Enabling systemic identification and functionality profiling for Cdc42 homeostatic modulators

IF 5.9 2区 化学 Q1 CHEMISTRY, MULTIDISCIPLINARY Communications Chemistry Pub Date : 2024-11-19 DOI:10.1038/s42004-024-01352-7
Satyaveni Malasala, Fereshteh Azimian, Yan-Hua Chen, Jeffery L. Twiss, Christi Boykin, Shayan Nik Akhtar, Qun Lu
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Abstract

Maintaining body homeostasis is the ultimate key to health. There are rich resources of bioactive materials for the functionality of homeostatic modulators (HMs) from both natural and synthetic chemical repertories1–3. HMs are powerful modern therapeutics for human diseases including neuropsychiatric diseases, mental disorders, and drug addiction (e.g. Buspirone and benzodiazepines)4–7. However, the identification of therapeutic HMs are often unpredictable and limited to membrane protein receptors and ion channels. Based on a serendipitously encountered small molecule ZCL278 with partial agonist (PA) profile as a model compound8–10, the Mant-GTP fluorophore-based Cdc42-GEF (guanine nucleotide exchange factor) screening uncovered a near holistic spectrum of HMs for Cdc42, a cytoplasmic small GTPase in the Ras superfamily11,12. We categorized these HMs as functionally distinct, with some previously understudied classes: Class I-competitive PAs, Class II-hormetic agonists, Class III-bona fide inhibitors, Class IV-bona fide activators, and Class V-ligand-enhanced agonists. The model HMs elicited striking biological functionalities in modulating bradykinin activation of Cdc42 signaling as well as actin remodeling while they ameliorated Alzheimer’s disease-like social behavior in mouse model. Furthermore, molecular structural modeling analyses led to the concept of preferential binding pocket order (PBPO) for profiling HMs that target Cdc42 complexed with intersectin (ITSN), a GEF selectively activating Cdc42. Remarkably, the PBPO enabled a prediction of HM class that mimics the pharmacological functionality. Therefore, our study highlights a model path to actively capture different classes of HM to broaden therapeutic landscape. Homeostatic modulators (HMs) are powerful modern therapeutics for human diseases including neuropsychiatric diseases, mental disorders, and drug addiction; however, their discovery is often unpredictable and limited to membrane protein receptors and ion channels. Here, the authors analyze a spectrum of novel HMs for Cdc42, a cytoplasmic small GTPase in the Ras superfamily, with striking biological functionalities and potential therapeutic applications.

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实现对 Cdc42 平衡调节剂的系统鉴定和功能分析。
维持体内平衡是健康的最终关键。天然和合成化学物质库中有丰富的生物活性材料,可用于平衡调节剂(HMs)的功能1-3。同调调节剂是治疗人类疾病(包括神经精神疾病、精神障碍和药物成瘾,如丁螺环酮和苯二氮卓)的强大现代疗法4-7。然而,治疗性 HMs 的鉴定往往难以预测,而且仅限于膜蛋白受体和离子通道。基于偶然发现的具有部分激动剂(PA)特征的小分子 ZCL278 作为模型化合物8-10,基于 Mant-GTP 荧光团的 Cdc42-GEF(鸟嘌呤核苷酸交换因子)筛选发现了 Cdc42(Ras 超家族中的一种细胞质小 GTP 酶11,12)的近乎全面的 HMs。我们将这些 HMs 分为不同的功能类别,其中包括一些以前未被充分研究的类别:一类是竞争性 PAs,二类是激素激动剂,三类是真正的抑制剂,四类是真正的激活剂,五类是配体增强激动剂。模型 HMs 在调节缓激肽激活 Cdc42 信号以及肌动蛋白重塑方面具有显著的生物学功能,同时它们还能改善小鼠模型中类似阿尔茨海默病的社会行为。此外,分子结构建模分析还提出了优先结合口袋顺序(PBPO)的概念,用于分析靶向与交联蛋白(ITSN)(一种选择性激活 Cdc42 的 GEF)复合物的 Cdc42 的 HMs。值得注意的是,PBPO 能够预测模拟药理功能的 HM 类别。因此,我们的研究强调了积极捕捉不同类别的 HM 以拓宽治疗领域的模型路径。
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来源期刊
Communications Chemistry
Communications Chemistry Chemistry-General Chemistry
CiteScore
7.70
自引率
1.70%
发文量
146
审稿时长
13 weeks
期刊介绍: Communications Chemistry is an open access journal from Nature Research publishing high-quality research, reviews and commentary in all areas of the chemical sciences. Research papers published by the journal represent significant advances bringing new chemical insight to a specialized area of research. We also aim to provide a community forum for issues of importance to all chemists, regardless of sub-discipline.
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