The checkpoint proteins Rad53 and Mec1-Ddc2 regulate many aspects of cell metabolism in response to DNA damage. We have examined the relative importance of downstream checkpoint effectors on cell viability. Checkpoint regulation of mitosis, gene expression, and late origin firing make only modest contributions to viability. By contrast, the checkpoint is essential for preventing irreversible breakdown of stalled replication forks. Moreover, recruitment of Ddc2 to nuclear foci and subsequent activation of the Rad53 kinase only occur during S phase and require the assembly of replication forks. Thus, DNA replication forks are both activators and primary effectors of the checkpoint pathway in S phase.

Tercero, J., Longhese, M., Diffley, J. (2003). A central role for DNA replication forks in checkpoint activation and response. MOLECULAR CELL, 11(5), 1323-1336 [10.1016/S1097-2765(03)00169-2].

A central role for DNA replication forks in checkpoint activation and response

LONGHESE, MARIA PIA;
2003

Abstract

The checkpoint proteins Rad53 and Mec1-Ddc2 regulate many aspects of cell metabolism in response to DNA damage. We have examined the relative importance of downstream checkpoint effectors on cell viability. Checkpoint regulation of mitosis, gene expression, and late origin firing make only modest contributions to viability. By contrast, the checkpoint is essential for preventing irreversible breakdown of stalled replication forks. Moreover, recruitment of Ddc2 to nuclear foci and subsequent activation of the Rad53 kinase only occur during S phase and require the assembly of replication forks. Thus, DNA replication forks are both activators and primary effectors of the checkpoint pathway in S phase.
Articolo in rivista - Articolo scientifico
DNA replication; checkpoint; DNA damage; replication forks
English
mag-2003
11
5
1323
1336
none
Tercero, J., Longhese, M., Diffley, J. (2003). A central role for DNA replication forks in checkpoint activation and response. MOLECULAR CELL, 11(5), 1323-1336 [10.1016/S1097-2765(03)00169-2].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10281/1826
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