DESIGN OF EFFICIENT HUMAN LEUKOCYTE ELASTASE INHIBITORS; VARIANTS OF HUMAN PANCREATIC SECRETORY TRYPSIN INHIBITOR (hPSTI)
Average rating
Cast your vote
You can rate an item by clicking the amount of stars they wish to award to this item.
When enough users have cast their vote on this item, the average rating will also be shown.
Star rating
Your vote was cast
Thank you for your feedback
Thank you for your feedback
Authors
Collins, JohnSzardenings, Michael
Maywald, Friedhelm
Fritz, Hans
Bruns, Wolfgang
Reinhardt, Gerd
Schnabel, Eugen
Schröder, Werner
Blöcker, Helmut
Reichelt, Joachim
Schomburg, Dietmar
Issue Date
1989Submitted date
2023-11-03
Metadata
Show full item recordAbstract
A set of hPSTI variants were constructed by total gene synthesis or site-specific mutagenesis, with the aim of producing human leukocyte elastase(HLE)-specific inhibitors and obtaining a better insight into the parameters effecting inhibitor/protease interaction. In the initial planning the structure of related Kazal-type inhibitors were taken into account. For subsequent protein design, models were made of HLE based on the structure of porcine pancreatic elastase, and of hPSTI based on the stucture of porcine PSTI. Models of the hPSTI/HLE and hPSTI/chymotrypsin complexes were generated by CAPD "docking". The modelled complexes could be used to rationalise a posteriori the inhibitory properties of the hPSTI variants, and to postulate the structure of better elastase inhibitors which were duly generated. Excellent specific inhibitors (Ky=1.5x107 4" M for SHEE) were obtained and the contribution of individual amino acid residues Or exchanges to the binding constant were estimated.Citation
Advances in protein design, 201 - 210Affiliation
GBF - Gesellschaft für Biotechnologische Forschung mbH, Braunschweig; *Institut für Klinische Chemie und Klinische Biochemie, Universität München; °Institut für Biochemie, Bayer AG, Wuppertal, F.R.G.Journal
Advances in protein design, 1988Type
Book chapterconference paper
Language
enSeries/Report no.
GBF monographs ; Volume 12ISSN
0930-4320ISBN
35272802430895739534
Collections
The following license files are associated with this item:
- Creative Commons
Except where otherwise noted, this item's license is described as Attribution-NonCommercial-ShareAlike 4.0 International