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Replacing CAR-T cell resistance with persistence by changing a single residue
Emily M. Hsieh, … , Lauren D. Scherer, Rayne H. Rouce
Emily M. Hsieh, … , Lauren D. Scherer, Rayne H. Rouce
Published May 4, 2020
Citation Information: J Clin Invest. 2020;130(6):2806-2808. https://doi.org/10.1172/JCI136872.
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Commentary

Replacing CAR-T cell resistance with persistence by changing a single residue

Abstract

Sustained persistence of chimeric antigen receptor T (CAR-T) cells is a key characteristic associated with long-term remission in patients with hematologic malignancies. Attempts to uncover mechanisms that enhance persistence and thus functionality will have a substantial impact in broadening application of CAR-T cell therapy, especially for solid tumors. In this issue of the JCI, Guedan et al. describe a promising strategy to limit T cell exhaustion and improve persistence by changing a single amino acid in the costimulatory domain of CD28. The authors demonstrated that this single amino acid substitution in CD28-based mesothelin CAR-T cells results in improved persistence and functionality in a xenograft model of pancreatic cancer. Furthermore, reciprocal alteration of the same residue in inducible costimulator–containing (ICOS-containing) CAR-T cells resulted in limited antitumor activity and persistence. These findings suggest that simple alterations in the costimulatory domain may enhance CAR-T cell persistence, warranting future evaluation in other CD28-costimulatory CARs in an effort to improve durable antitumor effects.

Authors

Emily M. Hsieh, Lauren D. Scherer, Rayne H. Rouce

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