Human papillomavirus E7 oncoprotein targets RNF168 to hijack the host DNA damage response

Sitz, Justine; Blanchet, Sophie; Gameiro, Steven F.; Biquand, Élise; Morgan, Tia; Galloy, Maxime; Dessapt, Julien; Lavoie, Élise G.; Blondeau, Andréanne; Smith, Brandon C.; Mymryk, Joe S.; Moody, Cary A.; Fradet-Turcotte, Amélie

doi:10.1073/pnas.1906102116

Cited by 51 publications

(44 citation statements)

References 77 publications

(100 reference statements)

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“…in G1), when a sister chromatid template is not present, thereby preventing completion of HR despite upregulation of HR-related genes 105 , 107 and by impairing the correct localization of RAD51 to DSBs, further hindering HR. There may be additional mechanisms contributing to ineffective HR and/or genomic instability, including decreased levels of RAD52, 108 hypermethylation-related downregulation of RAD51, 109 impaired recruitment of downstream repair factors due to E7-mediated interaction with the E3 ubiquitin ligase RNF168, 110 and suppression of NHEJ and shunting of DSB repair toward the more error-prone microhomology-mediated end joining. 111 Interestingly, in vitro analysis of nine patient-derived cervical-cancer cell lines, eight of which were HPV 16- or HPV 18-positive, found that none met the criteria of HR deficiency, defined using log2-ratios and allele frequencies to generate a loss of heterozygosity score in a method used previously in EOC trials.…”

Section: Perspectives For Gynecologic Cancersmentioning

confidence: 99%

PARP inhibition and immune modulation: scientific rationale and perspectives for the treatment of gynecologic cancers

Lee

Konstantinopoulos

2020

Ther Adv Med Oncol

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Poly[adenosine diphosphate (ADP) ribose]polymerase (PARP) has multifaceted roles in the maintenance of genomic integrity, deoxyribonucleic acid (DNA) repair and replication, and the maintenance of immune-system homeostasis. PARP inhibitors are an attractive oncologic therapy, causing direct cancer cell cytotoxicity by propagating DNA damage and indirectly, by various mechanisms of immunostimulation, including activation of the cGAS/STING pathway, paracrine stimulation of dendritic cells, increased T-cell infiltration, and upregulation of death-ligand receptors to increase susceptibility to natural-killer-cell killing. However, these immunostimulatory effects are counterbalanced by PARPi-mediated upregulation of programmed cell-death-ligand 1 (PD-L1), which leads to immunosuppression. Combining PARP inhibition with immune-checkpoint blockade seeks to exploit the immune stimulatory effects of PARP inhibition while negating the immunosuppressive effects of PD-L1 upregulation.

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Section: Perspectives For Gynecologic Cancersmentioning

confidence: 99%

PARP inhibition and immune modulation: scientific rationale and perspectives for the treatment of gynecologic cancers

Lee

Konstantinopoulos

2020

Ther Adv Med Oncol

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“…Additionally, a recent study by Sitz et al demonstrated a critical role for RNF168 in the productive replication of HPV31 [114]. RNF168 protein levels are substantially upregulated in HPV31-positive cells, and transient depletion of RNF168 using small hairpin RNAs blocks productive viral replication upon differentiation, while having minimal effect on episomal maintenance in undifferentiated cells [114]. Importantly, this study also showed that high-risk, but not low-risk, E7 proteins directly interact with RNF168 via E7's CR3 domain, hindering the function of RNF168 at cellular DSBs, resulting in decreased 53BP1 recruitment and an increase in HR repair [114].…”

Section: The Dna Damage Response Promotes Productive Replication Thromentioning

confidence: 99%

“…Indeed, Nbs1 and Mre11 of the MRN complex, along with the HR factors, Rad51 and BRCA1, are required for productive replication, indicating that HPV utilizes ATM activity to direct repair to HR on viral chromatin [112,113]. Additionally, a recent study by Sitz et al demonstrated a critical role for RNF168 in the productive replication of HPV31 [114]. RNF168 protein levels are substantially upregulated in HPV31-positive cells, and transient depletion of RNF168 using small hairpin RNAs blocks productive viral replication upon differentiation, while having minimal effect on episomal maintenance in undifferentiated cells [114].…”

Section: The Dna Damage Response Promotes Productive Replication Thromentioning

confidence: 99%

“…RNF168 protein levels are substantially upregulated in HPV31-positive cells, and transient depletion of RNF168 using small hairpin RNAs blocks productive viral replication upon differentiation, while having minimal effect on episomal maintenance in undifferentiated cells [114]. Importantly, this study also showed that high-risk, but not low-risk, E7 proteins directly interact with RNF168 via E7's CR3 domain, hindering the function of RNF168 at cellular DSBs, resulting in decreased 53BP1 recruitment and an increase in HR repair [114]. Interestingly, recent studies from the Laimins lab demonstrated that breaks in the HPV31 genome are preferentially repaired at the expense of cellular DNA upon differentiation [115].…”

Section: The Dna Damage Response Promotes Productive Replication Thromentioning

confidence: 99%

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Epigenetic Regulation of the Human Papillomavirus Life Cycle

Mac

Moody

2020

Pathogens

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Persistent infection with certain types of human papillomaviruses (HPVs), termed high risk, presents a public health burden due to their association with multiple human cancers, including cervical cancer and an increasing number of head and neck cancers. Despite the development of prophylactic vaccines, the incidence of HPV-associated cancers remains high. In addition, no vaccine has yet been licensed for therapeutic use against pre-existing HPV infections and HPV-associated diseases. Although persistent HPV infection is the major risk factor for cancer development, additional genetic and epigenetic alterations are required for progression to the malignant phenotype. Unlike genetic mutations, the reversibility of epigenetic modifications makes epigenetic regulators ideal therapeutic targets for cancer therapy. This review article will highlight the recent advances in the understanding of epigenetic modifications associated with HPV infections, with a particular focus on the role of these epigenetic changes during different stages of the HPV life cycle that are closely associated with activation of DNA damage response pathways.

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“…Alternatively, interactions of viral proteins with cellular replication factors may also contribute. For instance, E7 has been shown to bind to the E3 ubiquitin ligase, RNF168, which is critical for proper DNA repair leading to enhanced viral replication [ 67 ]. In addition to E6 and E7, high-level expression of E1 from heterologous promoters has also been shown to activate the ATM DNA damage response.…”

Section: Dna Damage Repair Pathways and Hpv Replicationmentioning

confidence: 99%

Regulation of the Human Papillomavirus Life Cycle by DNA Damage Repair Pathways and Epigenetic Factors

Albert

Laimins

2020

Viruses

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Human papillomaviruses are the causative agents of cervical and other anogenital cancers along with approximately 60% of oropharyngeal cancers. These small double-stranded DNA viruses infect stratified epithelia and link their productive life cycles to differentiation. HPV proteins target cellular factors, such as those involved in DNA damage repair, as well as epigenetic control of host and viral transcription to regulate the productive life cycle. HPVs constitutively activate the ATM and ATR DNA repair pathways and preferentially recruit these proteins to viral genomes to facilitate productive viral replication. In addition, the sirtuin deacetylases along with histone acetyltransferases, including Tip60, are targeted in HPV infections to regulate viral transcription and replication. These pathways provide potential targets for drug therapy to treat HPV-induced disease.

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Human papillomavirus E7 oncoprotein targets RNF168 to hijack the host DNA damage response

Cited by 51 publications

References 77 publications

PARP inhibition and immune modulation: scientific rationale and perspectives for the treatment of gynecologic cancers

PARP inhibition and immune modulation: scientific rationale and perspectives for the treatment of gynecologic cancers

Epigenetic Regulation of the Human Papillomavirus Life Cycle

Regulation of the Human Papillomavirus Life Cycle by DNA Damage Repair Pathways and Epigenetic Factors

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