Off-the-shelf invariant NKT cells expressing anti-PSCA CAR and IL-15 promote pancreatic cancer regression in mice
Zhenyu Dai, … , Michael A. Caligiuri, Jianhua Yu
Zhenyu Dai, … , Michael A. Caligiuri, Jianhua Yu
Published April 15, 2025
Citation Information: J Clin Invest. 2025;135(8):e179014. https://doi.org/10.1172/JCI179014.
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Off-the-shelf invariant NKT cells expressing anti-PSCA CAR and IL-15 promote pancreatic cancer regression in mice

Abstract

Pancreatic ductal adenocarcinoma cancer (PDAC) continues to pose a significant health burden, with a 5-year survival rate of only 10%. Prostate stem cell antigen (PSCA) is highly expressed on the surface of tumor cells of most PDAC patients, with minimum expression in most normal tissues. Here, we generated cryopreserved, off-the-shelf, allogeneic PSCA chimeric antigen receptor (CAR) invariant NKT (iNKT) cells using human peripheral blood mononuclear cells as a cell source. In multiple in vitro and in vivo PDAC models, freshly manufactured PSCA CAR_sIL-15 iNKT cells and frozen-thawed, off-the-shelf PSCA CAR_sIL-15 iNKT cells demonstrate comparable efficacies, and both show remarkable suppression of PSCA-positive and gemcitabine-resistant PDAC. Importantly, off-the-shelf cryopreserved PSCA CAR_sIL-15 iNKT cells show equivalent efficacy when compared with PSCA CAR T cells using the same PSCA CAR and in the same PDAC model; however, PSCA CAR_sIL-15 iNKT cells do not appear to induce systemic toxicity or graft-versus-host disease, thus allowing for multiple infusions to control recurrent disease. Collectively, our study suggests that PSCA CAR_sIL-15 iNKT cells merit clinical investigation for PDAC patients exhibiting positive PSCA expression. The therapy could be given as a single agent or in combination with established therapeutic modalities for PDAC.

Authors

Zhenyu Dai, Zheng Zhu, Zhiyao Li, Lei Tian, Kun-Yu Teng, Hanyu Chen, Li-Shu Wang, Jianying Zhang, Laleh Melstrom, Michael A. Caligiuri, Jianhua Yu

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Figure 3

PSCA CAR_sIL-15 iNKT cells demonstrate potent and specific cytotoxicity against human PSCA+ PDAC cell lines in vitro.

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PSCA CAR_sIL-15 iNKT cells demonstrate potent and specific cytotoxicity ...
(A) RTCA results measuring cytotoxicity of sIL-15 iNKT cells and PSCA CAR_sIL-15 iNKT cells against PSCA+ Capan-1, PSCA+ MIA Paca-2, and PSCA+ Aspc-1 or PSCA Panc-1 and PSCA BxPC-3 tumor cells at an E:T ratio of 1:1. Experiments were repeated with 3 donors. (B) Representative microscopic images show the killing as noted in A after 90 hours of coincubation. Experiments were repeated with 3 donors. (C) Freshly isolated human primary NK cells were cultured in the presence of supernatants from nontransduced iNKT (NT supernatant), sIL-15 iNKT, PSCA CAR iNKT, or PSCA CAR_sIL-15 cells for 2 days. Capan-1 cells were labeled with 51Cr and served as target cells. The labeled target cells were added to the cultured NK cells in the presence of respective supernatants for an additional 12 hours. The cytotoxicity levels were measured by 51Cr release assay. n = 4 donors. NT versus PSCA, P = 0.2218; NT versus sIL-15, P < 0.0001; PSCA versus PSCA CAR sIL-15, P < 0.0001; PSCA versus sIL-15, P < 0.0001; sIL-15 versus PSCA s15, P = 0.1157. Statistical analyses were performed by 1-way ANOVA with P values corrected for multiple comparisons by Bonferroni’s method.