Molecular origin of the hydrolytic activity and fixed regioselectivity of a Zr(IV) -substituted polyoxotungstate as artificial protease

Karen Stroobants; Vincent Goovaerts; Gregory Absillis; Gilles Bruylants; Eva Moelants; Paul Proost; Tatjana N Parac-Vogt

doi:10.1002/chem.201402683

Molecular origin of the hydrolytic activity and fixed regioselectivity of a Zr(IV) -substituted polyoxotungstate as artificial protease

Chemistry. 2014 Jul 28;20(31):9567-77. doi: 10.1002/chem.201402683. Epub 2014 Jun 24.

Authors

Karen Stroobants¹, Vincent Goovaerts, Gregory Absillis, Gilles Bruylants, Eva Moelants, Paul Proost, Tatjana N Parac-Vogt

Affiliation

¹ Department of Chemistry, KU Leuven, Celestijnenlaan 200F, 3001 Leuven (Belgium).

PMID: 24958622
DOI: 10.1002/chem.201402683

Abstract

A multitechnique approach has been applied in order to identify the thermodynamic and kinetic parameters related to the regioselective hydrolysis of human serum albumin (HSA) promoted by the Wells-Dawson polyoxometalate (POM), K15 H[Zr(α2 -P2 W17 O61 )2 ]. Isothermal titration calorimetry (ITC) studies indicate that up to four POM molecules interact with HSA. While the first interaction site is characterized by a 1:1 binding and an affinity constant of 2×10(8) M(-1) , the three remaining sites are characterized by a lower global affinity constant of 7×10(5) M(-1) . The higher affinity constant at the first site is in accordance with a high quenching constant of 2.2×10(8) M(-1) obtained for fluorescence quenching of the Trp214 residue located in the only positively charged cleft of HSA, in the presence of K15 H[Zr(α2 -P2 W17 O61 )2 ]. In addition, Eu(III) luminescence experiments with an Eu(III) -substituted POM analogue have shown the replacement of water molecules in the first coordination sphere of Eu(III) due to binding of the metal ion to amino acid side chain residues of HSA. All three interaction studies are in accordance with a stronger POM dominated binding at the positive cleft on the one hand, and interaction mainly governed by metal anchoring at the three remaining positions, on the other hand. Hydrolysis experiments in the presence of K15 H[Zr(α2 -P2 W17 O61 )2 ] have demonstrated regioselective cleavage of HSA at the Arg114Leu115, Ala257Asp258, Lys313Asp314 or Cys392Glu393 peptide bonds. This is in agreement with the interaction studies as the Arg114Leu115 peptide bond is located in the positive cleft of HSA and the three remaining peptide bonds are each located near an upstream acidic residue, which can be expected to coordinate to the metal ion. A detailed kinetic study has evidenced the formation of additional fragments upon prolonged reaction times. Edman degradation of the additional reaction products has shown that these fragments result from further hydrolysis at the initially observed cleavage positions, indicating a fixed selectivity for K15 H[Zr(α2 -P2 W17 O61 )2 ].

Keywords: human serum albumin; hydrolysis; polyoxometalates; regioselective protease; zirconium.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Calorimetry / methods
Humans
Hydrolysis
Kinetics
Peptide Hydrolases / chemistry*
Serum Albumin / chemistry
Stereoisomerism
Thermodynamics
Tungsten Compounds / chemistry*
Zirconium / chemistry*

Substances

Serum Albumin
Tungsten Compounds
polyoxometalate I
Zirconium
Peptide Hydrolases