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片段筛选的弱亲和层析法:与针对 HSP90 的筛选的既定技术比较。

Fragment screening by weak affinity chromatography: comparison with established techniques for screening against HSP90.

机构信息

Department of Chemistry and Biomedical Sciences, Linnaeus University, Kalmar, Sweden.

出版信息

Anal Chem. 2013 Jul 16;85(14):6756-66. doi: 10.1021/ac400715t. Epub 2013 Jun 27.

Abstract

The increasing use of fragment-based lead discovery (FBLD) in industry as well as in academia creates a high demand for sensitive and reliable methods to detect the binding of fragments to act as starting points in drug discovery programs. Nuclear magnetic resonance (NMR), surface plasmon resonance (SPR), and X-ray crystallography are well-established methods for fragment finding, and thermal shift and fluorescence polarization (FP) assays are used to a lesser extent. Weak affinity chromatography (WAC) was recently introduced as a new technology for fragment screening. The study presented here compares screening of 111 fragments against the ATPase domain of HSP90 by all of these methods, with isothermal titration calorimetry (ITC) used to confirm the most potent hits. The study demonstrates that WAC is comparable to the established methods of ligand-based NMR and SPR as a hit-id method, with hit correlations of 88% and 83%, respectively. The stability of HSP90 WAC columns was also evaluated and found to give 90% reproducibility even after 207 days of storage. A good correlation was obtained between the various technologies, validating WAC as an effective technology for fragment screening.

摘要

片段起始药物发现(FBLD)在工业和学术界的应用日益广泛,这对灵敏可靠的检测片段与靶标蛋白结合的方法产生了很高的需求,这些方法可以作为药物发现项目的起始点。核磁共振(NMR)、表面等离子体共振(SPR)和 X 射线晶体学是已经确立的片段发现方法,而热转移和荧光偏振(FP)检测法的应用则相对较少。弱亲和色谱(WAC)最近被引入作为一种新的片段筛选技术。本研究通过所有这些方法比较了 111 个片段与 HSP90 的 ATP 酶结构域的筛选,等温滴定量热法(ITC)用于确认最有效的命中物。研究表明,WAC 作为一种命中鉴定方法,与基于配体的 NMR 和 SPR 等已确立的方法相当,命中相关性分别为 88%和 83%。还评估了 HSP90 WAC 柱的稳定性,发现即使在储存 207 天后,仍具有 90%的重现性。各种技术之间存在良好的相关性,这验证了 WAC 作为一种有效的片段筛选技术。

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