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Rapid Fine Conformational Epitope Mapping Using Comprehensive Mutagenesis and Deep Sequencing.

J Biol Chem.. 2015-10;  290(44):26457-70
Kowalsky CA, Faber MS, Nath A, Dann HE, Kelly VW, Liu L, Shanker P, Wagner EK, Maynard JA, Chan C, Whitehead TA. Department of Chemical Engineering and Materials Science, Michigan State University, 428 S. Shaw Lane East Lansing, MI, USA.
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摘要

Knowledge of the fine location of neutralizing and non-neutralizing epitopes on human pathogens affords a better understanding of the structural basis of antibody efficacy, which will expedite rational design of vaccines, prophylactics, and therapeutics. However, full utilization of the wealth of information from single cell techniques and antibody repertoire sequencing awaits the development of a high throughput, inexpensive method to map the conformational epitopes for antibody-antigen interactions. Here we show such an approach that combines comprehensive mutagenesis, cell surface display, and DNA deep sequencing. We develop analytical equations to identify epitope positions and show the method effectiveness... More

關鍵詞

Bordetella pertussis; TROP2; antibody; antibody engineering; conformational epitope mapping; epitope mapping; protein-protein interaction; tumor necrosis factor (TNF)
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