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用于筛选调节分子伴侣DnaK的ATP酶活性的小分子的高通量筛选。

High-throughput screen for small molecules that modulate the ATPase activity of the molecular chaperone DnaK.

作者信息

Chang Lyra, Bertelsen Eric B, Wisén Susanne, Larsen Erik M, Zuiderweg Erik R P, Gestwicki Jason E

机构信息

Life Sciences Institute, University of Michigan, Ann Arbor, MI 48109, USA.

出版信息

Anal Biochem. 2008 Jan 15;372(2):167-76. doi: 10.1016/j.ab.2007.08.020. Epub 2007 Aug 22.

Abstract

DnaK is a molecular chaperone of Escherichia coli that belongs to a family of conserved 70-kDa heat shock proteins. The Hsp70 chaperones are well known for their crucial roles in regulating protein homeostasis, preventing protein aggregation, and directing subcellular traffic. Given the complexity of functions, a chemical method for controlling the activities of these chaperones might provide a useful experimental tool. However, there are only a handful of Hsp70-binding molecules known. To build this area, we developed a robust, colorimetric, high-throughput screening (HTS) method in 96-well plates that reports on the ATPase activity of DnaK. Using this approach, we screened a 204-member focused library of molecules that share a dihydropyrimidine core common to known Hsp70-binding leads and uncovered seven new inhibitors. Intriguingly, the candidates do not appear to bind the hydrophobic groove that normally interacts with peptide substrates. In sum, we have developed a reliable HTS method that will likely accelerate discovery of small molecules that modulate DnaK/Hsp70 function. Moreover, because this family of chaperones has been linked to numerous diseases, this platform might be used to generate new therapeutic leads.

摘要

DnaK是大肠杆菌的一种分子伴侣,属于保守的70 kDa热休克蛋白家族。Hsp70分子伴侣因其在调节蛋白质稳态、防止蛋白质聚集和指导亚细胞运输中的关键作用而闻名。鉴于功能的复杂性,一种控制这些分子伴侣活性的化学方法可能会提供一种有用的实验工具。然而,已知的Hsp70结合分子只有少数几种。为了拓展这一领域,我们在96孔板中开发了一种强大的比色高通量筛选(HTS)方法,用于报告DnaK的ATP酶活性。使用这种方法,我们筛选了一个由204个成员组成的聚焦分子库,这些分子共享已知Hsp70结合先导化合物共有的二氢嘧啶核心,并发现了七种新的抑制剂。有趣的是,这些候选物似乎并不结合通常与肽底物相互作用的疏水凹槽。总之,我们开发了一种可靠的HTS方法,这可能会加速发现调节DnaK/Hsp70功能的小分子。此外,由于这一家族的分子伴侣与多种疾病有关,这个平台可能会用于产生新的治疗先导化合物。

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