Volume 65, Issue 5 pp. 664-670
Experimental Cancer

Intramuscular immunisation with MUC1 cDNA can protect C57 mice challenged with MUC1-expressing syngeneic mouse tumour cells

Rosalind A. Graham

Rosalind A. Graham

Epithelial Cell Biology Laboratory, Imperial Cancer Research Fund, London WC2A 3PX, UK

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Joy M. Burchell

Joy M. Burchell

Epithelial Cell Biology Laboratory, Imperial Cancer Research Fund, London WC2A 3PX, UK

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Peter Beverley

Peter Beverley

Epithelial Cell Biology Laboratory, Imperial Cancer Research Fund, London WC2A 3PX, UK

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Joyce Taylor-Papadimitriou

Corresponding Author

Joyce Taylor-Papadimitriou

Epithelial Cell Biology Laboratory, Imperial Cancer Research Fund, London WC2A 3PX, UK

Epithelial Cell Biology Laboratory, Imperial Cancer Research Fund, 44 Lincoln's Inn Fields, London WC2A 3PX, UKSearch for more papers by this author

Abstract

Much interest is currently being shown in immunotherapy as a treatment for cancer since several tumour-associated antigens have been identified and the genes encoding them cloned. One such molecule is the tumour-associated human MUC1 gene product. In this report we describe tumour rejection studies in a C57BI murine model system with syngeneic MUC1-expressing tumour cells designed to examine the efficacy of MUC1 cDNA as an immunogen. Intra-muscular immunisation with 100 μg MUC1 cDNA 3 times at 3-weekly intervals resulted in tumour protection in approximately 80% of mice. Tumour protection was dose-dependent, with 50–100 μg being the most effective dose. Both humoral and cell-mediated MUC1-specific immune responses were detected. Anti-MUC1 antibodies were detected after immunisation with DNA alone, indicating that the injected DNA was expressed. Humoral immune responses did not correlate with tumour rejection. Tumour challenge with syngeneic tumour cells expressing MUC1 appeared to be a pre-requisite for the generation of MUC1-specific cytotoxic T lymphocytes. © 1996 Wiley-Liss, Inc.

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