Abstract

The major outer membrane protein (MOMP) of C. trachomatis is a putative vaccine candidate because of its association with protective immunity. Humoral responses to MOMP epitopes have been characterized and specific protective MOMP epitopes mapped. In contrast, the role of MOMP in cell- mediated immunity (CMI) is unresolved. The initial goal of the proposal will be to characterize specifics of MOMP sequence and structure, with respect to protective CMI, during chlamydial infection. This will involve: (i) use of defined MOMP epitopes as immunogens, and (ii) analyses of T lymphocyte responses to such antigens, both in vitro and with a mouse model. Based on these studies, T-cell clones to antigens which promote increased protective antibody response and/or stimulation of protective CMI will be exploited for T-cell epitope mapping. The protective abilities of these defined MOMP epitopes will be tested in a murine genital tract infection model by 1) examining the effects of adoptive transfer of T-cell clones and 2) immunizing mice with fusion proteins containing combinations of protective predicted B and T-cell epitopes. Because studies suggest that chlamydial heat shock protein (hsp600) promotes a delayed hypersensitivity (DTH) response, hsp60 may play a role in the pathology of chlamydial infection. The second goal of the proposal, analogous to the above goal, will be to characterize specifics of hsp60 sequence and structure, in this case with respect to the immunopathology of chlamydial upper tract infection in vivo. This will involve: (i) production of a suitable quantity of recombinant hsp60 as an immunogen, and (ii) characterization of T-cell lymphocyte response both in vitro and in vivo. The role of gammadelta T lymphocytes in response to hsp60 will be examined using a newly available transgenic murine line, deficient in gammadelta T- lymphocyte populations in order to complement studies in immunologically competent animals. Finally, we propose to use the results of our studies with MOMP to begin characterizing the role of CMI in patients exposed to or infected with Chlamydia spp.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI033087-03
Application #
3747341
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
3
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Boston Medical Center
Department
Type
DUNS #
005492160
City
Boston
State
MA
Country
United States
Zip Code
02118

  Publications

Muhlecker, W; Gulati, S; McQuillen, D P et al. (1999) An essential saccharide binding domain for the mAb 2C7 established for Neisseria gonorrhoeae LOS by ES-MS and MSn. Glycobiology 9:157-71
McQuillen, D P; Gulati, S; Ram, S et al. (1999) Complement processing and immunoglobulin binding to Neisseria gonorrhoeae determined in vitro simulates in vivo effects. J Infect Dis 179:124-35
Qureshi, N; Kaltashov, I; Walker, K et al. (1997) Structure of the monophosphoryl lipid A moiety obtained from the lipopolysaccharide of Chlamydia trachomatis. J Biol Chem 272:10594-600
Lo, S K; Golenbock, D T; Sass, P M et al. (1997) Engagement of the Lewis X antigen (CD15) results in monocyte activation. Blood 89:307-14
Gulati, S; McQuillen, D P; Mandrell, R E et al. (1996) Immunogenicity of Neisseria gonorrhoeae lipooligosaccharide epitope 2C7, widely expressed in vivo with no immunochemical similarity to human glycosphingolipids. J Infect Dis 174:1223-37
Gulati, S; McQuillen, D P; Sharon, J et al. (1996) Experimental immunization with a monoclonal anti-idiotope antibody that mimics the Neisseria gonorrhoeae lipooligosaccharide epitope 2C7. J Infect Dis 174:1238-48
Ingalls, R R; Rice, P A; Qureshi, N et al. (1995) The inflammatory cytokine response to Chlamydia trachomatis infection is endotoxin mediated. Infect Immun 63:3125-30
Ingalls, R R; Golenbock, D T (1995) CD11c/CD18, a transmembrane signaling receptor for lipopolysaccharide. J Exp Med 181:1473-9
Golenbock, D T; Bach, R R; Lichenstein, H et al. (1995) Soluble CD14 promotes LPS activation of CD14-deficient PNH monocytes and endothelial cells. J Lab Clin Med 125:662-71
Delude, R L; Savedra Jr, R; Zhao, H et al. (1995) CD14 enhances cellular responses to endotoxin without imparting ligand-specific recognition. Proc Natl Acad Sci U S A 92:9288-92

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