| Literature DB >> 34625299 |
Bhushan L Thakur1, Anagh Ray1, Christophe E Redon1, Mirit I Aladjem2.
Abstract
Cells activate distinctive regulatory pathways that prevent excessive initiation of DNA replication to achieve timely and accurate genome duplication. Excess DNA synthesis is constrained by protein-DNA interactions that inhibit initiation at dormant origins. In parallel, specific modifications of pre-replication complexes prohibit post-replicative origin relicensing. Replication stress ensues when the controls that prevent excess replication are missing in cancer cells, which often harbor extrachromosomal DNA that can be further amplified by recombination-mediated processes to generate chromosomal translocations. The genomic instability that accompanies excess replication origin activation can provide a promising target for therapeutic intervention. Here we review molecular pathways that modulate replication origin dormancy, prevent excess origin activation, and detect, encapsulate, and eliminate persistent excess DNA. Published by Elsevier Ltd.Entities:
Keywords: DNA damage; dormant origins; extrachromosomal DNA; extrachromosomal circular DNA; genomic instability; overreplication; re-replication; replication origins
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Year: 2021 PMID: 34625299 PMCID: PMC8752500 DOI: 10.1016/j.tig.2021.09.008
Source DB: PubMed Journal: Trends Genet ISSN: 0168-9525 Impact factor: 11.639