Disulfide bond structure of glycoprotein D of herpes simplex virus types 1 and 2.

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J Virol. 1992 November; 66(11): 6668-6685

Disulfide bond structure of glycoprotein D of herpes simplex virus types 1 and 2.

D Long, W C Wilcox, W R Abrams, G H Cohen and R J Eisenberg

Department of Microbiology, University of Pennsylvania, Philadelphia 19104-6003.

ABSTRACT

Glycoprotein D (gD) is a structural component of the herpessimplex virus envelope which is essential for virus penetration.The function of this protein is highly dependent on its structure,and its structure is dependent on maintenance of three intactdisulfide bonds. gD contains six cysteines in its ectodomainwhose spacing is conserved among all its homologs in other alphaherpesvirusesas well as Marek's disease virus. For other proteins, conservationof cysteine spacing correlates with conservation of disulfidebond structure. We have now solved the disulfide bond structureof gD-1 and gD-2 of herpes simplex virus types 1 and 2, respectively.Two approaches were used. First, we constructed 15 double-Cysmutants of gD-1, representing all possible disulfide pairs.In each case, codons for cysteines were changed to serine. Wereasoned that if two cysteines normally form a disulfide bond,double mutations which eliminate one proper bond should be lessharmful to gD structure than double mutations which eliminatetwo disulfide bonds. The mutated genes were cloned into a eucaryoticexpression vector, and the proteins were expressed in transientlytransfected cells. Three double mutations, Cys-1,5, Cys-2,6,and Cys-3,4 permitted gD-1 folding, processing, transport tothe cell surface, and function in virus infection, whereas 12other double mutations each produced a malfolded and nonfunctionalprotein. Thus, the three functional double-Cys mutants may representthe actual partners in disulfide bond linkages. The second approachwas to define the actual disulfide bond structure of gD by biochemicalmeans. Purified native gD-2 was cleaved by CNBr and proteases,and the peptides were separated by high-performance liquid chromatography.Disulfide-linked peptides were subjected to N-terminal aminoacid sequencing. The results show that cysteine 1 (amino acid[aa] 66) is bonded to cysteine 5 (aa 189), cysteine 2 (aa 106)is bonded to cysteine 6 (aa 202), and cysteine 3 (aa 118) isbonded to cysteine 4 (aa 127). Thus, the biochemical analysisof gD-2 agrees with the genetic analysis of gD-1. A similardisulfide bond arrangement is postulated to exist in other gDhomologs.

J Virol. 1992 November; 66(11): 6668-6685

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