OncoImmunology (Dec 2022)

Trogocytosis and fratricide killing impede MSLN-directed CAR T cell functionality

  • Esther Schoutrop,
  • Stefanie Renken,
  • Isabella Micallef Nilsson,
  • Paula Hahn,
  • Thomas Poiret,
  • Rolf Kiessling,
  • Stina L Wickström,
  • Jonas Mattsson,
  • Isabelle Magalhaes

DOI
https://doi.org/10.1080/2162402X.2022.2093426
Journal volume & issue
Vol. 11, no. 1

Abstract

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Successful translation of chimeric antigen receptor (CAR) T cell therapy for the treatment of solid tumors has proved to be troublesome, mainly due to the complex tumor microenvironment promoting T cell dysfunction and antigen heterogeneity. Mesothelin (MSLN) has emerged as an attractive target for CAR T cell therapy of several solid malignancies, including ovarian cancer. To improve clinical response rates with MSLN-CAR T cells, a better understanding of the mechanisms impacting CAR T cell functionality in vitro is crucial. Here, we demonstrated superior cytolytic capacity of CD28-costimulated MSLN-CAR T cells (M28z) relative to 4–1BB-costimulated MSLN-CAR T cells (MBBz). Furthermore, CD28-costimulated MSLN CAR T cells displayed enhanced cytolytic capacity against tumor spheroids with heterogeneous MSLN expression compared to MBBz CAR T cells. In this study, we identified CAR-mediated trogocytosis as a potential impeding factor for successful MSLN-CAR T cell therapy due to fratricide killing and contributing to tumor antigen heterogeneity. Moreover, we link antigen-dependent upregulation of LAG-3 with reduced CAR T cell functionality. Taken together, our study highlights the therapeutic potential and bottlenecks of MSLN-CAR T cells, providing a rationale for combinatorial treatment strategies.

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