In order to stabilize the C-terminal dodecapeptide of neuropeptide Y (NPY) we replaced Leu²⁸ and Thr³² by Lys and Glu, respectively, and subsequently linked these residues by lactamization. This peptide analog of NPY shows a more than 100-fold increase in affinity compared to the C-terminal linear dodecapeptide in receptor binding studies performed at human neuroblastoma cells SMS-KAN, which exclusively express the Y₂ receptor subtype. Signal transduction was investigated by measuring Ca²⁺ current inhibition in human SH-SY5Y cells and cyclic [Lys²⁸-Glu³²] NPY Ac-25–36 and NPY were shown to be equipotent in this assay. Thus, this molecule is the smallest Y₂ receptor selective full agonist of NPY. Using 2D-NMR experiments and molecular modelling techniques, the structures of the linear and cyclic peptides have been investigated and significant differences have been found, which may explain the improvement in biological activity. Thus, a model of the bioactive conformation of NPY at the human Y₂ receptor is suggested.