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Development of a T-cell Receptor Mimic Antibody Against Wild-Type P53 for Cancer Immunotherapy

Overview
Journal Cancer Res
Specialty Oncology
Date 2017 Apr 2
PMID 28363997
Citations 21
Authors
Demin Li
Carol Bentley
Amanda Anderson
Sarah Wiblin
Kirstie L S Cleary
Sofia Koustoulidou
Tasneem Hassanali
Jenna Yates
Jenny Greig
Marloes Olde Nordkamp
Iva Trenevska
Nicola Ternette
Benedikt M Kessler
Bart Cornelissen
Mark S Cragg
Alison H Banham
Affiliations
Soon will be listed here.
Abstract

The tumor suppressor p53 is widely dysregulated in cancer and represents an attractive target for immunotherapy. Because of its intracellular localization, p53 is inaccessible to classical therapeutic monoclonal antibodies, an increasingly successful class of anticancer drugs. However, peptides derived from intracellular antigens are presented on the cell surface in the context of MHC I and can be bound by T-cell receptors (TCR). Here, we report the development of a novel antibody, T1-116C, that acts as a TCR mimic to recognize an HLA-A*0201-presented wild-type p53 T-cell epitope, p53(RMPEAAPPV). The antibody recognizes a wide range of cancers, does not bind normal peripheral blood mononuclear cells, and can activate immune effector functions to kill cancer cells , the antibody targets p53 peptide-expressing breast cancer xenografts, significantly inhibiting tumor growth. This represents a promising new agent for future cancer immunotherapy. .

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