| Literature DB >> 28062646 |
Simon Krah1,2, Christian Schröter1,2, Carla Eller1, Laura Rhiel2, Nicolas Rasche2, Jan Beck1, Carolin Sellmann1,2, Ralf Günther2, Lars Toleikis2, Björn Hock2, Harald Kolmar1, Stefan Becker2.
Abstract
Bispecific antibodies (bsAbs) pave the way for novel therapeutic modes of action along with potential benefits in several clinical applications. However, their generation remains challenging due to the necessity of correct pairings of two different heavy and light chains and related manufacturability issues. We describe a generic approach for the generation of fully human IgG-like bsAbs. For this, heavy chain repertoires from immunized transgenic rats were combined with either a randomly chosen common light chain or a light chain of an existing therapeutic antibody and screened for binders against tumor-related targets CEACAM5 and CEACAM6 by yeast surface display. bsAbs with subnanomolar affinities were identified, wherein each separate binding arm mediated specific binding to the respective antigen. Altogether, the described strategy represents a combination of in vivo immunization with an in vitro selection method, which allows for the integration of existing therapeutic antibodies into a bispecific format.Entities:
Keywords: antibody; bispecific antibody; common light chain; high-throughput screening; yeast surface display
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Year: 2017 PMID: 28062646 DOI: 10.1093/protein/gzw077
Source DB: PubMed Journal: Protein Eng Des Sel ISSN: 1741-0126 Impact factor: 1.650