Frontiers in Immunology (Mar 2024)

Efficacy of the induced pluripotent stem cell derived and engineered CD276-targeted CAR-NK cells against human esophageal squamous cell carcinoma

  • Xiaolan Lin,
  • Tian Guan,
  • Tian Guan,
  • Yien Xu,
  • Yun Li,
  • Yun Li,
  • Yanchun Lin,
  • Yanchun Lin,
  • Shaobin Chen,
  • Yuping Chen,
  • Xiaolong Wei,
  • Dongsheng Li,
  • Yukun Cui,
  • Yan Lin,
  • Pingnan Sun,
  • Pingnan Sun,
  • Jianmin Guo,
  • Congzhu Li,
  • Jiang Gu,
  • Wei Yang,
  • Haoyu Zeng,
  • Haoyu Zeng,
  • Haoyu Zeng,
  • Changchun Ma,
  • Changchun Ma,
  • Changchun Ma

DOI
https://doi.org/10.3389/fimmu.2024.1337489
Journal volume & issue
Vol. 15

Abstract

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IntroductionChimeric antigen receptor natural killer (CAR-NK) cells have been found to be successful in treating hematologic malignancies and present potential for usage in solid tumors.MethodsIn this study, we created CD276-targeted CAR-expressing NK cells from pluripotent stem cells (iPSC CD276-targeted CAR-NK cells) and evaluated their cytotoxicity against esophageal squamous cell carcinoma (ESCC) using patient-specific organoid (PSO) models comprising of both CD276-positive and CD276-negative adjacent epithelium PSO models (normal control PSO, NC PSO) as well as primary culture of ESCC cell models. In addition, in vitro and in vivo models such as KYSE-150 were also examined. iPSC NK cells and NK-free media were used as the CAR-free and NK-free controls, respectively.ResultsThe positive CD276 staining was specifically detected on the ESCC membrane in 51.43% (54/105) of the patients of all stages, and in 51.35% (38/74) of stages III and IV. The iPS CD276-targeted CAR-NK cells, comparing with the iPS NK cells and the NK-free medium, exhibited specific and significant cytotoxic activity against CD276-positive ESCC PSO rather than CD276-negative NC PSO, and exhibited significant cytotoxicity against CD276-expressing cultured ESCC cells, as well as against CD276-expressing KYSE-150 in vitro and in BNDG mouse xenograft.DiscussionThe efficacy of the iPSC CD276-targeted CAR-NK cells demonstrated by their successful treatment of CD276-expressing ESCC in a multitude of pre-clinical models implied that they hold tremendous therapeutic potential for treating patients with CD276-expressing ESCC.

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