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Conformational and biochemical analysis of the cyclic peptides which modulate serine protease activity

✍ Scribed by Miikka Pakkala; Anu Jylhäsalmi; Ping Wu; Jari Leinonen; Ulf-Håkan Stenman; Harri Santa; Jouko Vepsäläinen; Mikael Peräkylä; Ale Närvänen


Book ID
105360368
Publisher
John Wiley and Sons
Year
2004
Tongue
English
Weight
175 KB
Volume
10
Category
Article
ISSN
1075-2617

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✦ Synopsis


Abstract

Prostate‐specific antigen (PSA), a member of the kallikrein sub‐group of the trypsin serine protease family, is a widely used marker for prostate cancer. Several sequences with specific binding to PSA have been identified by using phage display peptide libraries. The GST‐fusion proteins of the characterized sequences have been shown to increase the enzyme activity of PSA to a synthetic substrate. The corresponding three cyclic synthetic analogues CVFTSNYAFC (A‐1), CVFAHNYNYLVC (B‐2) and CVAYCIEHHCWTC (C‐4) have similar PSA promoting activity. Despite differences in the amino acid sequences, all three peptides bind to the same region of PSA. The conformation of the peptides was investigated by proton NMR spectroscopy. In addition, alanine replacement was used to characterize the prerequisites for binding. It is proposed that interactions with PSA are based on the aromatic and hydrophobic features of the amino acid side chains. Furthermore, it is suggested that peptides form β–turn structures forced by cysteine bridges directing important aromatic side chains to the same side of the turn‐structure. Copyright © 2004 European Peptide Society and John Wiley & Sons, Ltd.


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