Herpes simplex virus glycoproteins E and I facilitate cell-to-cell spread in vivo and across junctions of cultured cells

Dingwell, Kevin S.; Brunetti, Craig R.; Hendricks, Robert L.; Tang, Qizhi; Tang, Mary Y.; Rainbow, Andrew J.; Johnson, David C.

doi:10.1128/jvi.68.2.834-845.1994

Cited by 307 publications

(174 citation statements)

References 58 publications

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“…A naturally occurring VZV mutant with a point mutation in gE shows accelerated cell-to-cell spread in cell culture and in human cells in SCID-hu mice (Santos et al, 2000). HSV gE, which is homologous to the VZV glycoprotein, is necessary for directing egress of virus to the basolateral surface of polarized cells (Collins and Johnson, 2003;Dingwell et al, 1994).…”

Section: Discussionmentioning

confidence: 99%

Insulin Degrading Enzyme Is a Cellular Receptor Mediating Varicella-Zoster Virus Infection and Cell-to-Cell Spread

Ali

Cohen

2006

Cell

136

151

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Varicella-zoster virus (VZV) causes chickenpox and shingles. While varicella is likely spread as cell-free virus to susceptible hosts, the virus is transmitted by cell-to-cell spread in the body and in vitro. Since VZV glycoprotein E (gE) is essential for virus infection, we postulated that gE binds to a cellular receptor. We found that insulin-degrading enzyme (IDE) interacts with gE through its extracellular domain. Downregulation of IDE by siRNA, or blocking of IDE with antibody, with soluble IDE protein extracted from liver, or with bacitracin inhibited VZV infection. Cell-to-cell spread of virus was also impaired by blocking IDE. Transfection of cell lines impaired for VZV infection with a plasmid expressing human IDE resulted in increased entry and enhanced infection with cell-free and cell-associated virus. These studies indicate that IDE is a cellular receptor for both cell-free and cell-associated VZV.

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Section: Discussionmentioning

confidence: 99%

Insulin Degrading Enzyme Is a Cellular Receptor Mediating Varicella-Zoster Virus Infection and Cell-to-Cell Spread

Ali

Cohen

2006

Cell

136

151

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“…The minimal mutation introduced into the gE mutants affected the IgG-related functions of gE:gI, but did not interfere with the other important gE function, i.e. to mediate direct cell-to-cell spread of nascent virions [95].…”

Section: The Fccr Of the A-herpesviruses: The Ge:gi Complexmentioning

confidence: 98%

Herpesviral Fcγ receptors: culprits attenuating antiviral IgG?

Budt

Reinhard

Bigl

et al. 2004

International Immunopharmacology

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Production of IgG in response to virus infection is central to antiviral immune effector functions and a hallmark of B cell memory. Antiviral antibodies (Abs) recognising viral glycoproteins or protein antigen displayed on the surface of virions or virus-infected cells are crucial in rendering the virus noninfectious and in eliminating viruses or infected cells, either acting alone or in conjunction with complement. In many instances, passive transfer of Abs is sufficient to protect from viral infection. Herpesviruses (HV) are equipped with a large array of immunomodulatory functions which increase the efficiency of infection by dampening the antiviral immunity. Members of the alpha- and beta-subfamily of the Herpesviridae are distinct in encoding transmembrane glycoproteins which selectively bind IgG via its Fc domain. The Fc-binding proteins constitute viral Fcgamma receptors (vFcgammaRs) which are expressed on the cell surface of infected cells. Moreover, vFcgammaRs are abundantly incorporated into the envelope of virions. Despite their molecular and structural heterogeneity, the vFcgammaRs generally interfere with IgG-mediated effector functions like antibody (Ab)-dependent cellular cytolysis, complement activation and neutralisation of infectivity of virions. vFcgammaRs may thus contribute to the limited therapeutic potency of antiherpesviral IgG in clinical settings. A detailed molecular understanding of vFcgammaRs opens up the possibility to design recombinant IgG molecules resisting vFcgammaRs. Engineering IgG with a better antiviral efficiency represents a new therapeutic option against herpesviral diseases.

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“…4). In addition, herpesviruses can travel from infected cells to neighbouring cells via budding at the basolateral intercellular junction or by crossing the tight junctions between cells (Cocchi et al, 2000;Dingwell et al, 1994;York and Johnson, 1993). Whether these mechanisms are responsible for the accelerated spread of ILTV that we observed remains unclear.…”

Section: Discussionmentioning

confidence: 89%

“…Numerous efforts have been made to elucidate the mechanisms involved in the intercellular spread of viruses. The simplest and most widely used model of cell-to-cell spread is plaque formation in cell cultures with or without the addition of a neutralizing antibody, which reflects the cumulative processes of the host-virus interaction, including viral binding, penetration and replication, reorganization of cell-to-cell junctions, viral intercellular transport, and restriction mechanisms used by the host to resist infection, such as antiviral immune responses and factors (Dingwell et al, 1994;Johnson et al, 2001;Mettenleiter et al, 2009). Such models have been frequently used to investigate the processes of cell-to-cell spread and the essential viral and host factors for these processes (Farnsworth and Johnson, 2006;Krummenacher et al, 2003;Sourvinos and Everett, 2002).…”

Section: Discussionmentioning

confidence: 99%

Host Src controls gallid alpha herpesvirus 1 intercellular spread in a cellular fatty acid metabolism-dependent manner

et al. 2019

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A B S T R A C TViral spread is considered a promising target for antiviral therapeutics, but the associated mechanisms remain unclear for gallid alpha herpesvirus 1 (ILTV). We previously identified proto-oncogene tyrosine-protein kinase Src (Src) as a crucial host determinant of ILTV infection. The present study revealed accelerated spread of ILTV upon Src inhibition. This phenomenon was independent of either viral replication or the proliferation of infected cells and could not be compromised by neutralizing antibody. Neither extracellular vesicles nor the direct cytosol-to-cytosol connections between adjacent cells contributed to the enhanced spread of ILTV upon Src inhibition. Further genome-wide transcriptional profile analyses in combination with functional validation identified fatty acid metabolism as an essential molecular event during modulation of the intercellular spread and subsequent cytopathic effect of ILTV by Src. Overall, these data suggest that Src controls the cell-to-cell spread of ILTV in a cellular fatty acid metabolism-dependent manner, which determines the virus's cytopathic effect.

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Herpes simplex virus glycoproteins E and I facilitate cell-to-cell spread in vivo and across junctions of cultured cells

Cited by 307 publications

References 58 publications

Insulin Degrading Enzyme Is a Cellular Receptor Mediating Varicella-Zoster Virus Infection and Cell-to-Cell Spread

Insulin Degrading Enzyme Is a Cellular Receptor Mediating Varicella-Zoster Virus Infection and Cell-to-Cell Spread

Herpesviral Fcγ receptors: culprits attenuating antiviral IgG?

Host Src controls gallid alpha herpesvirus 1 intercellular spread in a cellular fatty acid metabolism-dependent manner

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