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Phage display technology for human monoclonal antibodies

Authors :
Marco Dal Ferro
Serena Rizzo
Emanuela Rizzo
Francesca Marano
Immacolata Luisi
Olga Tarasiuk
Daniele Sblattero
Dal Ferro, Marco
Rizzo, Serena
Rizzo, Emanuela
Marano, Francesca
Luisi, Immacolata
Tarasiuk, Olga
Sblattero, Daniele
Source :
Methods in Molecular Biology ISBN: 9781493989577
Publication Year :
2019
Publisher :
Humana Press Inc., 2019.

Abstract

During the last 20 years in vitro technologies opened powerful routes to combine the generation of large libraries together with fast selection and screening procedures to identify lead candidates. One of the most successful methods is based on the use of filamentous phages. Functional Antibodies (Abs) fragments can be displayed on the surface of phages by fusing the coding sequence of the antibody variable (V) regions to the phage minor coat protein pIII. By creating large libraries, antibodies with affinities comparable to those obtained using traditional hybridoma technology can be isolated by a series of cycles of selection on the antigen of interest. In this system, antibody genes can be recovered simultaneously with selection and can be easily further engineered, for example by increasing their affinity to levels unobtainable in the immune system, or by modulating their specificity and their effector functions (by recloning into a full-length immunoglobulin scaffold). This chapter describes the basic protocols for antibody library construction and selection of binder with desired specificity.

Details

Language :
English
ISBN :
978-1-4939-8957-7
ISBNs :
9781493989577
Database :
OpenAIRE
Journal :
Methods in Molecular Biology ISBN: 9781493989577
Accession number :
edsair.doi.dedup.....a981ffc1888e7ebce442f02fc552866e