Authors
E Randal Hofmann, Stuart Milstein, Simon J Boulton, Mianjia Ye, Jen J Hofmann, Lilli Stergiou, Anton Gartner, Marc Vidal, Michael O Hengartner
Publication date
2002/11/19
Journal
Current biology
Volume
12
Issue
22
Pages
1908-1918
Publisher
Elsevier
Description
Background: The inability to efficiently repair DNA damage or remove cells with severely damaged genomes has been linked to several human cancers. Studies in yeasts and mammals have identified several genes that are required for proper activation of cell cycle checkpoints following various types of DNA damage. However, in metazoans, DNA damage can induce apoptosis as well. How DNA damage activates the apoptotic machinery is not fully understood.
Results: We demonstrate here that the Caenorhabditis elegans gene hus-1 is required for DNA damage-induced cell cycle arrest and apoptosis. Following DNA damage, HUS-1 relocalizes and forms distinct foci that overlap with chromatin. Relocalization does not require the novel checkpoint protein RAD-5; rather, relocalization appears more frequently in rad-5 mutants, suggesting that RAD-5 plays a role in repair. HUS-1 is required for genome stability, as …
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