Antagonistic Relationship between Human Cytomegalovirus pUL27 and pUL97 Activities during Infection

Bigley, Tarin M.; Reitsma, Justin M.; Terhune, Scott S.

doi:10.1128/jvi.00986-15

Cited by 15 publications

(13 citation statements)

References 78 publications

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“…R25 blocks activity of CDK1, CDK2 and CDK5) (Sandal et al, 2002;Soni & Jacobberger, 2004). Consistent with our data, R25 treatment has been shown to reduce viral titres by approximately 1.2 log units, even at a much lower dose of 150 nM (Bigley et al, 2015). The identification of the CDK1-pUL50 interaction by CoIP analysis in the present study further suggests that at least CDK1 is directly involved in core NEC formation.…”

Section: Discussionsupporting

confidence: 91%

Cytomegalovirus pUL50 is the multi-interacting determinant of the core nuclear egress complex (NEC) that recruits cellular accessory NEC components

Sonntag

Hamilton

Hanife

et al. 2016

Journal of General Virology

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Nuclear egress of herpesvirus capsids through the nuclear envelope is mediated by the multimeric nuclear egress complex (NEC). The human cytomegalovirus (HCMV) core NEC is defined by an interaction between the membrane-anchored pUL50 and its nuclear co-factor pUL53, tightly associated through heterodimeric corecruitment to the nuclear envelope. Cellular proteins, such as p32/gC1qR, emerin and protein kinase C (PKC), are recruited by direct interaction with pUL50 for the multimeric extension of the NEC. As a functionally important event, the recruitment of both viral and cellular protein kinases leads to site-specific lamin phosphorylation and nuclear lamina disassembly. In this study, interaction domains within pUL50 for its binding partners were defined by co-immunoprecipitation. The interaction domain for pUL53 is located within the pUL50 N-terminus (residues 10-169), interaction domains for p32/gC1qR (100-358) and PKC (100-280) overlap in the central part of pUL50, and the interaction domain for emerin is located in the C-terminus (265-397). Moreover, expression and formation of core NEC proteins at the nuclear rim were consistently detected in cells permissive for productive HCMV replication, including two trophoblast-cell lines. Importantly, regular nuclear-rim formation of the core NEC was blocked by inhibition of cyclin-dependent kinase (CDK) activity. In relation to the recently published crystal structure of the HCMV core NEC, our findings result in a refined view of NEC assembly. In particular, we suggest that CDKs may play an important regulatory role in NEC formation during HCMV replication.

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Section: Discussionsupporting

confidence: 91%

Cytomegalovirus pUL50 is the multi-interacting determinant of the core nuclear egress complex (NEC) that recruits cellular accessory NEC components

Sonntag

Hamilton

Hanife

et al. 2016

Journal of General Virology

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“…Studies by Hamirally and Kamil et al [52] have demonstrated that phosphorylation of LMNA contributes to nuclear egress of HCMV particles. The antiviral compound, maribavir inhibits this process and its antiviral activity is further supported by increased steady-state levels of CDKN1A (p21 CIP1 ) ( Fig 6C) [51,54,70]. It is important to note that the kinetics of mitotic entry are regulated by the HCMV protein pUL21a which suppresses Cyclin A levels ( Fig 9A) [55].…”

Section: Plos Computational Biologymentioning

confidence: 95%

“…This state includes disruption of the nuclear lamina by and k 0 f 11 are high, respectively. https://doi.org/10.1371/journal.pcbi.1007733.g008 phosphorylation of LMNA by both HCMV pUL97 kinase and MPF kinase (CCNB1:CDK1) which is required for virion particle nuclear egress [51][52][53][54]. Disrupting these kinases is the defined mechanism of action for the antiviral, Maribavir [52,54].…”

Section: Defining the Contribution Of Apc/c Degradation To Mitotic Comentioning

confidence: 99%

“…https://doi.org/10.1371/journal.pcbi.1007733.g008 phosphorylation of LMNA by both HCMV pUL97 kinase and MPF kinase (CCNB1:CDK1) which is required for virion particle nuclear egress [51][52][53][54]. Disrupting these kinases is the defined mechanism of action for the antiviral, Maribavir [52,54]. Entry of the infected cell into mitosis is regulated HCMV pUL21a which limits Cyclin A levels and subsequently CCNB1 levels ( Fig 9A) [55].…”

Section: Defining the Contribution Of Apc/c Degradation To Mitotic Comentioning

confidence: 99%

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Network mechanisms and dysfunction within an integrated computational model of progression through mitosis in the human cell cycle

et al. 2020

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The cellular protein-protein interaction network that governs cellular proliferation (cell cycle) is highly complex. Here, we have developed a novel computational model of human mitotic cell cycle, integrating diverse cellular mechanisms, for the purpose of generating new hypotheses and predicting new experiments designed to help understand complex diseases. The pathogenic state investigated is infection by a human herpesvirus. The model starts at mitotic entry initiated by the activities of Cyclin-dependent kinase 1 (CDK1) and Polo-like kinase 1 (PLK1), transitions through Anaphase-promoting complex (APC/C) bound to Cell division cycle protein 20 (CDC20), and ends upon mitotic exit mediated by APC/C bound to CDC20 homolog 1 (CDH1). It includes syntheses and multiple mechanisms of degradations of the mitotic proteins. Prior to this work, no such comprehensive model of the human mitotic cell cycle existed. The new model is based on a hybrid framework combining Michaelis-Menten and mass action kinetics for the mitotic interacting reactions. It simulates temporal changes in 12 different mitotic proteins and associated protein complexes in multiple states using 15 interacting reactions and 26 ordinary differential equations. We have defined model parameter values using both quantitative and qualitative data and using parameter values from relevant published models, and we have tested the model to reproduce the cardinal features of human mitosis determined experimentally by numerous laboratories. Like cancer, viruses create dysfunction to support infection. By simulating infection of the human herpesvirus, cytomegalovirus, we hypothesize that virus-mediated disruption of APC/C is necessary to establish a unique mitotic collapse with sustained CDK1 activity, consistent with known mechanisms of virus egress. With the rapid discovery of cellular protein-protein interaction networks and regulatory mechanisms, we anticipate that this model will be highly valuable in helping us to understand the network dynamics and identify potential points of therapeutic interventions.

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“…Thus, in UL27-positive cells, p21 levels are high, cellular Cdks are inhibited, and Rb is phosphorylated during infection only if UL97 is present and active. In UL27-negative cells, p21 levels are low (54), and as a result, cellular Cdks are active and able to phosphorylate Rb. Rb phosphorylation by cellular Cdks or UL97 can be easily distinguished by monitoring the residues serine 249 and threonine 252, which are phosphorylated by cellular Cdks but not UL97 (2).…”

Section: Deoxyribonucleotides Are Limiting For Hcmv Dna Replicationmentioning

confidence: 99%

Human Cytomegalovirus Can Procure Deoxyribonucleotides for Viral DNA Replication in the Absence of Retinoblastoma Protein Phosphorylation

Kuny

Kalejta

2016

J Virol

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Viral DNA replication requires deoxyribonucleotide triphosphates (dNTPs). These molecules, which are found at low levels in noncycling cells, are generated either by salvage pathways or through de novo synthesis. Nucleotide synthesis utilizes the activity of a series of nucleotide-biosynthetic enzymes (NBEs) whose expression is repressed in noncycling cells by complexes between the E2F transcription factors and the retinoblastoma (Rb) tumor suppressor. Rb-E2F complexes are dissociated and NBE expression is activated during cell cycle transit by cyclin-dependent kinase (Cdk)-mediated Rb phosphorylation. The DNA virus human cytomegalovirus (HCMV) encodes a viral Cdk (v-Cdk) (the UL97 protein) that phosphorylates Rb, induces the expression of cellular NBEs, and is required for efficient viral DNA synthesis. A long-held hypothesis proposed that viral proteins with Rbinactivating activities functionally similar to those of UL97 facilitated viral DNA replication in part by inducing the de novo production of dNTPs. However, we found that dNTPs were limiting even in cells infected with wild-type HCMV in which UL97 is expressed and Rb is phosphorylated. Furthermore, we revealed that both de novo and salvage pathway enzymes contribute to viral DNA replication during HCMV infection and that Rb phosphorylation by cellular Cdks does not correct the viral DNA replication defect observed in cells infected with a UL97-deficient virus. We conclude that HCMV can obtain dNTPs in the absence of Rb phosphorylation and that UL97 can contribute to the efficiency of DNA replication in an Rb phosphorylation-independent manner. IMPORTANCETransforming viral oncoproteins, such as adenovirus E1A and papillomavirus E7, inactivate Rb. The standard hypothesis for how Rb inactivation facilitates infection with these viruses is that it is through an increase in the enzymes required for DNA synthesis, which include nucleotide-biosynthetic enzymes. However, HCMV UL97, which functionally mimics these viral oncoproteins through phosphorylation of Rb, fails to induce the production of nonlimiting amounts of dNTPs. This finding challenges the paradigm of the role of Rb inactivation during DNA virus infection and uncovers the existence of an alternative mechanism by which UL97 contributes to HCMV DNA synthesis. The ineffectiveness of the UL97 inhibitor maribavir in clinical trials might be better explained with a fuller understanding of the role of UL97 during infection. Furthermore, as the nucleoside analog ganciclovir is the current drug of choice for treating HCMV, knowing the provenance of the dNTPs incorporated into viral DNA may help inform antiviral therapeutic regimens. T wo members of the family of conserved protein kinases encoded by herpesviruses (UL13 of herpes simplex virus 1 [HSV-1] and BGLF4 of Epstein-Barr virus [EBV]) were found to phosphorylate two substrates on a residue also targeted by cyclindependent kinase 1 (Cdk1) (1), indicating that these proteins mimic at least some activities of cellular Cdks. Subsequently, UL97 (2) ...

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Antagonistic Relationship between Human Cytomegalovirus pUL27 and pUL97 Activities during Infection

Cited by 15 publications

References 78 publications

Cytomegalovirus pUL50 is the multi-interacting determinant of the core nuclear egress complex (NEC) that recruits cellular accessory NEC components

Cytomegalovirus pUL50 is the multi-interacting determinant of the core nuclear egress complex (NEC) that recruits cellular accessory NEC components

Network mechanisms and dysfunction within an integrated computational model of progression through mitosis in the human cell cycle

Human Cytomegalovirus Can Procure Deoxyribonucleotides for Viral DNA Replication in the Absence of Retinoblastoma Protein Phosphorylation

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