Regression of renal cell carcinoma by T cell receptor-engineered T cells targeting a human endogenous retrovirus

T细胞受体 细胞毒性T细胞 T细胞 CD8型 癌症研究 生物 抗原 异种移植 克隆(Java方法) 移植 分子生物学 免疫学 免疫系统 体外 医学 内科学 遗传学 DNA 生物化学
作者
Stefan Barisic,Elizabeth M. Brahmbhatt,Elena Cherkasova,Timothy T. Spear,Ujjawal Savani,Stéphanie Pierre,Gina Scurti,Long Chen,Muna Igboko,Rosa Nadal,Gang Zeng,Gordon Parry,David F. Stroncek,Steven L. Highfill,Annika V. Dalheim,Robert Reger,Michael I. Nishimura,Richard W. Childs
出处
期刊:Journal for ImmunoTherapy of Cancer [BMJ]
卷期号:12 (9): e009147-e009147 被引量:2
标识
DOI:10.1136/jitc-2024-009147
摘要

Background We discovered a novel human endogenous retrovirus (CT-RCC HERV-E) that was selectively expressed in most clear cell renal cell carcinomas (ccRCC) and served as a source of antigens for T cell-mediated killing. Here, we described the cloning of a novel T cell receptor (TCR) targeting a CT-RCC HERV-E-derived antigen specific to ccRCC and characterized antitumor activity of HERV-E TCR-transduced T cells (HERV-E T cells). Methods We isolated a CD8 + T cell clone from a patient with immune-mediated regression of ccRCC post-allogeneic stem cell transplant that recognized the CT-RCC-1 HERV-E-derived peptide in an HLA-A11-restricted manner. We used 5’Rapid Amplification of cDNA Ends (RACE) to clone the full length HERV-E TCR and generated retrovirus encoding this TCR for transduction of T cells. We characterized HERV-E T cells for phenotype and function in vitro and in a murine xenograft model. Lastly, we implemented a good manufacturing practice-compliant method for scalable production of HERV-E T cells. Results The HLA-A11-restricted HERV-E-reactive TCR exhibited a CD8-dependent phenotype and demonstrated specific recognition of the CT-RCC-1 peptide. CD8 + T cells modified to express HERV-E TCR displayed potent antitumor activity against HLA-A11 + ccRCC cells expressing CT-RCC HERV-E compared with unmodified T cells. Killing by HERV-E T cells was lost when cocultured against HERV-E knockout ccRCC cells. HERV-E T cells induced regression of established ccRCC tumors in a murine model and improved survival of tumor-bearing mice. Large-scale production of HERV-E T cells under good manufacturing practice conditions generated from healthy donors retained specific antigen recognition and cytotoxicity against ccRCC. Conclusions This is the first report showing that human ccRCC cells can be selectively recognized and killed by TCR-engineered T cells targeting a HERV-derived antigen. These preclinical findings provided the foundation for evaluating HERV-E TCR-transduced T cell infusions in patients with metastatic ccRCC in a clinical trial ( NCT03354390 ).
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