Centrosome-associated regulators of the G2/M checkpoint as targets for cancer therapy

被引:0
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作者
Yingmei Wang
Ping Ji
Jinsong Liu
Russell R Broaddus
Fengxia Xue
Wei Zhang
机构
[1] Tianjin Medical University,Tianjin General Hospital
[2] The University of Texas MD Anderson Cancer Center,Department of Pathology
来源
Molecular Cancer | / 8卷
关键词
Berberine; Daidzein; Cell Cycle Checkpoint; Aurora Kinase; Flavopiridol;
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摘要
In eukaryotic cells, control mechanisms have developed that restrain cell-cycle transitions in response to stress. These regulatory pathways are termed cell-cycle checkpoints. The G2/M checkpoint prevents cells from entering mitosis when DNA is damaged in order to afford these cells an opportunity to repair the damaged DNA before propagating genetic defects to the daughter cells. If the damage is irreparable, checkpoint signaling might activate pathways that lead to apoptosis. Since alteration of cell-cycle control is a hallmark of tumorigenesis, cell-cycle regulators represent potential targets for therapy. The centrosome has recently come into focus as a critical cellular organelle that integrates G2/M checkpoint control and repairs signals in response to DNA damage. A growing number of G2/M checkpoint regulators have been found in the centrosome, suggesting that centrosome has an important role in G2/M checkpoint function. In this review, we discuss centrosome-associated regulators of the G2/M checkpoint, the dysregulation of this checkpoint in cancer, and potential candidate targets for cancer therapy.
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