Frontiers in Immunology (Aug 2023)

CD62L as target receptor for specific gene delivery into less differentiated human T lymphocytes

  • Laura Kapitza,
  • Laura Kapitza,
  • Naphang Ho,
  • Thomas Kerzel,
  • Annika M. Frank,
  • Frederic B. Thalheimer,
  • Arezoo Jamali,
  • Thomas Schaser,
  • Christian J. Buchholz,
  • Christian J. Buchholz,
  • Christian J. Buchholz,
  • Jessica Hartmann

DOI
https://doi.org/10.3389/fimmu.2023.1183698
Journal volume & issue
Vol. 14

Abstract

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Chimeric antigen receptor (CAR)-expressing T cells are a complex and heterogeneous gene therapy product with variable phenotype compositions. A higher proportion of less differentiated CAR T cells is usually associated with improved antitumoral function and persistence. We describe in this study a novel receptor-targeted lentiviral vector (LV) named 62L-LV that preferentially transduces less differentiated T cells marked by the L-selectin receptor CD62L, with transduction rates of up to 70% of CD4+ and 50% of CD8+ primary T cells. Remarkably, higher amounts of less differentiated T cells are transduced and preserved upon long-term cultivation using 62L-LV compared to VSV-LV. Interestingly, shed CD62L neither altered the binding of 62L-LV particles to T cells nor impacted their transduction. The incubation of 2 days of activated T lymphocytes with 62L-LV or VSV-LV for only 24 hours was sufficient to generate CAR T cells that controlled tumor growth in a leukemia tumor mouse model. The data proved that potent CAR T cells can be generated by short-term ex vivo exposure of primary cells to LVs. As a first vector type that preferentially transduces less differentiated T lymphocytes, 62L-LV has the potential to circumvent cumbersome selections of T cell subtypes and offers substantial shortening of the CAR T cell manufacturing process.

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