Strategies for the development of recombinant vaccines for the immunotherapy of breast cancer |
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| Authors: | Jeffrey Schlom Judy Kantor Scott Abrams Kwong Y. Tsang Dennis Panicali J. Michael Hamilton |
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| Affiliation: | (1) Laboratory of Tumor Immunology and Biology, National Cancer Institute, National Institutes of Health, Building 10, Room 8B07, 20892-1750 Bethesda, MD, USA;(2) Therion Biologics Corporation, 76 Rogers Street, 02142 Cambridge, MA, USA;(3) NCI-Navy Oncology Branch, National Institutes of Health, 20892 Bethesda, MD, USA |
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| Abstract: | Summary The development of recombinant vaccines for specific immunotherapy of carcinoma represents a novel approach for the treatment of breast cancer and other tumor types. This article reviews the various parameters that should be considered in the development of recombinant vaccines. Several breast cancer associated antigens are also discussed which may provide potential target molecules. The human carcinoembryonic antigen (CEA), which is expressed on approximately 50% of breast cancers, represents one such target for immunotherapy. To enhance the immunogenicity of this antigen, a recombinant CEA-vaccinia vaccine, designated rV-CEA, was produced. To study the effects of this vaccine in an animal model, a murine colon carcinoma cell line was transduced with CEA and transplanted into immunocompetent mice for protection and therapy studies. Pre-clinical toxicity studies were also conducted in non-human primates. The results of these studies showed the rV-CEA vaccine to be immunogenic and safe in both rodents and primates, and to elicit good anti-tumor responses in the rodent model. In a Phase I clinical trial in metastatic breast, lung, and colorectal cancer patients involving three immunizations of rV-CEA, at three dose levels, enhancement of T-cell and antibody responses to vaccinia virus proteins were observed with no toxicity. Specific T-cell responses were studied via stimulation of peripheral blood lymphocytes with specific peptide epitopes from the CEA molecule. These studies demonstrated clear cut differences in establishment of T-cell lines pre- versus post-immunization. The T-cell lines were shown to be CD8+ and/or CD4+/CD8+, to lyse EBV transformed B-cells transduced with the CEA gene, and to lyse CEA positive carcinoma cells in a HLA restricted manner. Thus, in a Phase I clinical trial the rV-CEA vaccine has been shown to stimulate a CTL response specific for CEA defined epitopes in cancer patients.Presented at the symposium "New Approaches in the Therapy of Breast Cancer", Georgetown University Medical Canter, Washington DC, October 1994, generously supported by an education grant from Bristol-Myers Squibb. |
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| Keywords: | carcinoembryonic antigen (CEA) immunotherapy Phase I trial recombinant vaccines vaccinia virus |
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