Abstract

The overall goal of this revised application is to test immunogens and strategies of new conception for vaccination against MUC-1. MUC-1, a highly glycosylated mucin expressed on the luminal side of glandular epithelial, consists of 30-90 tandem repeats of 20 amino acids within which there exists an immunodominant epitope. During malignant transformation mucin is over-expressed, and mucin-producing cells lose luminal polarity with mucin becoming expressed all around the cell surface rendering tumor cells less susceptible to immune effector mechanisms and favoring apoptosis of T cells. Vaccination against MUC-1 is intended at generating two effects: (1) antibodies of sufficient specificity and avidity could cause redistribution (via cross-linking and capping) of the MUC-1 antigen at the surface of tumor cells hence reinstating the full immunological potential of the host against tumor cells expressing MUC-1; (2) T cells with cytotoxic activity that kill mucin-expressing tumor cells, particularly micro-metastasis. The vaccination experiments proposed herein are based on methods and principled developed in the laboratory and designed at maximizing the immunogenicity of MUC-1 oligopeptides by expressing them in the hyper-variable loops of antibodies, i.e., structures with limited flexibility anchored into the conserved immunoglobulin fold. This approach allows for their expression as conformationally-constrained units, a necessary prerequisite for the induction of biologically active B cell responses. Heterologous epitopes expressed in hyper-variable loops of antibodies are also site of preferential intracellular cleavage so that peptides for the activation of T cells are easily generated. Combined with the advantages of this pro protein engineering approach will be the use of a newly-developed method of DNA-based vaccination (Somatic Transgene Immunization), a method through which the genes of antibodies coding for MUC-1 epitopes are themselves utilized in vivo as vaccines to induce both antibodies and T cells. Studies will be done in normal C57B16 mice, in human MUC-1 transgenic mice to evaluate the limitations (if any) proposed by self tolerance, and in mice knock-out for the alpha (1->3) galactosyl transferase to determine if naturally-occurring antibodies (which are present in these KO mice) limit the extent to which specific cellular responses can be induced by vaccination. The efficacy of this type of vaccination will be evaluated in experiments of tumor protection (prevention or down-regulation of growth) in normal as well as transgenic mice.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA077427-01A2
Application #
2899962
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Program Officer
Yovandich, Jason L
Project Start
1999-07-23
Project End
2002-06-30
Budget Start
1999-07-23
Budget End
2000-06-30
Support Year
1
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of California San Diego
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
077758407
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Cortez-Gonzalez, Xochitl; Pellicciotta, Ilenia; Gerloni, Mara et al. (2006) TLR9-independent activation of B lymphocytes by bacterial DNA. DNA Cell Biol 25:253-61
Koch, Katherine S; Son, Kyung-Hwa; Maehr, Rene et al. (2006) Immune-privileged embryonic Swiss mouse STO and STO cell-derived progenitor cells: major histocompatibility complex and cell differentiation antigen expression patterns resemble those of human embryonic stem cell lines. Immunology 119:98-115
Gerloni, Mara; Castiglioni, Paola; Zanetti, Maurizio (2005) The cooperation between two CD4 T cells induces tumor protective immunity in MUC.1 transgenic mice. J Immunol 175:6551-9
Zanetti, Maurizio (2005) T for two: when helpers need help. Autoimmun Rev 4:571-8
Gerloni, Mara; Zanetti, Maurizio (2005) CD4 T cells in tumor immunity. Springer Semin Immunopathol 27:37-48
Gerloni, Mara; Rizzi, Marta; Castiglioni, Paola et al. (2004) T cell immunity using transgenic B lymphocytes. Proc Natl Acad Sci U S A 101:3892-7
Filaci, G; Gerloni, M; Rizzi, M et al. (2004) Spontaneous transgenesis of human B lymphocytes. Gene Ther 11:42-51
Zanetti, Maurizio; Castiglioni, Paola; Rizzi, Marta et al. (2004) B lymphocytes as antigen-presenting cell-based genetic vaccines. Immunol Rev 199:264-78
Castiglioni, Paola; Gerloni, Mara; Zanetti, Maurizio (2004) Genetically programmed B lymphocytes are highly efficient in inducing anti-virus protective immunity mediated by central memory CD8 T cells. Vaccine 23:699-708
Castiglioni, Paola; Lu, Christina; Lo, David et al. (2003) CD4 T cell priming in dendritic cell-deficient mice. Int Immunol 15:127-36

Showing the most recent 10 out of 15 publications