Literature DB >> 12885915

Cellular localization of nectin-1 and glycoprotein D during herpes simplex virus infection.

Claude Krummenacher1, Isabelle Baribaud, Roselyn J Eisenberg, Gary H Cohen.   

Abstract

During viral entry, herpes simplex virus (HSV) glycoprotein D (gD) interacts with a specific cellular receptor such as nectin-1 (PRR1/HveC/CD111) or the herpesvirus entry mediator A (HVEM/HveA). Nectin-1 is involved in cell-to-cell adhesion. It is located at adherens junctions, where it bridges cells through homophilic or heterophilic interactions with other nectins. Binding of HSV gD prevents nectin-1-mediated cell aggregation. Since HSV gD affects the natural function of nectin-1, we further investigated the effects of gD expression on nectin-1 during HSV infection or in transfected cells. We also studied the importance of the interaction between nectin-1 and the cytoplasmic protein afadin for HSV entry and spread as well as the effects of infection on this interaction. In these investigations, we used a panel of cells expressing nectin-1 or nectin-1-green fluorescent protein fusions as the only mediators of HSV entry. During HSV infection, nectin-1 localization at adherens junction was dramatically altered in a manner dependent on gD expression. Nectin-1 and gD colocalized at cell contact areas between infected and noninfected cells and at the edges of plaques. This specific accumulation of gD at junctions was driven by expression of nectin-1 in trans on the surface of adjacent cells. Reciprocally, nectin-1 was maintained at junctions by the trans expression of gD in the absence of a cellular natural ligand. Our observations indicate that newly synthesized gD substitutes for nectin-1 of infected cells at junctions with noninfected cells. We propose that gD attracts and maintains the receptor at junctions where it can be used for virus spread.

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Year:  2003        PMID: 12885915      PMCID: PMC167240          DOI: 10.1128/jvi.77.16.8985-8999.2003

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  77 in total

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3.  Use of chimeric nectin-1(HveC)-related receptors to demonstrate that ability to bind alphaherpesvirus gD is not necessarily sufficient for viral entry.

Authors:  R J Geraghty; A Fridberg; C Krummenacher; G H Cohen; R J Eisenberg; P G Spear
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4.  The V domain of herpesvirus Ig-like receptor (HIgR) contains a major functional region in herpes simplex virus-1 entry into cells and interacts physically with the viral glycoprotein D.

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5.  Requirement of interaction of nectin-1alpha/HveC with afadin for efficient cell-cell spread of herpes simplex virus type 1.

Authors:  T Sakisaka; T Taniguchi; H Nakanishi; K Takahashi; M Miyahara; W Ikeda; S Yokoyama; Y F Peng; K Yamanishi; Y Takai
Journal:  J Virol       Date:  2001-05       Impact factor: 5.103

6.  Chimeric nectin1-poliovirus receptor molecules identify a nectin1 region functional in herpes simplex virus entry.

Authors:  F Cocchi; M Lopez; P Dubreuil; G Campadelli Fiume; L Menotti
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7.  A novel role for 3-O-sulfated heparan sulfate in herpes simplex virus 1 entry.

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Journal:  Virology       Date:  2001-09-01       Impact factor: 3.616

9.  The first immunoglobulin-like domain of HveC is sufficient to bind herpes simplex virus gD with full affinity, while the third domain is involved in oligomerization of HveC.

Authors:  C Krummenacher; A H Rux; J C Whitbeck; M Ponce-de-Leon; H Lou; I Baribaud; W Hou; C Zou; R J Geraghty; P G Spear; R J Eisenberg; G H Cohen
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10.  Nectin/PRR: an immunoglobulin-like cell adhesion molecule recruited to cadherin-based adherens junctions through interaction with Afadin, a PDZ domain-containing protein.

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Journal:  J Cell Biol       Date:  1999-05-03       Impact factor: 10.539

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  40 in total

1.  Binding of herpes simplex virus glycoprotein D to nectin-1 exploits host cell adhesion.

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4.  The extracellular domain of herpes simplex virus gE is indispensable for efficient cell-to-cell spread: evidence for gE/gI receptors.

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5.  The herpesvirus glycoproteins B and H.L are sequentially recruited to the receptor-bound gD to effect membrane fusion at virus entry.

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Review 6.  The signaling networks of the herpesvirus entry mediator (TNFRSF14) in immune regulation.

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7.  Polarized cell migration during cell-to-cell transmission of herpes simplex virus in human skin keratinocytes.

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8.  Spatiotemporal changes of the herpes simplex virus entry receptor nectin-1 in murine brain during postnatal development.

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9.  Glycoprotein D actively induces rapid internalization of two nectin-1 isoforms during herpes simplex virus entry.

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10.  The antiapoptotic herpes simplex virus glycoprotein J localizes to multiple cellular organelles and induces reactive oxygen species formation.

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