Targeting Coronaviral Replication and Cellular JAK2 Mediated Dominant NF-κB Activation for Comprehensive and Ultimate Inhibition of Coronaviral Activity

Targeting Coronaviral Replication and Cellular JAK2 Mediated Dominant NF-κB Activation for Comprehensive and Ultimate Inhibition of Coronaviral Activity

Abstract Tylophorine-based compounds exert broad spectral, potent inhibition of coronaviruses. NF-κB activation is a common pro-inflammatory response of host cells to viral infection. The aims of this study were to (i) find an effective combination treatment for coronaviral infections through target...

Full description

Bibliographic Details
Main Authors: Cheng-Wei Yang, Yue-Zhi Lee, Hsing-Yu Hsu, Chuan Shih, Yu-Sheng Chao, Hwan-You Chang, Shiow-Ju Lee
Format: Article
Language:English
Published: Nature Publishing Group 2017-06-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-017-04203-9
id doaj-b63a6fb1851b4cd1a9d7bcee891a97ec
record_format Article
spelling doaj-b63a6fb1851b4cd1a9d7bcee891a97ec2020-12-08T01:16:12ZengNature Publishing GroupScientific Reports2045-23222017-06-017111310.1038/s41598-017-04203-9Targeting Coronaviral Replication and Cellular JAK2 Mediated Dominant NF-κB Activation for Comprehensive and Ultimate Inhibition of Coronaviral ActivityCheng-Wei Yang0Yue-Zhi Lee1Hsing-Yu Hsu2Chuan Shih3Yu-Sheng Chao4Hwan-You Chang5Shiow-Ju Lee6Institute of Biotechnology and Pharmaceutical Research, National Health Research InstitutesInstitute of Biotechnology and Pharmaceutical Research, National Health Research InstitutesInstitute of Biotechnology and Pharmaceutical Research, National Health Research InstitutesInstitute of Biotechnology and Pharmaceutical Research, National Health Research InstitutesInstitute of Biotechnology and Pharmaceutical Research, National Health Research InstitutesInstitute of Molecular Medicine, National Tsing Hua UniversityInstitute of Biotechnology and Pharmaceutical Research, National Health Research InstitutesAbstract Tylophorine-based compounds exert broad spectral, potent inhibition of coronaviruses. NF-κB activation is a common pro-inflammatory response of host cells to viral infection. The aims of this study were to (i) find an effective combination treatment for coronaviral infections through targeting of the virus per se and cellular NF-κB activity; and (ii) to study the underling mechanisms. We found that tylophorine-based compounds target the TGEV viral RNA and effectively inhibit TGEV replication. NF-κB inhibition also leads to anti-TGEV replication. NF-κB activation induced by TGEV infection was found to be associated with two convergent pathways, IKK-2_IκBα/p65 and JAK2 mediated p65 phosphorylation, in swine testicular cells. JAK2 inhibition either by CYT387 (a JAK family inhibitor) or by silencing JAK2-expression revealed a dominant JAK2 mediated p65 phosphorylation pathway for NF-κB activation and resulted in NF-κB inhibition, which overrode the IκBα regulation via the IKK-2. Finally, tylophorine-based compounds work cooperatively with CYT387 to impart comprehensive anti-TGEV activities. The combination treatment, wherein a tylophorine compound targets TGEV and a JAK2 inhibitor blocks the alternative dominant NF-κB activation mediated by JAK2, is more effective and comprehensive than either one alone and constitutes a feasible approach for the treatment of SARS-CoV or MERS-CoV.https://doi.org/10.1038/s41598-017-04203-9
collection DOAJ
language English
format Article
sources DOAJ
author Cheng-Wei Yang
Yue-Zhi Lee
Hsing-Yu Hsu
Chuan Shih
Yu-Sheng Chao
Hwan-You Chang
Shiow-Ju Lee
spellingShingle Cheng-Wei Yang
Yue-Zhi Lee
Hsing-Yu Hsu
Chuan Shih
Yu-Sheng Chao
Hwan-You Chang
Shiow-Ju Lee
Targeting Coronaviral Replication and Cellular JAK2 Mediated Dominant NF-κB Activation for Comprehensive and Ultimate Inhibition of Coronaviral Activity
Scientific Reports
author_facet Cheng-Wei Yang
Yue-Zhi Lee
Hsing-Yu Hsu
Chuan Shih
Yu-Sheng Chao
Hwan-You Chang
Shiow-Ju Lee
author_sort Cheng-Wei Yang
title Targeting Coronaviral Replication and Cellular JAK2 Mediated Dominant NF-κB Activation for Comprehensive and Ultimate Inhibition of Coronaviral Activity
title_short Targeting Coronaviral Replication and Cellular JAK2 Mediated Dominant NF-κB Activation for Comprehensive and Ultimate Inhibition of Coronaviral Activity
title_full Targeting Coronaviral Replication and Cellular JAK2 Mediated Dominant NF-κB Activation for Comprehensive and Ultimate Inhibition of Coronaviral Activity
title_fullStr Targeting Coronaviral Replication and Cellular JAK2 Mediated Dominant NF-κB Activation for Comprehensive and Ultimate Inhibition of Coronaviral Activity
title_full_unstemmed Targeting Coronaviral Replication and Cellular JAK2 Mediated Dominant NF-κB Activation for Comprehensive and Ultimate Inhibition of Coronaviral Activity
title_sort targeting coronaviral replication and cellular jak2 mediated dominant nf-κb activation for comprehensive and ultimate inhibition of coronaviral activity
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2017-06-01
description Abstract Tylophorine-based compounds exert broad spectral, potent inhibition of coronaviruses. NF-κB activation is a common pro-inflammatory response of host cells to viral infection. The aims of this study were to (i) find an effective combination treatment for coronaviral infections through targeting of the virus per se and cellular NF-κB activity; and (ii) to study the underling mechanisms. We found that tylophorine-based compounds target the TGEV viral RNA and effectively inhibit TGEV replication. NF-κB inhibition also leads to anti-TGEV replication. NF-κB activation induced by TGEV infection was found to be associated with two convergent pathways, IKK-2_IκBα/p65 and JAK2 mediated p65 phosphorylation, in swine testicular cells. JAK2 inhibition either by CYT387 (a JAK family inhibitor) or by silencing JAK2-expression revealed a dominant JAK2 mediated p65 phosphorylation pathway for NF-κB activation and resulted in NF-κB inhibition, which overrode the IκBα regulation via the IKK-2. Finally, tylophorine-based compounds work cooperatively with CYT387 to impart comprehensive anti-TGEV activities. The combination treatment, wherein a tylophorine compound targets TGEV and a JAK2 inhibitor blocks the alternative dominant NF-κB activation mediated by JAK2, is more effective and comprehensive than either one alone and constitutes a feasible approach for the treatment of SARS-CoV or MERS-CoV.
url https://doi.org/10.1038/s41598-017-04203-9
work_keys_str_mv AT chengweiyang targetingcoronaviralreplicationandcellularjak2mediateddominantnfkbactivationforcomprehensiveandultimateinhibitionofcoronaviralactivity
AT yuezhilee targetingcoronaviralreplicationandcellularjak2mediateddominantnfkbactivationforcomprehensiveandultimateinhibitionofcoronaviralactivity
AT hsingyuhsu targetingcoronaviralreplicationandcellularjak2mediateddominantnfkbactivationforcomprehensiveandultimateinhibitionofcoronaviralactivity
AT chuanshih targetingcoronaviralreplicationandcellularjak2mediateddominantnfkbactivationforcomprehensiveandultimateinhibitionofcoronaviralactivity
AT yushengchao targetingcoronaviralreplicationandcellularjak2mediateddominantnfkbactivationforcomprehensiveandultimateinhibitionofcoronaviralactivity
AT hwanyouchang targetingcoronaviralreplicationandcellularjak2mediateddominantnfkbactivationforcomprehensiveandultimateinhibitionofcoronaviralactivity
AT shiowjulee targetingcoronaviralreplicationandcellularjak2mediateddominantnfkbactivationforcomprehensiveandultimateinhibitionofcoronaviralactivity
_version_ 1724395176877621248

Similar Items