Dengue virus NS1 secretion is regulated via importin-subunit β1 controlling expression of the chaperone GRp78 and targeted by the clinical drug ivermectin

Dengue virus (DENV) is a major human pathogen. An important pathogenicity factor is non-structural protein 1 (NS1) required for viral replication and secreted from infected cells. A clinical study indicated that the anti-parasitic drug ivermectin lowers NS1 blood levels without affecting viremia. Iv...

Descripción completa

Detalles Bibliográficos
Autores principales: Denolly, Solène, Guo, Hongbo, Martens, Miriam, Płaszczyca, Anna, Scaturro, Pietro, Prasad, Vibhu, Kongmanas, Kessiri, Punyadee, Nuntaya, Songjaeng, Adisak, Mairiang, Dumrong, Pichlmair, Andreas, Avirutnan, Panisadee, Bartenschlager, Ralf
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10653883/
https://www.ncbi.nlm.nih.gov/pubmed/37702492
http://dx.doi.org/10.1128/mbio.01441-23
_version_ 1785136509137977344
author Denolly, Solène
Guo, Hongbo
Martens, Miriam
Płaszczyca, Anna
Scaturro, Pietro
Prasad, Vibhu
Kongmanas, Kessiri
Punyadee, Nuntaya
Songjaeng, Adisak
Mairiang, Dumrong
Pichlmair, Andreas
Avirutnan, Panisadee
Bartenschlager, Ralf
author_facet Denolly, Solène
Guo, Hongbo
Martens, Miriam
Płaszczyca, Anna
Scaturro, Pietro
Prasad, Vibhu
Kongmanas, Kessiri
Punyadee, Nuntaya
Songjaeng, Adisak
Mairiang, Dumrong
Pichlmair, Andreas
Avirutnan, Panisadee
Bartenschlager, Ralf
author_sort Denolly, Solène
collection PubMed
description Dengue virus (DENV) is a major human pathogen. An important pathogenicity factor is non-structural protein 1 (NS1) required for viral replication and secreted from infected cells. A clinical study indicated that the anti-parasitic drug ivermectin lowers NS1 blood levels without affecting viremia. Ivermectin targets nuclear transport by binding to importin-α, but how NS1 secretion in patients is suppressed by this drug is unknown. We show that ivermectin impairs folding and secretion of endoplasmic reticulum-luminal glycoproteins, including NS1. Proteomic analysis identified chaperones interacting with NS1, including GRp78 (78-kDa glucose-regulated protein, also known as HSPA5 or BIP). This chaperone increased in abundance on DENV infection via activation of the unfolded protein response (UPR). Ivermectin blocked the nuclear transport of transcription factors required for UPR, thus impairing GRp78 upregulation and NS1 secretion. Reduction of GRp78 and NS1 secretion was also observed in patients treated with ivermectin. These results link nuclear transport and its inhibition by ivermectin to folding and secretion of luminal glycoproteins, including DENV NS1. IMPORTANCE: Dengue virus (DENV) is a major human pathogen that can cause hemorrhagic fever and shock syndrome. One important factor of DENV pathogenicity is non-structural protein 1 (NS1), a glycoprotein that is secreted from infected cells. Here we study the mode of action of the widely used drug ivermectin, used to treat parasitic infections and recently shown to lower NS1 blood levels in DENV-infected patients. We found that ivermectin blocks the nuclear transport of transcription factors required for the expression of chaperones that support the folding and secretion of glycoproteins, including NS1. Impairing nuclear transport of these transcription factors by ivermectin or depleting them from infected cells dampens NS1 folding and thus its secretion. These results reveal a novel mode of action of ivermectin that might apply to other flaviviruses as well.
format Online
Article
Text
id pubmed-10653883
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher American Society for Microbiology
record_format MEDLINE/PubMed
spelling pubmed-106538832023-09-13 Dengue virus NS1 secretion is regulated via importin-subunit β1 controlling expression of the chaperone GRp78 and targeted by the clinical drug ivermectin Denolly, Solène Guo, Hongbo Martens, Miriam Płaszczyca, Anna Scaturro, Pietro Prasad, Vibhu Kongmanas, Kessiri Punyadee, Nuntaya Songjaeng, Adisak Mairiang, Dumrong Pichlmair, Andreas Avirutnan, Panisadee Bartenschlager, Ralf mBio Research Article Dengue virus (DENV) is a major human pathogen. An important pathogenicity factor is non-structural protein 1 (NS1) required for viral replication and secreted from infected cells. A clinical study indicated that the anti-parasitic drug ivermectin lowers NS1 blood levels without affecting viremia. Ivermectin targets nuclear transport by binding to importin-α, but how NS1 secretion in patients is suppressed by this drug is unknown. We show that ivermectin impairs folding and secretion of endoplasmic reticulum-luminal glycoproteins, including NS1. Proteomic analysis identified chaperones interacting with NS1, including GRp78 (78-kDa glucose-regulated protein, also known as HSPA5 or BIP). This chaperone increased in abundance on DENV infection via activation of the unfolded protein response (UPR). Ivermectin blocked the nuclear transport of transcription factors required for UPR, thus impairing GRp78 upregulation and NS1 secretion. Reduction of GRp78 and NS1 secretion was also observed in patients treated with ivermectin. These results link nuclear transport and its inhibition by ivermectin to folding and secretion of luminal glycoproteins, including DENV NS1. IMPORTANCE: Dengue virus (DENV) is a major human pathogen that can cause hemorrhagic fever and shock syndrome. One important factor of DENV pathogenicity is non-structural protein 1 (NS1), a glycoprotein that is secreted from infected cells. Here we study the mode of action of the widely used drug ivermectin, used to treat parasitic infections and recently shown to lower NS1 blood levels in DENV-infected patients. We found that ivermectin blocks the nuclear transport of transcription factors required for the expression of chaperones that support the folding and secretion of glycoproteins, including NS1. Impairing nuclear transport of these transcription factors by ivermectin or depleting them from infected cells dampens NS1 folding and thus its secretion. These results reveal a novel mode of action of ivermectin that might apply to other flaviviruses as well. American Society for Microbiology 2023-09-13 /pmc/articles/PMC10653883/ /pubmed/37702492 http://dx.doi.org/10.1128/mbio.01441-23 Text en Copyright © 2023 Denolly et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Denolly, Solène
Guo, Hongbo
Martens, Miriam
Płaszczyca, Anna
Scaturro, Pietro
Prasad, Vibhu
Kongmanas, Kessiri
Punyadee, Nuntaya
Songjaeng, Adisak
Mairiang, Dumrong
Pichlmair, Andreas
Avirutnan, Panisadee
Bartenschlager, Ralf
Dengue virus NS1 secretion is regulated via importin-subunit β1 controlling expression of the chaperone GRp78 and targeted by the clinical drug ivermectin
title Dengue virus NS1 secretion is regulated via importin-subunit β1 controlling expression of the chaperone GRp78 and targeted by the clinical drug ivermectin
title_full Dengue virus NS1 secretion is regulated via importin-subunit β1 controlling expression of the chaperone GRp78 and targeted by the clinical drug ivermectin
title_fullStr Dengue virus NS1 secretion is regulated via importin-subunit β1 controlling expression of the chaperone GRp78 and targeted by the clinical drug ivermectin
title_full_unstemmed Dengue virus NS1 secretion is regulated via importin-subunit β1 controlling expression of the chaperone GRp78 and targeted by the clinical drug ivermectin
title_short Dengue virus NS1 secretion is regulated via importin-subunit β1 controlling expression of the chaperone GRp78 and targeted by the clinical drug ivermectin
title_sort dengue virus ns1 secretion is regulated via importin-subunit β1 controlling expression of the chaperone grp78 and targeted by the clinical drug ivermectin
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10653883/
https://www.ncbi.nlm.nih.gov/pubmed/37702492
http://dx.doi.org/10.1128/mbio.01441-23
work_keys_str_mv AT denollysolene denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT guohongbo denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT martensmiriam denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT płaszczycaanna denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT scaturropietro denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT prasadvibhu denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT kongmanaskessiri denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT punyadeenuntaya denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT songjaengadisak denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT mairiangdumrong denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT pichlmairandreas denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT avirutnanpanisadee denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin
AT bartenschlagerralf denguevirusns1secretionisregulatedviaimportinsubunitb1controllingexpressionofthechaperonegrp78andtargetedbytheclinicaldrugivermectin

Ejemplares similares