Literature DB >> 16050137

Caspases-dependent cleavage of mitotic checkpoint proteins in response to microtubule inhibitor.

Kwan-Hyuck Baek1, Hyun-Jin Shin, Sook-Jung Jeong, Joong-Won Park, Frank McKeon, Chang-Woo Lee, Chang-Min Kim.   

Abstract

The mitotic checkpoint ensures the fidelity of chromosomal segregation by delaying the onset of anaphase until all chromosomes are aligned on the metaphase plate. After sustained mitotic arrest, however, cells eventually exit mitosis without the mitotic checkpoint being silenced. These cells then undergo apoptosis, an event that is important for prevention of the chromosomal instability observed in human cancers. An interesting question is to establish the biochemical link between the mitotic checkpoint and the subsequent apoptotic cell death. Here, we found that following prolonged spindle damage, the mitotic checkpoint kinases such as Bub1 and BubR1 were cleaved through a mechanism sensitive to caspases inhibitor. Interestingly, the expression of these mutants resistant to caspases-dependent cleavage led to increased apoptosis after sustained mitotic arrest, and a correspondingly more efficient elimination of the polyploid population than that seen in cells expressing wild-type proteins. These findings provide the novel biochemical properties of mitotic checkpoint proteins through its cleavage by caspases-dependent manner.

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Year:  2005        PMID: 16050137     DOI: 10.3727/096504005776367906

Source DB:  PubMed          Journal:  Oncol Res        ISSN: 0965-0407            Impact factor:   5.574


  17 in total

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8.  Caspase activity is not required for the mitotic checkpoint or mitotic slippage in human cells.

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Review 9.  Cell-Cycle Cross Talk with Caspases and Their Substrates.

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10.  Cell-based expression cloning for identification of polypeptides that hypersensitize mammalian cells to mitotic arrest.

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