Literature DB >> 23792919

Mammalian cell display for the discovery and optimization of antibody therapeutics.

Peter M Bowers1, Robert A Horlick1, Marilyn R Kehry1, Tamlyn Y Neben1, Geoffery L Tomlinson1, Larry Altobell1, Xue Zhang1, John L Macomber1, Irina P Krapf1, Betty F Wu1, Audrey D McConnell1, Betty Chau1, Ashley D Berkebile1, Eric Hare1, Petra Verdino1, David J King2.   

Abstract

Recent advances are described for the isolation and affinity maturation of antibodies that couple in vitro somatic hypermutation (SHM) with mammalian cell display, replicating key aspects of the adaptive immune system. SHM is dependent on the action of the B cell specific enzyme, activation-induced cytidine deaminase (AID). AID-directed SHM in vitro in non-B cells, combined with mammalian display of a library of human antibodies, initially naïve to SHM, can be used to isolate and affinity mature antibodies via iterative cycles of fluorescence-activated cell sorting (FACS) under increasingly stringent sort conditions. SHM observed in vitro closely resembles SHM observed in human antibodies in vivo in both mutation type and positioning in the antibody variable region. In addition, existing antibodies originating from mouse immunization, in vivo based libraries, or alternative display technologies such as phage can also be affinity matured in a similar manner. The display system has been developed to enable simultaneous high-level cell surface expression and secretion of the same protein through alternate splicing, where the displayed protein phenotype remains linked to genotype, allowing soluble secreted antibody to be simultaneously characterized in biophysical and cell-based functional assays. This approach overcomes many of the previous limitations of mammalian cell display, enabling direct selection and maturation of antibodies as full-length, glycosylated IgGs.
Copyright © 2013 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  AID; Antibody; Mammalian cell display; Somatic hypermutation

Mesh:

Substances:

Year:  2013        PMID: 23792919     DOI: 10.1016/j.ymeth.2013.06.010

Source DB:  PubMed          Journal:  Methods        ISSN: 1046-2023            Impact factor:   3.608


  22 in total

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