Issue 9, 2019
From the journal:

RSC Advances

Discovery of trisubstituted nicotinonitrile derivatives as novel human GCN5 inhibitors through AlphaScreen-based high throughput screening

Hongru Tao,ac   Jun Wang,bc   Wenchao Lu, ORCID logo cd   Rukang Zhang,cd   Yiqian Xie,c   Yu-Chih Liu,f   Rongfeng Liu,f   Liyan Yue,c   Kaixian Chen,cdg   Hualiang Jiang,cd   Yuanyuan Zhang, ORCID logo *c   Xiaohui Xu*a  and  Cheng Luo ORCID logo *ceg  

* Corresponding authors

a School of Life Sciences, Shanghai University, 99 Shangda Road, Shanghai 200444, China
E-mail: xxhxxh@shu.edu.cn

b Jiangsu Key Laboratory for High Technology Research of TCM Formulae, Nanjing University of Chinese Medicine, 138 Xianlin Road, Nanjing 210023, China

c State Key Laboratory of Drug Research, CAS Key Laboratory of Receptor Research, Shanghai Institute of Materia Medica, Chinese Academy of Sciences, 555 Zuchongzhi Road, Shanghai 201203, China
E-mail: zhangyy@simm.ac.cn, cluo@mail.shcnc.ac.cn

d University of Chinese Academy of Sciences, Beijing 100049, China

e School of Life Science and Technology, ShanghaiTech University, 100 Haike Road, Shanghai 201210, China

f In Vitro Biology, Shanghai ChemPartner Life Science Co., Ltd., #5 Building, 998 Halei Road, Shanghai 201203, China

g Open Studio for Druggability Research of Marine Natural Products, Pilot National Laboratory for Marine Science and Technology (Qingdao), 1 Wenhai Road, Aoshanwei, Jimo, Qingdao 266237, China

Abstract

The general control nonrepressed protein 5 (GCN5) is an important target for drug design and drug discovery largely owing to its pathogenic role in malignancies. Chemical probes that target GCN5 have been developed in recent decades, but their potencies are still unsatisfactory. In this study, through an in-house developed AlphaScreen-based high throughput screening platform, radioactive acetylation assays and 2D-similarity based analogue searching, we discovered DC_HG24-01 as the novel hGCN5 inhibitor with the IC50 value of 3.1 ± 0.2 μM. Further docking studies suggested that DC_HG24-01 could occupy the binding pocket of acetyl-CoA cofactor, which laid the foundation for the development of more potent hGCN5 inhibitors in the future. At the cellular level, DC_HG24-01 could retard cell proliferation and block the acetylation of H3K14 leading to cell apoptosis and cell cycle arrest at the G1 phase in MV4-11 cell lines. Taken together, the discovery of DC_HG24-01 may serve as a good starting point to accelerate the development of more potent hGCN5 inhibitors through further structural decoration and provide new insight into the pharmacological treatment of leukemia.

Graphical abstract: Discovery of trisubstituted nicotinonitrile derivatives as novel human GCN5 inhibitors through AlphaScreen-based high throughput screening

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Article information

DOI
https://doi.org/10.1039/C8RA10074H
Article type
Paper
Submitted
07 Dec 2018
Accepted
07 Jan 2019
First published
08 Feb 2019
This article is Open Access
Creative Commons BY-NC license

RSC Adv., 2019,9, 4917-4924

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Discovery of trisubstituted nicotinonitrile derivatives as novel human GCN5 inhibitors through AlphaScreen-based high throughput screening

H. Tao, J. Wang, W. Lu, R. Zhang, Y. Xie, Y. Liu, R. Liu, L. Yue, K. Chen, H. Jiang, Y. Zhang, X. Xu and C. Luo, RSC Adv., 2019, 9, 4917 DOI: 10.1039/C8RA10074H

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