Semi-rational design is combined with PCAs (protein-fragment complementation assays) and phage-display screening techniques to generate a range of iPEPs (interfering peptides) that target therapeutically relevant proteins with much higher interaction stability than their native complexes. PCA selection has been improved to impose a competitive and negative design initiative on the library screen, thus simultaneously improving the specificity of assay ‘winners’. The folding pathways of designed pairs imply that early events are dominated by hydrophobic collapse and helix formation, whereas later events account for the consolidation of more intricate intermolecular electrostatic interactions.

Keywords:
activator protein-1 (AP-1), basic leucine zipper (bZIP), interfering peptide, protein-fragment complementation assay (PCA), protein–protein interaction, semi-rational design
© The Authors Journal compilation © 2008 Biochemical Society
2008
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