Vaccinia Virus Envelope H3L Protein Binds to Cell Surface Heparan Sulfate and Is Important for Intracellular Mature Virion Morphogenesis and Virus Infection In Vitro and In Vivo

doi:10.1128/JVI.74.7.3353-3365.2000

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Journal of Virology, April 2000, p. 3353-3365, Vol. 74, No. 7
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Vaccinia Virus Envelope H3L Protein Binds to Cell Surface Heparan Sulfate and Is Important for Intracellular Mature Virion Morphogenesis and Virus Infection In Vitro and In Vivo

Chi-Long Lin,¹ Che-Sheng Chung,¹ Hans G. Heine,² and Wen Chang¹^,^*

Graduate Institute of Life Science, National Defense Medical Center and Institute of Molecular Biology, Academia Sinica, Taipei, Taiwan, Republic of China,¹ and Australian Animal Health Laboratory, CSIRO Animal Health, Geelong, Victoria, Australia²

Received 30 September 1999/Accepted 4 January 2000

An immunodominant antigen, p35, is expressed on the envelope of intracellular mature virions (IMV) of vaccinia virus. p35is encoded by the viral late gene H3L, but its role in the viruslife cycle is not known. This report demonstrates that solubleH3L protein binds to heparan sulfate on the cell surface and competeswith the binding of vaccinia virus, indicating a role for H3Lprotein in IMV adsorption to mammalian cells. A mutant virus defectivein expression of H3L (H3L) was constructed; the mutant virus has a small plaque phenotypeand 10-fold lower IMV and extracellular enveloped virion titersthan the wild-type virus. Virion morphogenesis is severely blockedand intermediate viral structures such as viral factories andcrescents accumulate in cells infected with the H3L mutant virus. IMV from the H3L mutant virus are somewhat altered and less infectious than wild-typevirions. However, cells infected by the mutant virus form multinucleatedsyncytia after low pH treatment, suggesting that H3L protein isnot required for cell fusion. Mice inoculated intranasally withwild-type virus show high mortality and severe weight loss, whereasmice infected with H3L mutant virus survive and recover faster, indicating that inactivationof the H3L gene attenuates virus virulence in vivo. In summary,these data indicate that H3L protein mediates vaccinia virus adsorptionto cell surface heparan sulfate and is important for vacciniavirus infection in vitro and in vivo. In addition, H3L proteinplays a role in virionassembly.

^* Corresponding author. Mailing address: Institute of Molecular Biology, Academia Sinica, Nankang, Taipei, Taiwan 11529, Republicof China. Phone: 886-2-2789-9230. Fax: 886-2-2782-6085. E-mail:mbwen{at}ccvax.sinica.edu.tw.

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