Abstract
In response to replication hindrances, DNA replication forks frequently stall and are remodelled into a four-way junction. In such a structure the annealed nascent strand is thought to resemble a DNA double-strand break and remodelled forks are vulnerable to nuclease attack by MRE11 and DNA2. Proteins that promote the recruitment, loading and stabilisation of RAD51 onto single-stranded DNA for homology search and strand exchange in homologous recombination (HR) repair and inter-strand cross-link repair also act to set up RAD51-mediated protection of nascent DNA at stalled replication forks. However, despite the similarities of these pathways, several lines of evidence indicate that fork protection is not simply analogous to the RAD51 loading step of HR. Protection of stalled forks not only requires separate functions of a number of recombination proteins, but also utilises nucleases important for the resection steps of HR in alternative ways. Here we discuss how fork protection arises and how its differences with HR give insights into the differing contexts of these two pathways.
Original language | English |
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Pages (from-to) | 14-26 |
Journal | Seminars in Cell and Developmental Biology |
Volume | 113 |
Early online date | 9 Jul 2020 |
DOIs | |
Publication status | Published - May 2021 |
Keywords
- BRCA1
- BRCA2
- Fork reversal
- Homologous recombination
- RAD51
- Replication fork protection
ASJC Scopus subject areas
- Developmental Biology
- Cell Biology