Litcius/Paper detail

Spleen SORT LNP Generated in situ CAR T Cells Extend Survival in a Mouse Model of Lymphoreplete B Cell Lymphoma

Ester Álvarez‐Benedicto, Zeru Tian, Sumanta Chatterjee, Domenico Orlando, Minjung Kim, Erick Guerrero, Xu Wang, Daniel J. Siegwart

2023Angewandte Chemie International Edition118 citationsDOIOpen Access PDF

Abstract

Chimeric Antigen Receptor (CAR) T cell immunotherapy is revolutionizing treatment for patients suffering from B-cell lymphoma (BL). However, the current method of CAR T cell production is complicated and expensive, requiring collection of patient blood to enrich the T cell population, ex vivo engineering/activation, and quality assessment before the patient can receive the treatment. Herein we leverage Spleen Selective ORgan Targeted (SORT) Lipid Nanoparticles (LNPs) to produce CAR T cells in situ and bypass the extensive and laborious process currently used. Optimized Spleen SORT LNPs containing 10 % 18 : 1 PA transfected CD3+, CD8+, and CD4+ T cells in wild-type mice. Spleen SORT LNPs delivered Cre recombinase mRNA and CAR encoding mRNA to T cells in reporter mice and in a lymphoreplete B cell lymphoma model (respectively) after intravenous injection without the need for active targeting ligands. Moreover, in situ CAR T cells increased the overall survival of mice with a less aggressive form of B cell lymphoma. In addition, in situ transfected CAR T cells reduced tumor metastasis to the liver by increasing tumor infiltrating lymphocytes. Overall, these results offer a promising alternative method for CAR T cell production with pre-clinical potential to treat hematological malignancies.

Topics & Concepts

Chimeric antigen receptorSpleenCD8LymphomaT cellCancer researchImmunologyAntigenBiologyMedicineImmune systemCAR-T cell therapy researchViral Infectious Diseases and Gene Expression in InsectsNanowire Synthesis and Applications