1,2,4-Oxadiazoles Identified by Virtual Screening and their Non-Covalent Inhibition of the Human 20S Proteasome

被引:24
作者
Marechal, X. [1 ]
Genin, E. [2 ]
Qin, L. [1 ]
Sperandio, O. [3 ]
Montes, M. [3 ]
Basse, N. [1 ]
Richy, N. [2 ]
Miteva, M. A.
Reboud-Ravaux, M. [1 ]
Vidal, J. [2 ]
Villoutreix, B. O. [3 ]
机构
[1] Univ Paris 04, UPMC, UR4, F-75252 Paris 05, France
[2] Univ Rennes 1, CNRS UMR 6226, CS 74205, F-35042 Rennes, France
[3] Univ Paris Diderot, INSERM, UMR S 973, F-75013 Paris, France
来源
CURRENT MEDICINAL CHEMISTRY | 2013年 / 20卷 / 18期
关键词
Chymotrypsin-like subsite S5 binding; cytotoxicity; non-covalent inhibitors; oxadiazoles; proteasome; virtual screening; TMC-95A ANALOGS; 3D CONFORMATION; DRUG DISCOVERY; BINDING MODE; OPTIMIZATION; DESIGN; BORTEZOMIB; KNOWLEDGE; PROTEINS; PROFILE;
D O I
10.2174/0929867311320180006
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Although several constitutive proteasome inhibitors have been reported these recent years, potent organic, non-covalent and readily available inhibitors are still poorly documented. Here we used a structure- and ligand-based in silico approach to identify commercially available 1,2,4-oxadiazole derivatives as non-covalent human 20S proteasome inhibitors. Their optimization led to the newly synthesized compound 4h that is a mixed proteasomal inhibitor of the chymotrypsin-like activity (K-i of 26,1 nM and K of 7.5 nM) which is in addition selective versus the challenging cathepsin B and calpain proteases. Molecular modelling studies corroborated the mechanism of inhibition and suggest an unusual binding of the inhibitor within the S5 binding pocket (beta 6 subunit). The cellular effects of our compounds validate their utility as potential pharmacological agents for anti-cancer pre-clinical studies.
引用
收藏
页码:2351 / 2362
页数:12
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