Abstract
Faithful chromosome segregation and genome maintenance requires the removal of all DNA bridges that physically link chromosomes before cells divide. Using C. elegans embryos we show that the LEM-3/Ankle1 nuclease defines a previously undescribed genome integrity mechanism by processing DNA bridges right before cells divide. LEM-3 acts at the midbody, the structure where abscission occurs at the end of cytokinesis. LEM-3 localization depends on factors needed for midbody assembly, and LEM-3 accumulation is increased and prolonged when chromatin bridges are trapped at the cleavage plane. LEM-3 locally processes chromatin bridges that arise from incomplete DNA replication, unresolved recombination intermediates, or the perturbance of chromosome structure. Proper LEM-3 midbody localization and function is regulated by AIR-2/Aurora B kinase. Strikingly, LEM-3 acts cooperatively with the BRC-1/BRCA1 homologous recombination factor to promote genome integrity. These findings provide a molecular basis for the suspected role of the LEM-3 orthologue Ankle1 in human breast cancer.
Original language | English |
---|---|
Article number | 728 |
Number of pages | 11 |
Journal | Nature Communications |
Volume | 9 |
Issue number | 1 |
DOIs | |
Publication status | Published - 20 Feb 2018 |
Austrian Fields of Science 2012
- 106023 Molecular biology
- 106052 Cell biology
Keywords
- C. ELEGANS EMBRYOS
- CAENORHABDITIS-ELEGANS
- ANAPHASE BRIDGES
- OVARIAN-CANCER
- CYTOKINESIS
- RESOLUTION
- REPAIR
- CELLS
- SUSCEPTIBILITY
- COMPLETION