Identification of Functional HLA-A∗01:01-Restricted Epstein-Barr Latent Membrane Protein 2-Specific T-Cell Receptors

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Abstract

Background: Adoptive transfer of genetically engineered T cells expressing antigen-specific T-cell receptors (TCRs) is an appealing therapeutic approach for Epstein-Barr virus (EBV)-associated malignancies of latency type II/III that express EBV antigens (LMP1/2). Patients who are HLA-A∗01:01 positive could benefit from such products, since no T cells recognizing any EBV-derived peptide in this common HLA allele have been found thus far. Methods: HLA-A∗01:01-restricted EBV-LMP2-specific T cells were isolated using peptide major histocompatibility complex (pMHC) tetramers. Functionality was assessed by production of interferon gamma (IFN-γ) and cytotoxicity when stimulated with EBV-LMP2-expressing cell lines. Functionality of primary T cells transduced with HLA-A∗01:01-restricted EBV-LMP2-specific TCRs was optimized by knocking out the endogenous TCRs of primary T cells (ΔTCR) using CRISPR-Cas9 technology. Results: EBV-LMP2-specific T cells were successfully isolated and their TCRs were characterized. TCR gene transfer in primary T cells resulted in specific pMHC tetramer binding and reactivity against EBV-LMP2-expressing cell lines. The mean fluorescence intensity of pMHC-tetramer binding was increased 1.5-2 fold when the endogenous TCRs of CD8+ T cells was knocked out. CD8+/ΔTCR T cells modified to express EBV-LMP2-specific TCRs showed IFN-γsecretion and cytotoxicity toward EBV-LMP2-expressing malignant cell lines. Conclusions: We isolated the first functional HLA-A∗01:01-restricted EBV-LMP2-specific T-cell populations and TCRs, which can potentially be used in future TCR gene therapy to treat EBV-associated latency type II/III malignancies.

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APA

Huisman, W., Gille, I., Van Der Maarel, L. E., Hageman, L., Morton, L. T., De Jong, R. C. M., … Jedema, I. (2022). Identification of Functional HLA-A∗01:01-Restricted Epstein-Barr Latent Membrane Protein 2-Specific T-Cell Receptors. Journal of Infectious Diseases, 226(5), 833–842. https://doi.org/10.1093/infdis/jiaa512

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