Single-Molecule-Based, Label-Free Monitoring of Molecular Glue Efficacies for Promoting Protein-Protein Interactions Using YaxAB Nanopores.

IF 15.8 1区 材料科学 Q1 CHEMISTRY, MULTIDISCIPLINARY ACS Nano Pub Date : 2024-11-12 Epub Date: 2024-10-31 DOI:10.1021/acsnano.4c11436
Minju Ryu, Sohee Oh, Ki-Baek Jeong, Sungbo Hwang, Jin-Sik Kim, Minji Chung, Seung-Wook Chi
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Abstract

Modulating protein-protein interactions (PPIs) is an attractive strategy in drug discovery. Molecular glues, bifunctional small-molecule drugs that promote PPIs, offer an approach to targeting traditionally undruggable targets. However, the efficient discovery of molecular glues has been hampered by the current limitations of conventional ensemble-averaging-based methods. In this study, we present a YaxAB nanopore for probing the efficacy of molecular glues in inducing PPIs. Using YaxAB nanopores, we demonstrate single-molecule-based, label-free monitoring of protein complex formation between mammalian target of rapamycin (mTOR) and FK506-binding proteins (FKBPs) triggered by the molecular glue, rapamycin. Owing to its wide entrance and adjustable pore size, in combination with potent electro-osmotic flow (EOF), a single funnel-shaped YaxAB nanopore enables the simultaneous detection and single-molecule-level quantification of multiprotein states, including single proteins, binary complexes, and ternary complexes induced by rapamycin. Notably, YaxAB nanopores could sensitively discriminate between the binary complexes or ternary complexes induced by rapamycin and its analogues, despite the subtle size differences of ∼122 or ∼116 Da, respectively. Taken together, our results provide proof-of-concept for single-molecule-based, label-free, and ultrasensitive screening and structure-activity relationship (SAR) analysis of molecular glues, which will contribute to low-cost, highly efficient discovery, and rational design of bifunctional modality of drugs, such as molecular glues.

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利用 YaxAB 纳米孔,基于单分子、无标记监测分子胶促进蛋白质-蛋白质相互作用的功效。
调节蛋白质与蛋白质之间的相互作用(PPIs)是一种极具吸引力的药物发现策略。分子粘合剂是一种能促进 PPIs 的双功能小分子药物,它为靶向传统上无法药物治疗的靶点提供了一种方法。然而,目前基于集合平均法的传统方法的局限性阻碍了分子胶的高效发现。在本研究中,我们提出了一种 YaxAB 纳米孔,用于探测分子胶在诱导 PPIs 方面的功效。利用 YaxAB 纳米孔,我们展示了基于单分子、无标记监测雷帕霉素分子胶引发的哺乳动物雷帕霉素靶蛋白(mTOR)与 FK506 结合蛋白(FKBPs)之间蛋白质复合物的形成。由于 YaxAB 纳米孔具有宽入口和可调孔径的特点,再加上强大的电渗透流(EOF),一个漏斗状的 YaxAB 纳米孔就能同时检测和在单分子水平上定量多蛋白状态,包括雷帕霉素诱导的单个蛋白、二元复合物和三元复合物。值得注意的是,尽管雷帕霉素及其类似物诱导的二元复合物或三元复合物的大小分别为 ∼122 或 ∼116 Da,YaxAB 纳米孔仍能灵敏地区分这两种复合物。综上所述,我们的研究结果为基于单分子、无标记、超灵敏的分子胶筛选和结构-活性关系(SAR)分析提供了概念验证,有助于低成本、高效率地发现和合理设计分子胶等双功能药物。
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来源期刊
ACS Nano
ACS Nano 工程技术-材料科学:综合
CiteScore
26.00
自引率
4.10%
发文量
1627
审稿时长
1.7 months
期刊介绍: ACS Nano, published monthly, serves as an international forum for comprehensive articles on nanoscience and nanotechnology research at the intersections of chemistry, biology, materials science, physics, and engineering. The journal fosters communication among scientists in these communities, facilitating collaboration, new research opportunities, and advancements through discoveries. ACS Nano covers synthesis, assembly, characterization, theory, and simulation of nanostructures, nanobiotechnology, nanofabrication, methods and tools for nanoscience and nanotechnology, and self- and directed-assembly. Alongside original research articles, it offers thorough reviews, perspectives on cutting-edge research, and discussions envisioning the future of nanoscience and nanotechnology.
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