Add to ORKGCheckpoint kinase 1 (Chk1) is a checkpoint gene that is activated after DNA damage. It phosphorylates and inactivates the Cdc2 activating phosphatase Cdc25C. This in turn inactivates Cdc2, which leads to G2/M arrest. We report that blocking Chk1 expression by antisense or ribozymes in mammalian cells induces apoptosis and interferes with the G2/M arrest induced by adriamycin. The Chk1 inhibitor UCN-01 also blocks the G2 arrest after DNA damage and renders cells more susceptible to adriamycin. These results indicate that Chk1 is an essential gene for the checkpoint mechanism during normal cell proliferation as well as in the DNA damage response. Neoplasia (2001) 3, 411–419
Besides the well-understood DNA damage response via establishment of G2 checkpoint arrest, novel stu...
The E2F-1 transcription factor is regulated during cell cycle progression and induced by cellular st...
SummaryBackgroundCheckpoint signaling pathways are of crucial importance for the maintenance of geno...
AbstractCheckpoint kinase 1 (Chki) is a checkpoint gene that is activated after DNA damage. It phosp...
Topoisomerase II poisons like Adriamycin (ADR, doxorubicin) are clinically important chemotherapeuti...
Mammalian Chk1 is an essential kinase for embryonic development and plays an important role in the c...
Checkpoint kinase 1 (CHK1) is a key mediator that links the machineries that monitor DNA integrity t...
Cell cycle ckeckpoints are activated in response to DNA damage. Their role consists in blocking the ...
Cyclin-dependent kinases (Cdks) promote cellular proliferation, are often deregulated in human cance...
AbstractThe cellular response to DNA damage involves checkpoint controls that delay cell cycle progr...
Genotoxic antitumor agents continue to be the mainstay of current cancer chemotherapy. These drugs c...
The role of Chk1 in the cellular response to DNA replication stress is well established. However rec...
In the presence of sustained DNA damage occurring in S-phase or G2, normal cells arrest before mitos...
Tumor cells often become resistant to DNA damage–based therapy; however, the underlying mechanisms a...
The conserved protein kinase Chk1 is believed to play an important role in checkpoint responses to a...
Besides the well-understood DNA damage response via establishment of G2 checkpoint arrest, novel stu...
The E2F-1 transcription factor is regulated during cell cycle progression and induced by cellular st...
SummaryBackgroundCheckpoint signaling pathways are of crucial importance for the maintenance of geno...
AbstractCheckpoint kinase 1 (Chki) is a checkpoint gene that is activated after DNA damage. It phosp...
Topoisomerase II poisons like Adriamycin (ADR, doxorubicin) are clinically important chemotherapeuti...
Mammalian Chk1 is an essential kinase for embryonic development and plays an important role in the c...
Checkpoint kinase 1 (CHK1) is a key mediator that links the machineries that monitor DNA integrity t...
Cell cycle ckeckpoints are activated in response to DNA damage. Their role consists in blocking the ...
Cyclin-dependent kinases (Cdks) promote cellular proliferation, are often deregulated in human cance...
AbstractThe cellular response to DNA damage involves checkpoint controls that delay cell cycle progr...
Genotoxic antitumor agents continue to be the mainstay of current cancer chemotherapy. These drugs c...
The role of Chk1 in the cellular response to DNA replication stress is well established. However rec...
In the presence of sustained DNA damage occurring in S-phase or G2, normal cells arrest before mitos...
Tumor cells often become resistant to DNA damage–based therapy; however, the underlying mechanisms a...
The conserved protein kinase Chk1 is believed to play an important role in checkpoint responses to a...
Besides the well-understood DNA damage response via establishment of G2 checkpoint arrest, novel stu...
The E2F-1 transcription factor is regulated during cell cycle progression and induced by cellular st...
SummaryBackgroundCheckpoint signaling pathways are of crucial importance for the maintenance of geno...