Data from Preclinical Development and Evaluation of Allogeneic CAR T Cells Targeting CD70 for the Treatment of Renal Cell Carcinoma

Adit Ghosh,Barbra J Sasu,Bryan Smith,Dinali Wijewarnasuriya,Hongxiu Ning,Javier Chaparro-Riggers,Jonathan R Heyen,Jonathan Villanueva,Mathilde Dusseaux,Nguyen Tan,Roman Galetto,Shanshan Lang,Siler H Panowski,Silvia K Tacheva-Grigorova,Surabhi Srinivasan,Tao Sai,Thomas Van Blarcom,Yvonne S.L Mak,Zea Melton

doi:10.1158/0008-5472.c.6514085

Abstract

<div>AbstractCD70 is highly expressed in renal cell carcinoma (RCC), with limited expression in normal tissue, making it an attractive CAR T target for an immunogenic solid tumor indication. Here we generated and characterized a panel of anti-CD70 single-chain fragment variable (scFv)–based CAR T cells. Despite the expression of CD70 on T cells, production of CAR T cells from a subset of scFvs with potent in vitro activity was achieved. Expression of CD70 CARs masked CD70 detection in cis and provided protection from CD70 CAR T cell–mediated fratricide. Two distinct classes of CAR T cells were identified with differing memory phenotype, activation status, and cytotoxic activity. Epitope mapping revealed that the two classes of CARs bind unique regions of CD70. CD70 CAR T cells displayed robust antitumor activity against RCC cell lines and patient-derived xenograft mouse models. Tissue cross-reactivity studies identified membrane staining in lymphocytes, thus matching the known expression pattern of CD70. In a cynomolgus monkey CD3-CD70 bispecific toxicity study, expected findings related to T-cell activation and elimination of CD70-expressing cells were observed, including cytokine release and loss of cellularity in lymphoid tissues. Finally, highly functional CD70 allogeneic CAR T cells were produced at large scale through elimination of the T-cell receptor by TALEN-based gene editing. Taken together, these efficacy and safety data support the evaluation of CD70 CAR T cells for the treatment of RCC and has led to the advancement of an allogeneic CD70 CAR T-cell candidate into phase I clinical trials.Significance:These findings demonstrate the efficacy and safety of fratricide-resistant, allogeneic anti-CD70 CAR T cells targeting renal cell carcinoma and the impact of CAR epitope on functional activity.<a href="https://aacrjournals.org/cancerres/article/doi/10.1158/0008-5472.CAN-22-1739" target="_blank">See related commentary by Adotévi and Galaine, p. 2517</a></div>

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