Digestive Diseases Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland.
Digestive Diseases Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland
J Pharmacol Exp Ther. 2022 Aug;382(2):66-78. doi: 10.1124/jpet.121.001033. Epub 2022 May 29.
Allosteric ligands of various G-protein-coupled receptors are being increasingly described and are providing important advances in the development of ligands with novel selectivity and efficacy. These unusual properties allow expanded opportunities for pharmacologic studies and treatment. Unfortunately, no allosteric ligands are yet described for the bombesin receptor family (BnRs), which are proposed to be involved in numerous physiologic/pathophysiological processes in both the central nervous system and peripheral tissues. In this study, we investigate the possibility that the bombesin receptor subtype-3 (BRS-3) specific nonpeptide receptor agonist MK-5046 [(2S)-1,1,1-trifluoro-2-[4-(1H-pyrazol-1-yl)phenyl]-3-(4-[[1-(trifluoromethyl)cyclopropyl]methyl]-1H-imidazol-2-yl)propan-2-ol] functions as a BRS-3 allosteric receptor ligand. We find that in BRS-3 cells, MK-5046 only partially inhibits iodine-125 radionuclide (I)-Bantag-1 [Boc-Phe-His-4-amino-5-cyclohexyl-2,4,5-trideoxypentonyl-Leu-(3-dimethylamino) benzylamide N-methylammonium trifluoroacetate] binding and that both peptide-1 (a universal BnR-agonist) and MK-5046 activate phospholipase C; however, the specific BRS-3 peptide antagonist Bantag-1 inhibits the action of peptide-1 competitively, whereas for MK-5046 the inhibition is noncompetitive and yields a curvilinear Schild plot. Furthermore, MK-5046 shows other allosteric behaviors, including slowing dissociation of the BRS-3 receptor ligand I-Bantag-1, dose-inhibition curves being markedly affected by increasing ligand concentration, and MK-5046 leftward shifting the peptide-1 agonist dose-response curve. Lastly, receptor chimeric studies and site-directed mutagenesis provide evidence that MK-5046 and Bantag-1 have different binding sites determining their receptor high affinity/selectivity. These results provide evidence that MK-5046 is functioning as an allosteric agonist at the BRS-3 receptor, which is the first allosteric ligand described for this family of receptors. SIGNIFICANCE STATEMENT: G-protein-coupled receptor allosteric ligands providing higher selectivity, selective efficacy, and safety that cannot be obtained using usual orthosteric receptor-based strategies are being increasingly described, resulting in enhanced usefulness in exploring receptor function and in treatment. No allosteric ligands exist for any of the mammalian bombesin receptor (BnR) family. Here we provide evidence for the first such example of a BnR allosteric ligand by showing that MK-5046, a nonpeptide agonist for bombesin receptor subtype-3, is functioning as an allosteric agonist.
各种 G 蛋白偶联受体的别构配体越来越多地被描述出来,并为开发具有新型选择性和疗效的配体提供了重要进展。这些不寻常的特性为药理学研究和治疗提供了更多的机会。不幸的是,目前尚未描述蛙皮素受体家族(BnR)的别构配体,据推测该家族参与中枢神经系统和外周组织中许多生理/病理生理过程。在这项研究中,我们研究了蛙皮素受体亚型 3(BRS-3)特异性非肽受体激动剂 MK-5046[(2S)-1,1,1-三氟-2-[4-(1H-吡唑-1-基)苯基]-3-(4-[[1-(三氟甲基)环丙基]甲基]-1H-咪唑-2-基)丙-2-醇]作为 BRS-3 别构受体配体的可能性。我们发现,在 BRS-3 细胞中,MK-5046 仅部分抑制碘-125 放射性核素(I)-Bantag-1[Boc-Phe-His-4-氨基-5-环己基-2,4,5-三脱氧戊酮基-Leu-(3-二甲基氨基)苄基酰胺 N-甲基铵三氟乙酸盐]结合,并且肽-1(通用 BnR-激动剂)和 MK-5046 均激活磷脂酶 C;然而,特异性 BRS-3 肽拮抗剂 Bantag-1 竞争性抑制肽-1 的作用,而对于 MK-5046,抑制是非竞争性的,并产生曲线的 Schild 图。此外,MK-5046 还表现出其他别构行为,包括减缓 BRS-3 受体配体 I-Bantag-1 的解离,剂量抑制曲线受配体浓度增加的显著影响,以及 MK-5046 使肽-1 激动剂剂量反应曲线向左移位。最后,受体嵌合研究和定点突变提供的证据表明,MK-5046 和 Bantag-1 具有不同的结合位点,决定了它们的受体高亲和力/选择性。这些结果提供了证据,表明 MK-5046 作为 BRS-3 受体的别构激动剂起作用,这是该受体家族描述的第一个别构配体。
越来越多地描述了 G 蛋白偶联受体的别构配体,这些配体提供了更高的选择性、选择性疗效和通常的基于受体的策略无法获得的安全性,从而增强了在探索受体功能和治疗中的有用性。哺乳动物蛙皮素受体(BnR)家族中不存在任何别构配体。在这里,我们通过证明非肽蛙皮素受体亚型 3 激动剂 MK-5046 作为别构激动剂起作用,提供了第一个此类 BnR 别构配体的例子。
