Highly flexible, IgG-shaped, trivalent antibodies effectively target tumor cells and induce T cell-mediated killing

Author:

Dickopf Steffen1,Lauer Matthias E.2,Ringler Philippe3,Spick Christian1,Kern Peter1,Brinkmann Ulrich1

Affiliation:

1. Roche Pharma Research and Early Development, Large Molecule Research, Roche Innovation Center Munich , Nonnenwald 2 , D-82377 Penzberg , Germany

2. Roche Pharma Research and Early Development, Chemical Biology, Roche Innovation Center Basel , Grenzacherstraße 124 , CH-4070 Basel , Switzerland

3. Center for Cellular Imaging and Nano Analytics, Biozentrum University of Basel , Mattenstrasse 26 , CH-4058 Basel , Switzerland

Abstract

Abstract A novel bispecific antibody format was applied to generate T cell-engaging antibodies. The TriFab format is a trivalent IgG-shaped entity composed of two Fab arms that bind to antigens on the surface of tumor cells, which are linked via flexible peptides to a CD3 binding moiety that replaces the CH2 domains of conventional IgGs. The distinctive feature of these T cell recruiting bispecifics is that their CD3 variable regions are incorporated between domains, rather than N- or C-terminally fused to an Fc or antibody fragments. T cell recruiting TriFabs resemble in size and shape, are expressed and show biophysical properties similar to regular IgGs. Transmission electron microscopy (TEM) demonstrates high flexibility of the cell surface binding arms as well as target antigen accessibility of the interspersed CD3 binding domain. Functional co-culturing assays of peripheral blood mononuclear cells (PBMCs) and different tumor cell lines (MCF7 and A431) revealed a dose-dependent T cell-mediated cytotoxicity that was induced by the TriFabs targeting either LeY or EGFR cell surface antigens.

Publisher

Walter de Gruyter GmbH

Subject

Clinical Biochemistry,Molecular Biology,Biochemistry

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