Abstract
Serine proteases and their natural inhibitors have long been served as excellent models for studying (primary, secondary and tertiary) structure - activity relationships of biologically interacting proteins. As protein flexibility has been accepted as a “fourth dimension” of the protein structure, its contribution to the binding process has gained much interest. In this article we review extreme cases of serine protease interactions with canonical serine protease inhibitors that provide unique insights into the dynamics of protein- protein interactions. The major conclusions of our review article are: a) taxon-specific inhibitory effects of two highly homologous protease inhibitors from Schistocerca gregaria (SGCI and SGTI), as investigated by H/D exchange experiments and NMR spectroscopy, are due to their differential flexibilities, b) stabilities of some protease and inhibitor complexes, the wide-spread and increased flexibility of some segments in the protein-protein complexes, as studied by X-ray crystallography and NMR-spectroscopy, appear to be proportional to the physical stability of the complex.
Keywords: Canonical inhibitors, flexibility, protein-protein interactions, serine proteases, serpins, stability.
Current Protein & Peptide Science
Title:The Role of Structural Flexibility and Stability in the Interaction of Serine Proteases with their Inhibitors
Volume: 16 Issue: 6
Author(s): Laszlo Graf, Tamas Molnar, Jozsef Kardos, Zoltan Gaspari and Gergely Katona
Affiliation:
Keywords: Canonical inhibitors, flexibility, protein-protein interactions, serine proteases, serpins, stability.
Abstract: Serine proteases and their natural inhibitors have long been served as excellent models for studying (primary, secondary and tertiary) structure - activity relationships of biologically interacting proteins. As protein flexibility has been accepted as a “fourth dimension” of the protein structure, its contribution to the binding process has gained much interest. In this article we review extreme cases of serine protease interactions with canonical serine protease inhibitors that provide unique insights into the dynamics of protein- protein interactions. The major conclusions of our review article are: a) taxon-specific inhibitory effects of two highly homologous protease inhibitors from Schistocerca gregaria (SGCI and SGTI), as investigated by H/D exchange experiments and NMR spectroscopy, are due to their differential flexibilities, b) stabilities of some protease and inhibitor complexes, the wide-spread and increased flexibility of some segments in the protein-protein complexes, as studied by X-ray crystallography and NMR-spectroscopy, appear to be proportional to the physical stability of the complex.
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Cite this article as:
Graf Laszlo, Molnar Tamas, Kardos Jozsef, Gaspari Zoltan and Katona Gergely, The Role of Structural Flexibility and Stability in the Interaction of Serine Proteases with their Inhibitors, Current Protein & Peptide Science 2015; 16 (6) . https://dx.doi.org/10.2174/1389203716666150429123733
DOI https://dx.doi.org/10.2174/1389203716666150429123733 |
Print ISSN 1389-2037 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-5550 |
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