The RAD51 recombinase protects mitotic chromatin in human cells

Wassing, Isabel E.; Saayman, Xanita; Rampazzo, Lucia; Ralf, Christine; Bassett, Andrew; Esashi, Fumiko

doi:10.1101/2020.08.11.246231

Cited by 6 publications

(11 citation statements)

References 58 publications

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Section: Resultssupporting

confidence: 89%

“…Moreover, treatment of mitotic cells with a PLK1 inhibitor prior to EdU incubation severely reduces MiDAS in both the parental as well as the TopBP1Δ284-301 cell line (Fig. 3D and E) consistent with other studies (Minocherhomji et al, 2015;Wassing et al, 2021). This indicates that the identified PLK1 docking site in TopBP1 is important for MiDAS and moreover suggests that the PLK1 TopBP1 interaction via the identified PLK1 docking site is facilitating the involvement of PLK1 in MiDAS.…”

Section: The Plk1 Docking Site Is Important For the Mitotic Functions...supporting

confidence: 88%

“…PLK1 was shown to promote loading of RAD51 in interphase cells (Moudry et al, 2016) in a process that relies on BRCT7 and BRCT8 of TopBP1 for coordinating the PLK1-mediated phosphorylation of RAD51 (Moudry et al, 2016). Interestingly, PLK1-mediated RAD51-phoshorylation promotes MiDAS (Wassing et al, 2021). Furthermore, PLK1 activity is important for suppressing recruitment of NHEJ factors to camptothecin (CPT)-induced replication problems (Nakamura et al, 2021).…”

Section: Introductionmentioning

confidence: 99%

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A conserved PLK1 docking site in TopBP1 maintains genome integrity during mitosis

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et al. 2022

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TopBP1 is a large scaffold protein with multiple functions in genome integrity. We previously identified a novel role for TopBP1 during M phase by showing that TopBP1 reduces carry-over of DNA damage to daughter cells. This function emerges as a critical backup pathway in BRCA deficient cells, yet many aspects of TopBP1 regulation during mitosis are unclear. The mitotic kinase PLK1 has been reported to interact with TopBP1 but the functional relevance of this is unclear. Here, we identify and characterize a conserved PLK1 docking site in TopBP1. Endogenous deletion of the PLK1 docking site in TopBP1 results in increased number of mitotic TopBP1 foci, increased DNA damage in daughter cells, deficient mitotic DNA repair synthesis and increased frequency of binucleation. At the same time, cell cycle distribution and ATR activation are normal in cells with the PLK1 docking site deletion in TopBP1. Interestingly, mutation of this site in TopBP1 renders cells sensitive to PARP inhibitors but not to camptothecin hinting to different cellular effects of the two chemotherapeutics. Altogether, our data indicate that the PLK1-TopBP1 interaction is critical for the mitotic function of TopBP1.

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Section: Resultssupporting

confidence: 89%

Section: The Plk1 Docking Site Is Important For the Mitotic Functions...supporting

confidence: 88%

Section: Introductionmentioning

confidence: 99%

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A conserved PLK1 docking site in TopBP1 maintains genome integrity during mitosis

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et al. 2022

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“…Recent studies have indicated that defects in DNA replication or broken chromosome bridges formed during interphase can result in aberrant DNA synthesis during subsequent mitoses, on a path toward high levels of genome instability (51,52). We did not detect DNA synthesis in Ki-67-depleted mitotic cells (Fig.…”

Section: Resultsmentioning

confidence: 56%

The chromatin-binding domain of Ki-67 together with p53 protects human chromosomes from mitotic damage

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Sun

Iyer

et al. 2021

Proc. Natl. Acad. Sci. U.S.A.

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Vertebrate mammals express a protein called Ki-67 which is most widely known as a clinically useful marker of highly proliferative cells. Previous studies of human cells indicated that acute depletion of Ki-67 can elicit a delay at the G1/S boundary of the cell cycle, dependent on induction of the checkpoint protein p21. Consistent with those observations, we show here that acute Ki-67 depletion causes hallmarks of DNA damage, and the damage occurs even in the absence of checkpoint signaling. This damage is not observed in cells traversing S phase but is instead robustly detected in mitotic cells. The C-terminal chromatin-binding domain of Ki-67 is necessary and sufficient to protect cells from this damage. We also observe synergistic effects when Ki-67 and p53 are simultaneously depleted, resulting in increased levels of chromosome bridges at anaphase, followed by the appearance of micronuclei. Therefore, these studies identify the C terminus of Ki-67 as an important module for genome stability.

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“…Importantly, the physical association of Rad51 with microtubules was revealed in a co-immunoprecipitation assay, thereby indicating that an efficient response to DNA damage involves a cytoplasmic-to-nuclear transport of Rad51 and might be tubulin-dependent [ 51 ]. Lastly, Rad51 recombinase was proposed to be a key factor protecting mitotic chromatin by promoting the mitotic DNA synthesis of the underreplicated DNA [ 52 ], thereby suggesting that cancer cells lacking this DDR protein might be extremely sensitive to mitotic DNA damage when the cells enter mitosis before completion of DNA replication [ 53 ]. Thus, the ability of 2-APCAs to induce apoptosis of cancer cells might be due to the dual mode of action—mitotic arrest due to the enhancement of tubulin polymerization, which in turn substantially reduces Rad51 expression and triggers the cancer cell death due to the unrepairable mitotic DNA damage.…”

Section: Discussionmentioning

confidence: 99%

2-APCAs, the Novel Microtubule Targeting Agents Active against Distinct Cancer Cell Lines

et al. 2021

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Microtubules are known as the most attractive molecular targets for anti-cancer drugs. However, the number of serious limitations of the microtubule targeting agents (MTAs) including poor bioavailability, adverse effects (e.g., systemic and neural toxicity), and acquired resistance after initiation of MTA-based therapy remain the driving forces to develop the novel therapeutic agents effectively targeting microtubules and exhibiting potent anti-tumor activities. Here, we report the discovery of 2-amino-pyrrole-carboxamides (2-APCAs), a novel class of MTA, which effectively inhibited the growth of the broad spectrum of cancer cell lines in vitro, including various types of breast, prostate, and non-small lung cancer (NSLC), soft tissue sarcomas (STS) (e.g., leio-, rhabdomyo-, and fibrosarcomas), osteosarcomas and gastrointestinal stromal tumors (GISTs). Importantly, 2-APCAs were also effective in cancer cell lines exhibiting resistance to certain chemotherapeutic agents, including MTAs and topoisomerase II inhibitors. The anti-proliferative effect of 2-APCAs was due to their ability to interfere with the polymerization of tubulin and thereby leading to the accumulation of tumor cells in the M-phase. As an outcome of the mitotic arrest, cancer cells underwent apoptotic cell death which was evidenced by increased expression of cleaved forms of the poly-ADP-ribose polymerase (PARP) and caspase-3 and the increased numbers of Annexin V-positive cells, as well. Among the compounds exhibiting the potent anti-cancer activities against the various cancer cell lines indicated above, 2-APCA-III was found the most active. Importantly, its cytotoxic activities correlated with its highest potency to interfere with the dynamics of tubulin polymerization and inducement of cell cycle arrest in the G2/M phase. Interestingly, the cytotoxic and tubulin polymerization activities of 2-APCAs correlated with the stability of the «tubulin—2-АРСА» complexes, illustrating the “tubulin-2-APCA-III” complex as the most stable. Molecular docking showed that the binding site for 2-АРСА-III is located in α tubulin by forming a hydrogen bond with Leu23. Of note, single-cell electrophoresis (Comet assay) data illustrated the low genotoxic activities of 2-APCAs when compared to certain anti-cancer chemotherapeutic agents. Taken together, our study describes the novel MTAs with potent anti-proliferative and pro-apoptotic activities, thereby illustrating them as a scaffold for the development of successful chemotherapeutic anti-cancer agent targeting microtubules.

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The RAD51 recombinase protects mitotic chromatin in human cells

Cited by 6 publications

References 58 publications

A conserved PLK1 docking site in TopBP1 maintains genome integrity during mitosis

A conserved PLK1 docking site in TopBP1 maintains genome integrity during mitosis

The chromatin-binding domain of Ki-67 together with p53 protects human chromosomes from mitotic damage

2-APCAs, the Novel Microtubule Targeting Agents Active against Distinct Cancer Cell Lines

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