Literature DB >> 31996390

Antigen Experienced T Cells from Peripheral Blood Recognize p53 Neoantigens.

Parisa Malekzadeh1, Rami Yossef1, Gal Cafri1, Biman C Paria1, Frank J Lowery1, Mohammad Jafferji1, Meghan L Good1, Abraham Sachs1, Amy R Copeland1, Sanghyun P Kim1, Scott Kivitz1, Maria R Parkhurst1, Paul F Robbins1, Satyajit Ray1, Liqiang Xi2, Mark Raffeld2, Zhiya Yu1, Nicholas P Restifo1, Robert P T Somerville1, Steven A Rosenberg3, Drew C Deniger1.   

Abstract

PURPOSE: The purpose of this study was to evaluate antigen experienced T cells in peripheral blood lymphocytes (PBL) for responses to p53 neoantigens. EXPERIMENTAL
DESIGN: PBLs from patients with a mutated TP53 tumor were sorted for antigen-experienced T cells and in vitro stimulation (IVS) was performed with p53 neoantigens. The IVS cultures were stimulated with antigen-presenting cells expressing p53 neoantigens, enriched for 41BB/OX40 and grown with rapid expansion protocol.
RESULTS: T-cell responses were not observed in the PBLs of 4 patients who did not have tumor-infiltrating lymphocyte (TIL) responses to mutated TP53. In contrast, 5 patients with TIL responses to mutated TP53 also had similar T-cell responses in their PBLs, indicating that the PBLs and TILs were congruent in p53 neoantigen reactivity. CD4+ and CD8+ T cells were specific for p53R175H, p53Y220C, or p53R248W neoantigens, including a 78% reactive T-cell culture against p53R175H and HLA-A*02:01. Tracking TCRB clonotypes (clonality, top ranked, and TP53 mutation-specific) supported the enrichment of p53 neoantigen-reactive T cells from PBLs. The same T-cell receptor (TCR) from the TIL was found in the IVS cultures in three cases and multiple unique TCRs were found in another patient. TP53 mutation-specific T cells also recognized tumor cell lines bearing the appropriate human leukocyte antigen restriction element and TP53 mutation, indicating these T cells could recognize processed and presented p53 neoantigens.
CONCLUSIONS: PBL was a noninvasive source of T cells targeting TP53 mutations for cell therapy and can provide a window into intratumoral p53 neoantigen immune responses.See related commentary by Olivera et al., p. 1203. ©2020 American Association for Cancer Research.

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Year:  2020        PMID: 31996390      PMCID: PMC7424598          DOI: 10.1158/1078-0432.CCR-19-1874

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


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