Oncogenes create a unique landscape of fragile sites

Karin Miron, Tamar Golan-Lev, Raz Dvir, Eyal Ben-David, Batsheva Kerem*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

62 Scopus citations


Recurrent genomic instability in cancer is attributed to positive selection and/or the sensitivity of specific genomic regions to breakage. Among these regions are fragile sites (FSs), genomic regions sensitive to replication stress conditions induced by the DNA polymerase inhibitor aphidicolin. However, the basis for the majority of cancer genomic instability hotspots remains unclear. Aberrant oncogene expression induces replication stress, leading to DNA breaks and genomic instability. Here we map the cytogenetic locations of oncogene-induced FSs and show that in the same cells, each oncogene creates a unique fragility landscape that only partially overlaps with aphidicolin-induced FSs. Oncogene-induced FSs colocalize with cancer breakpoints and large genes, similar to aphidicolin-induced FSs. The observed plasticity in the fragility landscape of the same cell type following oncogene expression highlights an additional level of complexity in the molecular basis for recurrent fragility in cancer.

Original languageAmerican English
Article number7094
JournalNature Communications
StatePublished - 11 May 2015

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