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通过酰腙部分的优化发现β-连环蛋白/T细胞因子蛋白-蛋白相互作用的选择性小分子抑制剂。

Discovery of Selective Small-Molecule Inhibitors for the β-Catenin/T-Cell Factor Protein-Protein Interaction through the Optimization of the Acyl Hydrazone Moiety.

作者信息

Catrow J Leon, Zhang Yongqiang, Zhang Min, Ji Haitao

机构信息

Department of Chemistry, Center for Cell and Genome Science, University of Utah, 315 South 1400 East, Salt Lake City, Utah 84112-0850, United States.

出版信息

J Med Chem. 2015 Jun 11;58(11):4678-92. doi: 10.1021/acs.jmedchem.5b00223. Epub 2015 May 22.

Abstract

Acyl hydrazone is an important functional group for the discovery of bioactive small molecules. This functional group is also recognized as a pan assay interference structure. In this study, a new small-molecule inhibitor for the β-catenin/Tcf protein-protein interaction (PPI), ZINC02092166, was identified through AlphaScreen and FP assays. This compound contains an acyl hydrazone group and exhibits higher inhibitory activities in cell-based assays than biochemical assays. Inhibitor optimization resulted in chemically stable derivatives that disrupt the β-catenin/Tcf PPI. The binding mode of new inhibitors was characterized by site-directed mutagenesis and structure-activity relationship studies. This series of inhibitors with a new scaffold exhibits dual selectivity for β-catenin/Tcf over β-catenin/cadherin and β-catenin/APC PPIs. One derivative of this series suppresses canonical Wnt signaling, downregulates the expression of Wnt target genes, and inhibits the growth of cancer cells. This compound represents a solid starting point for the development of potent and selective β-catenin/Tcf inhibitors.

摘要

酰腙是发现生物活性小分子的重要官能团。该官能团也被认为是一种泛分析干扰结构。在本研究中,通过AlphaScreen和荧光偏振(FP)分析鉴定了一种用于β-连环蛋白/Tcf蛋白-蛋白相互作用(PPI)的新型小分子抑制剂ZINC02092166。该化合物含有一个酰腙基团,并且在基于细胞的分析中比生化分析表现出更高的抑制活性。抑制剂优化产生了破坏β-连环蛋白/Tcf PPI的化学稳定衍生物。通过定点诱变和构效关系研究对新型抑制剂的结合模式进行了表征。这一系列具有新骨架的抑制剂对β-连环蛋白/Tcf相对于β-连环蛋白/钙黏蛋白和β-连环蛋白/APC PPI表现出双重选择性。该系列的一种衍生物抑制经典Wnt信号传导,下调Wnt靶基因的表达,并抑制癌细胞的生长。该化合物是开发强效和选择性β-连环蛋白/Tcf抑制剂的坚实起点。

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