Re-replication is a driving force of tumorigenesis and genomic instability. Here, the authors show that upon re-replication, FANCD2 localizes at early origins to limit replisome progression, ssDNA gap accumulation and fork breakage, revealing a vulnerability for selective targeting of cancer cells.
- Nibal Badra-Fajardo
- Elena Karydi
- Zoi Lygerou
