Human Metallothionein Gene Expression Is Upregulated by β-Thujaplicin : Possible Involvement of Protein Kinase C and Reactive Oxygen Species(Molecular and Cell Biology)
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概要
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Recently, we discovered that β-thujaplicin (BT) induces metallothionein (MT) expression in mouse keratinocytes, both in vivo and in vitro. However, the molecular mechanisms by which BT exerts its biological effects have not been elucidated. The purpose of this study is to explore the signal transduction pathway involved in the MT mRNA induction by BT. Using a HaCaT keratinocyte cell line, Northern blotting was performed for analyzing the human MT-IIA mRNA expression levels in combination with BT and a number of protein kinase (PK) inhibitors including H7, HA1004 and a PKC-specific inhibitor chelerythrin. CAT assays with the MT-IIA gene promorter-CAT construct were conducted for examining the transcriptional regulation by BT of MT. A free radical scavenger N-acetylcysteine (NAC) was used for analyzing a role of oxidative stress for the MT gene induction by BT. BT increased MT-IIA gene transcript levels and CAT activity in a dose-dependent fashion in HaCaT cells. The increase in MT-IIA mRNA levels and CAT activity were completely suppressed by H7 but not by HA1004. In addition, chelerythrin prevented BT-inducible MT-IIA promoter activation. Furthermore, NAC suppressed BT-inducible MT-IIA promoter activation. These results demonstrate that BT is a potent activator of the MT-IIA gene promoter and that PKC activation and reactive oxygen species are implicated in BT-inducible MT-IIA gene expression. BT may be a useful tool for dissecting the signal transduction pathway mediating MT-IIA promoter activation.
- 公益社団法人日本薬学会の論文
- 2006-01-01
著者
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Matsuzaki Yasushi
Department of Dermatology, Hirosaki University Graduate School of Medicine
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Nakano Hajime
Department of Dermatology, Hirosaki University Graduate School of Medicine
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KANEKO Takahide
Department of Dermatology, Hirosaki University School of Medicine
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Nakano H
Department Of Dermatology Hirosaki University Graduate School Of Medicine
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Nakano Hajime
弘前大学 医学部皮膚科学
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Nakano Hajime
駿河台日本大学病院 皮膚科
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Hanada Katsumi
Department Of Dermatology Hirosaki University School Of Medicine
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Nakano Hajime
Department Of Dermatology Hirosaki University Graduate School Of Medicine
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TSUCHIDA Shigeki
Second Department of Biochemistry, Hirosaki University School of Medicine
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Hanada K
Department Of Dermatology Hirosaki University School Of Medicine
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AIZU Takayuki
Department of Dermatology, Hirosaki University School of Medicine
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IKENAGA Satsuki
Department of Dermatology, Hirosaki University Graduate School of Medicine
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ARIMA Yaeno
Department of Dermatology, Kyoto University Graduate School of Medicine
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Tsuchida Shigeki
Second Department Of Biochemistry Hirosaki University School Of Medicine
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Aizu Takayuki
Department Of Dermatology Hirosaki University School Of Medicine
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Arima Yaeno
Department Of Dermatology Kyoto University Graduate School Of Medicine
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Arima Yaeno
Department Of Analytical And Bionorganic Chemistry Kyoto Pharmaceutical University
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Kaneko Takahide
Department Of Dermatology Hirosaki University Graduate School Of Medicine
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Tsuchida S
Second Department Of Biochemistry Hirosaki University School Of Medicine
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Ikenaga Satsuki
Department Of Dermatology Hirosaki University Graduate School Of Medicine
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Matsuzaki Yasushi
Department Of Dermatology Hirosaki University Graduate School Of Medicine
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Aizu Takayuki
Department Of Dermatology Hirosaki University Graduate School Of Medicine
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Takeuchi Sonoko
弘前大学 医学研究科皮膚科学
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Hanada Katsumi
Department Of Dermatology Hirosaki University Graduate School Of Medicine
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Nakano Hajime
Department Of Cardiovascular Medicine Ohmori Hospital Toho University School Of Medicine
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