| Literature DB >> 31526159 |
Claudio Sustmann1, Steffen Dickopf1, Jörg T Regula1, Hubert Kettenberger1, Michael Mølhøj1, Christian Gassner1, Diana Weininger1, Sebastian Fenn1, Tobias Manigold2, Lothar Kling1, Klaus-Peter Künkele1, Manfred Schwaiger2, Birgit Bossenmaier1, Julia J Griese3, Karl-Peter Hopfner3, Alexandra Graff-Meyer4, Henning Stahlberg4, Philippe Ringler4, Matthias E Lauer5, Ulrich Brinkmann1, Wolfgang Schaefer1, Christian Klein6.
Abstract
High specificity accompanied with the ability to recruit immune cells has made recombinant therapeutic antibodies an integral part of drug development. Here we present a generic approach to generate two novel IgG-derived antibody formats that are based on a modification of the CrossMab technology. MoAbs harbor two heavy chains (HCs) resulting in one binding entity and one fragment crystallizable region (Fc), whereas DuoMabs are composed of four HCs harboring two binding entities and two Fc regions linked at a disulfide-bridged hinge. The latter bivalent format is characterized by avidity-enhanced target cell binding while simultaneously increasing the 'Fc-load' on the surface. DuoMabs were shown to be producible in high yield and purity and bind to surface cells with affinities comparable to IgGs. The increased Fc load directed at the surface of target cells by DuoMabs modulates their antibody-dependent cell-mediated cytotoxicity competency toward target cells, making them attractive for applications that require or are modulated by FcR interactions.Entities:
Keywords: ADCC; CrossMab; IGF-1R; antibody; cancer therapy; domain exchange
Mesh:
Substances:
Year: 2019 PMID: 31526159 PMCID: PMC6816436 DOI: 10.1080/19420862.2019.1661736
Source DB: PubMed Journal: MAbs ISSN: 1942-0862 Impact factor: 5.857