Decoding Selection Bias Imparted by Unpaired Cysteines: a Tug of War Between Expression and Affinity |
| |
| Authors: | B. Vijayalakshmi Ayyar Stephen Hearty Richard O’Kennedy |
| |
| Affiliation: | 1.Biomedical Diagnostics Institute, National Centre for Sensor Research,Dublin City University,Dublin 9,Ireland;2.School of Biotechnology,Dublin City University,Dublin 9,Ireland;3.Department of Molecular Virology and Microbiology,Baylor College of Medicine,Houston,USA;4.Immunocore Ltd,Abingdon,UK;5.Research Complex, Hamid Bin Khalifa University,Doha,Qatar |
| |
| Abstract: | In a recombinant antibody scFv format, the presence of an unpaired cysteine (Cys) is implicated in reduced soluble expression and inefficient presentation in phage display. Compared to other species, antibodies derived from rabbits are more likely to contain this unpaired Cys residue at position 80 (Cys80), when generated in a scFv format. In a screening campaign to isolate rabbit scFv against cardiac troponin I (cTnI), it was found that, a large proportion of isolated cTnI-specific clones contained unpaired Cys80. To analyze the factors that led to the selection of anti-cTnI Cys80 scFv, after five rounds of biopanning, the biopanning experiments were repeated with a Cys80 scFv (MG4Cys), its alanine variant (MG4Ala), and an irrelevant high expressing scFv control. It was found that the selection and subsequent enrichment of MG4Cys scFv was ousted by the superior expressing variant MG4Ala, indicating that the Cys80 scFv was selected primarily due to its affinity. It is evident that phage-based selection is influenced by specific sequence characteristics affecting the expression as well as the binding specificity and this needs to be taken into account for selection of optimal antibody derivatives. |
| |
| Keywords: | |
| 本文献已被 SpringerLink 等数据库收录! |
|
