Distinctive binding modes and inhibitory mechanisms of two peptidic inhibitors of urokinase-type plasminogen activator with isomeric P1 residues

Longguang Jiang; Baoyu Zhao; Peng Xu; Hans Peter Sørensen; Jan K Jensen; Anni Christensen; Masood Hosseini; Niels Christian Nielsen; Knud J Jensen; Peter A Andreasen; Mingdong Huang

doi:10.1016/j.biocel.2015.02.016

Distinctive binding modes and inhibitory mechanisms of two peptidic inhibitors of urokinase-type plasminogen activator with isomeric P1 residues

Int J Biochem Cell Biol. 2015 May:62:88-92. doi: 10.1016/j.biocel.2015.02.016. Epub 2015 Mar 2.

Affiliations

¹ Fujian Institute of Research on the Structure of Matter, Chinese Academy of Sciences, Fuzhou 350002, China(1); Danish-Chinese Centre for Proteases and Cancer, China.
² Department of Chemistry, Aarhus University, Aarhus, Denmark; Danish-Chinese Centre for Proteases and Cancer, China.
³ Department of Molecular Biology and Genetics, Aarhus University, Aarhus, Denmark(2); Danish-Chinese Centre for Proteases and Cancer, China.
⁴ Department of Chemistry, Faculty of Science, University of Copenhagen, Copenhagen, Denmark(3); Danish-Chinese Centre for Proteases and Cancer, China.
⁵ Fujian Institute of Research on the Structure of Matter, Chinese Academy of Sciences, Fuzhou 350002, China(1); Danish-Chinese Centre for Proteases and Cancer, China. Electronic address: mhuang@fjirsm.ac.cn.

PMID: 25744057
DOI: 10.1016/j.biocel.2015.02.016

Abstract

Two isomeric piperidine derivatives (meta and para isomers) were used as arginine mimics in the P1 position of a cyclic peptidic inhibitor (CPAYSRYLDC) of urokinase-type plasminogen activator. The two resulting cyclic peptides showed vastly different affinities (∼70 fold) to the target enzyme. X-ray crystal structure analysis showed that the two P1 residues were inserted into the S1 specificity pocket in indistinguishable manners. However, the rest of the peptides bound in entirely different ways on the surface of the enzyme, and the two peptides have different conformations, despite the highly similar sequence. These results demonstrate how the subtle difference in P1 residue can dictate the exosite interactions and the potencies of peptidic inhibitors, and highlight the importance of the P1 residue for protease inhibition. This study provides important information for the development of peptidic agents for pharmacological intervention.

Keywords: Cyclic peptide; Inhibitor; Protease; Urokinase; X-ray crystal structure.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Amino Acid Sequence
Catalytic Domain
Crystallography, X-Ray
Humans
Models, Molecular
Peptide Fragments / chemistry
Peptide Fragments / metabolism
Peptide Fragments / pharmacology
Peptides, Cyclic / chemistry
Peptides, Cyclic / pharmacology
Protease Inhibitors / chemistry
Protease Inhibitors / metabolism*
Protease Inhibitors / pharmacology
Protein Binding
Protein Interaction Domains and Motifs*
Urokinase-Type Plasminogen Activator / antagonists & inhibitors*
Urokinase-Type Plasminogen Activator / chemistry*
Urokinase-Type Plasminogen Activator / metabolism*

Substances

Peptide Fragments
Peptides, Cyclic
Protease Inhibitors
mupain-1
Urokinase-Type Plasminogen Activator

Associated data

PDB/4X0W
PDB/4X1N
PDB/4X1P