Frontiers in Oncology (Jan 2022)

Development of a Novel Anti-CD19 CAR Containing a Fully Human scFv and Three Costimulatory Domains

  • Yupanun Wutti-in,
  • Yupanun Wutti-in,
  • Jatuporn Sujjitjoon,
  • Jatuporn Sujjitjoon,
  • Nunghathai Sawasdee,
  • Nunghathai Sawasdee,
  • Aussara Panya,
  • Aussara Panya,
  • Katesara Kongkla,
  • Katesara Kongkla,
  • Pornpimon Yuti,
  • Pornpimon Yuti,
  • Petlada Yongpitakwattana,
  • Petlada Yongpitakwattana,
  • Chutamas Thepmalee,
  • Chutamas Thepmalee,
  • Mutita Junking,
  • Mutita Junking,
  • Thaweesak Chieochansin,
  • Thaweesak Chieochansin,
  • Naravat Poungvarin,
  • Montarop Yamabhai,
  • Pa-thai Yenchitsomanus,
  • Pa-thai Yenchitsomanus

DOI
https://doi.org/10.3389/fonc.2021.802876
Journal volume & issue
Vol. 11

Abstract

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Second-generation anti-CD19-chimeric antigen receptor T cells (anti-CD19-CAR2 T cells) are effective for treating B-cell malignancies; however, anti-CD19-CAR2 T cells can induce human anti-mouse immune responses because anti-CD19 single-chain variable fragment (scFv) in the CAR molecules is derived from a murine FMC63 (mFMC63) monoclonal antibody. Consequently, the persistence of mFMC63-CAR2 T cells and their therapeutic efficiency in patients are decreased, which results in tumor relapse. In an attempt to remedy this shortcoming, we generated a new anti-CD19-CAR T cells containing fully human anti-CD19 scFv (Hu1E7-CAR4 T cells) to pre-clinically evaluate and compare with mFMC63-CAR4 T cells. The human anti-CD19 scFv (Hu1E7) was isolated from a human scFv phage display library and fused to the hinge region of CD8α, the transmembrane domain of CD28, three intracellular costimulatory domains (CD28, 4-1BB, and CD27), and a CD3ζ signaling domain (28BB27ζ). Compared to mFMC63-CAR2 T cells (BBζ) and mFMC63-CAR3 (BB27ζ), the mFMC63-CAR4 T cells (28BB27ζ) exerted superior anti-tumor activity against Raji (CD19+) target cell. The Hu1E7-CAR4 and mFMC63-CAR4 T cells demonstrated comparable cytotoxicity and proliferation. Interestingly, compared to mFMC63-CAR4 T cells, the Hu1E7-CAR4 T cells secreted lower levels of cytokines (IFN-γ and TNF-α), which may be due to the lower binding affinity of Hu1E7-CAR4 T cells. These findings demonstrated the successfulness in creation of a new CAR T cells containing a novel fully human-derived scFv specific to CD19+ cancer cells. In vivo studies are needed to further compare the anti-tumor efficacy and safety of Hu1E7-CAR4 T cells and mFMC63-CAR4 T cells.

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