Drug Discovery Biology Laboratory, Monash Institute of Pharmaceutical Sciences and Department of Pharmacology, Monash University, Parkville, Victoria, Australia.
Mol Pharmacol. 2010 Sep;78(3):456-65. doi: 10.1124/mol.110.065664. Epub 2010 Jun 14.
The glucagon-like peptide-1 (GLP-1) receptor is a key regulator of insulin secretion and a major therapeutic target for treatment of diabetes. However, GLP-1 receptor function is complex, with multiple endogenous peptides that can interact with the receptor, including full-length (1-37) and truncated (7-37) forms of GLP-1 that can each exist in an amidated form and the related peptide oxyntomodulin. We have investigated two GLP-1 receptor allosteric modulators, Novo Nordisk compound 2 (6,7-dichloro2-methylsulfonyl-3-tert-butylaminoquinoxaline) and quercetin, and their ability to modify binding and signaling (cAMP formation, intracellular Ca(2+) mobilization, and extracellular signal-regulated kinase 1/2 phosphorylation) of each of the naturally occurring endogenous peptide agonists, as well as the clinically used peptide mimetic exendin-4. We identified and quantified stimulus bias across multiple endogenous peptides, with response profiles for truncated GLP-1 peptides distinct from those of either the full-length GLP-1 peptides or oxyntomodulin, the first demonstration of such behavior at the GLP-1 receptor. Compound 2 selectively augmented cAMP signaling but did so in a peptide-agonist dependent manner having greatest effect on oxyntomodulin, weaker effect on truncated GLP-1 peptides, and negligible effect on other peptide responses; these effects were principally driven by parallel changes in peptide agonist affinity. In contrast, quercetin selectively modulated calcium signaling but with effects only on truncated GLP-1 peptides or exendin and not oxyntomodulin or full-length peptides. These data have significant implications for how GLP-1 receptor targeted drugs are screened and developed, whereas the allosterically driven, agonist-selective, stimulus bias highlights the potential for distinct clinical efficacy depending on the properties of individual drugs.
胰高血糖素样肽-1 (GLP-1) 受体是胰岛素分泌的关键调节剂,也是治疗糖尿病的主要治疗靶点。然而,GLP-1 受体的功能很复杂,有多种内源性肽可以与受体相互作用,包括全长 (1-37) 和截断 (7-37) 形式的 GLP-1,它们都可以以酰胺化形式存在,以及相关肽促胃液素。我们研究了两种 GLP-1 受体别构调节剂,诺和诺德化合物 2(6,7-二氯-2-甲基磺酰基-3-叔丁基氨基喹喔啉)和槲皮素,以及它们对每种天然内源性肽激动剂结合和信号转导(cAMP 形成、细胞内 Ca(2+)动员和细胞外信号调节激酶 1/2 磷酸化)的修饰能力,以及临床使用的肽模拟物 exendin-4。我们确定并量化了多种内源性肽的刺激偏倚,截断的 GLP-1 肽的反应谱与全长 GLP-1 肽或促胃液素不同,这是在 GLP-1 受体上首次证明这种行为。化合物 2 选择性增强 cAMP 信号,但以肽激动剂依赖性方式进行,对促胃液素的作用最大,对截断的 GLP-1 肽的作用较弱,对其他肽反应的作用可以忽略不计;这些影响主要是由肽激动剂亲和力的平行变化驱动的。相比之下,槲皮素选择性调节钙信号,但仅对截断的 GLP-1 肽或 exendin 有作用,而对促胃液素或全长肽没有作用。这些数据对 GLP-1 受体靶向药物的筛选和开发具有重要意义,而别构驱动、激动剂选择性、刺激偏倚突出了个体药物的特性可能导致不同的临床疗效。
