Impaired Replication Timing Promotes Tissue-Specific Expression of Common Fragile Sites

Maccaroni, Klizia; Balzano, Elisa; Mirimao, Federica; Giunta, Simona; Pelliccia, Franca

doi:10.3390/genes11030326

Cited by 24 publications

(29 citation statements)

References 74 publications

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“…Furthermore, the effect was independent of fragile site coincidence even though fragile sites are renowned harbours of long genes ( 56 , 78 ) and the mean length of established fusions also significantly exceeded that of a simulated dataset produced using the same mapping pipeline (Figure 3E ). Operationally, the replication of long genes is limited by their transcription that may be incomplete over more than one round of cell division ( 79 ). Where long genes are also poor in initiation sites, delayed replication in concert with the extended distance of fork travel renders these sites vulnerable to instability ( 78 ).…”

Section: Discussionmentioning

confidence: 99%

Tracking telomere fusions through crisis reveals conflict between DNA transcription and the DNA damage response

et al. 2021

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Identifying attributes that distinguish pre-malignant from senescent cells provides opportunities for targeted disease eradication and revival of anti-tumour immunity. We modelled a telomere-driven crisis in four human fibroblast lines, sampling at multiple time points to delineate genomic rearrangements and transcriptome developments that characterize the transition from dynamic proliferation into replicative crisis. Progression through crisis was associated with abundant intra-chromosomal telomere fusions with increasing asymmetry and reduced microhomology usage, suggesting shifts in DNA repair capacity. Eroded telomeres also fused with genomic loci actively engaged in transcription, with particular enrichment in long genes. Both gross copy number alterations and transcriptional responses to crisis likely underpin the elevated frequencies of telomere fusion with chromosomes 9, 16, 17, 19 and most exceptionally, chromosome 12. Juxtaposition of crisis-regulated genes with loci undergoing de novo recombination exposes the collusive contributions of cellular stress responses to the evolving cancer genome.

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Section: Discussionmentioning

confidence: 99%

Tracking telomere fusions through crisis reveals conflict between DNA transcription and the DNA damage response

et al. 2021

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“…Unlike constitutively fragile locations, such as fragile X, CFSs form in a cell-type-specific manner, leading to suggestions that an epigenetic component has a role in their fragility ( Letessier et al., 2011 ; Le Tallec et al., 2011 ). A number of factors have been identified, including late replication timing, transcription of long genes, and features of the underlying DNA sequence ( Blin et al., 2019 ; Brison et al., 2019 ; Fungtammasan et al., 2012 ; Helmrich et al., 2011 ; Maccaroni et al., 2020 ; Okamoto et al., 2018 ; Le Tallec et al., 2014 ; Wei et al., 2016 ; Wilson et al., 2015 ). CFSs also require FANCD2 for efficient replication ( Madireddy et al., 2016 ; Pentzold et al., 2018 ) and have been identified as regions in which active DNA synthesis is apparent on mitotic chromosomes in a process dependent on POLD3 and the Mus81 nuclease ( Minocherhomji et al., 2015 ).…”

Section: Introductionmentioning

confidence: 99%

Common Fragile Sites Are Characterized by Faulty Condensin Loading after Replication Stress

et al. 2020

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Summary Cells coordinate interphase-to-mitosis transition, but recurrent cytogenetic lesions appear at common fragile sites (CFSs), termed CFS expression, in a tissue-specific manner after replication stress, marking regions of instability in cancer. Despite such a distinct defect, no model fully provides a molecular explanation for CFSs. We show that CFSs are characterized by impaired chromatin folding, manifesting as disrupted mitotic structures visible with molecular fluorescence in situ hybridization (FISH) probes in the presence and absence of replication stress. Chromosome condensation assays reveal that compaction-resistant chromatin lesions persist at CFSs throughout the cell cycle and mitosis. Cytogenetic and molecular lesions are marked by faulty condensin loading at CFSs, a defect in condensin-I-mediated compaction, and are coincident with mitotic DNA synthesis (MIDAS). This model suggests that, in conditions of exogenous replication stress, aberrant condensin loading leads to molecular defects and CFS expression, concomitantly providing an environment for MIDAS, which, if not resolved, results in chromosome instability.

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“…As cells differentiate from a highly proliferative pluripotent stem cell, they alter replication timing in a cell-type-dependent manner as well as origin usage [ 206 , 207 , 208 ]. Furthermore, common fragile sites show lineage specificity, indicating that different regions of the genome are sensitive to perturbation of the replication program depending on the cell type [ 209 ]. It is therefore conceivable that differences in the replication program sensitize specific cell types to depletion of origin licensing or origin firing factors [ 209 , 210 , 211 ].…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, common fragile sites show lineage specificity, indicating that different regions of the genome are sensitive to perturbation of the replication program depending on the cell type [ 209 ]. It is therefore conceivable that differences in the replication program sensitize specific cell types to depletion of origin licensing or origin firing factors [ 209 , 210 , 211 ]. For example, we recently proposed that NK cells are sensitive to MCM10 depletion due to enhanced telomere erosion [ 85 ].…”

Section: Discussionmentioning

confidence: 99%

Congenital Diseases of DNA Replication: Clinical Phenotypes and Molecular Mechanisms

Schmit

Bielinsky

2021

IJMS

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Deoxyribonucleic acid (DNA) replication can be divided into three major steps: initiation, elongation and termination. Each time a human cell divides, these steps must be reiteratively carried out. Disruption of DNA replication can lead to genomic instability, with the accumulation of point mutations or larger chromosomal anomalies such as rearrangements. While cancer is the most common class of disease associated with genomic instability, several congenital diseases with dysfunctional DNA replication give rise to similar DNA alterations. In this review, we discuss all congenital diseases that arise from pathogenic variants in essential replication genes across the spectrum of aberrant replisome assembly, origin activation and DNA synthesis. For each of these conditions, we describe their clinical phenotypes as well as molecular studies aimed at determining the functional mechanisms of disease, including the assessment of genomic stability. By comparing and contrasting these diseases, we hope to illuminate how the disruption of DNA replication at distinct steps affects human health in a surprisingly cell-type-specific manner.

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Impaired Replication Timing Promotes Tissue-Specific Expression of Common Fragile Sites

Cited by 24 publications

References 74 publications

Tracking telomere fusions through crisis reveals conflict between DNA transcription and the DNA damage response

Tracking telomere fusions through crisis reveals conflict between DNA transcription and the DNA damage response

Common Fragile Sites Are Characterized by Faulty Condensin Loading after Replication Stress

Congenital Diseases of DNA Replication: Clinical Phenotypes and Molecular Mechanisms

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