) have been widely used as abrasives, wear-resistant coatings on propeller
shafts of ships, to increase the specific impulse per weight of composite propellants used in
solid rocket fuel and as drug delivery systems to increase solubility. However, recent studies
have shown that nano-sized aluminum (110 nm in diameter) can generate adverse effects, such as
pulmonary response. The cytotoxicity and genotoxicity of Al2O3 NP were investigated using the dye
exclusion assay, the comet assay, and the mouse lymphoma thymidine kinase (tk(+/-)) gene mutation
assay (MLA). IC20 values of Al2O3 NP in BEAS-2B cells were determined the concentration of 273.44
mu g/mL and 390.63 mu g/mL with and without S-9. However IC20 values of Al2O3 NP were found
nontoxic in L5178Y cells both of with and without S-9 fraction. In the comet assay, L5178Y cells
and BEAS-2B cells were treated with Al2O3 NP which significantly increased 2-fold tail moment
with and without S-9. Also, the mutant frequencies in the Al2O3 NP treated L5178Y cells were
increased compared to the vehicle controls with S-9. The results of this study indicate that
Al2O3 NP can cause primary DNA damage and cytotoxicity but not mutagenicity in cultured mammalian
cells.
Keywords
Nanoparticle; Aluminum oxide; Comet assay; Gene mutation assay (MLA); Cytotoxicity; Genotoxicity
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