Litcius/Paper detail

Dendritic cell-mimicking scaffolds for ex vivo T cell expansion

Hye Sung Kim, Tzu‐Chieh Ho, Moshe J. Willner, Michael W. Becker, Hae‐Won Kim, Kam W. Leong

2022Bioactive Materials22 citationsDOIOpen Access PDF

Abstract

We propose an ex vivo T cell expansion system that mimics natural antigen-presenting cells (APCs) for adoptive cell therapy (ACT). Microfiber scaffolds coated with dendritic cell (DC) membrane replicate physicochemical properties of dendritic cells specific for T cell activation such as rapid recognition by T cells, long duration of T cell tethering, and DC-specific co-stimulatory cues. The DC membrane-coated scaffold is first surface-immobilized with T cell stimulatory ligands, anti-CD3 (αCD3) and anti-CD28 (αCD28) antibodies, followed by adsorption of releasable interleukin-2 (IL-2). The scaffolds present both surface and soluble cues to T cells ex vivo in the same way that these cues are presented by natural APCs in vivo. We demonstrate that the DC-mimicking scaffold promotes greater polyclonal expansion of primary human T cells as compared to αCD3/αCD28-functionalized Dynabead. More importantly, major histocompatibility complex molecules derived from the DC membrane of the scaffold allow antigen-specific T cell expansion with target cell-specific killing ability. In addition, most of the expanded T cells (∼97%) can be harvested from the scaffold by density gradient centrifugation. Overall, the DC-mimicking scaffold offers a scalable, modular, and customizable platform for rapid expansion of highly functional T cells for ACT.

Topics & Concepts

CD28T cellCell biologyChemistryEx vivoAntigen-presenting cellScaffoldDendritic cellAntigenIn vitroImmunologyBiologyImmune systemBiomedical engineeringBiochemistryMedicineCAR-T cell therapy researchImmunotherapy and Immune ResponsesImmune Cell Function and Interaction