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Integration of ζ-deficient CARs into theCD3-zetagene conveys potent cytotoxicity in T and NK cells

细胞毒性 Zeta电位 生物 基因技术 基因 化学 CD3型 细胞生物学 分子生物学 免疫学 纳米技术 体外 抗原 生物化学 生物技术 CD8型 材料科学 纳米颗粒
作者
Jonas Kath,Clemens Franke,Vanessa Drosdek,Weijie Du,Viktor Glaser,Carla Fuster‐García,Maik Stein,Tatiana Zittel,Sarah Schulenberg,Caroline E. Porter,Lena Andersch,Annette Künkele,Joshua Alcaniz,Jens Hoffmann,Hinrich Abken,Mohamed Abou‐El‐Enein,Axel Pruß,Masataka Suzuki,Toni Cathomen,Renata Stripecke,Hans‐Dieter Volk,Petra Reinke,Michael Schmueck‐Henneresse,Dimitrios L. Wagner
标识
DOI:10.1101/2023.11.10.565518
摘要

I. Abstract Chimeric antigen receptor (CAR)-reprogrammed immune cells hold significant therapeutic potential for oncology, autoimmune diseases, transplant medicine, and infections. All approved CAR-T therapies rely on personalized manufacturing using undirected viral gene transfer, which results in non-physiological regulation of CAR-signaling and limits their accessibility due to logistical challenges, high costs and biosafety requirements. Here, we propose a novel approach utilizing CRISPR-Cas gene editing to redirect T cells and natural killer (NK) cells with CARs. By transferring shorter, truncated CAR-transgenes lacking a main activation domain into the human CD3 ζ (CD247) gene, functional CAR fusion-genes are generated that exploit the endogenous CD3 ζ gene as the CAR’s activation domain. Repurposing this T/NK-cell lineage gene facilitated physiological regulation of CAR-expression and reprogramming of various immune cell types, including conventional T cells, TCRγ/δ T cells, regulatory T cells, and NK cells. In T cells, CD3 ζ in-frame fusion eliminated TCR surface expression, reducing the risk of graft-versus-host disease in allogeneic off-the-shelf settings. CD3 ζ-CD19-CAR-T cells exhibited comparable leukemia control to T cell receptor alpha constant ( TRAC )-replaced and lentivirus-transduced CAR-T cells in vivo . Tuning of CD3 ζ-CAR-expression levels significantly improved the in vivo efficacy. Compared to TRAC -edited CAR-T cells, integration of a Her2-CAR into CD3 ζ conveyed similar in vitro tumor lysis but reduced susceptibility to activation-induced cell death and differentiation, presumably due to lower CAR-expression levels. Notably, CD3 ζ gene editing enabled reprogramming of NK cells without impairing their canonical functions. Thus, CD3 ζ gene editing is a promising platform for the development of allogeneic off-the-shelf cell therapies using redirected killer lymphocytes. Key points Integration of ζ-deficient CARs into CD3 ζ gene allows generation of functional TCR-ablated CAR-T cells for allogeneic off-the-shelf use CD3 ζ-editing platform allows CAR reprogramming of NK cells without affecting their canonical functions
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