Literature DB >> 31113828

Mitotic DNA Synthesis Is Differentially Regulated between Cancer and Noncancerous Cells.

Cari L Graber-Feesl1, Kayla D Pederson1, Katherine J Aney1, Naoko Shima2.   

Abstract

Mitotic DNA synthesis is a recently discovered mechanism that resolves late replication intermediates, thereby supporting cell proliferation under replication stress. This unusual form of DNA synthesis occurs in the absence of RAD51 or BRCA2, which led to the identification of RAD52 as a key player in this process. Notably, mitotic DNA synthesis is predominantly observed at chromosome loci that colocalize with FANCD2 foci. However, the role of this protein in mitotic DNA synthesis remains largely unknown. In this study, we investigated the role of FANCD2 and its interplay with RAD52 in mitotic DNA synthesis using aphidicolin as a universal inducer of this process. After examining eight human cell lines, we provide evidence for FANCD2 rather than RAD52 as a fundamental supporter of mitotic DNA synthesis. In cancer cell lines, FANCD2 exerts this role independently of RAD52. Surprisingly, RAD52 is dispensable for mitotic DNA synthesis in noncancerous cell lines, but these cells strongly depend on FANCD2 for this process. Therefore, RAD52 functions selectively in cancer cells as a secondary regulator in addition to FANCD2 to facilitate mitotic DNA synthesis. As an alternative to aphidicolin, we found partial inhibition of origin licensing as an effective way to induce mitotic DNA synthesis preferentially in cancer cells. Importantly, cancer cells still perform mitotic DNA synthesis by dual regulation of FANCD2 and RAD52 under such conditions. IMPLICATIONS: These key differences in mitotic DNA synthesis between cancer and noncancerous cells advance our understanding of this mechanism and can be exploited for cancer therapies. ©2019 American Association for Cancer Research.

Entities:  

Year:  2019        PMID: 31113828      PMCID: PMC6677588          DOI: 10.1158/1541-7786.MCR-19-0057

Source DB:  PubMed          Journal:  Mol Cancer Res        ISSN: 1541-7786            Impact factor:   5.852


  50 in total

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4.  A double-hexameric MCM2-7 complex is loaded onto origin DNA during licensing of eukaryotic DNA replication.

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5.  RAD52 Facilitates Mitotic DNA Synthesis Following Replication Stress.

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8.  Alternative Lengthening of Telomeres Mediated by Mitotic DNA Synthesis Engages Break-Induced Replication Processes.

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9.  DNA synthesis by Pol η promotes fragile site stability by preventing under-replicated DNA in mitosis.

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10.  FANCI and FANCD2 have common as well as independent functions during the cellular replication stress response.

Authors:  Elizabeth L Thompson; Jung E Yeo; Eun-A Lee; Yinan Kan; Maya Raghunandan; Constanze Wiek; Helmut Hanenberg; Orlando D Schärer; Eric A Hendrickson; Alexandra Sobeck
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Review 2.  Processing DNA lesions during mitosis to prevent genomic instability.

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3.  SMC5/6 is required for replication fork stability and faithful chromosome segregation during neurogenesis.

Authors:  Alisa Atkins; Michelle J Xu; Maggie Li; Nathaniel P Rogers; Marina V Pryzhkova; Philip W Jordan
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4.  High-resolution mapping of mitotic DNA synthesis regions and common fragile sites in the human genome through direct sequencing.

Authors:  Morgane Macheret; Rahul Bhowmick; Katarzyna Sobkowiak; Laura Padayachy; Jonathan Mailler; Ian D Hickson; Thanos D Halazonetis
Journal:  Cell Res       Date:  2020-06-19       Impact factor: 46.297

5.  Expression of SnoRNA U50A Is Associated with Better Prognosis and Prolonged Mitosis in Breast Cancer.

Authors:  Jie-Ning Li; Ming-Yang Wang; Yi-Ting Chen; Yao-Lung Kuo; Pai-Sheng Chen
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  5 in total

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