Abstract

Cholera toxin and the similar heat labile toxin of E. coli are among the most effective adjuvants known for enhancing mucosal immune responses. These toxins have been shown to enhance immune responses after both oral and intranasal immunization. The mechanism(s) which these molecules use to enhance immune responses are not well established, however, and their inherent toxicity is a major problem which makes their use in humans impractical. As probes into the mechanism(s) by which these toxin molecules enhance immune responses, the investigators have assembled a panel of genetically engineered toxin derivatives, many with reduced or absent toxicity. Using both model antigens and infectious challenge models in mice, they will investigate the mechanisms by which native and altered toxins enhance oral and intranasal immune responses. The investigators will determine how native and engineered toxin molecules affect uptake of model antigens into mucosal tissues such as Peyer's patches and enterocytes and whether antigen presentation and intracellular antigen processing is up regulated. They will also study the direct effects of cholera toxin/heat labile toxin and engineered derivatives upon antigen responsive B lymphocytes and the effects upon patterns of cytokine secretion by T lymphocytes. Ultimately, if non-toxic derivatives of cholera toxin or heat labile toxin which still stimulate mucosal immune responses are identified, they may find use as adjuvants for mucosal vaccines versus pathogenic organisms or even dietary carcinogens. Thus, they will also investigate the effectiveness of non-toxic-engineered cholera toxin/heat labile toxin derivatives in promoting protective immune responses in two infectious challenge models. The models which the investigators have chosen are intranasal Sendai virus infection and oral Helicobacter felis infection. Sendai virus infects the respiratory tract and is a murine parainfluenza virus. Helicobacter infections of gastric tissue have been implicated as causes of gastroduodenal ulcers and gastric cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
1R01AI040701-01
Application #
2005263
Study Section
Immunological Sciences Study Section (IMS)
Project Start
1997-02-01
Project End
2000-01-31
Budget Start
1997-02-01
Budget End
1998-01-31
Support Year
1
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Case Western Reserve University
Department
Pathology
Type
Schools of Medicine
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106

  Publications

Garhart, Christine A; Nedrud, John G; Heinzel, Frederick P et al. (2003) Vaccine-induced protection against Helicobacter pylori in mice lacking both antibodies and interleukin-4. Infect Immun 71:3628-33
Garhart, Christine A; Heinzel, Frederick P; Czinn, Steven J et al. (2003) Vaccine-induced reduction of Helicobacter pylori colonization in mice is interleukin-12 dependent but gamma interferon and inducible nitric oxide synthase independent. Infect Immun 71:910-21
Garhart, Christine A; Redline, Raymond W; Nedrud, John G et al. (2002) Clearance of Helicobacter pylori Infection and Resolution of Postimmunization Gastritis in a Kinetic Study of Prophylactically Immunized Mice. Infect Immun 70:3529-38
Johansson, M; Lycke, N (2001) Immunological memory in B-cell-deficient mice conveys long-lasting protection against genital tract infection with Chlamydia trachomatis by rapid recruitment of T cells. Immunology 102:199-208
Chintalacharuvu, S R; Nagy, N U; Sigmund, N et al. (2001) T cell cytokines determine the severity of experimental IgA nephropathy by regulating IgA glycosylation. Clin Exp Immunol 126:326-33
Gardby, E; Chen, X J; Lycke, N Y (2001) Impaired CD40-signalling in CD19-deficient mice selectively affects Th2-dependent isotype switching. Scand J Immunol 53:13-23
Gottwein, J M; Blanchard, T G; Targoni, O S et al. (2001) Protective anti-Helicobacter immunity is induced with aluminum hydroxide or complete Freund's adjuvant by systemic immunization. J Infect Dis 184:308-14
Agren, L; Sverremark, E; Ekman, L et al. (2000) The ADP-ribosylating CTA1-DD adjuvant enhances T cell-dependent and independent responses by direct action on B cells involving anti-apoptotic Bcl-2- and germinal center-promoting effects. J Immunol 164:6276-86
Gardby, E; Lycke, N Y (2000) CD19-deficient mice exhibit poor responsiveness to oral immunization despite evidence of unaltered total IgA levels, germinal centers and IgA-isotype switching in Peyer's patches. Eur J Immunol 30:1861-71
Nedrud, J G (1999) Animal models for gastric Helicobacter immunology and vaccine studies. FEMS Immunol Med Microbiol 24:243-50

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