Παρασκευή 1 Ιουλίου 2016

PCNA Retention on DNA into G2/M Phase Causes Genome Instability in Cells Lacking Elg1

Publication date: Available online 30 June 2016
Source:Cell Reports
Author(s): Catherine Johnson, Vamsi K. Gali, Tatsuro S. Takahashi, Takashi Kubota
Loss of the genome maintenance factor Elg1 causes serious genome instability that leads to cancer, but the underlying mechanism is unknown. Elg1 forms the major subunit of a replication factor C-like complex, Elg1-RLC, which unloads the ring-shaped polymerase clamp PCNA from DNA during replication. Here, we show that prolonged retention of PCNA on DNA into G2/M phase is the major cause of genome instability in elg1Δ yeast. Overexpression-induced accumulation of PCNA on DNA causes genome instability. Conversely, disassembly-prone PCNA mutants that relieve PCNA accumulation rescue the genome instability of elg1Δ cells. Covalent modifications to the retained PCNA make only a minor contribution to elg1Δ genome instability. By engineering cell-cycle-regulated ELG1 alleles, we show that abnormal accumulation of PCNA on DNA during S phase causes moderate genome instability and its retention through G2/M phase exacerbates genome instability. Our results reveal that PCNA unloading by Elg1-RLC is critical for genome maintenance.

Graphical abstract

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Teaser

Loss of the genome maintenance factor Elg1 causes serious genome instability. Johnson et al. find that PCNA unloading by Elg1 is critical for genome maintenance, and that PCNA retention on DNA into G2/M phase causes genome instability in cells lacking Elg1.


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