Characterization and optimization of peptide arrays for the study of epitope-antibody interactions using surface plasmon resonance imaging

Greta J. Wegner, Hye Jin Lee, Robert M. Corn

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261 Scopus citations

Abstract

The characterization of peptide arrays on gold surfaces designed for the study of peptide-antibody interactions using surface plasmon resonance (SPR) imaging is described. A two-step process was used to prepare the peptide arrays: (i) a set of parallel microchannels was used to deliver chemical reagents to covalently attach peptide probes to the surface by a thiol-disulfide exchange reaction; (ii) a second microchannel with a wrap-around design was used as a small-volume flow cell (5 μL) to introduce antibody solutions to the peptide surface. As a demonstration, the interactions of the FLAG epitope tag and monoclonal anti-FLAG M2 were monitored by SPR imaging using a peptide array. This peptide-antibody pair was studied because of its importance as a means to purify fusion proteins. The surface coverage of the FLAG peptide was precisely controlled by creating the peptide arrays on mixed monolayers of alkanethiols containing an amine-terminated surface and an inert alkanethiol. The mole fraction of peptide epitopes was also controlled by reacting solutions containing FLAG peptide and the non-interacting peptide HA or cysteine. By studying variants based on the FLAG binding motif, it was possible to distinguish peptides differing by a single amino acid substitution using SPR imaging. In addition, quantitative analysis of the signal was accomplished using the peptide array to simultaneously determine the binding constants of the antibody-peptide interactions for four peptides. The binding constant, Kads, for the FLAG peptide was measured and found to be 1.5 × 108 M-1 while variants made by the substitution of alanine for residues based on the binding motif had binding constants of 2.8 × 107, 5.0 × 106, and 2.0 × 106 M-1.

Original languageEnglish
Pages (from-to)5161-5168
Number of pages8
JournalAnalytical Chemistry
Volume74
Issue number20
DOIs
StatePublished - 15 Oct 2002

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