Relocalization of the Mre11-Rad50-Nbs1 Complex by the Adenovirus E4 ORF3 Protein Is Required for Viral Replication

Evans, Jared D.; Hearing, Patrick

doi:10.1128/jvi.79.10.6207-6215.2005

Cited by 135 publications

(230 citation statements)

References 34 publications

(62 reference statements)

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“…It has previously been reported that p53 and MRN are relocalized to cytoplasmic aggresomes and nuclear track-like structures during Ad5 infection by E1B-55K and E4orf3, before degradation by E1B-55K and E4orf6 (23,24). However, we did not observe either type of staining for TOPBP1 in Ad5-or Ad12-infected cells (Fig.…”

Section: Topbp1contrasting

confidence: 47%

Adenovirus 12 E4orf6 inhibits ATR activation by promoting TOPBP1 degradation

Blackford

Patel

Forrester

et al. 2010

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

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Activation of the cellular DNA damage response is detrimental to adenovirus (Ad) infection. Ad has therefore evolved a number of strategies to inhibit ATM-and ATR-dependent signaling pathways during infection. Recent work suggests that the Ad5 E4orf3 protein prevents ATR activation through its ability to mislocalize the MRN complex. Here we provide evidence to indicate that Ad12 has evolved a different strategy from Ad5 to inhibit ATR. We show that Ad12 utilizes a CUL2/RBX1/elongin C-containing ubiquitin ligase to promote the proteasomal degradation of the ATR activator protein topoisomerase-IIβ-binding protein 1 (TOPBP1). Ad12 also uses this complex to degrade p53 during infection, in contrast to Ad5, which requires a CUL5-based ubiquitin ligase. Although Ad12-mediated degradation of p53 is dependent upon both E1B-55K and E4orf6, Ad12-mediated degradation of TOPBP1 is solely dependent on E4orf6. We propose that Ad12 E4orf6 has two principal activities: to recruit the CUL2-based ubiquitin ligase and to act as substrate receptor for TOPBP1. In support of the idea that Ad12 E4orf6 specifically prevents ATR activation during infection by targeting TOPBP1 for degradation, we demonstrate that Ad12 E4orf6 can inhibit the ATR-dependent phosphorylation of CHK1 in response to replication stress. Taken together, these data provide insights into how Ad modulates ATR signaling pathways during infection.DNA damage | cullin-RING ubiquitin ligases | DNA damage | proteasome

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Section: Topbp1contrasting

confidence: 47%

Adenovirus 12 E4orf6 inhibits ATR activation by promoting TOPBP1 degradation

Blackford

Patel

Forrester

et al. 2010

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

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“…To prove the principle that HMGA2-promoted PML degradation is biologically relevant, we showed that this process can be stimulated by ATO treatment and that HMGA2 counteracts PMLmediated enhancement of GR transactivation. Besides stimulating GR function (13,42), PML nuclear bodies are reportedly involved in the cellular response to DNA damage (43). For example, components of the DNA damage sensor MRN complex are also reported to be colocalized with PML or PML nuclear bodies (43 -47).…”

Section: Discussionmentioning

confidence: 99%

SUMOylation of HMGA2: selective destabilization of promyelocytic leukemia protein via proteasome

Cao

Clavijo

et al. 2008

Molecular Cancer Therapeutics

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The HMGA2 architectural protein functions in a variety of cellular processes, such as cell growth, transcription regulation, neoplastic transformation, and progression. Up-regulation of HMGA2 protein is observed in many tumors and is associated with advanced cancers with poor prognoses. Although the expression and biochemical properties of HMGA2 protein are regulated by microRNA and phosphorylation, it is unknown whether HMGA2 activity can also be regulated by SUMOylation, and that is what is investigated in this report. We identified HMGA2 as a SUMOylation target and showed that the expression of wild-type HMGA2, but not SUMOylation-defective HMGA2(2K/R), selectively lowered the steady-state level of PML protein. Consequently, the HMGA2-elicited PML down-regulation rendered a reduction in the average number of PML nuclear bodies per cell and the volume of PML assembled per PML nuclear body. Using small interfering RNA to suppress endogenous ubiquitin expression and proteasome inhibitor to repress ubiquitin-mediated protein degradation, we showed that HMGA2 confers PML down-regulation through ubiquitin-proteasomedependent protein degradation. Importantly, arsenic trioxide treatment stimulated HMGA2 SUMOylation, leading to the formation of HMGA2 nuclear foci surrounding PML nuclear bodies and the stimulation of PML degradation.Collectively, our results unveil a previously unrecognized effect by HMGA2 on the modulation of PML protein level, providing a novel mechanism underlying HMGA2 function and underscoring the molecular basis for oncogenic progression by HMGA2. [Mol Cancer Ther 2008;7(4):923-34]

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“…For E1B-55K mutants, viral DNA replication is normal in p53-minus cells (Harada and Berk, 1999) even though MRN subunits are not degraded. This is because E4orf3 and E4orf6 proteins also inhibit MRN function (Boyer J et al, 1999;Shepard and Ornelles, 2004;Evans and Hearing, 2005). In HeLa and KB cells, the defect in E1B-55K mutant late viral protein synthesis results from a defect in export of late viral mRNAs from the nucleus to the cytoplasm (Babiss et al, 1985;Pilder et al, 1986;Leppard and Shenk, 1989;O'Shea et al, 2004).…”

Section: Kmentioning

confidence: 99%

“…The results with E1B-55K in adenovirus-infected cells indicate that aggresome formation is a protective response that increases the rate of degradation of polyubiquitinated proteins. In infected cells, MRN first interacts with E4orf3 in PML nuclear domains of altered morphology (Carvalho et al, 1995;Doucas et al, 1996;Evans and Hearing, 2005). E1B-55K then interacts with MRN in these modified PML nuclear bodies.…”

Section: Kmentioning

confidence: 99%

Recent lessons in gene expression, cell cycle control, and cell biology from adenovirus

2005

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Adenovirus continues to be an important model system for investigating basic aspects of cell biology. Interactions of several cellular proteins with E1A conserved regions (CR) 1 and 2, and inhibition of apoptosis by E1B proteins are required for oncogenic transformation. CR2 binds RB family members, de-repressing E2F transcription factors, thus activating genes required for cell cycling. E1B-19K is a BCL2 homolog that binds and inactivates proapoptotic BAK and BAX. E1B-55K binds p53, inhibiting its transcriptional activation function. In productively infected cells, E1B-55K and E4orf6 assemble a ubiquitin ligase with cellular proteins Elongins B and C, Cullin 5 and RBX1 that polyubiquitinates p53 and one or more subunits of the MRN complex involved in DNA doublestrand break repair, directing them to proteosomal degradation. E1A CR3 activates viral transcription by interacting with the MED23 Mediator subunit, stimulating preinitiation complex assembly on early viral promoters and probably also the rate at which they initiate transcription. The viral E1B-55K/E4orf6 ubiquitin ligase is also required for efficient viral late protein synthesis in many cell types, but the mechanism is not understood. E1A CR1 binds several chromatin-modifying complexes, but how this contributes to stimulation of cellular DNA synthesis and transformation is not clear. E1A CR4 binds the CtBP corepressor, but the mechanism by which this modulates the frequency of transformation remains to be determined. Clearly, adenovirus has much left to teach us about fundamental cellular processes.

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Relocalization of the Mre11-Rad50-Nbs1 Complex by the Adenovirus E4 ORF3 Protein Is Required for Viral Replication

Cited by 135 publications

References 34 publications

Adenovirus 12 E4orf6 inhibits ATR activation by promoting TOPBP1 degradation

Adenovirus 12 E4orf6 inhibits ATR activation by promoting TOPBP1 degradation

SUMOylation of HMGA2: selective destabilization of promyelocytic leukemia protein via proteasome

Recent lessons in gene expression, cell cycle control, and cell biology from adenovirus

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