Figure 1
Figure 1. VST manufacturing strategies. Donor blood is drawn and PBMCs are then manipulated using different approaches for the manufacture of VSTs for clinical use. (A) Direct selection utilizes either: (1) multimers specific for a virus-derived peptide in the setting of a class-I HLA molecule, or (2) column selection where T cells are stimulated with viral antigen followed by selection of IFN-γ or CD154–expressing T cells using antibody coated immunomagnetic beads. (B) Ex vivo T-cell expansion requires the in vitro stimulation and expansion of T cells using APCs pulsed, infected, or transfected with viral peptide(s)/protein(s), viral lysate, or viral vectors/plasmids, respectively. (C) Genetic modification requires the gene transfer of high affinity VST receptors or chimeric-antigen receptors to redirect specificity of T cells to viral targets. CAR, chimeric antigen receptor.

VST manufacturing strategies. Donor blood is drawn and PBMCs are then manipulated using different approaches for the manufacture of VSTs for clinical use. (A) Direct selection utilizes either: (1) multimers specific for a virus-derived peptide in the setting of a class-I HLA molecule, or (2) column selection where T cells are stimulated with viral antigen followed by selection of IFN-γ or CD154–expressing T cells using antibody coated immunomagnetic beads. (B) Ex vivo T-cell expansion requires the in vitro stimulation and expansion of T cells using APCs pulsed, infected, or transfected with viral peptide(s)/protein(s), viral lysate, or viral vectors/plasmids, respectively. (C) Genetic modification requires the gene transfer of high affinity VST receptors or chimeric-antigen receptors to redirect specificity of T cells to viral targets. CAR, chimeric antigen receptor.

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