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research article

Phage-encoded combinatorial chemical libraries based on bicyclic peptides

Heinis, Christian  
•
Rutherford, Trevor
•
Freund, Stefan
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2009
Nature Chemical Biology

Here we describe a phage strategy for the selection of ligands based on bicyclic or linear peptides attached covalently to an organic core. We designed peptide repertoires with three reactive cysteine residues, each spaced apart by several random amino acid residues, and we fused the repertoires to the phage gene-3-protein. Conjugation with tris-(bromomethyl)benzene via the reactive cysteines generated repertoires of peptide conjugates with two peptide loops anchored to a mesitylene core. Iterative affinity selections yielded several enzyme inhibitors; after further mutagenesis and selection, we were able to chemically synthesize a lead inhibitor (PK15; K(i) = 1.5 nM) specific to human plasma kallikrein that efficiently interrupted the intrinsic coagulation pathway in human plasma tested ex vivo. This approach offers a powerful means of generating and selecting bicyclic macrocycles (or if cleaved, linear derivatives thereof) as ligands poised at the interface of small-molecule drugs and biologics.

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Type
research article
DOI
10.1038/nchembio.184
Web of Science ID

WOS:000267266100016

Author(s)
Heinis, Christian  
Rutherford, Trevor
Freund, Stefan
Winter, Greg
Date Issued

2009

Published in
Nature Chemical Biology
Volume

5

Issue

7

Start page

502

End page

507

Subjects

Messenger-Rna Display

•

Filamentous Phage

•

Escherichia-Coli

•

Variable Domains

•

Protein Surfaces

•

Binding

•

Selection

•

Dna

•

Macrocycles

•

Evolution

Editorial or Peer reviewed

REVIEWED

Written at

OTHER

EPFL units
LPPT  
Available on Infoscience
October 5, 2009
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/43087
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