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Sleeping Beauty (SB) transposon, a type of nonviral integrative vectors, provides an alternative to modify primary T cells. Creative biolabs has developed SB transposon CAR vector pSBCAR1 CD20 (1F5) h(BBζ), which is constructed for the engineering of T cells to target human CD20. The T cells are genetically modified through transduction with a nonviral vector expressing scFv of anti-CD20 antibody linked to 4-1BB and CD3ζ signaling domains. And the vector product was designed for the treatment of Acute lymphoblastic leukemia (ALL).
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CAR Construction : 1F5-CD28-41BB-CD3ζ
Fig.1 Transduced T cells exhibit CD20-specific cytolytic activity in vitro. iC9-CD20CAR-Δ19 T cells transduced with CD20-CAR (CD20-CAR T), or non-transduced (mock) T cells were co-cultured with EL4, Daudi, and Granta in various effector to target (E:T) ratios. Budde L E, Berger C, Lin Y, et al. Combining a CD20 chimeric antigen receptor and an inducible caspase 9 suicide switch to improve the efficacy and safety of T cell adoptive immunotherapy for lymphoma[J]. PloS one, 2013, 8(12): e82742. |
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CAR Construction : 1F5-CD28-41BB-CD3ζ
Fig.2 Anti-tumor effect of the transduced T cells. Mock or iC9-CD20CAR-Δ19 transduced T cells were co-cultured with CD20+ Ramos cells in various Effector to Target ratios (E:T) for 48 hours. Cells were then stained with antibodies recognizing CD22 and CD3. Flow cytometric analysis was used to determine the presence of Ramos cells (CD22+CD3-) and T cells (CD22-CD3+). Budde L E, Berger C, Lin Y, et al. Combining a CD20 chimeric antigen receptor and an inducible caspase 9 suicide switch to improve the efficacy and safety of T cell adoptive immunotherapy for lymphoma[J]. PloS one, 2013, 8(12): e82743. |
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CAR Construction : 1F5-CD28-41BB-CD3ζ
Fig.3 Cytokine production. Expanded T cells secreted IL2, IFN-γ and TNF-α after co-culture with CD20-expressing Ramos target cells for 48 hours. Budde L E, Berger C, Lin Y, et al. Combining a CD20 chimeric antigen receptor and an inducible caspase 9 suicide switch to improve the efficacy and safety of T cell adoptive immunotherapy for lymphoma[J]. PloS one, 2013, 8(12): e82744. |
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CAR Construction : 1F5-CD28-41BB-CD3ζ
Fig.4 Anti-tumor activity of transduced T cells in vivo. Eradication of CD20+ Raji tumors in NOD-SCID mice by CD20-CAR T cells but not non-transduced T cells (Mock T) as measured by in vivo bioluminescent imaging. Budde L E, Berger C, Lin Y, et al. Combining a CD20 chimeric antigen receptor and an inducible caspase 9 suicide switch to improve the efficacy and safety of T cell adoptive immunotherapy for lymphoma[J]. PloS one, 2013, 8(12): e82745. |
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CAR Construction : 1F5-CD28-41BB-CD3ζ
Fig.5 Anti-tumor activity of transduced T cells in vivo. Kaplan-Meier survival curves of mice receiving iC9-CD20CAR-Δ19 T treatment (CD20-CAR T) or non-transduced mock T cell treatment (NT). Budde L E, Berger C, Lin Y, et al. Combining a CD20 chimeric antigen receptor and an inducible caspase 9 suicide switch to improve the efficacy and safety of T cell adoptive immunotherapy for lymphoma[J]. PloS one, 2013, 8(12): e82746. |
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CAR Construction :
Fig.6 CD20 binding assay. Binding of 1F5-IgG1 or 1F5-IgA2 and respective control antibodies to human CD20 transfected CHO-K1 cells was analysed by indirect immunofluorescence using a fluorescein isothicyanate (FITC)-labelled human jlight chain antibody. Lohse S, Loew S, Kretschmer A, et al. Effector mechanisms of IgA antibodies against CD20 include recruitment of myeloid cells for antibody-dependent cell-mediated cytotoxicity and complement-dependent cytotoxicity[J]. British journal of haematology, 2018, 181(3): 413-417. |
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CAR Construction :
Fig.7 Binding activity of 1F5 scFv-Ig compared with 1F5. A total of 10^5 Ramos cells were incubated with various concentrations of 1F5 scFv-Ig (GS1) or 1F5, followed by incubation with a peroxidase-conjugated GAH or GAM secondary Ab. Shan, D., Press, O. W., Tsu, T. T., Hayden, M. S., & Ledbetter, J. A. (1999). Characterization of scFv-Ig constructs generated from the anti-CD20 mAb 1F5 using linker peptides of varying lengths. The Journal of Immunology, 162(11), 6589-6595. |
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