Discovery and validation of a novel inhibitor of HYPE-mediated AMPylation

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-04-09 DOI:10.1016/j.cstres.2024.04.001
Ali Camara , Heerak Chugh , Alyssa George , Lukas Dolidze , Kevin Ryu , Katrina J. Holly , Daniel P. Flaherty , Seema Mattoo
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Abstract

Adenosyl monophosphate (AMP)ylation (the covalent transfer of an AMP from Adenosine Triphosphate (ATP) onto a target protein) is catalyzed by the human enzyme Huntingtin Yeast Interacting Partner E (HYPE)/FicD to regulate its substrate, the heat shock chaperone binding immunoglobulin protein (BiP). HYPE-mediated AMPylation of BiP is critical for maintaining proteostasis in the endoplasmic reticulum and mounting a unfolded protein response in times of proteostatic imbalance. Thus, manipulating HYPE’s enzymatic activity is a key therapeutic strategy toward the treatment of various protein misfolding diseases, including neuropathy and early-onset diabetes associated with two recently identified clinical mutations of HYPE. Herein, we present an optimized, fluorescence polarization-based, high-throughput screening (HTS) assay to discover activators and inhibitors of HYPE-mediated AMPylation. After challenging our HTS assay with over 30,000 compounds, we discovered a novel AMPylase inhibitor, I2.10. We also determined a low micromolar IC50 for I2.10 and employed biorthogonal counter-screens to validate its efficacy against HYPE’s AMPylation of BiP. Further, we report low cytotoxicity of I2.10 on human cell lines. We thus established an optimized, high-quality HTS assay amenable to tracking HYPE’s enzymatic activity at scale, and provided the first novel small-molecule inhibitor capable of perturbing HYPE-directed AMPylation of BiP in vitro. Our HTS assay and I2.10 compound serve as a platform for further development of HYPE-specific small-molecule therapeutics.

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发现并验证 HYPE 介导的 AMPylation 的新型抑制剂
单磷酸腺苷(AMP)酰化(将三磷酸腺苷(ATP)中的 AMP 以共价方式转移到目标蛋白质上)由人类的亨廷汀酵母相互作用伙伴 E(HYPE)/FicD 酶催化,以调节其底物--热休克伴侣结合免疫球蛋白(BiP)。HYPE 介导的 BiP 的 AMPylation 对维持内质网中的蛋白稳态以及在蛋白稳态失衡时启动未折叠蛋白反应至关重要。因此,操纵 HYPE 的酶活性是治疗各种蛋白质错误折叠疾病的关键治疗策略,包括与最近发现的两种 HYPE 临床突变相关的神经病变和早发糖尿病。在此,我们介绍了一种优化的、基于荧光偏振的高通量筛选(HTS)测定法,用于发现 HYPE 介导的 AMPylation 的激活剂和抑制剂。在用 30,000 多种化合物对我们的 HTS 试验进行挑战之后,我们发现了一种新型 AMPylase 抑制剂 I2.10。我们还确定了 I2.10 较低的微摩尔 IC50 值,并采用生物对映方法验证了它对 HYPE 对 BiP 的 AMPylation 的有效性。此外,我们还报告了 I2.10 对人类细胞系的低细胞毒性。因此,我们建立了一种适合大规模跟踪 HYPE 酶活性的优化、高质量 HTS 检测方法,并提供了第一种能够在体外扰乱 HYPE 引导的 BiP AMPylation 的新型小分子抑制剂。我们的 HTS 检测方法和 I2.10 化合物可作为进一步开发 HYPE 特异性小分子疗法的平台。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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