Kinetic and computational analysis of the reversible inhibition of porcine pancreatic elastase: a structural and mechanistic approach

  • J Enzyme Inhib Med Chem. 2016;31(sup3):131-139. doi: 10.1080/14756366.2016.1210137.
Panagiota-Yiolanda Stergiou  1 Athanasios Foukis  1 Olga A Gkini  1 Joseph G Bieth  2 Emmanuel M Papamichael  1
Affiliations
  • 1. a Department of Chemistry , Enzyme Biotechnology and Genetic Engineering Group, University of Ioannina , Ioannina , Greece and.
  • 2. b Laboratory of Enzymology-Unistra , University of Strasbourg , Strasbourg , France.
Abstract

Structural and mechanistic insights were revealed for the reversible inhibition of Porcine Pancreatic Elastase (PPE); the kinetics of uninhibited and inhibited hydrolysis of substrate Suc-AAA-pNA was analyzed thoroughly. Additionally, the interactions between PPE and its inhibitor were studied by computational techniques. The uninhibited hydrolysis of Suc-AAA-pNA by PPE proceeds through a virtual transition state, involving an inferior physical and another dominating chemical step, where two stabilized reactant states precede the predominant acyl-enzyme. Different kinds of bonding with the PPE-backbone residues, including those of the catalytic triad, were found during the MD simulation of 5 ns, as key interactions favoring a higher stabilization of the best ranked complex PPE-CF3C(O)-KA-NHPh-p-CF3. The proton inventories of the inhibited hydrolysis of Suc-AAA-pNA by PPE, were ruled out the existence of any virtual transition state and thus they argue for a different mode of catalysis involving a structurally disturbed PPE molecule. Thereafter, a novel inhibition mechanism was suggested.

Keywords
Inhibition mechanism; molecular docking; molecular dynamics; proton inventories.
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