Herpes Simplex Virus gD and Virions Accumulate in Endosomes by Mannose 6-Phosphate-Dependent and -Independent Mechanisms

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J Virol, April 1998, p. 3330-3339, Vol. 72, No. 4
0022-538X/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.

Herpes Simplex Virus gD and Virions Accumulate in Endosomes by Mannose 6-Phosphate-Dependent and -Independent Mechanisms

Craig R. Brunetti,¹^, Kevin S. Dingwell,¹^,² Cathy Wale,¹ Frank L. Graham,¹^,² and David C. Johnson³^,^*

McMaster Cancer Research Group¹ and Department of Biology,² McMaster University, Hamilton, Ontario, Canada L8N 3Z5, and Department of Molecular Microbiology and Immunology, Oregon Health Sciences University, Portland, Oregon 97201³

Received 16 October 1997/Accepted 12 January 1998

Herpes simplex virus (HSV) glycoprotein D (gD) is modified with mannose 6-phosphate (M6P) and binds to M6P receptors (MPRs).MPRs are involved in the well-characterized pathway by which lysosomalenzymes are directed to lysosomes via a network of endosomal membranes.Based on the impaired ability of HSV to form plaques under conditionsin which glycoproteins could not interact with MPRs, we proposedthat MPRs may function during HSV egress or cell-to-cell spread(C. R. Brunetti, R. L. Burke, B. Hoflack, T. Ludwig, K. S. Dingwell,and D. C. Johnson, J. Virol. 69:3517-3528, 1995). To further analyzeM6P modification and intracellular trafficking of gD in the absenceof other HSV proteins, adenovirus (Ad) vectors were used to expresssoluble and membrane-anchored forms of gD. Both membrane-boundand soluble gD were modified with M6P residues and were localizedto endosomes that contained the 275-kDa MPR or the transferrinreceptor. Similar results were observed in HSV-infected cells.Cell fractionation experiments showed that gD was not presentin lysosomes. However, a mutant form of gD and another HSV glycoprotein,gI, that were not modified with M6P were also found in endosomesin HSV-infected cells. Moreover, a substantial fraction of theHSV nucleocapsid protein VP6 was found in endosomes, consistentwith accumulation of virions in an endosomal compartment. Therefore,it appears that HSV glycoproteins and virions are directed toendosomes, by M6P-dependent as well as by M6P-independent mechanisms,either as part of the virus egress pathway or by endocytosis fromthe cell surface.

^* Corresponding author. Mailing address: L-220, Dept. of Molecular Microbiology and Immunology, Oregon Health Sciences University,3181 S.W. Sam Jackson Park Rd., Portland, OR 97201. Phone: (503)494-0834. Fax: (503) 494-6862. E-mail: johnsoda{at}ohsu.edu.

Present address: Howard Hughes Medical Institute, University of Wisconsin, Madison, WI 53706.

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