[摘要] Terminally protectedpentapeptides with 2 histidines (Ac-HHVGD-NH2and Ac-HVGDH-NH2) and the terminally free peptides containing both internal aspartyl and C-terminal histidyl residues (FDAH and VIDAH) have been synthesized, and copper(II) complexes studied bypotentiometric, UV-Vis, CD, and EPR spectroscopic techniques in solution. Both thermodynamic and spectroscopic data reveal that side chain donor atoms of aspartyl and histidyl residues have a significant contribution to the metal binding affinity of peptide molecules. In the case of terminally protected peptides, the role of the imidazole-N donor functions is reflected in the enhanced stability of the 3N and 4N coordinatedcopper(II) complexes. The amino andβ-carboxylate groups ofFDAH and VIDAH create a very effective metal binding site with the (NH2,N−,β-COO−) and(NH2,N−,N−,β-COO−) coordination modes including the N-termini, while the histidine sites are available for the formation of the (Nim,N−,N−) binding mode resulting in the preference of dinuclear complex formation.