Issue 22, 2015

State-of-the-art strategies for targeting protein–protein interactions by small-molecule inhibitors

Abstract

Targeting protein–protein interactions (PPIs) has emerged as a viable approach in modern drug discovery. However, the identification of small molecules enabling us to effectively interrupt their interactions presents significant challenges. In the recent past, significant advances have been made in the development of new biological and chemical strategies to facilitate the discovery process of small-molecule PPI inhibitors. This review aims to highlight the state-of-the-art technologies and the achievements made recently in this field. The “hot spots” of PPIs have been proved to be critical for small molecules to bind. Three strategies including screening, designing, and synthetic approaches have been explored for discovering PPI inhibitors by targeting the “hot spots”. Although the classic high throughput screening approach can be used, fragment screening, fragment-based drug design and newly improved virtual screening are demonstrated to be more effective in the discovery of PPI inhibitors. In addition to screening approaches, design strategies including anchor-based and small molecule mimetics of secondary structures involved in PPIs have become powerful tools as well. Finally, constructing new chemically spaced libraries with high diversity and complexity is becoming an important area of interest for PPI inhibitors. The successful cases from the recent five year studies are used to illustrate how these approaches are implemented to uncover and optimize small molecule PPI inhibitors and notably some of them have become promising therapeutics.

Graphical abstract: State-of-the-art strategies for targeting protein–protein interactions by small-molecule inhibitors

Associated articles

Article information

Article type
Review Article
Submitted
21 Mar 2015
First published
06 Aug 2015

Chem. Soc. Rev., 2015,44, 8238-8259

Author version available

State-of-the-art strategies for targeting protein–protein interactions by small-molecule inhibitors

C. Sheng, G. Dong, Z. Miao, W. Zhang and W. Wang, Chem. Soc. Rev., 2015, 44, 8238 DOI: 10.1039/C5CS00252D

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