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Development of pyrrole-imidazole polyamide for specific regulation of human aurora kinase-A and -B gene expression
Authors:Takahashi Teruyuki  Asami Yukihiro  Kitamura Eiko  Suzuki Tsukasa  Wang Xiaofei  Igarashi Jun  Morohashi Aiko  Shinojima Yui  Kanou Hisao  Saito Kosuke  Takasu Toshiaki  Nagase Hiroki  Harada Yuichi  Kuroda Kazumichi  Watanabe Takayoshi  Kumamoto Satoshi  Aoyama Takahiko  Matsumoto Yoshiaki  Bando Toshikazu  Sugiyama Hiroshi  Yoshida-Noro Chikako  Fukuda Noboru  Hayashi Nariyuki
Institution:Advanced Research Institute for the Sciences and Humanities, Nihon University, Tokyo, Japan. teruyuk@med.nihon-u.ac.jp
Abstract:Pyrrole-imidazole polyamide (PIP) is a nuclease-resistant novel compound that inhibits gene expression through binding to the minor groove of DNA. Human aurora kinase-A (AURKA) and -B (AURKB) are important regulators in mitosis during the cell cycle. In this study, two specific PIPs (PIP-A and PIP-B) targeting AURKA and AURKB promoter regions were designed and synthesized, and their biological effects were investigated by several in vitro assays. PIP-A and PIP-B significantly inhibited the promoter activities, mRNA expression, and protein levels of AURKA and AURKB, respectively, in a concentration-dependent manner. Moreover, 1:1 combination treatment with both PIPs demonstrated prominent antiproliferative synergy (CI value ED(50)] = 0.256) to HeLa cells as a result of inducing apoptosis-mediated severe catastrophe of cell-cycle progression. The novel synthesized PIP-A and PIP-B are potent and specific gene-silencing agents for AURKA and AURKB.
Keywords:CHEMBIO  SIGNALING  CELLBIO
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