Directed evolution-based discovery of ligands for in vivo restimulation of CAR-T cells

嵌合抗原受体 癌症研究 T细胞 CD19 体内 白血病 抗原 免疫学 化学 生物 免疫系统 生物技术
作者
Tomasz M. Grzywa,Alexandra Neeser,Ranjani Ramasubramanian,Anna Romanov,Ryan Tannir,Naveen K. Mehta,Benjamin Cossette,Duncan M. Morgan,Beatriz Gonçalves,Ina Sukaj,Elisa Bergaggio,Stephan Kadauke,Regina M. Myers,Luca Paruzzo,Guido Ghilardi,Aj Cozzone,Stephen J. Schuster,Norbert Frey,Libin Zhang,Parisa Yousefpour
标识
DOI:10.1101/2024.04.16.589780
摘要

Chimeric antigen receptor (CAR) T cell therapy targeting CD19 elicits remarkable clinical efficacy in B-cell malignancies, but many patients relapse due to failed expansion and/or progressive loss of CAR-T cells. We recently reported a strategy to potently restimulate CAR-T cells in vivo, enhancing their functionality by administration of a vaccine-like stimulus comprised of surrogate peptide ligands for a CAR linked to a lymph node-targeting amphiphilic PEG-lipid (termed CAR-T-vax). Here, we demonstrate a general strategy to generate and optimize peptide mimotopes enabling CAR-T-vax generation for any CAR. Using the clinical CD19 CAR FMC63 as a test case, we employed yeast surface display to identify peptide binders to soluble IgG versions of FMC63, which were subsequently affinity matured by directed evolution. CAR-T vaccines using these optimized mimotopes triggered marked expansion of both murine CD19 CAR-T cells in a syngeneic model and human CAR-T cells in a humanized mouse model of B cell acute lymphoblastic leukemia (B-ALL), and enhanced control of leukemia progression. This approach thus enables vaccine boosting to be applied to any clinically-relevant CAR-T cell product.
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