Antigen Presenting Cell Mimetic Lipid Nanoparticles for Rapid mRNA CAR T Cell Cancer Immunotherapy.
Ann E MetzloffMarshall S PadillaNingqiang GongMargaret M BillingsleyXuexiang HanMaria MerolleDavid MaiChristian G Figueroa-EspadaAjay S ThatteRebecca M HaleyAlvin J MukalelAlex G HamiltonMohamad-Gabriel AlamehDrew WeissmanNeil C SheppardCarl H JuneMichael J MitchellPublished in: Advanced materials (Deerfield Beach, Fla.) (2024)
Chimeric antigen receptor (CAR) T cell therapy has achieved remarkable clinical success in the treatment of hematological malignancies. However, producing these bespoke cancer-killing cells is a complicated ex vivo process involving leukapheresis, artificial T cell activation, and CAR construct introduction. The activation step requires the engagement of CD3/TCR and CD28 and is vital for T cell transfection and differentiation. Though antigen-presenting cells (APCs) facilitate activation in vivo, ex vivo activation relies on antibodies against CD3 and CD28 conjugated to magnetic beads. While effective, this artificial activation adds to the complexity of CAR T cell production as the beads must be removed prior to clinical implementation. To overcome this challenge, this work develops activating lipid nanoparticles (aLNPs) that mimic APCs to combine the activation of magnetic beads and the transfection capabilities of LNPs. It is shown that aLNPs enable one-step activation and transfection of primary human T cells with the resulting mRNA CAR T cells reducing tumor burden in a murine xenograft model, validating aLNPs as a promising platform for the rapid production of mRNA CAR T cells.
Keyphrases
- cell therapy
- induced apoptosis
- single cell
- squamous cell carcinoma
- endothelial cells
- signaling pathway
- bone marrow
- high throughput
- fatty acid
- mass spectrometry
- nk cells
- young adults
- quality improvement
- molecularly imprinted
- regulatory t cells
- replacement therapy
- oxide nanoparticles
- loop mediated isothermal amplification