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The successful cocrystallization of the noncovalent complex formed between (Et2NH2)8[{α-PW11O39Zr-(μ-OH)(H2O)}2]·7H2O Keggin polyoxometalate (2) and Hen Egg White Lysozyme (HEWL) protein is reported. The resulting structural model revealed inter­action between monomeric [Zr(PW11O39)]4−(1), which is a postulated catalytically active species, and the protein in two positions in the asymmetric unit. The first position (occupancy 36%) confirms the previously observed binding sites on the protein surface, whereas the second position (occupancy 14%) provides novel insights into the hydrolytic mechanisms of ZrIV-substituted polyoxometalates. The new inter­action site occurs at the Asn65 residue, which is directly next to the Asp66–Gly67 peptide bond that was identified recently as a cleavage site in the polyoxometalate-catalysed hydrolysis of HEWL. Furthermore, in this newly discovered binding site, the monomeric polyoxometalate 1 is observed to bind directly to the side chain of the Asn65 residue. This binding of ZrIV as a Lewis-acid metal to the carbonyl O atom of the Asn65 side chain is very similar to the inter­mediate state proposed in density functional theory (DFT) studies in which ZrIV activates the peptide bond via inter­action with its carbonyl O atom, and can be thus regarded as a model for inter­action between ZrIV and a peptide bond.

Supporting information

pdf

Portable Document Format (PDF) file https://doi.org/10.1107/S2053229618010690/jr3021sup1.pdf
Additional figures: image of the cocrystal and a view of the steric clashing

pdf

Portable Document Format (PDF) file https://doi.org/10.1107/S2053229618010690/jr3021sup2.pdf
PDB validation report

PDB reference: hen egg white lysozyme, 6gnl


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