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DOI: 10.1038/srep26240
¤ OpenAccess: Gold
This work has “Gold” OA status. This means it is published in an Open Access journal that is indexed by the DOAJ.

Targeting membrane proteins for antibody discovery using phage display

Martina L. Jones,Mohamed A. Alfaleh,Sumukh Kumble,Shuo Zhang,Geoffrey W. Osborne,Michael W. Yeh,Neetika Arora,Jeff Jia Cheng Hou,Christopher B. Howard,David Y. Chin,Stephen M. Mahler

Panning (audio)
Phage display
Antigen
2016
Abstract A critical factor in the successful isolation of new antibodies by phage display is the presentation of a correctly folded antigen. While this is relatively simple for soluble proteins which can be purified and immobilized onto a plastic surface, membrane proteins offer significant challenges for antibody discovery. Whole cell panning allows presentation of the membrane protein in its native conformation, but is complicated by a low target antigen density, high background of irrelevant antigens and non-specific binding of phage particles to cell surfaces. The method described here uses transient transfection of alternating host cell lines and stringent washing steps to address each of these limitations. The successful isolation of antibodies from a naive scFv library is described for three membrane bound proteins; human CD83, canine CD117 and bat CD11b.
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    Targeting membrane proteins for antibody discovery using phage display” is a paper by Martina L. Jones Mohamed A. Alfaleh Sumukh Kumble Shuo Zhang Geoffrey W. Osborne Michael W. Yeh Neetika Arora Jeff Jia Cheng Hou Christopher B. Howard David Y. Chin Stephen M. Mahler published in 2016. It has an Open Access status of “gold”. You can read and download a PDF Full Text of this paper here.