Title of article
Elaborate Manifold of Short Hydrogen Bond Arrays Mediating Binding of Active Site-directed Serine Protease Inhibitors
Author/Authors
Mary E. McGrath and Bradley A. Katz، نويسنده , , Kyle Elrod، نويسنده , , Erik Verner، نويسنده , , Richard L. Mackman، نويسنده , , Christine Luong، نويسنده , , William D. Shrader، نويسنده , , Martin Sendzik، نويسنده , , Jeffrey R. Spencer، نويسنده , , Paul A. Sprengeler، نويسنده , , Aleks Kolesnikov، نويسنده , , Vincent W.-F. Tai، نويسنده , , Hon C. Hui، نويسنده , , J. Guy Breitenbucher، نويسنده , , Darin Allen، نويسنده , , James W. Janc، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2003
Pages
28
From page
93
To page
120
Abstract
An extensive structural manifold of short hydrogen bond-mediated, active site-directed, serine protease inhibition motifs is revealed in a set of over 300 crystal structures involving a large suite of small molecule inhibitors (2-(2-phenol)-indoles and 2-(2-phenol)-benzimidazoles) determined over a wide range of pH (3.5–11.4). The active site hydrogen-bonding mode was found to vary markedly with pH, with the steric and electronic properties of the inhibitor, and with the type of protease (trypsin, thrombin or urokinase type plasminogen activator (uPA)). The pH dependence of the active site hydrogen-bonding motif is often intricate, constituting a distinct fingerprint of each complex. Isosteric replacements or minor substitutions within the inhibitor that modulate the pKa of the phenol hydroxyl involved in short hydrogen bonding, or that affect steric interactions distal to the active site, can significantly shift the pH-dependent structural profile characteristic of the parent scaffold, or produce active site-binding motifs unique to the bound analog.
Keywords
inhibition mechanism , short hydrogen bond , serine protease , Trypsin , shift of pKa of His57
Journal title
Journal of Molecular Biology
Serial Year
2003
Journal title
Journal of Molecular Biology
Record number
1242679
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