高通量筛选 SARS-CoV-2 螺旋酶抑制剂。

IF 2.7 4区 生物学 Q2 BIOCHEMICAL RESEARCH METHODS
Yuka Otsuka , Eunjung Kim , Austin Krueger , Justin Shumate , Chao Wang , Bilel Bdiri , Sultan Ullah , HaJeung Park , Louis Scampavia , Thomas D. Bannister , Donghoon Chung , Timothy P. Spicer
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引用次数: 0

摘要

严重急性呼吸系统综合征冠状病毒 2(SARS-CoV-2)自 2019 年底爆发以来,已造成全球近 700 万人死亡。尽管疫苗的开发和生产速度很快,研究工作也很深入,但人们仍然非常需要针对迅速出现的新变种的特异性抗病毒药物。为了解决这一问题,美国国家过敏与传染病研究所(NIAID)成立了九个抗病毒药物研发中心(AViDD),负责探索针对具有流行潜力的病原体(包括 SARS-CoV-2)的方法。在这项研究中,我们寻找 SARS-CoV2 非结构蛋白 13 (nsP13) 的抑制剂作为潜在的抗病毒药物,首先开发了一种 HTS 兼容测定法来测量 SARS-CoV2 nsP13 螺旋酶的活性。在此,我们介绍了我们在 1,536 孔板格式中实施该测定法的工作,以及从一个 ∼650,000 个化合物库中鉴定 nsP13 抑制剂命中化合物的工作。初筛结果十分可靠(平均 Z' = 0.86 ± 0.05),初筛出 7,009 个化合物。其中 1,763 个化合物经反复复试后得到进一步确认,显示出一致的抑制作用。在进行内部分析、额外的正交试验和滴定试验后,我们确定了 674 个化合物的 IC50
本文章由计算机程序翻译,如有差异,请以英文原文为准。
High throughput screening for SARS-CoV-2 helicase inhibitors

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is responsible for nearly 7 million deaths worldwide since its outbreak in late 2019. Even with the rapid development and production of vaccines and intensive research, there is still a huge need for specific anti-viral drugs that address the rapidly arising new variants. To address this concern, the National Institute of Allergy and Infectious Diseases (NIAID) established nine Antiviral Drug Discovery (AViDD) Centers, tasked with exploring approaches to target pathogens with pandemic potential, including SARS-CoV-2. In this study, we sought inhibitors of SARS-CoV2 non-structural protein 13 (nsP13) as potential antivirals, first developing a HTS-compatible assay to measure SARS-CoV2 nsP13 helicase activity. Here we present our effort in implementing the assay in a 1,536 well-plate format and in identifying nsP13 inhibitor hit compounds from a ∼650,000 compound library. The primary screen was robust (average Z’ = 0.86 ± 0.05) and resulted in 7,009 primary hits. 1,763 of these compounds upon repeated retests were further confirmed, showing consistent inhibition. Following in-silico analysis, an additional orthogonal assay and titration assays, we identified 674 compounds with IC50 <10 μM. We confirmed activity of independent compound batches from de novo powders while also incorporating multiple counterscreen assays. Our study highlights the potential of this assay for use on HTS platforms to discover novel compounds inhibiting SARS-CoV2 nsP13, which merit further development as an effective SARS-CoV2 antiviral.

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来源期刊
SLAS Discovery
SLAS Discovery Chemistry-Analytical Chemistry
CiteScore
7.00
自引率
3.20%
发文量
58
审稿时长
39 days
期刊介绍: Advancing Life Sciences R&D: SLAS Discovery reports how scientists develop and utilize novel technologies and/or approaches to provide and characterize chemical and biological tools to understand and treat human disease. SLAS Discovery is a peer-reviewed journal that publishes scientific reports that enable and improve target validation, evaluate current drug discovery technologies, provide novel research tools, and incorporate research approaches that enhance depth of knowledge and drug discovery success. SLAS Discovery emphasizes scientific and technical advances in target identification/validation (including chemical probes, RNA silencing, gene editing technologies); biomarker discovery; assay development; virtual, medium- or high-throughput screening (biochemical and biological, biophysical, phenotypic, toxicological, ADME); lead generation/optimization; chemical biology; and informatics (data analysis, image analysis, statistics, bio- and chemo-informatics). Review articles on target biology, new paradigms in drug discovery and advances in drug discovery technologies. SLAS Discovery is of particular interest to those involved in analytical chemistry, applied microbiology, automation, biochemistry, bioengineering, biomedical optics, biotechnology, bioinformatics, cell biology, DNA science and technology, genetics, information technology, medicinal chemistry, molecular biology, natural products chemistry, organic chemistry, pharmacology, spectroscopy, and toxicology. SLAS Discovery is a member of the Committee on Publication Ethics (COPE) and was published previously (1996-2016) as the Journal of Biomolecular Screening (JBS).
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