Vasoactive intestinal polypeptide VPAC1 and VPAC2 receptor chimeras identify domains responsible for the specificity of ligand binding and activation

Abstract

In order to identify the receptor domains responsible for the VPAC₁ selectivity of the VIP₁ agonist, [Lys15, Arg16, Leu27] VIP (1–7)/GRF (8–27) and VIP₁ antagonist, Ac His1 [D‐Phe2, Lys15, Arg16, Leu27] VIP (3–7)/GRF (8–27), we evaluated their binding and functional properties on chimeric VPAC₁/VPAC₂ receptors. Our results suggest that the N‐terminal extracellular domain is responsible for the selectivity of the VIP₁ antagonist. Selective recognition of the VIP₁ agonist was supported by a larger receptor area: in addition to the N‐terminal domain, the first extracellular loop, as well as additional determinants in the distal part of the VPAC₁ receptor were involved. Furthermore, these additional domains were critical for an efficient receptor activation, as replacement of EC₁ in VPAC₁ by its counter part in the VPAC₂ receptor markedly reduced the maximal response.