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research article

Dithiol amino acids can structurally shape and enhance the ligand-binding properties of polypeptides

Chen, Shiyu  
•
Gopalakrishnan, Ranganath  
•
Schaer, Tifany
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2014
Nature Chemistry

The disulfide bonds that form between two cysteine residues are important in defining and rigidifying the structures of proteins and peptides. In polypeptides containing multiple cysteine residues, disulfide isomerization can lead to multiple products with different biological activities. Here, we describe the development of a dithiol amino acid (Dtaa) that can form two disulfide bridges at a single amino acid site. Application of Dtaas to a serine protease inhibitor and a nicotinic acetylcholine receptor inhibitor that contain disulfide constraints enhanced their inhibitory activities 40- and 7.6-fold, respectively. X-ray crystallographic and NMR structure analysis show that the peptide ligands containing Dtaas have retained their native tertiary structures. We furthermore show that replacement of two cysteines by Dtaas can avoid the formation of disulfide bond isomers. With these properties, Dtaas are likely to have broad application in the rational design or directed evolution of peptides and proteins with high activity and stability.

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Type
research article
DOI
10.1038/nchem.2043
Web of Science ID

WOS:000344476000015

Author(s)
Chen, Shiyu  
•
Gopalakrishnan, Ranganath  
•
Schaer, Tifany
•
Marger, Fabrice
•
Hovius, Ruud  
•
Bertrand, Daniel
•
Pojer, Florence
•
Heinis, Christian  
Date Issued

2014

Publisher

Nature Publishing Group

Published in
Nature Chemistry
Volume

6

Start page

1009

End page

1016

Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LPPT  
LCPPM  
Available on Infoscience
September 2, 2014
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/106647
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