MEPE/OF45 protects cells from DNA damage induced killing via stabilizing CHK1.
Matrix extracellular phosphoglycoprotein/osteoblast factor 45 (MEPE/OF45) was cloned in 2000 with functions related to bone metabolism. We identified MEPE/OF45 for the first time as a new co-factor of CHK1 in mammalian cells to protect cells from DNA damage induced killing. We demonstrate here that MEPE/OF45 directly interacts with CHK1. Knocking ... down MEPE/OF45 decreases CHK1 levels and sensitizes the cells to DNA damage inducers such as ionizing radiation (IR) or camptothicin (CPT)-induced killing. Over-expressing wild-type MEPE/OF45, but not the mutant MEPE/OF45 (depleted the key domain to interact with CHK1) increases CHK1 levels in the cells and increases the resistance of the cells to IR or CPT. MEPE/OF45, interacting with CHK1, increases CHK1 half-life and decreases CHK1 degradation through the ubiquitine-mediated pathway. In addition, the interaction of MEPE/OF45 with CHK1 decreases CHK1 levels in the ubiquitin E3 ligases (Cul1 and Cul4A) complex, which suggests that MEPE/OF45 competes with the ubiquitin E3 ligases binding to CHK1 and thus decreases CHK1 from ubiquitin-mediated proteolysis. These findings reveal an important role of MEPE/OF45 in protecting cells from DNA damage induced killing through stabilizing CHK1, which would provide MEPE/OF45 as a new target for sensitizing tumor cells to radiotherapy or chemotherapy.
Mesh Terms:
Animals, Cell Line, Transformed, Cytoprotection, DNA Damage, Enzyme Stability, Extracellular Matrix Proteins, Glycoproteins, Phosphoproteins, Protein Kinases, Rats, Ubiquitins
Animals, Cell Line, Transformed, Cytoprotection, DNA Damage, Enzyme Stability, Extracellular Matrix Proteins, Glycoproteins, Phosphoproteins, Protein Kinases, Rats, Ubiquitins
Nucleic Acids Res.
Date: Dec. 01, 2009
PubMed ID: 19808933
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