Replication stress at microsatellites causes DNA double-strand breaks and break-induced replication

Journal of Biological Chemistry(2020)

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摘要
Short tandemly repeated DNA sequences, termed microsatellites, are abundant in the human genome. These microsatellites exhibit length instability and susceptibility to DNA double-strand breaks (DSBs) due to their tendency to form stable non-B DNA structures. Replication-dependent microsatellite DSBs are linked to genome instability signatures in human developmental diseases and cancers. To probe the causes and consequences of microsatellite DSBs, we designed a dual-fluorescence reporter system to detect DSBs at expanded (CTG/CAG)(n) and polypurine/polypyrimidine (Pu/Py) mirror repeat structures alongside the c-myc replication origin integrated at a single ectopic chromosomal site. Restriction cleavage near the (CTG/CAG)(100) microsatellite leads to homology-directed single-strand annealing between flanking AluY elements and reporter gene deletion that can be detected by flow cytometry. However, in the absence of restriction cleavage, endogenous and exogenous replication stressors induce DSBs at the (CTG/CAG)(100) and Pu/Py microsatellites. DSBs map to a narrow region at the downstream edge of the (CTG)(100) lagging-strand template. (CTG/CAG)(n) chromosome fragility is repeat length-dependent, whereas instability at the (Pu/Py) microsatellites depends on replication polarity. Strikingly, restriction-generated DSBs and replication-dependent DSBs are not repaired by the same mechanism. Knockdown of DNA damage response proteins increases (Rad18, polymerase (Pol) eta, Pol kappa) or decreases (Mus81) the sensitivity of the (CTG/CAG)(100) microsatellites to replication stress. Replication stress and DSBs at the ectopic (CTG/CAG)(100) microsatellite lead to break-induced replication and high-frequency mutagenesis at a flanking thymidine kinase gene. Our results show that non-B structure-prone microsatellites are susceptible to replication-dependent DSBs that cause genome instability.
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关键词
DNA replication,DNA repair,trinucleotide repeat disease,genomic instability,mutagenesis,myotonic dystrophy,cancer,break-induced replication,microsatellite instability,polycystic kidney disease
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