Journal of Enzyme Inhibition and Medicinal Chemistry (Jan 2017)

Allosteric inhibition of carnosinase (CN1) by inducing a conformational shift

  • Verena Peters,
  • Claus P. Schmitt,
  • Tim Weigand,
  • Kristina Klingbeil,
  • Christian Thiel,
  • Antje van den Berg,
  • Vittorio Calabrese,
  • Peter Nawroth,
  • Thomas Fleming,
  • Elisabete Forsberg,
  • Andreas H. Wagner,
  • Markus Hecker,
  • Giulio Vistoli

DOI
https://doi.org/10.1080/14756366.2017.1355793
Journal volume & issue
Vol. 32, no. 1
pp. 1102 – 1110

Abstract

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In humans, low serum carnosinase (CN1) activity protects patients with type 2 diabetes from diabetic nephropathy. We now characterized the interaction of thiol-containing compounds with CN1 cysteine residue at position 102, which is important for CN1 activity. Reduced glutathione (GSH), N-acetylcysteine and cysteine (3.2 ± 0.4, 2.0 ± 0.3, 1.6 ± 0.2 µmol/mg/h/mM; p < .05) lowered dose-dependently recombinant CN1 (rCN1) efficiency (5.2 ± 0.2 µmol/mg/h/mM) and normalized increased CN1 activity renal tissue samples of diabetic mice. Inhibition was allosteric. Substitution of rCN1 cysteine residues at position 102 (Mut1C102S) and 229 (Mut2C229S) revealed that only cysteine-102 is influenced by cysteinylation. Molecular dynamic simulation confirmed a conformational rearrangement of negatively charged residues surrounding the zinc ions causing a partial shift of the carnosine ammonium head and resulting in a less effective pose of the substrate within the catalytic cavity and decreased activity. Cysteine-compounds influence the dynamic behaviour of CN1 and therefore present a promising option for the treatment of diabetes.

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