Identification of three antiviral inhibitors against Japanese encephalitis virus from library of pharmacologically active compounds 1280.

Identification of three antiviral inhibitors against Japanese encephalitis virus from library of pharmacologically active compounds 1280.

Japanese encephalitis virus (JEV) can cause severe central nervous disease with a high mortality rate. There is no antiviral drug available for JEV-specific treatment. In this study, a cytopathic-effect-based, high-throughput screening assay was developed and applied to screen JEV inhibitors from Li...

Full description

Bibliographic Details
Main Authors: Jin'e Fang, Leqiang Sun, Guiqing Peng, Jia Xu, Rui Zhou, Shengbo Cao, Huanchun Chen, Yunfeng Song
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3857149?pdf=render
id doaj-a3bd7bf3c7354f44bdad0f9ef9611b3e
record_format Article
spelling doaj-a3bd7bf3c7354f44bdad0f9ef9611b3e2020-11-25T01:24:51ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-01811e7842510.1371/journal.pone.0078425Identification of three antiviral inhibitors against Japanese encephalitis virus from library of pharmacologically active compounds 1280.Jin'e FangLeqiang SunGuiqing PengJia XuRui ZhouShengbo CaoHuanchun ChenYunfeng SongJapanese encephalitis virus (JEV) can cause severe central nervous disease with a high mortality rate. There is no antiviral drug available for JEV-specific treatment. In this study, a cytopathic-effect-based, high-throughput screening assay was developed and applied to screen JEV inhibitors from Library of Pharmacologically Active Compounds 1280. The antiviral effects of three hit compounds including FGIN-1-27, cilnidipine, and niclosamide were evaluated in cells by western blotting, indirect immunofluorescence assay, and plaque reduction assay. A time-of-addition assay proved that all three compounds inhibited JEV at the stage of replication. The EC50s of FGIN-1-27, cilnidipine, and niclosamide were 3.21, 6.52, and 5.80 µM, respectively, while the selectivity indexes were 38.79, 30.67, and 7.49. FGIN-1-27 and cilnidipine have high efficiency and selectivity against JEV. This study provided two JEV antiviral inhibitors as candidates for treatment of JEV infection.http://europepmc.org/articles/PMC3857149?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Jin'e Fang
Leqiang Sun
Guiqing Peng
Jia Xu
Rui Zhou
Shengbo Cao
Huanchun Chen
Yunfeng Song
spellingShingle Jin'e Fang
Leqiang Sun
Guiqing Peng
Jia Xu
Rui Zhou
Shengbo Cao
Huanchun Chen
Yunfeng Song
Identification of three antiviral inhibitors against Japanese encephalitis virus from library of pharmacologically active compounds 1280.
PLoS ONE
author_facet Jin'e Fang
Leqiang Sun
Guiqing Peng
Jia Xu
Rui Zhou
Shengbo Cao
Huanchun Chen
Yunfeng Song
author_sort Jin'e Fang
title Identification of three antiviral inhibitors against Japanese encephalitis virus from library of pharmacologically active compounds 1280.
title_short Identification of three antiviral inhibitors against Japanese encephalitis virus from library of pharmacologically active compounds 1280.
title_full Identification of three antiviral inhibitors against Japanese encephalitis virus from library of pharmacologically active compounds 1280.
title_fullStr Identification of three antiviral inhibitors against Japanese encephalitis virus from library of pharmacologically active compounds 1280.
title_full_unstemmed Identification of three antiviral inhibitors against Japanese encephalitis virus from library of pharmacologically active compounds 1280.
title_sort identification of three antiviral inhibitors against japanese encephalitis virus from library of pharmacologically active compounds 1280.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Japanese encephalitis virus (JEV) can cause severe central nervous disease with a high mortality rate. There is no antiviral drug available for JEV-specific treatment. In this study, a cytopathic-effect-based, high-throughput screening assay was developed and applied to screen JEV inhibitors from Library of Pharmacologically Active Compounds 1280. The antiviral effects of three hit compounds including FGIN-1-27, cilnidipine, and niclosamide were evaluated in cells by western blotting, indirect immunofluorescence assay, and plaque reduction assay. A time-of-addition assay proved that all three compounds inhibited JEV at the stage of replication. The EC50s of FGIN-1-27, cilnidipine, and niclosamide were 3.21, 6.52, and 5.80 µM, respectively, while the selectivity indexes were 38.79, 30.67, and 7.49. FGIN-1-27 and cilnidipine have high efficiency and selectivity against JEV. This study provided two JEV antiviral inhibitors as candidates for treatment of JEV infection.
url http://europepmc.org/articles/PMC3857149?pdf=render
work_keys_str_mv AT jinefang identificationofthreeantiviralinhibitorsagainstjapaneseencephalitisvirusfromlibraryofpharmacologicallyactivecompounds1280
AT leqiangsun identificationofthreeantiviralinhibitorsagainstjapaneseencephalitisvirusfromlibraryofpharmacologicallyactivecompounds1280
AT guiqingpeng identificationofthreeantiviralinhibitorsagainstjapaneseencephalitisvirusfromlibraryofpharmacologicallyactivecompounds1280
AT jiaxu identificationofthreeantiviralinhibitorsagainstjapaneseencephalitisvirusfromlibraryofpharmacologicallyactivecompounds1280
AT ruizhou identificationofthreeantiviralinhibitorsagainstjapaneseencephalitisvirusfromlibraryofpharmacologicallyactivecompounds1280
AT shengbocao identificationofthreeantiviralinhibitorsagainstjapaneseencephalitisvirusfromlibraryofpharmacologicallyactivecompounds1280
AT huanchunchen identificationofthreeantiviralinhibitorsagainstjapaneseencephalitisvirusfromlibraryofpharmacologicallyactivecompounds1280
AT yunfengsong identificationofthreeantiviralinhibitorsagainstjapaneseencephalitisvirusfromlibraryofpharmacologicallyactivecompounds1280
_version_ 1725116685442088960

Similar Items