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Oxidative stress and apoptosis induced by ZnO nanoparticles in HaCaT cells

Authors
Bae, Hyun CheolRyu, Hwa JungJeong, Sang HoonLee, Eun YoungPark, Yoon-HeeLee, Kyung GooChoi, Byeong HyeokMaeng, Eun HoKim, Meyoung-KonSon, Sang Wook
Issue Date
31-12월-2011
Publisher
KOREAN SOCIETY TOXICOGENOMICS & TOXICOPROTEOMICS-KSTT
Keywords
ZnO; Cytotoxicity; ROS; Keratinocyte
Citation
MOLECULAR & CELLULAR TOXICOLOGY, v.7, no.4, pp.333 - 337
Indexed
SCIE
SCOPUS
KCI
OTHER
Journal Title
MOLECULAR & CELLULAR TOXICOLOGY
Volume
7
Number
4
Start Page
333
End Page
337
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/110889
DOI
10.1007/s13273-011-0042-9
ISSN
1738-642X
Abstract
Zinc oxide (ZnO) nanoparticles (NPs) are used in the cosmetic industry in cosmetics and sunscreen. ZnO NPs have been reported to elicit various adverse cellular effects, including cytotoxicity. However, the underlying mechanisms of these adverse effects have not been fully characterized. To investigate the potential of cytotoxicity induced by ZnO NPs, we evaluated cytosolic reactive oxygen species levels in human keratinocyte HaCaT cells treated with ZnO NPs having different surface charges and particle sizes. A short period of treatment (30 min) with 100 nm ZnO NPs resulted in a greater increase of cytosolic ROS levels, compared to treatment with 20 nm ZnO NPs at the same concentration. During a long period of treatment (24 h) with ZnO NPs, intracellular ROS was increased in cells treated with 20 mu g/mL 20 nm (+/-) charged ZnO. No significant difference according to differences in surface charge was observed. In addition, total levels of caspase-7 and PARP were decreased by ZnO NPs. These results demonstrated that ZnO NPs could induce ROS mediated apoptosis.
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