Bispecific CD3/HER2 targeting FynomAb induces redirected t cell-mediated cytolysis with high potency and enhanced tumor selectivity

23Citations
Citations of this article
30Readers
Mendeley users who have this article in their library.

Abstract

CD3 bispecific therapies retargeting T cells to tumors have recently demonstrated striking activity in patients. Several CD3 bispecific antibodies directed against various tumor targets are currently being investigated in the clinic across different tumors. One limitation of these therapies is the risk of target-related toxicity due to low-level expression of tumor antige in normal tissue. In this study we have engineered a bispecific CD3/HER2 FynomAb, COVA420, which redirects T cells with high potency and selectivity to tumor cells with high HER2 expression in vitro and in vivo. COVA420 activity depends on high HER2 density as no activity was observed on cells with lower HER2 levels as found in human normal tissue. These results suggest that COVA420 may spare normal tissue expressing low levels of HER2 while still having uncompromised efficacy on tumor cells with high HER2 expression. This concept may be applied to other cancer antigens that otherwise cannot be targeted by T cell redirecting approaches, and may therefore expand the applicability of CD3 bispecific FynomAbs to a larger number of solid tumors.

Cite

CITATION STYLE

APA

Wuellner, U., Klupsch, K., Buller, F., Attinger-Toller, I., Santimari, R., Zbinden, I., … Brack, S. (2015). Bispecific CD3/HER2 targeting FynomAb induces redirected t cell-mediated cytolysis with high potency and enhanced tumor selectivity. Antibodies, 4(4), 426–440. https://doi.org/10.3390/antib4040426

Register to see more suggestions

Mendeley helps you to discover research relevant for your work.

Already have an account?

Save time finding and organizing research with Mendeley

Sign up for free