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Journal of Virology, October 2000, p. 9106-9114, Vol. 74, No. 19
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
Herpes Simplex Virus Types 1 and 2 Differ in Their
Interaction with Heparan Sulfate
Edward
Trybala,
Jan-Åke
Liljeqvist,
Bo
Svennerholm, and
Tomas
Bergström*
Department of Clinical Virology, University
of Göteborg, S-413 46 Göteborg, Sweden
Received 28 February 2000/Accepted 13 July 2000
Cell surface heparan sulfate (HS) serves as an initial receptor for
many different viruses, including herpes simplex virus types 1 and 2 (HSV-1 and 2, respectively). Glycoproteins C and B (gC and gB) are
the major components of the viral envelope that mediate
binding to HS. In this study, purified gB and gC homologous proteins as well as purified HSV-1 and HSV-2 virions were compared for
the ability to bind isolated HS receptor molecules. HSV-1 gC and HSV-2
gC bound comparable amounts of HS. Similarly, HSV-1 gB and its HSV-2
counterpart showed no difference in the HS-binding capabilities.
Despite the similar HS-binding potentials of gB and gC homologs, HSV-1
virions bound more HS than HSV-2 particles. Purified gC and gB proteins
differed with respect to sensitivity of their interaction with HS to
increased concentrations of sodium chloride in the order gB-2 > gB-1 > gC-1 > gC-2. The corresponding pattern for binding
of whole HSV virions to cells in the presence of increased ionic
strength of the medium was HSV-2 gC-neg1 > HSV-1
gC
39 > HSV-1 KOS 321 > HSV-2 333. These
results relate the HS-binding activities of individual glycoproteins
with the cell-binding abilities of whole virus particles. In addition,
these data suggest a greater contribution of electrostatic forces for
binding of gB proteins and gC-negative mutants compared with binding of
gC homologs and wild-type HSV strains. Binding of wild-type HSV-2
virions was the least sensitive to increased ionic strength of the
medium, suggesting that the less extensive binding of HS molecules by HSV-2 than by HSV-1 can be compensated for by a relatively weak contribution of electrostatic forces to the binding. Furthermore, gB
and gC homologs exhibited different patterns of sensitivity of binding
to cells to inhibition with selectively N-, 2-O-, and 6-O-desulfated
heparin compounds. The O-sulfate groups of heparin were found to be
more important for interaction with gB-1 than gB-2. These results
indicate that HSV-1 and HSV-2 differ in their interaction with HS.
*
Corresponding author. Mailing address: Department of
Clinical Virology, Göteborg University, Guldhedsgatan 10B, S-413
46 Göteborg, Sweden. Phone: 46-31-604735. Fax: 46-31-827032. E-mail: tomas.bergstrom{at}microbio.gu.se.
Journal of Virology, October 2000, p. 9106-9114, Vol. 74, No. 19
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
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