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Characterization of a dengue NS4B inhibitor originating from an HCV small molecule library

Authors :
Ilane Hernandez-Morales
Peggy Geluykens
Marleen Clynhens
Rudy Strijbos
Olivia Goethals
Sarah Megens
Nick Verheyen
Stefaan Last
David McGowan
Erwin Coesemans
Benoît De Boeck
Bart Stoops
Benoit Devogelaere
Frederik Pauwels
Koen Vandyck
Jan Martin Berke
Pierre Raboisson
Kenneth Simmen
Pedro Lory
Marnix Van Loock
Source :
Antiviral research. 147
Publication Year :
2017

Abstract

Dengue is the most important mosquito-transmitted viral disease and a major global health concern. Over the last decade, dengue virus (DENV) drug discovery and development has intensified, however, this has not resulted in approved DENV-specific antiviral treatments yet. DENV and hepatitis C virus (HCV) belong to the same Flaviviridae family and, in contrast to DENV, antiviral treatments for HCV have been licensed. Therefore, applying the knowledge gained on anti-HCV drugs may foster the discovery and development of dengue antiviral drugs. Here, we screened a library of compounds with established anti-HCV activity in a DENV-2 sub-genomic replicon inhibition assay and selected compounds with single-digit micromolar activity. These compounds were advanced into a hit-to-lead medicinal chemistry program resulting in lead compound JNJ-1A, which inhibited the DENV-2 sub-genomic replicon at 0.7 μM, in the absence of cytotoxicity. In addition, JNJ-1A showed equipotent antiviral activity against DENV serotypes 1, 2, and 4. In vitro resistance selection experiments with JNJ-1A induced mutation T108I in non-structural protein 4B (NS4B), pointing towards a mechanism of action linked to this protein. Collectively, we described the discovery and characterization of a novel DENV inhibitor potentially targeting NS4B.

Details

ISSN :
18729096
Volume :
147
Database :
OpenAIRE
Journal :
Antiviral research
Accession number :
edsair.doi.dedup.....a6caa7a244de6b850d843aa7cef9ecf9