Limited Effects of Disrupted Gap Junctions in the Liver on Multi-organ Carcinogenesis Induced by Diisopropanolnitrosamine in the Mutant Connexin 32 Transgenic Rat
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概要
- 論文の詳細を見る
Gap junctions, composed from molecules called connexins, play important roles in cell-to-cell communication and aberrant gap junctional intercellular communication (GJIC) has been reported in many types of cancers. We have established transgenic rats bearing a dominant negative mutant of the connexin 32 gene under control of the albumin promoter. In these rats, GJIC is markedly decreased in the liver, and is associated with increased induction of preneoplastic foci after a single treatment of diethylnitrosamine. In the present study, in order to explore whether organs other than the liver would demonstrate increased susceptibility to a carcinogen, we treated these transgenic rats (having disrupted GJIC of the liver) with diisopropanolnitrosamine (DHPN), a carcinogen targeting multiple organs, such as the liver, lung, kidney and thyroid gland. We found that increased susceptibility for the carcinogenicity was evident only in the liver, but not in the lung, kidney and thyroid gland. This result indicates that disrupted GJIC in the liver influences the liver carcinogenesis, but has no effect on carcinogenesis in other organs.
- 日本毒性病理学会の論文
- 2006-06-01
著者
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高橋 智
首都大学東京 大学院理工学研究科機械工学専攻
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SHIRAI Tomoyuki
Department of Pathology, Nagoya City University Medical School
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Tamano S
Dims Institute Of Medical Science Inc.
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OGAWA Kumiko
Department of Experimental Pathology and Tumor Biology, Nagoya City University Graduate School of Me
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ASAMOTO Makoto
Department of Experimental Pathology and Tumor Biology, Nagoya City University Graduate School of Me
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Shirai T
Experimental Pathology And Tumor Biology Graduate School Of Medical Sciences Nagoya City University
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Shirai Tomoyuki
ボゾリサーチセンター御殿場研究所
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Ogawa Kumiko
名古屋市立大学 医学研究科実験病態病理学
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Ogawa K
Nagoya City Univ. Medical School Nagoya
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Asamoto M
Department Of Experimental Pathology And Tumor Biology Graduate School Of Medical Sciences Nagoya Ci
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Asamoto M
Department Of Experimental Pathology And Tumor Biology Nagoya City University Graduate School Of Med
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Asamoto Makoto
国立がんセンター
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Asamoto Makoto
住友製薬大阪研究所
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HOKAIWADO Naomi
Department of Experimental Pathology and Tumor Biology, Nagoya City University, Graduate School of M
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MURASAKI Toshiya
Department of Experimental Pathology and Tumor Biology, Nagoya City University Graduate School of Me
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Sugimura T
Cancer Prevention Basic Research Project National Cancer Center Research Institute
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Mutai Mamoru
First Department Of Pathology Nagoya City University Medical School
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Shimokawa T
National Cancer Center Res. Inst. Tokyo Jpn
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SHIRAI Tomoyuki
Nagoya City University Medical School
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Shirai Tomoyuki
Graduate School Of Medical Sciences Nagoya City University
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Takahashi S
Department Of Experimental Pathology And Tumor Biology Nagoya City University Graduate School Of Med
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Hokaiwado Naomi
Department Of Experimental Pathology And Tumor Biology Nagoya City University Graduate School Of Med
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Hokaiwado Naomi
Experimental Pathology And Chemotherapy Division National Cancer Center Research Institute
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Murasaki Toshiya
Department Of Experimental Pathology And Tumor Biology Nagoya City University Graduate School Of Med
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Shirai Tomoyuki
Department Of Biochemistry Niigata College Of Pharmacy
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Shirai T
大雄会医科学研究所
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Tamano Seiko
First Department Of Pathology Nagoya City University Medical School
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Asamoto Makoto
Department Of Experimental Pathology And Tumor Biology Graduate School Of Medical Sciences Nagoya Ci
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Sugimura T
Carcinogenesis Division National Cancer Center Research Institute
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Shirai Tomoyuki
Pathology Group Yakult Central Inst.
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Ogawa Kumiko
Department Of Experimental Pathology And Tumor Biology Nagoya City University Graduate School Of Med
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Ogawa Kumiko
Department Of Experimental Pathology And Tumor Biology Graduate School Of Medical Sciences Nagoya Ci
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