Neoantigen-specific stimulation of tumor-infiltrating lymphocytes enables effective TCR isolation and expansion while preserving stem-like memory phenotypes

表型 T细胞受体 癌症研究 T细胞 分离(微生物学) 医学 刺激 干细胞 生物 免疫学 生物信息学 细胞生物学 免疫系统 遗传学 基因 神经科学
作者
Noam Levin,Sanghyun P. Kim,Charles Marquardt,Nolan R. Vale,Zhiya Yu,Sivasish Sindiri,Jared J. Gartner,Maria R. Parkhurst,Sri Krishna,Frank J. Lowery,Nikolaos Zacharakis,L Lévy,Todd D. Prickett,Tiffany Benzine,Satyajit Ray,Robert V. Masi,Billel Gasmi,Yong Li,M. Rafiqul Islam,Alakesh Bera
出处
期刊:Journal for ImmunoTherapy of Cancer [BMJ]
卷期号:12 (5): e008645-e008645 被引量:12
标识
DOI:10.1136/jitc-2023-008645
摘要

Background Tumor-infiltrating lymphocytes (TILs) targeting neoantigens can effectively treat a selected set of metastatic solid cancers. However, harnessing TILs for cancer treatments remains challenging because neoantigen-reactive T cells are often rare and exhausted, and ex vivo expansion can further reduce their frequencies. This complicates the identification of neoantigen-reactive T-cell receptors (TCRs) and the development of TIL products with high reactivity for patient treatment. Methods We tested whether TILs could be in vitro stimulated against neoantigens to achieve selective expansion of neoantigen-reactive TILs. Given their prevalence, mutant p53 or RAS were studied as models of human neoantigens. An in vitro stimulation method, termed “NeoExpand”, was developed to provide neoantigen-specific stimulation to TILs. 25 consecutive patient TILs from tumors harboring p53 or RAS mutations were subjected to NeoExpand. Results We show that neoantigenic stimulation achieved selective expansion of neoantigen-reactive TILs and broadened the neoantigen-reactive CD4 + and CD8 + TIL clonal repertoire. This allowed the effective isolation of novel neoantigen-reactive TCRs. Out of the 25 consecutive TIL samples, neoantigenic stimulation enabled the identification of 16 unique reactivities and 42 TCRs, while conventional TIL expansion identified 9 reactivities and 14 TCRs. Single-cell transcriptome analysis revealed that neoantigenic stimulation increased neoantigen-reactive TILs with stem-like memory phenotypes expressing IL-7R, CD62L, and KLF2. Furthermore, neoantigenic stimulation improved the in vivo antitumor efficacy of TILs relative to the conventional OKT3-induced rapid TIL expansion in p53-mutated or KRAS-mutated xenograft mouse models. Conclusions Taken together, neoantigenic stimulation of TILs selectively expands neoantigen-reactive TILs by frequencies and by their clonal repertoire. NeoExpand led to improved phenotypes and functions of neoantigen-reactive TILs. Our data warrant its clinical evaluation. Trial registration number NCT00068003 , NCT01174121 , and NCT03412877 .

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