FHA Domain-mediated DNA Checkpoint Regulation of Rad53

Overview

Journal Cell Cycle

Specialty Cell Biology

Date 2003 Jul 10

PMID 12851493

Citations 29

Authors

Marc F Schwartz

Soo-Jung Lee

Jimmy K Duong

Seda Eminaga

David F Stern

Affiliations

Soon will be listed here.

Abstract

Saccharomyces cerevisiae Rad53 is a protein kinase central to the DNA damage and DNA replication checkpoint signaling pathways. In addition to its catalytic domain, Rad53 contains two forkhead homology-associated (FHA) domains (FHA1 and FHA2), which are phosphopeptide binding domains. The Rad53 FHA domains are proposed to mediate the interaction of Rad53 with both upstream and downstream branches of the DNA checkpoint signaling pathways. Here we show that concurrent mutation of Rad53 FHA1 and FHA2 causes DNA checkpoint defects approaching that of inactivation or loss of RAD53 itself. Both FHA1 and FHA2 are required for the robust activation of Rad53 by the RAD9-dependent DNA damage checkpoint pathway, while an intact FHA1 or FHA2 allows the activation of Rad53 in response to replication block. Mutation of Rad53 FHA1 causes the persistent activation of the RAD9-dependent DNA damage checkpoint pathway in response to replicational stress, suggesting that the RAD53-dependent stabilization of stalled replication forks functions through FHA1. Rad53 FHA1 is also required for the phosphorylation-dependent association of Rad53 with the chromatin assembly factor Asf1, although Asf1 itself is apparently not required for the prevention of DNA damage in response to replication block.

Citing Articles

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Checkpoint Responses to DNA Double-Strand Breaks.

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Replication checkpoint: tuning and coordination of replication forks in s phase.

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Chen E, Hoch N, Wang S, Pellicioli A, Heierhorst J, Tsai M Mol Cell Proteomics. 2013; 13(2):551-65.

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