Destruxin E, a Cyclodepsipeptide Antibiotic, Reduces Cyclin D1 Levels and Inhibits Anchorage-Independent Growth of v-Ki-ras-Expressed pMAM-ras-REF Cells (Biopharmacy)
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概要
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Destruxin E (DE), a cyclodepsipeptide isolated from fermentation broths of Metarhizium sp. MA324, inhibited the growth of v-Ki-ras-expressed pMAM-ras-REF (rasREF) cells in the suspension (anchorage-independent) culture (a) more strongly than that in the substratum-attached (anchorage-dependent) culture (b) or that of v-Ki-ras-unexpressed pMAM-ras-REF (REF) cells in the substratum-attached culture (c); the IC_<50> values of DE were 0.07μM (a), 0.4μM (b), and 1.2μM (c). DE arrested G1 phase cell cycle progression of rasREF cells in the substratum-attached culture (b). In rasREF cells treated with DE for 72 h in suspension culture (a), the levels of cyclin D1, cyclin A, p27^<Kip1>, and hyperphosphorylated Rb were decreased, but the levels of cdk4, cdk6, cdk2, p16^<INK4a>, and p21^<Cip1> were not affected. Among these effects, the decrease in cyclin D1 was prominent. DE decreased the level of cyclin D1 in rasREF cells in the suspension culture (a) at 0.1μM and in the substratum-attached culture (b) at 1 μM, while the level of cyclin D1 in REF cells in the substratum-attached culture (c) was not decreased at 1 μM. The extent of growth inhibition correlated with the decrease in cyclin D1. The level of cyclin D1 mRNA of rasREF cells in the suspension culture (a) was also decreased by DE. DE decreased cyclin D1 mRNA, resulting in inhibition of anchorage-independent growth of rasREF cells.
- 公益社団法人日本薬学会の論文
- 2004-04-01
著者
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Hori M
Showa Pharmaceutical University
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HOSOKAWA Nobuo
Institute of Microbial Chemistry
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TSUCHIYA Kayoko
Showa College of Pharmaceutical Sciences
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HORI Makoto
Showa College of Pharmaceutical Sciences
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UEHARA Yoshimasa
Department of Bioactive Molecules, National Institute of Infectious Diseases
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Hosokawa Nobuo
Microbial Chemistry Research Center
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Hori M
Hokkaido Univ. Graduate School Of Pharmaceutical Sci. Sapporo Jpn
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IKENO Souichi
Showa College of Pharmaceutical Sciences
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Hosokawa N
Microbial Chemistry Research Center
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KOBAYASHI Takanori
Showa Pharmaceutical University
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Tsuchiya Kayoko
Showa Pharmaceutical University
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Uehara Yoshimasa
Department Of Bioactive Molecules National Institute Of Infectious Diseases
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Ikeno S
Showa Pharmaceutical University
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Tsuchiya K
Showa Pharmaceutical University
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Matsumoto Hiroshi
Tokushima Research Center Taiho Pharmaceutical Co. Ltd.
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