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Avidity characterization of genetically engineered T-cells with novel and established approaches

18

Citations

22

References

2016

Year

Abstract

The combination of binding assay with functional assays yields data suggesting that TARP-TCR-engineered T-cells bind to their target, but need more antigen stimulation compared to the pp65-TCR to achieve full effector response. Nonetheless, we believe that the TARP-TCR is an attractive candidate for immunotherapy development for prostate and/or breast cancer.

References

YearCitations

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