Frontiers in Immunology (Nov 2018)

Efficient and Non-genotoxic RNA-Based Engineering of Human T Cells Using Tumor-Specific T Cell Receptors With Minimal TCR Mispairing

  • Diana Campillo-Davo,
  • Fumihiro Fujiki,
  • Johan M. J. Van den Bergh,
  • Hans De Reu,
  • Evelien L. J. M. Smits,
  • Evelien L. J. M. Smits,
  • Evelien L. J. M. Smits,
  • Herman Goossens,
  • Herman Goossens,
  • Haruo Sugiyama,
  • Eva Lion,
  • Eva Lion,
  • Zwi N. Berneman,
  • Zwi N. Berneman,
  • Zwi N. Berneman,
  • Viggo Van Tendeloo

DOI
https://doi.org/10.3389/fimmu.2018.02503
Journal volume & issue
Vol. 9

Abstract

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Genetic engineering of T cells with tumor specific T-cell receptors (TCR) is a promising strategy to redirect their specificity against cancer cells in adoptive T cell therapy protocols. Most studies are exploiting integrating retro- or lentiviral vectors to permanently introduce the therapeutic TCR, which can pose serious safety issues when treatment-related toxicities would occur. Therefore, we developed a versatile, non-genotoxic transfection method for human unstimulated CD8+ T cells. We describe an optimized double sequential electroporation platform whereby Dicer-substrate small interfering RNAs (DsiRNA) are first introduced to suppress endogenous TCR α and β expression, followed by electroporation with DsiRNA-resistant tumor-specific TCR mRNA. We demonstrate that double sequential electroporation of human primary unstimulated T cells with DsiRNA and TCR mRNA leads to unprecedented levels of transgene TCR expression due to a strongly reduced degree of TCR mispairing. Importantly, superior transgenic TCR expression boosts epitope-specific CD8+ T cell activation and killing activity. Altogether, DsiRNA and TCR mRNA double sequential electroporation is a rapid, non-integrating and highly efficient approach with an enhanced biosafety profile to engineer T cells with antigen-specific TCRs for use in early phase clinical trials.

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