Projects per year
Abstract
Replisome disassembly is the final step of DNA replication in eukaryotes, involving the ubiquitylation and CDC48-dependent dissolution of the CMG helicase (Cdc45-MCM-GINS). Using Caenorhabditis elegans early embryos and Xenopus egg extracts, we show that the E3 ligase CUL-2LRR-1 associates with the replisome and drives ubiquitylation and disassembly of CMG, together with the CDC-48 co-factors UFD-1 and NPL-4. Removal of CMG from chromatin in frog egg extracts requires CUL2 neddylation, and our data identify chromatin recruitment of CUL2LRR1 as a key regulated step during DNA replication termination. Interestingly, however, CMG persists on chromatin until prophase in worms that lack CUL-2LRR-1, but is then removed by a mitotic pathway that requires the CDC-48 co-factor UBXN-3, orthologous to the human tumour suppressor FAF1. Partial inactivation of lrr-1 and ubxn-3 leads to synthetic lethality, suggesting future approaches by which a deeper understanding of CMG disassembly in metazoa could be exploited therapeutically.
Original language | English |
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Pages (from-to) | 468–479 |
Journal | Nature Cell Biology |
Volume | 19 |
Early online date | 3 Apr 2017 |
DOIs | |
Publication status | Published - May 2017 |
Keywords
- DNA replication termination
- replisome disassembly
- CMG helicase
- Caenorhabditis elegans
- Xenopus laevis
- Cullin
- CUL-2
- LRR-1
- UBXN-3
- FAF1
- CUL2
- LRR1
- CDC-48
- UFD-1
- NPL-4
- p97
- VCP
- ULP-4
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Dive into the research topics of 'CUL-2LRR-1 and UBXN-3 drive replisome disassembly during DNA replication termination and mitosis'. Together they form a unique fingerprint.Projects
- 1 Finished
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Replisome disassembly at sites of DNA damage
LISTER INSTITUTE OF PREVENTATIVE MEDICINE
13/03/17 → 21/05/17
Project: Research
Prizes
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MRC Career Development Fellowship
Gambus, Aga (Recipient), 1 Mar 2013
Prize: Fellowship awarded competitively