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Clinical and Diagnostic Laboratory Immunology, May 1999, p. 356-363, Vol. 6, No. 3
Department of Pathology, University of
California
Received 26 October 1998/Returned for modification 17 December
1998/Accepted 25 January 1999
C3H (H-2k) mice are susceptible to a
vaginal challenge with human strains of Chlamydia
trachomatis and thus are a useful strain for testing potential
Chlamydia vaccine candidates. However, C3H mice are fairly
poor responders in terms of the level of antibody resulting from
immunization with potential protective peptides representing variable
domains (VDs) of the major outer membrane protein (MOMP). C57BL/6
(H-2b) mice, on the other hand, are moderately
resistant to a vaginal challenge but are good responders to the
chlamydial MOMP VDs. Peptides representing universal T-cell helper
epitopes were employed to determine whether the antibody response to a
peptide representing VD4 of the MOMP, which has been shown to contain
neutralizing epitopes, could be enhanced in C3H and C57 mice. Universal
T-cell helper peptides from tetanus toxin, the pre-S2 region of
hepatitis B virus, and the mouse heat shock protein 60, as well as the
corresponding segment of the Chlamydia heat shock protein
60 (hspct), were coadministered with the VD4 peptide.
Peptides were coencapsulated in liposomes containing the adjuvant
monophosphoryl lipid A and administered by using a combination of
mucosal and intramuscular injection. The only T-cell helper peptide
that improved the immune response as judged by antibody level, in vitro
neutralization assays, and T-cell proliferation was hspct.
The response in the C57BL/6 strain was not significantly enhanced with
hspct over levels achieved with VD4 alone; however, in C3H
mice the levels of serum antibody to C. trachomatis
increased to that seen in C57 mice. However, the molecular specificity
and immunoglobulin subclass distribution differed from those of the C57
response, and the neutralizing titers and T-cell proliferation
responses were lower. In both strains of mice, titers of vaginal
antibody to C. trachomatis were low. In summary, of the
T-helper peptides used, only hspct significantly enhanced
the immune response of C3H mice to the VD4 peptide, but it had only a
modest effect on the immune response of C57 mice.
1071-412X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Immunization with a Peptide Corresponding to Chlamydial Heat
Shock Protein 60 Increases the Humoral Immune Response in C3H Mice
to a Peptide Representing Variable Domain 4 of the Major Outer
Membrane Protein of Chlamydia trachomatis
Irvine, Irvine, California 92697-4800
*
Corresponding author. Mailing address: Department of
Pathology, Medical Science Building, Room D440, University of
California, Irvine, Irvine, CA 92697-4800. Phone: (949) 824-4169. Fax:
(949) 824-2160. E-mail: epeterso{at}uci.edu.
Present address: Lawrence Livermore National Laboratory, Human
Genome Center, Livermore, CA 94550.
Clinical and Diagnostic Laboratory Immunology, May 1999, p. 356-363, Vol. 6, No. 3
1071-412X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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