| Literature DB >> 30078706 |
Anthony Tubbs1, Sriram Sridharan1, Niek van Wietmarschen1, Yaakov Maman1, Elsa Callen1, Andre Stanlie1, Wei Wu1, Xia Wu2, Amanda Day1, Nancy Wong1, Mianmian Yin3, Andres Canela1, Haiqing Fu4, Christophe Redon4, Steven C Pruitt5, Yan Jaszczyszyn6, Mirit I Aladjem4, Peter D Aplan3, Olivier Hyrien2, André Nussenzweig7.
Abstract
Replication origins, fragile sites, and rDNA have been implicated as sources of chromosomal instability. However, the defining genomic features of replication origins and fragile sites are among the least understood elements of eukaryote genomes. Here, we map sites of replication initiation and breakage in primary cells at high resolution. We find that replication initiates between transcribed genes within nucleosome-depleted structures established by long asymmetrical poly(dA:dT) tracts flanking the initiation site. Paradoxically, long (>20 bp) (dA:dT) tracts are also preferential sites of polar replication fork stalling and collapse within early-replicating fragile sites (ERFSs) and late-replicating common fragile sites (CFSs) and at the rDNA replication fork barrier. Poly(dA:dT) sequences are fragile because long single-strand poly(dA) stretches at the replication fork are unprotected by the replication protein A (RPA). We propose that the evolutionary expansion of poly(dA:dT) tracts in eukaryotic genomes promotes replication initiation, but at the cost of chromosome fragility. Published by Elsevier Inc.Entities:
Keywords: DNA breaks; fragile sites; genome instability; poly(dA:dT) tracts; replication fork barrier; replication origins; replication stress; ribosomal DNA
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Year: 2018 PMID: 30078706 PMCID: PMC6591735 DOI: 10.1016/j.cell.2018.07.011
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582