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Pro-oxidant status and Nrf2 levels in psoriasis vulgaris skin tissues and dimethyl fumarate-treated HaCaT cells

Authors
Lee, Yoon JinBae, Jin HoKang, Sang-GueCho, Sung WooChun, Dong-IlNam, Seung MinKim, Chul HanNam, Hae SeonLee, Seon HwaLee, Sang HanCho, Moon Kyun
Issue Date
Sep-2017
Publisher
대한약학회
Keywords
Antioxidant protein; Nrf2; Psoriasis; DMF
Citation
Archives of Pharmacal Research, v.40, no.9, pp 1105 - 1116
Pages
12
Journal Title
Archives of Pharmacal Research
Volume
40
Number
9
Start Page
1105
End Page
1116
URI
https://scholarworks.bwise.kr/sch/handle/2021.sw.sch/7288
DOI
10.1007/s12272-017-0955-5
ISSN
0253-6269
1976-3786
Abstract
Reactive oxygen species (ROS) contribute to pathogenesis of many inflammatory skin diseases, including psoriasis. The aim of this study is to compare antioxidant protein expression in psoriasis vulgaris (PV) skin tissues with that in normal skin tissues in vivo and to evaluate the effects of dimethyl fumarate (DMF), used for the treatment of psoriasis, on ROS generation and apoptosis in a human keratinocyte cell line HaCaT. Compared with normal skin tissues, PV skin tissues showed increased protein oxidation as well as down-regulation of Nrf2 and its regulatory proteins such as HO-1 and AKR1C3. Using HaCaT cells to model DMF-induced pro-oxidant effects in the skin cells, we found that DMF treatment induced increased ROS levels and apoptotic cell death, as signified by increased proportion of cells with Annexin V-PE(+) staining and a sub-G(0)/G(1) peak in the cell cycle. Preceding these changes, DMF treatment resulted in up-regulation of Nrf2, HO-1, and AKR1C3 proteins in these cells. Collectively, increased oxidative stress and impaired cellular anti-oxidant enzyme systems may participate in the pathogenesis of PV. DMF may exert an additive therapeutic efficacy in PV by attenuating the redox burden and subsequent oxidative damage to normal keratinocytes through activation of Nrf2 pathway relative to PV.
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College of Medicine > Department of Clinical Parasitology > 1. Journal Articles
College of Medicine > Department of Plastic Surgery > 1. Journal Articles
College of Medicine > Department of Plastic Surgery > 1. Journal Articles
College of Medicine > Department of Orthopedic Surgery > 1. Journal Articles
College of Medicine > Department of General Surgery > 1. Journal Articles
College of Medicine > Department of Biochemistry > 1. Journal Articles

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