| Literature DB >> 30189101 |
Xia Wu1,2, Hadi Kabalane3, Malik Kahli1, Nataliya Petryk1, Bastien Laperrousaz3,4, Yan Jaszczyszyn5, Guenola Drillon3, Frank-Emmanuel Nicolini4,6, Gaëlle Perot7, Aude Robert8, Cédric Fund9, Frédéric Chibon7, Ruohong Xia2, Joëlle Wiels8, Françoise Argoul10, Véronique Maguer-Satta4, Alain Arneodo10, Benjamin Audit3, Olivier Hyrien1.
Abstract
The spatiotemporal program of metazoan DNA replication is regulated during development and altered in cancers. We have generated novel OK-seq, Repli-seq and RNA-seq data to compare the DNA replication and gene expression programs of twelve cancer and non-cancer human cell types. Changes in replication fork directionality (RFD) determined by OK-seq are widespread but more frequent within GC-poor isochores and largely disconnected from transcription changes. Cancer cell RFD profiles cluster with non-cancer cells of similar developmental origin but not with different cancer types. Importantly, recurrent RFD changes are detected in specific tumour progression pathways. Using a model for establishment and early progression of chronic myeloid leukemia (CML), we identify 1027 replication initiation zones (IZs) that progressively change efficiency during long-term expression of the BCR-ABL1 oncogene, being twice more often downregulated than upregulated. Prolonged expression of BCR-ABL1 results in targeting of new IZs and accentuation of previous efficiency changes. Targeted IZs are predominantly located in GC-poor, late replicating gene deserts and frequently silenced in late CML. Prolonged expression of BCR-ABL1 results in massive deletion of GC-poor, late replicating DNA sequences enriched in origin silencing events. We conclude that BCR-ABL1 expression progressively affects replication and stability of GC-poor, late-replicating regions during CML progression.Entities:
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Year: 2018 PMID: 30189101 PMCID: PMC6212843 DOI: 10.1093/nar/gky797
Source DB: PubMed Journal: Nucleic Acids Res ISSN: 0305-1048 Impact factor: 16.971