Abstract

The long term goal of the Papillomavirus Research Unit of the University of Queensland is to study the immunobiology of HPV infection and hence develop vaccines that could be used: I) as a treatment for patients with HPV associated cervical cancer or precancer, or II) to prevent HPV infection, for all women at risk. The detailed aims of the present proposal are: 1) to create transgenic mouse models of HPV infection in which epithelial cells express HPV E6 and E7 proteins, using a number of strategies to avoid the lethal effects of these proteins on the developing embryo. Such mice should constitute an immunological model for HPV infected human cervical epithelium: peptides derived from HPV proteins will be presented by epithelial cells to the immune system without local inflammation. Mice immunologically naive with regard to HPV protein will be produced by induction of transgene expression in adult life, using an inducible binary transgene system, and by grafting transgenic skin to naive HPV transgene negative but otherwise syngeneic mice. Mice constitutively expressing the HPV transgene, and hence tolerant of it, will also be studied. 2) to test the effect of acquired immunity to HPV proteins on HPV E6 and E7 transgenic epithelium using our mouse models. Immunity will be induced by a number of vaccine strategies, including i) iscoms and HPV peptides, ii) baculovirus derived HPV proteins with 'Algammulin', iii) HPV peptides coupled to P3CSSS, iv) HPV recombinant adenoviruses, and v) HPV recombinant vaccinia viruses. 3) to determine, using in vitro assays for antigen specific cell mediated immunity, how the immune response to natural HPV infection in man compares with the vaccine induced immune response in mice, and the natural immune responses in naive and HPV tolerant transgenic mice. 4) to conduct a phase 1/2 clinical trial of the appropriate HPV16 E6 or E7 based vaccine in patients with advanced cervical cancer who have failed conventional therapy, and who have an HPV16 associated cancer expressing HPV16 E7 protein in tumor cells. The appropriate vaccine will be one producing immune responses which result in rejection of HPV transgenic epithelium in both naive and HPV tolerant mice.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA057789-02
Application #
3202135
Study Section
Special Emphasis Panel (SRC (66))
Project Start
1992-08-01
Project End
1995-07-31
Budget Start
1993-08-15
Budget End
1994-07-31
Support Year
2
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Queensland University of Technology
Department
Type
DUNS #
City
Brisbane
State
Country
Australia
Zip Code
4001

  Publications

Leggatt, Graham R; Dunn, Linda A; De Kluyver, Rachel L et al. (2002) Interferon-gamma enhances cytotoxic T lymphocyte recognition of endogenous peptide in keratinocytes without lowering the requirement for surface peptide. Immunol Cell Biol 80:415-24
Frazer, I H; De Kluyver, R; Leggatt, G R et al. (2001) Tolerance or immunity to a tumor antigen expressed in somatic cells can be determined by systemic proinflammatory signals at the time of first antigen exposure. J Immunol 167:6180-7
Fernando, G J; Murray, B; Zhou, J et al. (1999) Expression, purification and immunological characterization of the transforming protein E7, from cervical cancer-associated human papillomavirus type 16. Clin Exp Immunol 115:397-403
Zhou, J; Liu, W J; Peng, S W et al. (1999) Papillomavirus capsid protein expression level depends on the match between codon usage and tRNA availability. J Virol 73:4972-82
Peng, S; Frazer, I H; Fernando, G J et al. (1998) Papillomavirus virus-like particles can deliver defined CTL epitopes to the MHC class I pathway. Virology 240:147-57
Dunn, L A; Evander, M; Tindle, R W et al. (1997) Presentation of the HPV16E7 protein by skin grafts is insufficient to allow graft rejection in an E7-primed animal. Virology 235:94-103
Qi, Y M; Peng, S W; Hengst, K et al. (1996) Epithelial cells display separate receptors for papillomavirus VLPs and for soluble L1 capsid protein. Virology 216:35-45
Frazer, I H (1996) The role of vaccines in the control of STDs: HPV vaccines. Genitourin Med 72:398-403
Frazer, I H; Leippe, D M; Dunn, L A et al. (1995) Immunological responses in human papillomavirus 16 E6/E7-transgenic mice to E7 protein correlate with the presence of skin disease. Cancer Res 55:2635-9
Fernando, G J; Stenzel, D J; Tindle, R W et al. (1995) Peptide polymerisation facilitates incorporation into ISCOMs and increases antigen-specific IgG2a production. Vaccine 13:1460-7

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