Recombinant Mouse Antibody binds selectively to Mouse CD3E.
Figure 1 Concanavalin A expanded γδ T cells staining
Concanavalin A expanded γδ T cells were stained with UCHT1, Fab, Fabred, or left untreated, followed by an APC-labeled anti-mouse IgG antibody as a secondary reagent. Fluorescence intensities were quantified by flow cytometry (n > 3).
Juraske, C., Wipa, P., Morath, A., Hidalgo, J. V., Hartl, F. A., Raute, K., ... & Pongcharoen, S. (2018). Anti-CD3 Fab fragments enhance tumor killing by human γδ T cells independent of Nck recruitment to the γδ T cell antigen receptor. Frontiers in immunogy, 9, 1579.
Figure 2 Close proximity between the TCR and Nck was detected by in situ PLA.
Zoledronate-expanded γδ T cells were either left untreated (−) or treated with 5 µg/ml UCHT1 in the absence or presence of 10 nM AX-024 at 37°C for 5 min. After fixation and permeabilization, PLA was performed using the primary antibodies goat anti-CD3ε (M20) and rabbit anti-Nck1, and the corresponding secondary antibodies. Nuclei were stained with DAPI.
Juraske, C., Wipa, P., Morath, A., Hidalgo, J. V., Hartl, F. A., Raute, K., ... & Pongcharoen, S. (2018). Anti-CD3 Fab fragments enhance tumor killing by human γδ T cells independent of Nck recruitment to the γδ T cell antigen receptor. Frontiers in immunogy, 9, 1579.
Figure 3 UCHT1 increased tumor killing by γδ T cells.
51Cr-labeled Daudi and Raji cells were incubated with zoledronate-expanded human γδ T cells without (−) or with the addition of 5 µg/ml UCHT1 using an effector to target (T cell to tumor cell) ratio of 12.5:1.
Juraske, C., Wipa, P., Morath, A., Hidalgo, J. V., Hartl, F. A., Raute, K., ... & Pongcharoen, S. (2018). Anti-CD3 Fab fragments enhance tumor killing by human γδ T cells independent of Nck recruitment to the γδ T cell antigen receptor. Frontiers in immunology, 9, 1579.
Figure 4 Using its SH3.1(Nck) domain Nck binds to the UCHT1-stimulated γδ T cell antigen receptor (TCR).
Zoledronate-expanded γδ T cells were left untreated (−) or stimulated with 5 µg/ml UCHT1 at 37°C for 5 min
Juraske, C., Wipa, P., Morath, A., Hidalgo, J. V., Hartl, F. A., Raute, K., ... & Pongcharoen, S. (2018). Anti-CD3 Fab fragments enhance tumor killing by human γδ T cells independent of Nck recruitment to the γδ T cell antigen receptor. Frontiers in immunology, 9, 1579.
Figure 5 Preparation of UCHT1 Fab fragments.
The anti-CD3ε antibody UCHT1 was digested with papain using a kit from Thermo Fisher Scientific. The Fab fragments were purified with protein A coupled beads.
Juraske, C., Wipa, P., Morath, A., Hidalgo, J. V., Hartl, F. A., Raute, K., ... & Pongcharoen, S. (2018). Anti-CD3 Fab fragments enhance tumor killing by human γδ T cells independent of Nck recruitment to the γδ T cell antigen receptor. Frontiers in immunogy, 9, 1579.
Figure 6 Fab and Fabred fragments enhanced tumor killing by γδ T cells.
51Cr-labeled Daudi and Raji cells were incubated with zoledronate or with 5 µg/ml UCHT1, 3.33 µg/ml Fab, or 3.33 µg/ml Fabred (these concentrations were chosen to obtain equimolar amounts of the different reagents). The effector to target ratio was 12.5:1.
Juraske, C., Wipa, P., Morath, A., Hidalgo, J. V., Hartl, F. A., Raute, K., ... & Pongcharoen, S. (2018). Anti-CD3 Fab fragments enhance tumor killing by human γδ T cells independent of Nck recruitment to the γδ T cell antigen receptor. Frontiers in immunogy, 9, 1579.
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CAT | Product Name | Application | Type |
---|---|---|---|
TAB-H28 | Anti-Human CD3E Recombinant Antibody (Ertumaxomab) | ELISA, FC, IP, FuncS, IF, Neut, ICC | IgG2a / G2b |
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(Creative Biolabs Cat# DrMAB-989, RRID: AB_3111289)
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For research use only. Not intended for any clinical use. No products from Creative Biolabs may be resold, modified for resale or used to manufacture commercial products without prior written approval from Creative Biolabs.
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