Pharmacological characterization of allosteric modulators: A case for chemokine receptors

IF 10.9 1区 医学 Q1 CHEMISTRY, MEDICINAL Medicinal Research Reviews Pub Date : 2024-04-18 DOI:10.1002/med.22043
Lisa S. den Hollander, Adriaan P. IJzerman, Laura H. Heitman
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Abstract

Chemokine receptors are relevant targets for a multitude of immunological diseases, but drug attrition for these receptors is remarkably high. While many drug discovery programs have been pursued, most prospective drugs failed in the follow-up studies due to clinical inefficacy, and hence there is a clear need for alternative approaches. Allosteric modulators of receptor function represent an excellent opportunity for novel drugs, as they modulate receptor activation in a controlled manner and display increased selectivity, and their pharmacological profile can be insurmountable. Here, we discuss allosteric ligands and their pharmacological characterization for modulation of chemokine receptors. Ligands are included if (1) they show clear signs of allosteric modulation in vitro and (2) display evidence of binding in a topologically distinct manner compared to endogenous chemokines. We discuss how allosteric ligands affect binding of orthosteric (endogenous) ligands in terms of affinity as well as binding kinetics in radioligand binding assays. Moreover, their effects on signaling events in functional assays and how their binding site can be elucidated are specified. We substantiate this with examples of published allosteric ligands targeting chemokine receptors and hypothetical graphs of pharmacological behavior. This review should serve as an effective starting point for setting up assays for characterizing allosteric ligands to develop safer and more efficacious drugs for chemokine receptors and, ultimately, other G protein-coupled receptors.

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异位调节剂的药理学特征:趋化因子受体案例
趋化因子受体是多种免疫疾病的相关靶点,但这些受体的药物损耗率非常高。虽然已经开展了许多药物发现项目,但大多数前瞻性药物都因临床疗效不佳而在后续研究中失败,因此显然需要寻找替代方法。受体功能的异构调节剂是开发新型药物的绝佳机会,因为它们以可控的方式调节受体的活化,并显示出更高的选择性,其药理特征可能是难以逾越的。在此,我们将讨论用于调节趋化因子受体的异构配体及其药理学特征。如果配体(1)在体外显示出明显的异构调节迹象,并且(2)显示出与内源性趋化因子相比以拓扑学上不同的方式结合的证据,则被列入异构配体。我们讨论了异位配体如何在亲和力方面影响正位(内源性)配体的结合,以及在放射性配体结合试验中的结合动力学。此外,还具体说明了异位配体在功能测定中对信号传导事件的影响,以及如何阐明其结合位点。我们以已发表的针对趋化因子受体的异构配体和药理学行为假设图为例,证实了这一点。这篇综述应作为一个有效的起点,用于建立表征异构配体的试验,为趋化因子受体以及其他 G 蛋白偶联受体开发更安全、更有效的药物。
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来源期刊
CiteScore
29.30
自引率
0.00%
发文量
52
审稿时长
2 months
期刊介绍: Medicinal Research Reviews is dedicated to publishing timely and critical reviews, as well as opinion-based articles, covering a broad spectrum of topics related to medicinal research. These contributions are authored by individuals who have made significant advancements in the field. Encompassing a wide range of subjects, suitable topics include, but are not limited to, the underlying pathophysiology of crucial diseases and disease vectors, therapeutic approaches for diverse medical conditions, properties of molecular targets for therapeutic agents, innovative methodologies facilitating therapy discovery, genomics and proteomics, structure-activity correlations of drug series, development of new imaging and diagnostic tools, drug metabolism, drug delivery, and comprehensive examinations of the chemical, pharmacological, pharmacokinetic, pharmacodynamic, and clinical characteristics of significant drugs.
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