Literature DB >> 11679575

Sustained activation of p34(cdc2) is required for noscapine-induced apoptosis.

K Ye1, J Zhou, J W Landen, E M Bradbury, H C Joshi.   

Abstract

Mitotic arrest and subsequent apoptosis has been observed in many types of cells treated with anti-microtubule agents. However, the molecular mechanisms underlying the two events as well as their relationship are not well understood; on the contrary, there has been increasing evidence indicating that anti-microtubule agents might induce apoptosis via signaling pathways independent of mitosis. In this study, we found that apoptosis induced by noscapine, an anti-microtubule drug previously shown to cause both mitotic arrest and apoptotic cell death, was blocked by inhibiting p34(cdc2) activity with olomoucine in FM3A murine mammary carcinoma cells or by reducing the level and activity of p34(cdc2) in a mutant cell line FT210 derived from FM3A. Furthermore, transfection of the mutant FT210 cells with wild-type p34(cdc2) restored their ability to undergo mitotic arrest and then apoptosis in response to noscapine. Thus, we conclude that sustained activation of the p34(cdc2) kinase during mitotic arrest is required for subsequent apoptosis induced by noscapine, establishing a link between the two events.

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Year:  2001        PMID: 11679575     DOI: 10.1074/jbc.C100550200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  11 in total

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Authors:  Ritu Aneja; Jun Zhou; Surya N Vangapandu; Binfei Zhou; Ramesh Chandra; Harish C Joshi
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Review 5.  Drugs that target dynamic microtubules: a new molecular perspective.

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10.  Proteomics to display tissue repair opposing injury response to LPS-induced liver injury.

Authors:  Xiao-Wei Liu; Fang-Gen Lu; Guang-Sen Zhang; Xiao-Ping Wu; Yu You; Chun-Hui Ouyang; Dong-Ye Yang
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