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A Small-Molecule Dengue Virus Entry Inhibitor
Author(s) -
Qingyin Wang,
Sejal Patel,
Eric Vangrevelinghe,
Hao Xu,
Ranga Rao,
Deana Jaber,
Wouter Schul,
Feng Gu,
Olivier Heudi,
Ngai Ling,
Mee Kian Poh,
Wai Yee Phong,
Thomas H. Keller,
Edgar Jacoby,
Subhash G. Vasudevan
Publication year - 2009
Publication title -
antimicrobial agents and chemotherapy
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.07
H-Index - 259
eISSN - 1070-6283
pISSN - 0066-4804
DOI - 10.1128/aac.01148-08
Subject(s) - dengue virus , dengue fever , flavivirus , antibody dependent enhancement , virology , dengue vaccine , virus , viral entry , lipid bilayer fusion , entry inhibitor , viral envelope , biology , ns3 , docking (animal) , chemistry , viral replication , hepatitis c virus , medicine , nursing
The incidence of dengue fever epidemics has increased dramatically over the last few decades. However, no vaccine or antiviral therapies are available. Therefore, the need for safe and effective antiviral drugs has become imperative. The entry of dengue virus into a host cell is mediated by its major envelope (E) protein. The crystal structure of the E protein reveals a hydrophobic pocket that is presumably important for low-pH-mediated membrane fusion. High-throughput docking with this hydrophobic pocket was performed, and hits were evaluated in cell-based assays. Compound 6 was identified as one of the inhibitors and had an average 50% effective concentration of 119 nM against dengue virus serotype 2 in a human cell line. Mechanism-of-action studies demonstrated that compound 6 acts at an early stage during dengue virus infection. It arrests dengue virus in vesicles that colocalize with endocytosed dextran and inhibits NS3 expression. The inhibitors described in this report can serve as molecular probes for the study of the entry of flavivirus into host cells.

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