| Literature DB >> 27694443 |
Carolin Sellmann1,2, Achim Doerner2, Christine Knuehl3, Nicolas Rasche2, Vanita Sood4, Simon Krah1,2, Laura Rhiel2, Annika Messemer1, John Wesolowski4, Mark Schuette2, Stefan Becker2, Lars Toleikis2, Harald Kolmar5, Bjoern Hock6.
Abstract
Bispecific antibodies (bsAbs) and antibody-drug conjugates (ADCs) have already demonstrated benefits for the treatment of cancer in several clinical studies, showing improved drug selectivity and efficacy. In particular, simultaneous targeting of prominent cancer antigens, such as EGF receptor (EGFR) and c-MET, by bsAbs has raised increasing interest for potentially circumventing receptor cross-talk and c-MET-mediated acquired resistance during anti-EGFR monotherapy. In this study, we combined the selectivity of EGFR × c-MET bsAbs with the potency of cytotoxic agents via bispecific antibody-toxin conjugation. Affinity-attenuated bispecific EGFR × c-MET antibody-drug conjugates demonstrated high in vitro selectivity toward tumor cells overexpressing both antigens and potent anti-tumor efficacy. Due to basal EGFR expression in the skin, ADCs targeting EGFR in general warrant early safety assessments. Reduction in EGFR affinity led to decreased toxicity in keratinocytes. Thus, the combination of bsAb affinity engineering with the concept of toxin conjugation may be a viable route to improve the safety profile of ADCs targeting ubiquitously expressed antigens.Entities:
Keywords: antibody engineering; anticancer drug; epidermal growth factor receptor (EGFR); sortase A; toxicity
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Year: 2016 PMID: 27694443 PMCID: PMC5122778 DOI: 10.1074/jbc.M116.753491
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157