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Targeting mutant p53-expressing tumours with a T cell receptor-like antibody specific for a wild-type antigen

Nat Commun.. 2019; 
Low L1, Goh A1, Koh J2, Lim S2, Wang CI3.
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Peptide Synthesis All peptides were synthesized by Genscript USA Inc. at >90% purity and dissolved in dimethyl sulphoxide at 40 mg mL−1 and frozen at −80 °C. The peptides hTERT324–332 and hTERT461–469, WT1235–243, WT1417–425, p53125–134 and p53204–212 were all previously described by various groups as HLA*A24:02-binding peptides17,56,66–68. Get A Quote

摘要

Accumulation of mutant p53 proteins is frequently found in a wide range of cancers. While conventional antibodies fail to target intracellular proteins, proteosomal degradation results in the presentation of p53-derived peptides on the tumour cell surface by class I molecules of the major histocompatibility complex (MHC). Elevated levels of such p53-derived peptide-MHCs on tumour cells potentially differentiate them from healthy tissues. Here, we report the engineering of an affinity-matured human antibody, P1C1TM, specific for the unmutated p53125-134 peptide in complex with the HLA-A24 class I MHC molecule. We show that P1C1TM distinguishes between mutant and wild-type p53 expressing HLA-A24+ cells, and media... More

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