The novel VIP-like hypothalamic polypeptide PACAP interacts with high affinity receptors in the human neuroblastoma cell line NB-OK.

Peptides1990PMID: 2172943

Plain Language Summary

Researchers discovered that the newly identified brain peptide PACAP binds to specific high-affinity receptors on human neuroblastoma cells that are distinct from VIP receptors. PACAP was 300 to 1,000 times more potent than VIP at these receptors and powerfully stimulated the enzyme adenylate cyclase, while GRF and other related peptides had no effect. This establishes PACAP as acting through its own dedicated receptor system rather than through existing VIP or GRF receptors.

Abstract

We investigated the ability of two forms of Pituitary Adenylate Cyclase Activating Polypeptide [PACAP-38, the 38 amino acid peptide isolated from ovine hypothalamus, and PACAP-27, a shorter N-terminal (1-27) amidated version] to interact with specific receptors in membranes from the human neuroblastoma cell line NB-OK. [125I]PACAP-27 bound rapidly and specifically to one class of high affinity sites (Kd 0.5 nM). VIP inhibited [125I]PACAP-27 binding 300- to 1000-fold less potently than PACAP-27 and PACAP-38. One microM PHI prevented tracer binding only partially and secretin, glucagon and GRF(1-29)NH2 were ineffective in this respect. PACAP-27 and PACAP-38 stimulated adenylate cyclase activity dose dependently and with similar efficacy (Kact 0.2-0.3 nM), this activation being compatible with the occupancy of specific high affinity PACAP receptor. VIP was markedly less potent and less efficient on this enzyme than PACAP. Chemical cross-linking of [125I]PACAP-27 followed by SDS-PAGE and autoradiography revealed specific cross-linking with a 68 kDa protein.

Authors

Cauvin, A; Buscail, L; Gourlet, P; De Neef, P; Gossen, D; Arimura, A; Miyata, A; Coy, D H; Robberecht, P; Christophe, J