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利用微量热泳动技术从高通量筛选中鉴定命中化合物:欧洲先导化合物工厂的视角。

Using Microscale Thermophoresis to Characterize Hits from High-Throughput Screening: A European Lead Factory Perspective.

机构信息

1 European Screening Centre Newhouse, Biocity Scotland, University of Dundee, Newhouse, UK.

出版信息

SLAS Discov. 2018 Mar;23(3):225-241. doi: 10.1177/2472555217744728.

Abstract

High-throughput screening (HTS) is a proven method for discovering new lead matter for drug discovery and chemical biology. To maximize the likelihood of identifying genuine binders to a molecular target, and avoid wasting resources following up compounds with unproductive/nonspecific mechanisms of action, it is important to employ a range of assays during an HTS campaign that build confidence of target engagement for hit compounds. Biophysical methods that measure direct target/compound engagement have established themselves as key techniques in generating this confidence, and they are now integral to the latter stages of HTS triage at the European Lead Factory (ELF). One relatively new technique that the ELF is using is microscale thermophoresis (MST), which measures the differences in rate of movement through a temperature gradient that are caused when single molecular species form complexes. Here we provide an overview of the MST assay development workflow that the ELF employs and a perspective of our experience to date of using MST to triage the output of HTS campaigns and how it compares and contrasts with the use of other biophysical techniques.

摘要

高通量筛选(HTS)是发现新药和化学生物学新先导物质的一种经过验证的方法。为了最大限度地提高鉴定分子靶标真正结合物的可能性,并避免浪费资源跟踪具有非生产性/非特异性作用机制的化合物,在 HTS 活动中采用一系列可建立靶标结合物置信度的测定方法非常重要。测量直接靶标/化合物结合的生物物理方法已成为产生这种置信度的关键技术,现在已成为欧洲先导工厂(ELF)HTS 分类后期的组成部分。ELF 使用的一种相对较新的技术是微量热泳动(MST),它测量了当单分子物种形成复合物时,通过温度梯度的移动速度差异。在这里,我们提供了 ELF 采用的 MST 测定开发工作流程概述,并介绍了我们迄今为止使用 MST 对 HTS 活动的输出进行分类的经验,以及它与使用其他生物物理技术的比较。

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