Engineered Jurkat Cells for Targeting Prostate-Specific Membrane Antigen on Prostate Cancer Cells by Nanobody-Based Chimeric Antigen Receptor

نویسندگان

  • Arash Arashkia Department of Virology, Pasteur Institute of Iran, Tehran, Iran
  • Fatemeh Hajari Taheri Department of Immunology, Hybridoma Lab, Pasteur Institute of Iran, Tehran, Iran
  • Jamshid Hadjati Department of Immunology, School of Medicine, Tehran University of Medical Sciences, Tehran, Iran
  • Mahmoud Hassani Department of Molecular Medicine, School of Advanced Technologies in Medicine, Tehran University of Medical Sciences, Tehran, Iran
  • Mohammad Hossein Modarressi Department of Molecular Medicine, School of Advanced Technologies in Medicine, Tehran University of Medical Sciences, Tehran, Iran
  • Mohsen Abolhassani Department of Immunology, Hybridoma Lab, Pasteur Institute of Iran, Tehran, Iran
  • Shahriyar Abdoli Department of Virology, Pasteur Institute of Iran, Tehran, Iran
  • Wytske M. van Weerden Department of Urology, Erasmus Medical Center, Rotterdam, Netherlands
  • Zahra Sharifzadeh Department of Immunology, Hybridoma Lab, Pasteur Institute of Iran, Tehran, Iran
چکیده مقاله:

Background: Recently, modification of T cells with chimeric antigen receptor (CAR) has been an attractive approach for adoptive immunotherapy of cancers. Typically, CARs contain a single-chain variable domain fragment (scFv). Most often, scfvs are derived from a monoclonal antibody of murine origin and may be a trigger for host immune system that leads to the T-cell clearance. Nanobody is a specific antigen-binding fragment derived from camelid that has great homology to human VH and low immunogenic potential. Therefore, in this study, nanobody was employed instead of scFv in CAR construct. Methods: In this study, a CAR was constructed based on a nanobody against PSMA (NBPII-CAR). At first, Jurkat cells were electroporated with NBPII-CAR, and then flow cytometry was performed for NBPII-CAR expression. For functional analysis, CAR T cells were co-cultured with prostate cancer cells and analyzed for IL-2 secretion, CD25 expression, and cell proliferation. Results: Flow cytometry results confirmed the expression of NBPII-CAR on the transfected Jurkat cells. Our data showed the specificity of engineered Jurkat cells against prostate cancer cells by not only increasing the IL-2 cytokine (about 370 pg/ml) but also expressing the T-cell activation marker CD25 (about 30%). In addition, proliferation of engineered Jurkat cells increased nearly 60% when co-cultured with LNCaP (PSMA+), as compared with DU145 (PSMA-). Conclusion: Here, we describe the ability of nanobody-based CAR to recognize PSMA that leads to the activation of Jurkat cells. This construct might be used as a promising candidate for clinical applications in prostate cancer therapy.

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عنوان ژورنال

دوره 24  شماره 2

صفحات  81- 88

تاریخ انتشار 2020-03

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