Identification of a Unique Ligand Which Has High Affinity for All Four Bombesin Receptor Subtypes

Overview

Journal Eur J Pharmacol

Specialty Pharmacology

Date 1998 May 7

PMID 9570477

Citations 35

Authors

T K PRADHAN

T Katsuno

J E Taylor

S H Kim

R R Ryan

S A Mantey

P J Donohue

H C Weber

E Sainz

J F Battey

D H Coy

R T Jensen

Affiliations

Soon will be listed here.

Abstract

Four subtypes of bombesin receptors are identified (gastrin-releasing peptide receptor, neuromedin B receptor, the orphan receptor bombesin receptor subtype 3 (BB3 or BRS-3) and bombesin receptor subtype 4 (BB4)), however, only the pharmacology of the gastrin-releasing peptide receptor has been well studied. This lack of data is due in part to the absence of a general ligand. Recently we have discovered a ligand, 125I-[D-Tyr6,betaAla11,Phe13,Nle14]bombesin-(6-1 4) that binds to BRS-3 receptors. In this study we investigate its ability to interact with all four bombesin receptor subtypes. In rat pancreatic acini containing only gastrin-releasing peptide receptor and in BB4 transfected BALB cells, this ligand and 125I-[Tyr4]bombesin, the conventional gastrin-releasing peptide receptor ligand, gave similar results for receptor number, affinity for bombesin and affinity for the unlabeled ligand. In neuromedin B receptor transfected BALB cells, this ligand and 125I-[D-Tyr0]neuromedin B, the generally used neuromedin B receptor ligand, gave similar results for receptor number, neuromedin B affinity or the unlabeled ligand affinity. Lastly, in BRS-3 transfected BALB cells, only this ligand had high affinity. For all four bombesin receptors this ligand had an affinity of 1-8 nM and was equal or greater in affinity than any other specific ligands for any receptor. The unlabeled ligand is specific for gastrin-releasing peptide receptors on rat pancreatic acini and did not inhibit binding of 125I-cholecystokinin octapeptide (125I-CCK-8), 125I-vasoactive intestinal peptide (125I-VIP) or 125I-endothelin to their receptors. The unlabeled ligand was an agonist only at the gastrin-releasing peptide receptor in rat acini and did not interact with CCK(A) receptors or muscarinic M3 acetylcholine receptors to increase [3H]inositol phosphates. These results demonstrate 125I-[D-Tyr6,betaAla11,Phe13,Nle14]bombesin-(6-1 4) is a unique ligand with high affinity for all subtypes of bombesin receptors. Because of the specificity for bombesin receptors, this ligand will be a valuable addition for such pharmacological studies as screening for bombesin receptor agonists or antagonists and, in particular, for investigating BRS-3 cell biology, a receptor for which no ligand currently exists.

Citing Articles

Bombesins: A New Frontier in Hybrid Compound Development.

Serafin P, Kleczkowska P Pharmaceutics. 2023; 15(11).

PMID: 38004575 PMC: 10674911. DOI: 10.3390/pharmaceutics15112597.

The Nonpeptide Agonist MK-5046 Functions As an Allosteric Agonist for the Bombesin Receptor Subtype-3.

Ramos-Alvarez I, Iordanskaia T, Mantey S, Jensen R J Pharmacol Exp Ther. 2022; 382(2):66-78.

PMID: 35644465 PMC: 9341266. DOI: 10.1124/jpet.121.001033.

Development and Characterization of a Novel, High-Affinity, Specific, Radiolabeled Ligand for BRS-3 Receptors.

Ramos-Alvarez I, Lee L, Mantey S, Jensen R J Pharmacol Exp Ther. 2019; 369(3):454-465.

PMID: 30971479 PMC: 6519687. DOI: 10.1124/jpet.118.255141.

Easy formulation of liposomal doxorubicin modified with a bombesin peptide analogue for selective targeting of GRP receptors overexpressed by cancer cells.

Accardo A, Mannucci S, Nicolato E, Vurro F, Diaferia C, Bontempi P Drug Deliv Transl Res. 2018; 9(1):215-226.

PMID: 30569349 DOI: 10.1007/s13346-018-00606-x.

A possible new target in lung-cancer cells: The orphan receptor, bombesin receptor subtype-3.

Moreno P, Mantey S, Lee S, Ramos-Alvarez I, Moody T, Jensen R Peptides. 2018; 101:213-226.

PMID: 29410320 PMC: 6159918. DOI: 10.1016/j.peptides.2018.01.016.