Design, Solid-Phase Synthesis, and Evaluation of a Phenyl-Piperazine-Triazine Scaffold as α-Helix Mimetics

被引:19
|
作者
Moon, Heejo [1 ]
Lee, Woo Sirl [1 ]
Oh, Misook [1 ,2 ]
Lee, Huisun [3 ,4 ]
Lee, Ji Hoon [1 ]
Im, Wonpil [3 ,4 ]
Lim, Hyun-Suk [1 ,2 ]
机构
[1] Pohang Univ Sci & Technol, Dept Chem, Pohang 790784, South Korea
[2] Indiana Univ, Sch Med, Dept Biochem & Mol Biol, Indianapolis, IN 46032 USA
[3] Univ Kansas, Dept Mol Biosci, Lawrence, KS 66047 USA
[4] Univ Kansas, Ctr Bioinformat, Lawrence, KS 66047 USA
基金
美国国家科学基金会; 新加坡国家研究基金会;
关键词
alpha-helix mimetics; solid-phase synthesis; combinatorial library; protein-protein interaction inhibitor; PROTEIN-PROTEIN INTERACTIONS; SMALL-MOLECULE INHIBITORS; DRUG DISCOVERY; MCL-1; DERIVATIVES; MIMICS; STRATEGIES; INTERFACES; PEPTIDES; AGENTS;
D O I
10.1021/co500114f
中图分类号
O69 [应用化学];
学科分类号
081704 ;
摘要
alpha-Helices play a critical role in mediating many protein-protein interactions (PPIs) as recognition motifs. Therefore, there is a considerable interest in developing small molecules that can mimic helical peptide segments to modulate alpha-helix-mediated PPIs. Due to the relatively low aqueous solubility and synthetic difficulty of most current alpha-helix mimetic small molecules, one important goal in this area is to develop small molecules with favorable physicochemical properties and ease of synthesis. Here we designed phenyl-piperazine-triazine-based alpha-helix mimetics that possess improved water solubility and excellent synthetic accessibility. We developed a facile solid-phase synthetic route that allows for rapid creation of a large, diverse combinatorial library of alpha-helix mimetics. Further, we identified a selective inhibitor of the Mcl-1/BH3 interaction by screening a focused library of phenyl-piperazine-triazines, demonstrating that the scaffold is able to serve as functional mimetics of alpha-helical peptides. We believe that our phenyl-piperazine-triazine-based alpha-helix mimetics, along with the facile and divergent solid-phase synthetic method, have great potential as powerful tools for discovering potent inhibitors of given alpha-helix-mediated PPIs.
引用
收藏
页码:695 / 701
页数:7
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