Roscovitine Inhibits Activation of Promoters in Herpes Simplex Virus Type 1 Genomes Independently of Promoter-Specific Factors

Diwan, Prerna; Lacasse, Jonathan J; Schang, Luis M.

doi:10.1128/jvi.78.17.9352-9365.2004

Cited by 45 publications

(63 citation statements)

References 89 publications

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“…Accordingly, FIT-039 reduced the expression levels of HSV-1 IEGs and early and late genes ( Figure 2B and Supplemental Figure 4). IEGs are transcribed immediately after the viral infection, and their encoded proteins regulate the transcription of early and late viral genes (30). These results indicated that the antiviral mechanism may be attributed to the inhibition of the viral transcription through suppression of the CTD phosphorylation of RNA polymerase II.…”

Section: Introductionmentioning

confidence: 82%

CDK9 inhibitor FIT-039 prevents replication of multiple DNA viruses

Yamamoto¹,

Onogi²,

Kii³

et al. 2014

J. Clin. Invest.

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Section: Introductionmentioning

confidence: 82%

CDK9 inhibitor FIT-039 prevents replication of multiple DNA viruses

Yamamoto¹,

Onogi²,

Kii³

et al. 2014

J. Clin. Invest.

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“…2 D and E). We therefore tested entry using reporter cells containing a red fluorescence protein (RFP) gene driven by a VP16-responsive promoter (35). VP16 is in the tegument of HSV-1 virions, a protein layer underneath the envelope but outside the capsid.…”

Section: Resultsmentioning

confidence: 99%

“…Vero Clone 57 cells express RFP under the control of the HSV-1 ICP0 promoter (35). Huh7.5 cells were obtained from C. Rice (The Rockefeller University, New York, NY).…”

Section: Methodsmentioning

confidence: 99%

Rigid amphipathic fusion inhibitors, small molecule antiviral compounds against enveloped viruses

St.Vincent¹,

Colpitts

Устинов

et al. 2010

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

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139

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Antiviral drugs targeting viral proteins often result in prompt selection for resistance. Moreover, the number of viral targets is limited. Novel antiviral targets are therefore needed. The unique characteristics of fusion between virion envelopes and cell membranes may provide such targets. Like all fusing bilayers, viral envelopes locally adopt hourglass-shaped stalks during the initial stages of fusion, a process that requires local negative membrane curvature. Unlike cellular vesicles, however, viral envelopes do not redistribute lipids between leaflets, can only use the energy released by virion proteins, and fuse to the extracellular leaflets of cell membranes. Enrichment in phospholipids with hydrophilic heads larger than their hydrophobic tails in the convex outer leaflet of vesicles favors positive curvature, therefore increasing the activation energy barrier for fusion. Such phospholipids can increase the activation barrier beyond the energy provided by virion proteins, thereby inhibiting viral fusion. However, phospholipids are not pharmacologically useful. We show here that a family of synthetic rigid amphiphiles of shape similar to such phospholipids, RAFIs (rigid amphipathic fusion inhibitors), inhibit the infectivity of several otherwise unrelated enveloped viruses, including hepatitis C and HSV-1 and -2 (lowest apparent IC 50 48 nM), with no cytotoxic or cytostatic effects (selectivity index > 3,000) by inhibiting the increased negative curvature required for the initial stages of fusion.lipid bilayer fusion | DNA virus | RNA virus | Sindbis virus | nucleosides

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“…These authors found that emerin hyperphosphorylation depended upon US3 in HSV-2-infected cells and that it could be inhibited by an inhibitor of the cyclin-dependent kinase CDK1. The dependence on CDK1 activity is interesting, since inhibitors of CDKs, including CDK1, inhibit multiple steps in the virus life cycle (8,11,28,(56)(57)(58), and a dominant-negative CDK1 inhibits viral-DNA replication and late-gene expression (1). CDK1 inhibition may depress expression of late genes, and the CDK1 dependence of emerin phosphorylation may reflect lower UL34 expression and recruitment of PKC␦.…”

Section: Discussionmentioning

confidence: 99%

Emerin Is Hyperphosphorylated and Redistributed in Herpes Simplex Virus Type 1-Infected Cells in a Manner Dependent on both UL34 and US3

Leach

Bjerke

Christensen

et al. 2007

J Virol

105

160

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Cells infected with wild-type herpes simplex virus type 1 (HSV-1) show disruption of the organization of the nuclear lamina that underlies the nuclear envelope. This disruption is reflected in changes in the localization and phosphorylation of lamin proteins. Here, we show that HSV-1 infection causes relocalization of the LEM domain protein emerin. In cells infected with wild-type virus, emerin becomes more mobile in the nuclear membrane, and in cells infected with viruses that fail to express UL34 protein (pUL34) and US3 protein (pUS3), emerin no longer colocalizes with lamins, suggesting that infection causes a loss of connection between emerin and the lamina. Infection causes hyperphosphorylation of emerin in a manner dependent upon both pUL34 and pUS3. Some emerin hyperphosphorylation can be inhibited by the protein kinase C␦ (PKC␦) inhibitor rottlerin. Emerin and pUL34 interact physically, as shown by pull-down and coimmunoprecipitation assays. Emerin expression is not, however, necessary for infection, since virus growth is not impaired in cells derived from emerin-null transgenic mice. The results suggest a model in which pUS3 and PKC␦ that has been recruited by pUL34 hyperphosphorylate emerin, leading to disruption of its connections with lamin proteins and contributing to the disruption of the nuclear lamina. Changes in emerin localization, nuclear shape, and lamin organization characteristic of cells infected with wild-type HSV-1 also occur in cells infected with recombinant virus that does not make viral capsids, suggesting that these changes occur independently of capsid envelopment.During primary envelopment, herpes simplex virus type 1 (HSV-1) nucleocapsids translocate from the nucleus to the cytoplasm by budding into the inner nuclear membrane and then fusing with the outer nuclear membrane. The capsid does not, however, have unimpeded access to the inner nuclear membrane. Lining the inside of the inner nuclear membrane is the nuclear lamina, which is composed of a meshwork of proteins with spaces too small for the capsid to move through without some disruption (2,19,65). The lamina meshwork is made up of intermediate filament family proteins called lamins that are linked to the inner nuclear membrane and to intranuclear proteins by association with lamin-associated proteins (LAPs) (reviewed in reference 65). Connection of the network of lamin proteins to the inner nuclear membrane is mediated by integral membrane LAPs, including emerin, lamin B receptor, LAP2-␤, and MAN-1 (26).Emerin is a member of a family of nuclear envelope proteins that share a common sequence called the LEM domain that mediates association with BAF (barrier to autointegration factor) and is important for the assembly of LEM domain proteins into the re-forming nuclear envelope following mitosis (21,37,39). Emerin also contains a lamin-binding domain that helps retain it in the interphase nuclear envelope (6,14,25,37). Emerin is ubiquitously expressed but is not essential for the viability of cells in culture (36). Failure to ...

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Roscovitine Inhibits Activation of Promoters in Herpes Simplex Virus Type 1 Genomes Independently of Promoter-Specific Factors

Cited by 45 publications

References 89 publications

CDK9 inhibitor FIT-039 prevents replication of multiple DNA viruses

CDK9 inhibitor FIT-039 prevents replication of multiple DNA viruses

Rigid amphipathic fusion inhibitors, small molecule antiviral compounds against enveloped viruses

Emerin Is Hyperphosphorylated and Redistributed in Herpes Simplex Virus Type 1-Infected Cells in a Manner Dependent on both UL34 and US3

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