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   WIP1 phosphatase as pharmacological target in cancer therapy  
   
نویسنده Pecháčková Soňa ,Burdová Kamila ,Macurek Libor
منبع journal of molecular medicine - 2017 - دوره : 95 - شماره : 6 - صفحه:589 -599
چکیده    Dna damage response (ddr) pathway protects cells from genome instability and prevents cancer development. tumor suppressor p53 is a key molecule that interconnects ddr, cell cycle checkpoints, and cell fate decisions in the presence of genotoxic stress. inactivating mutations in tp53 and other genes implicated in ddr potentiate cancer development and also influence the sensitivity of cancer cells to treatment. protein phosphatase 2c delta (referred to as wip1) is a negative regulator of ddr and has been proposed as potential pharmaceutical target. until recently, exploitation of wip1 inhibition for suppression of cancer cell growth was compromised by the lack of selective small-molecule inhibitors effective at cellular and organismal levels. here, we review recent advances in development of wip1 inhibitors and discuss their potential use in cancer treatment.
کلیدواژه Cancer ,Phosphatase ,Checkpoint ,DNA damage response ,Inhibitor ,p53
آدرس Institute of Molecular Genetics of the ASCR, Department of Cancer Cell Biology, Czech Republic, Institute of Molecular Genetics of the ASCR, Department of Cancer Cell Biology, Czech Republic, Institute of Molecular Genetics of the ASCR, Department of Cancer Cell Biology, Czech Republic
 
     
   
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