| Literature DB >> 29624387 |
Stephen J Capuzzi1, Wei Sun2, Eugene N Muratov1,3, Carles Martínez-Romero4,5, Shihua He6, Wenjun Zhu6,7, Hao Li2, Gregory Tawa2, Ethan G Fisher2, Miao Xu2, Paul Shinn2, Xiangguo Qiu6,7, Adolfo García-Sastre4,5,8, Wei Zheng2, Alexander Tropsha1.
Abstract
The Ebola virus (EBOV) causes severe human infection that lacks effective treatment. A recent screen identified a series of compounds that block EBOV-like particle entry into human cells. Using data from this screen, quantitative structure-activity relationship models were built and employed for virtual screening of a ∼17 million compound library. Experimental testing of 102 hits yielded 14 compounds with IC50 values under 10 μM, including several sub-micromolar inhibitors, and more than 10-fold selectivity against host cytotoxicity. These confirmed hits include FDA-approved drugs and clinical candidates with non-antiviral indications, as well as compounds with novel scaffolds and no previously known bioactivity. Five selected hits inhibited BSL-4 live-EBOV infection in a dose-dependent manner, including vindesine (0.34 μM). Additional studies of these novel anti-EBOV compounds revealed their mechanisms of action, including the inhibition of NPC1 protein, cathepsin B/L, and lysosomal function. Compounds identified in this study are among the most potent and well-characterized anti-EBOV inhibitors reported to date.Entities:
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Year: 2018 PMID: 29624387 PMCID: PMC6548547 DOI: 10.1021/acs.jmedchem.8b00035
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446