Genome-wide CRISPR screens reveal synthetic lethality of RNASEH2 deficiency and ATR inhibition

Wang, Chao; Wang, Gang; Feng, Xu; Shepherd, Peter D.A.; Zhang, Jie; Tang, Mengfan; Chen, Zhen; Srivastava, Mrinal; McLaughlin, Megan; Navone, Nora M.; Hart, Glen Traver; Chen, Junjie

doi:10.1038/s41388-018-0606-4

Cited by 104 publications

(143 citation statements)

References 54 publications

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“…This is supported by the notion that PARP1 can sense unligated Okazaki fragments due to the presence of DNA nicks between them, and signal for their repair (Hanzlikova et al, 2018). The loss of RNase H2 activity further renders cells hypersensitive to ATR inhibition, which is likely linked to replication stress when rNMPs are encountered by the replisome (Wang et al, 2018;Hustedt et al, 2019).…”

Section: Rnase H2 Mutations Are Implicated In Cancermentioning

confidence: 96%

“…This is particularly important given the recent findings with regard to RNase H2 status and sensitivity to PARP or ATR inhibitors, as it may have important consequences with respect to therapeutic approaches in patients (Wang et al, 2018;Zimmermann et al, 2018;Hustedt et al, 2019). This is particularly important given the recent findings with regard to RNase H2 status and sensitivity to PARP or ATR inhibitors, as it may have important consequences with respect to therapeutic approaches in patients (Wang et al, 2018;Zimmermann et al, 2018;Hustedt et al, 2019).…”

Section: Rnase H2 Mutations Are Implicated In Cancermentioning

confidence: 98%

“…A detailed analysis of existing human cancer genomes could reveal other types of cancer that coincide with a loss of RNase H2 function. This is particularly important given the recent findings with regard to RNase H2 status and sensitivity to PARP or ATR inhibitors, as it may have important consequences with respect to therapeutic approaches in patients (Wang et al, 2018;Zimmermann et al, 2018;Hustedt et al, 2019). Therefore, it seems that the status of the p53 and/or pRb checkpoints may be critical in the fate of RER-defective cells.…”

Section: Rnase H2 Mutations Are Implicated In Cancermentioning

confidence: 99%

“…Mouse xenograft studies confirmed that tumors arising from implanted RER-deficient CLL cells are similarly sensitized. The loss of RNase H2 activity further renders cells hypersensitive to ATR inhibition, which is likely linked to replication stress when rNMPs are encountered by the replisome (Wang et al, 2018;Hustedt et al, 2019). However, substrates for PARP1 could also arise in a TOP1-independent manner through spontaneous hydrolysis of DNA at unrepaired rNMPs.…”

Section: Rnase H2 Mutations Are Implicated In Cancermentioning

confidence: 99%

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Molecular and physiological consequences of faulty eukaryotic ribonucleotide excision repair

Kellner

Luke

2019

The EMBO Journal

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The duplication of the eukaryotic genome is an intricate process that has to be tightly safe-guarded. One of the most frequently occurring errors during DNA synthesis is the mis-insertion of a ribonucleotide instead of a deoxyribonucleotide. Ribonucleotide excision repair (RER) is initiated by RNase H2 and results in errorfree removal of such mis-incorporated ribonucleotides. If left unrepaired, DNA-embedded ribonucleotides result in a variety of alterations within chromosomal DNA, which ultimately lead to genome instability. Here, we review how genomic ribonucleotides lead to chromosomal aberrations and discuss how the tight regulation of RER timing may be important for preventing unwanted DNA damage. We describe the structural impact of unrepaired ribonucleotides on DNA and chromatin and comment on the potential consequences for cellular fitness. In the context of the molecular mechanisms associated with faulty RER, we have placed an emphasis on how and why increased levels of genomic ribonucleotides are associated with severe autoimmune syndromes, neuropathology, and cancer. In addition, we discuss therapeutic directions that could be followed for pathologies associated with defective removal of ribonucleotides from doublestranded DNA.

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Section: Rnase H2 Mutations Are Implicated In Cancermentioning

confidence: 96%

Section: Rnase H2 Mutations Are Implicated In Cancermentioning

confidence: 98%

Section: Rnase H2 Mutations Are Implicated In Cancermentioning

confidence: 99%

Section: Rnase H2 Mutations Are Implicated In Cancermentioning

confidence: 99%

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Molecular and physiological consequences of faulty eukaryotic ribonucleotide excision repair

Kellner

Luke

2019

The EMBO Journal

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“…Our work identifies the importance of the MCM8IP-MCM8-9 complex in mediating cellular resistance to cisplatin and olaparib. Interestingly, MCM8IP and MCM8-9 have recently been identified in genetic screens for mediators of ATR inhibitor and temozolomide resistance 66,67 . Collectively, these studies implicate a broad role for the MCM8IP-MCM8-9 complex in promoting chemoresistance to clinically relevant chemotherapeutic agents.…”

Section: Mcm8ip As a Therapeutic Target In Cancermentioning

confidence: 99%

Identification of MCM8IP, an interactor of MCM8-9 and RPA1 that promotes homologous recombination and DNA synthesis in response to DNA damage

Huang

Taglialatela

Acharya

et al. 2019

Preprint

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Homologous recombination (HR) mediates the error-free repair of DNA double-strand breaks to maintain genomic stability. HR is carried out by a complex network of DNA repair factors. Here we identify C17orf53/MCM8IP, an OB-fold containing protein that binds ssDNA, as a novel DNA repair factor involved in HR. MCM8IP-deficient cells exhibit HR defects, especially in long-tract gene conversion, occurring downstream of RAD51 loading, consistent with a role for MCM8IP in HR-dependent DNA synthesis. Moreover, loss of MCM8IP confers cellular sensitivity to crosslinking agents and PARP inhibition.Importantly, we identify a direct interaction with MCM8-9, a putative helicase complex mutated in Primary Ovarian Insufficiency, that is crucial for MCM8IP's ability to promote resistance to DNA damaging agents. In addition to its association with MCM8-9, MCM8IP also binds directly to RPA1. We show that the interactions of MCM8IP with both MCM8-9 and RPA are required to maintain replication fork progression in response to treatment with crosslinking agents. Collectively, our work identifies MCM8IP as a key regulator of DNA damage-associated DNA synthesis during DNA recombination and replication.

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Resistance to DNA repair inhibitors in cancer

et al. 2022

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The DNA damage response (DDR) represents a complex network of proteins which detect and repair DNA damage, thereby maintaining the integrity of the genome and preventing the transmission of mutations and rearranged chromosomes to daughter cells. Faults in the DDR are a known driver and hallmark of cancer. Furthermore, inhibition of DDR enzymes can be used to treat the disease. This is exemplified by PARP inhibitors (PARPi) used to treat cancers with defects in the homologous recombination DDR pathway. A series of novel DDR targets are now also under pre-clinical or clinical investigation, including inhibitors of ATR kinase, WRN helicase or the DNA polymerase/helicase Polh (Pol-Theta). Drug resistance is a common phenomenon that impairs the overall effectiveness of cancer treatments and there is already some understanding of how resistance to PARPi occurs. Here, we discuss how an understanding of PARPi resistance could inform how resistance to new drugs targeting the DDR emerges. We also discuss potential strategies that could limit the impact of these therapy resistance mechanisms in cancer.Abbreviations ATR, Ataxia telangiectasia and Rad3 related gene; BRCA1, BRCA1 DNA repair-associated gene; BRCA2, BRCA2 DNA repair-associated gene; ctDNA, circulating tumour DNA; DDR, DNA damage response network; HR, homologous recombination; MMR, mismatch DNA repair; NAD+, nicotinamide adenine dinucleotide; PAR, poly-ADP-ribose; PARP1, poly-(ADP-ribose) polymerase 1 gene; PARPi, PARP inhibitor; POLQ, DNA polymerase theta gene, protein known as Polh; RS, replication stress; SWI/SNF, SWItch/sucrose non-fermentable chromatin remodelling complex; TMEJ, theta-mediated end joining; VEGF, vascular endothelial growth factor; WGR, protein domain containing tryptophan (W), glycine (G), arginine (R); WRN, Werner syndrome ATP-dependent helicase gene; ZnF, Zinc Finger protein domain.

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Genome-wide CRISPR screens reveal synthetic lethality of RNASEH2 deficiency and ATR inhibition

Cited by 104 publications

References 54 publications

Molecular and physiological consequences of faulty eukaryotic ribonucleotide excision repair

Molecular and physiological consequences of faulty eukaryotic ribonucleotide excision repair

Identification of MCM8IP, an interactor of MCM8-9 and RPA1 that promotes homologous recombination and DNA synthesis in response to DNA damage

Resistance to DNA repair inhibitors in cancer

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