A Pharmacophore for Drugs Targeting the α4α4 Binding Site of the (α4)3(β2)2 Nicotinic Acetylcholine Receptor

IF 4.2 3区医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Journal of Neurochemistry Pub Date : 2025-02-18 DOI:10.1111/jnc.70000

Ali S. Kusay, Yujia Luo, Megan L. O'Mara, Thomas Balle

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Abstract

Neuronal nicotinic acetylcholine receptors (nAChRs) have an established role in pain pathways and devastating neurodegenerative diseases; however, few drugs have been successfully developed to target them. The most abundant nAChR in the brain, the α4β2 nAChR, is assembled from five subunits in a 3α:2β stoichiometry—(α4)₃(β2)₂. This receptor contains a unique agonist-binding site at the α4α4 interface in addition to two classical agonist-binding sites at α4β2 interfaces. Most known agonists target both α4α4 and α4β2 sites, however, a few compounds with selectivity for the α4α4 site have been identified. These α4α4 selective compounds have a modulator-like effect akin to benzodiazepines in the γ-aminobutyric acid type A receptor, which is desirable from a drug development perspective. The two most well characterised α4α4 selective compounds are CMPI and NS9283. Both are structurally very different from classical agonists, and it is puzzling how they occupy the same binding site. In the search for a common pharmacophore, we conducted extensive molecular dynamics simulations with both classical agonists and site-selective non-classical compounds. Analyses of the simulations revealed that the α4α4 binding site contains a unique pocket not found in the α4β2 binding site. CMPI and NS9283 were observed to bind in this pocket, thereby explaining why they are selective for the α4α4 binding site. The proposed binding mode featured a closed-loop C conformation, which is strongly correlated with agonism in nAChRs and explained key site-directed mutagenesis data for both compounds. Based on this binding mode, we proposed a pharmacophore for drugs targeting the α4α4 binding site. The proposed pharmacophore captures the essence of the original model, that is, nicotinic agonists act as a bridge between protein subunits. The pharmacophore model we propose is unique to the α4α4 binding site and provides a template for developing new site-selective therapeutic agents.

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靶向（α4）3(β2)2烟碱乙酰胆碱受体α4α4结合位点的药物药效团

神经元烟碱乙酰胆碱受体（nAChRs）在疼痛通路和破坏性神经退行性疾病中具有确定的作用；然而，很少有药物能够成功地针对它们。大脑中最丰富的nAChR是α4β2 nAChR，它由5个亚基以3α:2β化学计量- (α4)3(β2)2的方式组装而成。该受体在α4 - α4界面上含有一个独特的激动剂结合位点，在α4 - β2界面上含有两个经典的激动剂结合位点。大多数已知的激动剂都靶向α4α4和α4β2位点，然而，已经发现了一些对α4α4位点具有选择性的化合物。这些α4α4选择性化合物在γ-氨基丁酸a型受体中具有类似于苯二氮卓类药物的调节作用，从药物开发的角度来看是理想的。两种表征最好的α4α4选择性化合物是CMPI和NS9283。两者在结构上都与传统的激动剂非常不同，它们如何占据相同的结合位点令人困惑。为了寻找一种常见的药效团，我们对经典激动剂和位点选择性非经典化合物进行了广泛的分子动力学模拟。模拟分析表明，α4α4结合位点含有α4β2结合位点所没有的独特口袋。观察到CMPI和NS9283在这个口袋中结合，从而解释了为什么它们对α4α4结合位点具有选择性。所提出的结合模式具有闭环C构象，这与nachr的激动作用密切相关，并解释了两种化合物的关键位点定向突变数据。基于这种结合模式，我们提出了一种靶向α4α4结合位点的药物药效团。提出的药效团抓住了原始模型的本质，即尼古丁激动剂作为蛋白质亚基之间的桥梁。我们提出的药效团模型是α4α4结合位点特有的，为开发新的位点选择性治疗剂提供了模板。

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来源期刊

Journal of Neurochemistry 医学-神经科学

CiteScore

9.30

自引率

2.10%

发文量

181

审稿时长

2.2 months

期刊介绍： Journal of Neurochemistry focuses on molecular, cellular and biochemical aspects of the nervous system, the pathogenesis of neurological disorders and the development of disease specific biomarkers. It is devoted to the prompt publication of original findings of the highest scientific priority and value that provide novel mechanistic insights, represent a clear advance over previous studies and have the potential to generate exciting future research.