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Beyond CAR T cells: exploring alternative cell sources for CAR-like cellular therapies

Christina Angeliki Tsiverioti, Adrian Gottschlich, Marcel P. Trefny, Sebastian Theurich, Hans‐Joachim Anders, Matthias Kroiß, Sebastian Kobold

2024Biological Chemistry18 citationsDOIOpen Access PDF

Abstract

Chimeric antigen receptor (CAR)-T cell therapy has led to remarkable clinical outcomes in the treatment of hematological malignancies. However, challenges remain, such as limited infiltration into solid tumors, inadequate persistence, systemic toxicities, and manufacturing insufficiencies. The use of alternative cell sources for CAR-based therapies, such as natural killer cells (NK), macrophages (MΦ), invariant Natural Killer T (iNKT) cells, γδT cells, neutrophils, and induced pluripotent stem cells (iPSC), has emerged as a promising avenue. By harnessing these cells' inherent cytotoxic mechanisms and incorporating CAR technology, common CAR-T cell-related limitations can be effectively mitigated. We herein present an overview of the tumoricidal mechanisms, CAR designs, and manufacturing processes of CAR-NK cells, CAR-MΦ, CAR-iNKT cells, CAR-γδT cells, CAR-neutrophils, and iPSC-derived CAR-cells, outlining the advantages, limitations, and potential solutions of these therapeutic strategies.

Topics & Concepts

Chimeric antigen receptorInduced pluripotent stem cellCytotoxic T cellCell therapyCellImmunologyCancer researchImmunotherapyBiologyStem cellImmune systemCell biologyEmbryonic stem cellGeneIn vitroGeneticsBiochemistryCAR-T cell therapy researchImmune Cell Function and Interaction