Basic amino acids as modulators of an O-linked glycosylation signal of the herpes simplex virus type 1 glycoprotein gC: functional roles in viral infectivity

doi:10.1093/glycob/cwh075

Glycobiology Advance Access originally published online on March 24, 2004
Glycobiology 2004 14(7):571-581; doi:10.1093/glycob/cwh075

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Basic amino acids as modulators of an O-linked glycosylation signal of the herpes simplex virus type 1 glycoprotein gC: functional roles in viral infectivity

Kristina Mårdberg², Kristina Nyström², Mads Agervig Tarp³, Edward Trybala², Henrik Clausen³, Tomas Bergström² and Sigvard Olofsson¹^,2

² Department of Virology, University of Göteborg, Guldhedsgatan 10B; S-413 46 Göteborg, Sweden; and ³ Faculty of Health Sciences, School of Dentistry, Nørre Alle 20 DK-2200 N, Denmark

Received on September 22, 2003; revised on February 2, 2004; accepted on March 5, 2004

The herpes simplex virus type 1 (HSV-1) glycoprotein gC-1 isengaged both in viral attachment and viral immune evasion mechanismsin the infected host. Besides several N-linked glycans, gC-1contains numerous O-linked glycans, mainly localized in twopronase-resistant clusters in the N-terminal domain of gC-1.In the present study we construct and characterize one gC-1mutant virus, in which two basic amino acids (114K and 117R)in a putative O-glycosylation sequon were changed to alanine.We found that this modification did not modify the N-linkedglycosylation but increased the content of O-linked glycansconsiderably. Analysis of the O-glycosylation capacity of wild-typeand mutant gC-1 was performed by in vitro glycosylation assayswith synthetic peptides derived from the mutant region predictedto present new O-glycosylation sites. Thus the mutant peptideregion served as a better substrate for polypeptide GalNAc-transferase2 than the wild-type peptide, resulting in increased rate andnumber of O-glycan attachment sites. The predicted increasein O-linked glycosylation resulted in two modifications of thebiological properties of mutant virus—that is, an impairedbinding to cells expressing chondroitin sulfate but not heparansulfate on the cell surface and a significantly reduced plaquesize in cultured cells. The results suggested that basic aminoacids present within O-glycosylation signals may down-regulatethe amount of O-linked glycans attached to a protein and thatsubstitution of such amino acid residues may have functionalconsequences for a viral glycoprotein involving virus attachmentto permissive cells as well as viral cell-to-cell spread.

¹ To whom correspondence should be addressed; e-mail: sigvard.olofsson{at}microbio.gu.se

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