1. Production of a mono-biotinylated EGFR nanobody in the E. coli periplasm using the pET22b vector
- Author
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Matthijs Wesseling, Peter Kronenberger, Philippe Giron, Fatima Haddouchi, Gudrun Walser, Albert-Menno Laffra, Alfiah Noor, and Jacques De Greve
- Subjects
Single-domain antibody ,0301 basic medicine ,Immunoprecipitation ,EGFR ,lcsh:Medicine ,General Biochemistry, Genetics and Molecular Biology ,03 medical and health sciences ,0302 clinical medicine ,Mono-biotinylation ,Cell Line, Tumor ,Escherichia coli ,Humans ,Epidermal growth factor receptor ,lcsh:Science (General) ,lcsh:QH301-705.5 ,Cancer ,VHH domain ,biology ,Chemistry ,lcsh:R ,HEK 293 cells ,General Medicine ,Single-Domain Antibodies ,Molecular biology ,ErbB Receptors ,Research Note ,HEK293 Cells ,030104 developmental biology ,lcsh:Biology (General) ,Epidermoid carcinoma ,Cell culture ,030220 oncology & carcinogenesis ,Biotinylation ,Periplasm ,Cancer cell ,Nanobody ,biology.protein ,Streptavidin ,Nanocarriers ,lcsh:Q1-390 - Abstract
Objective Our aim was to produce a mono-biotinylated single domain antibody (‘nanobody’) specific for the epidermal growth factor receptor (EGFR), which is overexpressed in many cancer cells. The binding of the nanobody and its function are tested in cancer cells. The construct could be used to carry variable therapeutic or diagnostic load using biotin-streptavidin bridging. Results The EGFR-specific 7D12 nanobody was genetically fused to an IgA hinge linker and to a C-terminal biotin ligase acceptor sequence, allowing mono-biotinylation in E. coli. Expression was in strain BL21-DE3 from a T7 RNA polymerase driven pET22b vector. The biotinylated nanobody, isolated from the periplasm, was purified using streptavidin-mutein affinity chromatography. Final yields were up to 5 mg/l of cell culture. We showed that the construct could bind to EGFR expressing A431 epidermoid carcinoma cells, and to transiently transformed EGFR overexpressing HEK293T cells and not to EGFR negative control cells. The specificity for the EGFR was further demonstrated by immunoprecipitation. To test the functionality, PC9 non-small cell lung cancer cells were treated with mono-biotinylated nanobody or with streptavidin-coupled tetravalent nanobodies. Both were able to block mutant EGFR phosphorylation and slow down growth of PC9 cells. Tetravalent nanobodies were able to downregulate AKT phosphorylation. Electronic supplementary material The online version of this article (10.1186/s13104-018-3852-1) contains supplementary material, which is available to authorized users.
- Published
- 2018
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