CHARACTERIZATION OF RESISTANCE TO BROMOBENZENE-INDUCED HEPATOTOXICITY BY MICROARRAY
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概要
- 論文の詳細を見る
In our previous study, we demonstrated that the initial hepatic injury caused by bromobenzene (BB) was no longer detected in rats despite subsequent dosing, indicating that the liver acquired resistance to BB-induced hepatotoxicity. In this experiment, microarray analysis was conducted to characterize this resistance. The liver samples for the analysis utilized were obtained from previous experiments where F344 rats were treated intraperitoneally with BB (150 mg/kg). At 24 hr post-dose, hepatic injury was confirmed by monitoring the AST values and then the rats were maintained at the same dosing regimen for an additional 8 days. The gene expression profiles of the BB-treated rat livers were compared with a vehicle-treated group by Affymetrix RG_U34A arrays. As results, a decreased expression level of CYP3A9 and an increased expression level of GST Yc2 and glutathione peroxidase (GPX) were detected. These changes indicated suppression of the phase I reaction and induction of the phase II reaction (glutathione conjugation). Increased expression levels of epoxide hydrolase (EH) and NAD(P)H:quinone oxidoreductase (NQO1) also suggested the involvement of EH- and NQO1-mediated hydrolysis other than glutathione conjugation with resistance in the phase II reaction. Moreover, an increased expression level of abcc3 (multidrug resistance protein 3; Mrp3) was significantly noted. Based on the present findings, it was suggested that Mrp3 in the phase III reaction (drug elimination) contributed to the resistance to BB hepatotoxicity in addition to the suppression of the phase I reaction (metabolic activation) and the induction of the phase II reaction (detoxification). Among them, the factors which contributed most were considered to be the increased GST Yc2 and Mrp3, based on the degree of the gene expression changes.
- 日本トキシコロジー学会の論文
- 2007-05-16
著者
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Tanaka Kohji
Medicinal Safety Research Laboratories, Daiichi Sankyo Co., Ltd.
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Manabe Sunao
Medicinal Safety Research Laboratories, Daiichi Sankyo Co., Ltd.
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KIYOSAWA Naoki
Medical Safety Research Labs., Sankyo Co., Ltd.
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WATANABE Kyoko
Medical Safety Research Labs., Sankyo Co., Ltd.
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真鍋 淳
Medicinal Safety Research Laboratories Daiichi-sankyo Co. Ltd.
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真鍋 淳
三共
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真鍋 淳
Laboratory Animal Science And Toxicology Laboratories Sankyo Co. Ltd.
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Tanaka K
Institute Of Earth And Space Science Graduate School Of Science Osaka University
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Manabe Sunao
Medicinal Safety Research Laboratories Daiichi Sankyo Co. Ltd.
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Manabe Sunao
Medical Safety Research Laboratories Sankyo Co. Ltd.
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田中 宏治
Med.safe.res.labs. Sankyo Co. Ltd. Of Shizuoka Pref.
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Tanaka K
Department Of Toxicology Graduate School Of Pharmaceutical Sciences Osaka University:(present Office
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Kiyosawa Naoki
Toxicogenomics Project National Inst. Of Biomedical Innovation
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Kiyosawa Naoki
Medical Safety Research Laboratories Sankyo Co. Ltd.
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Kiyosawa Naoki
Dpt. Of Veterinary Pathology Graduate School Of Agricultural And Life Sciences The University Of Tok
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Watanabe Kyoko
Medicinal Safety Research Labs. Daiichi Sankyo Co. Ltd.
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Manabe Sunao
Med.safe.res.labs. Sankyo Co. Ltd. Of Shizuoka Pref.
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Tanaka Kohji
Med.safe.res.labs. Sankyo Co. Ltd. Of Shizuoka Pref.
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Manabe Sunao
Lab. Anim. Sci. & Toxicol. Lab. Sankyo Co. Ltd.
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Tanaka Katsushi
Department Of Materials Science And Engineering Graduate School Of Engineering Kyoto University
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Tanaka Keiichi
Dep. Toxicol. Grad. School Pharmaceut. Sci. Osaka Univ.
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Tanaka K
Kumamoto Univ. Kumamoto Jpn
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Manabe Sunao
Medicinal Safety Research Labs. Daiichi Sankyo Co. Ltd.
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Kojitani Takatoshi
Res. Inst. Of Pharmaceutical Sciences Musashino Univ.
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Kiyosawa Naoki
Medicinal Safety Research Labs. Daiichi Sankyo Co. Ltd.
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Tanaka K
Kobe‐gakuin Univ. Kobe Jpn
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