| Literature DB >> 30208333 |
Katy L Everett1, Matthew Kraman2, Francisca P G Wollerton2, Carlo Zimarino2, Katarzyna Kmiecik2, Miguel Gaspar2, Sarka Pechouckova2, Natalie L Allen2, Jacqueline F Doody2, Mihriban Tuna2.
Abstract
The immunoglobulin superfamily protein lymphocyte-activation gene 3 (LAG-3) participates in immune suppression and has been identified as a suitable target for cancer therapies. In order to generate bispecific antibodies targeting LAG-3, Fcabs (Fc-region with antigen binding) targeting human and murine LAG-3 were generated from phage libraries. These Fcabs bind to LAG-3, inhibiting its interaction with MHC class II, and induce IL-2 production in a T cell assay. Bispecific antibodies, known as mAb2, were produced by replacing the Fc region of a monoclonal antibody with Fcab sequences in the CH3 domain. mAb2 containing anti-LAG-3 Fcabs have mAb-like biophysical characteristics and retain LAG-3 binding and functional activity. mAb2 can thus be generated using multiple Fabs to investigate bispecific parings and develop novel therapeutics.Entities:
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Year: 2018 PMID: 30208333 DOI: 10.1016/j.ymeth.2018.09.003
Source DB: PubMed Journal: Methods ISSN: 1046-2023 Impact factor: 3.608