Copper(II) complexes of the N-terminal peptide fragments of tau protein have been studied by potentiometric and various spectroscopic techniques (UV-vis, CD, ESR and ESI-MS). The octapeptide Tau(9-16) (Ac-EVMEDHAG-NH ) contains the H14 residue of the native protein, while Tau(26-33) (Ac-QGGYTMHQ-NH ) and its mutants Tau(Q26K-Q33K) (Ac-KGGYTMHK-NH ) and Tau(Q26K-Y29A-Q33K) (Ac-KGGATMHK-NH ) include the H32 residue. To compare the binding ability of H14 and H32 in a single molecule the decapeptide Ac-EDHAGTMHQD-NH (Tau(12-16)(30-34)) has also been synthesized and studied. The histidyl residue is the primary metal binding site for metal ions in all the peptide models studied. In the case of Tau(9-16) the side chain carboxylate functions enhance the stability of the M-N coordinated complexes compared to Tau(26-33) (logK(Cu-N )=5.04 and 3.78, respectively). Deprotonation and metal ion coordination of amide groups occur around the physiological pH range for copper(II). The formation of the imidazole- and amide-coordinated species changes the metal ion preference and the complexes formed with the peptides containing the H32 residue predominate over those of H14 at physiological pH values (90 %-10 %) and in alkaline samples (96 %-4 %).

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http://dx.doi.org/10.1002/cplu.201900504DOI Listing

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