Herpes Simplex Virus 1 Induces Phosphorylation and Reorganization of Lamin A/C through the γ
            <sub>1</sub>
            34.5 Protein That Facilitates Nuclear Egress

Wu, Songfang; Pan, Shuang; Zhang, Liming; Baines, Joel D.; Roller, Richard J.; Ames, Joshua; Mu, Yang; Wang, Jiyan; Chen, Da; Liu, Yaohui; Zhang, Cuizhu; Cao, Youjia; He, Bin

doi:10.1128/jvi.01392-16

Cited by 45 publications

(49 citation statements)

References 43 publications

(55 reference statements)

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“…Furthermore, a virus lacking 147 amino acids from the N terminus of ICP34.5 failed to control TBK1-dependent interferon responses (18,19). Contained within this N-terminal deletion of ICP34.5 tested by Ma et al in 2012 are regions that are also required for beclin1 and p32 interactions (20,36,46). In this study, we genetically dissected domains of ICP34.5 to evaluate the influence of beclin1 and TBK1 interaction on replication and virulence of the virus.…”

Section: Discussionmentioning

confidence: 94%

Role of Herpes Simplex Virus 1 γ34.5 in the Regulation of IRF3 Signaling

Manivanh

Mehrbach

Knipe

et al. 2017

J Virol

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During viral infection, pattern recognition receptors (PRRs) and their associated adaptors recruit TANK-binding kinase 1 (TBK1) to activate interferon regulatory factor 3 (IRF3), resulting in production of type I interferons (IFNs). ICP0 and ICP34.5 are among the proteins encoded by herpes simplex virus 1 (HSV-1) that modulate type I IFN signaling. We constructed a recombinant virus (ΔXX) that lacks amino acids 87 to 106, a portion of the previously described TBK1-binding domain of the γ34.5 gene (D. Verpooten, Y. Ma, S. Hou, Z. Yan, and B. He, J Biol Chem 284:1097-1105, 2009, https://doi.org/10.1074/JBC.M805905200). These 20 residues are outside the γ34.5 beclin1-binding domain (BBD) that interacts with beclin1 and regulates autophagy. Unexpectedly, ΔXX showed no deficit in replication in a variety of tissues and showed virulence comparable to that of wild-type and marker-rescued viruses following intracerebral infection. ΔXX was fully capable of mediating the dephosphorylation of eIF2α, and the virus was capable of controlling the phosphorylation of IRF3. In contrast, a null mutant in γ34.5 failed to control IRF3 phosphorylation due to an inability of the mutant to sustain expression of ICP0. Our data show that while γ34.5 regulates IRF3 phosphorylation, the TBK1-binding domain itself has no impact on IRF3 phosphorylation or on replication and pathogenesis in mice. Interferons (IFNs) are potent activators of a variety of host responses that serve to control virus infections. The have evolved countermeasures to IFN responses. Herpes simplex virus 1 (HSV-1) encodes the multifunctional neurovirulence protein ICP34.5. In this study, we investigated the biological relevance of the interaction between ICP34.5 and TANK-binding kinase 1 (TBK1), an activator of IFN responses. Here, we establish that although ICP34.5 binds TBK1 under certain conditions through a TBK1-binding domain (TBD), there was no direct impact of the TBD on viral replication or virulence in mice. Furthermore, we showed that activation of IRF3, a substrate of TBK1, was independent of the TBD. Instead, we provided evidence that the ability of ICP34.5 to control IRF3 activation is through its ability to reverse translational shutoff and sustain the expression of other IFN inhibitors encoded by the virus. This work provides new insights into the immunomodulatory functions of ICP34.5.

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Section: Discussionmentioning

confidence: 94%

Role of Herpes Simplex Virus 1 γ34.5 in the Regulation of IRF3 Signaling

Manivanh

Mehrbach

Knipe

et al. 2017

J Virol

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“…Given evidence that HSV-1 infected cell protein (ICP) 34.5 is involved in regulation of the interferon system and viral egress (Jing et al, 2004; Wang et al, 2014; Wu et al, 2016), we investigated whether this protein could serve as a viral activator of HPSE. Infection of HCE cells with a mutant virus lacking the γ 34.5 gene was markedly impaired in its ability to upregulate HPSE mRNA expression (Figure 5A).…”

Section: Resultsmentioning

confidence: 99%

Viral Activation of Heparanase Drives Pathogenesis of Herpes Simplex Virus-1

et al. 2017

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Summary Herpes simplex virus type-1 (HSV-1) causes lifelong recurrent pathologies without a cure. How infection by HSV-1 triggers disease processes, especially in the immune-privileged avascular human cornea, remains a major unresolved puzzle. It has been speculated that a cornea-resident molecule must tip the balance in favor of pro-inflammatory and pro-angiogenic conditions observed with herpetic as well as non-herpetic ailments of the cornea. Here, we demonstrate that heparanase (HPSE), a host enzyme, is the molecular trigger for multiple pathologies associated with HSV-1 infection. In human corneal epithelial cells, HSV-1 infection upregulates HPSE in a manner dependent on HSV-1 infected cell protein 34.5. HPSE then relocates to the nucleus to regulate cytokine production, inhibits wound closure, enhances viral spread, and thus generates a toxic local environment. Overall, our findings implicate activated HPSE as a driver of viral pathogenesis, and call for further attention to this host protein in infection and other inflammatory disorders.

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“…Conversely, HSV-1 enzymes may also alter the regulation of PTMs on host proteins and histones. For example, HSV-1 UL13 directly phosphorylates host nuclear lamin proteins and this phosphorylation induces partial lamin disassembly or reorganization that allows virions to reach the inner nuclear membranes (16,17). However, even though a prior study identified phosphorylation on HSV-1 proteins (18), a global picture of regulation of host phosphorylation upon HSV-1 infection has not been fully investigated.…”

Section: Herpes Simplex Virus (Hsv-1)mentioning

confidence: 99%

Time-resolved Global and Chromatin Proteomics during Herpes Simplex Virus Type 1 (HSV-1) Infection

Kulej

Avgousti

Sidoli

et al. 2017

Molecular & Cellular Proteomics

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Herpes simplex virus (HSV-1) lytic infection results in global changes to the host cell proteome and the proteins associated with host chromatin. We present a system level characterization of proteome dynamics during infection by performing a multi-dimensional analysis during HSV-1 lytic infection of human foreskin fibroblast (HFF) cells. Our study includes identification and quantification of the host and viral proteomes, phosphoproteomes, chromatin bound proteomes and post-translational modifications (PTMs) on cellular histones during infection. We analyzed proteomes across six time points of virus infection (0, 3, 6, 9, 12 and 15 h post-infection) and clustered trends in abundance using fuzzy c-means. Globally, we accurately quantified more than 4000 proteins, 200 differently modified histone peptides and 9000 phosphorylation sites on cellular proteins. In addition, we identified 67 viral proteins and quantified 571 phosphorylation events (465 with high confidence site localization) on viral proteins, which is currently the most comprehensive map of HSV-1 phosphoproteome. We investigated chromatin bound proteins by proteomic analysis of the high-salt chromatin fraction and identified 510 proteins that were significantly different in abundance during infection. We found 53 histone marks significantly regulated during virus infection, including a steady increase of histone H3 acetylation (H3K9ac and H3K14ac). Our data provide a resource of unprecedented depth for human and viral proteome dynamics during infection. Collectively, our results indicate that the proteome composition of the chromatin of HFF cells is highly affected during HSV-1 infection, and that phosphorylation events are abundant on viral proteins. We propose that our epi-proteomics approach will prove to be important in the characterization of other model infectious systems that involve changes to chromatin composition. Molecular & Cellular Proteomics 16: 10.1074/mcp.M116.065987, S92-S107, 2017. Herpes simplex virus (HSV-1)1 leads to a contagious and persistent infection that affects about 95% of the human population. The HSV-1 genome is a double-stranded DNA molecule that replicates in the host cell nucleus (1). HSV-1 initially infects epithelial cells as a lytic infection, and then enters peripheral neurons where it establishes latency (2, 3). Processes such as viral transcription, viral DNA synthesis, virion assembly and DNA packaging take place in discrete virus-induced structures within the nucleus called replication compartments (1, 4). These processes are temporally regulated by the viral cascades of immediate-early (IE), early (E), and late (L) gene expression. The IE proteins are primarily responsible for counteracting intrinsic host defenses and for activating expression of early-phase genes (1). Early viral pro-

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Herpes Simplex Virus 1 Induces Phosphorylation and Reorganization of Lamin A/C through the γ ₁ 34.5 Protein That Facilitates Nuclear Egress

Cited by 45 publications

References 43 publications

Role of Herpes Simplex Virus 1 γ34.5 in the Regulation of IRF3 Signaling

Role of Herpes Simplex Virus 1 γ34.5 in the Regulation of IRF3 Signaling

Viral Activation of Heparanase Drives Pathogenesis of Herpes Simplex Virus-1

Time-resolved Global and Chromatin Proteomics during Herpes Simplex Virus Type 1 (HSV-1) Infection

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Herpes Simplex Virus 1 Induces Phosphorylation and Reorganization of Lamin A/C through the γ 1 34.5 Protein That Facilitates Nuclear Egress

Cited by 45 publications

References 43 publications

Role of Herpes Simplex Virus 1 γ34.5 in the Regulation of IRF3 Signaling

Role of Herpes Simplex Virus 1 γ34.5 in the Regulation of IRF3 Signaling

Viral Activation of Heparanase Drives Pathogenesis of Herpes Simplex Virus-1

Time-resolved Global and Chromatin Proteomics during Herpes Simplex Virus Type 1 (HSV-1) Infection

Contact Info

Product

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Herpes Simplex Virus 1 Induces Phosphorylation and Reorganization of Lamin A/C through the γ ₁ 34.5 Protein That Facilitates Nuclear Egress