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Anti-p53-directed immunotherapy of malignant disease

Published online by Cambridge University Press:  13 February 2004

Matthias Theobald
Affiliation:
Department of Hematology and Oncology, Johannes Gutenberg-University, 55101 Mainz, Germany.
Rienk Offringa
Affiliation:
Tumor Immunology Group, Department of Immunohematology and Bloodtransfusion, Leiden University Medical Center, 2300 ZA Leiden, The Netherlands.

Abstract

Mutation and aberrant expression of the p53 tumour suppressor protein are the most frequent molecular alterations in human malignancy. Peptides derived from the p53 protein and presented by major histocompatibility complex molecules for T-cell recognition could serve as universal tumour-associated antigens for cancer immunotherapy. Because p53 normally functions as a ubiquitously expressed self-protein, controlling cell-cycle progression and apoptosis, it also represents a paradigm target molecule for tumour-reactive yet self-antigen-specific T cells. Tailoring p53-based cancer immunotherapy thus requires both interference with p53-specific self-tolerance and induction of the entire repertoire of p53-reactive T cells. Transferring selected T-cell receptor genes into human T cells offers a novel and appealing strategy to meet these requirements.

Type
Review Article
Copyright
© Cambridge University Press 2003

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