TRIM26 Facilitates HSV-2 Infection by Downregulating Antiviral Responses through the IRF3 Pathway

TRIM26 Facilitates HSV-2 Infection by Downregulating Antiviral Responses through the IRF3 Pathway

Herpes simplex virus type 2 (HSV-2) is the primary cause of genital herpes which results in significant morbidity and mortality, especially in women, worldwide. HSV-2 is transmitted primarily through infection of epithelial cells at skin and mucosal surfaces. Our earlier work to examine interactions...

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Main Authors: Tushar Dhawan, Muhammad Atif Zahoor, Nishant Heryani, Samuel Tekeste Workenhe, Aisha Nazli, Charu Kaushic
Format: Article
Language:English
Published: MDPI AG 2021-01-01
Series:Viruses
Subjects:
TRIM26
intrinsic immunity
interferon
ISG
HSV-2
epithelial cell
Online Access:https://www.mdpi.com/1999-4915/13/1/70
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spelling doaj-10e794423f8a433981ceec51ea666dda2021-01-07T00:04:09ZengMDPI AGViruses1999-49152021-01-0113707010.3390/v13010070TRIM26 Facilitates HSV-2 Infection by Downregulating Antiviral Responses through the IRF3 PathwayTushar Dhawan0Muhammad Atif Zahoor1Nishant Heryani2Samuel Tekeste Workenhe3Aisha Nazli4Charu Kaushic5Department of Pathology and Molecular Medicine, McMaster University, Hamilton, ON L8S 4M3, CanadaDepartment of Pathology and Molecular Medicine, McMaster University, Hamilton, ON L8S 4M3, CanadaDepartment of Pathology and Molecular Medicine, McMaster University, Hamilton, ON L8S 4M3, CanadaDepartment of Pathobiology, Ontario Veterinary College, University of Guelph, Guelph, ON N1G 2W1, CanadaDepartment of Pathology and Molecular Medicine, McMaster University, Hamilton, ON L8S 4M3, CanadaDepartment of Pathology and Molecular Medicine, McMaster University, Hamilton, ON L8S 4M3, CanadaHerpes simplex virus type 2 (HSV-2) is the primary cause of genital herpes which results in significant morbidity and mortality, especially in women, worldwide. HSV-2 is transmitted primarily through infection of epithelial cells at skin and mucosal surfaces. Our earlier work to examine interactions between HSV-2 and vaginal epithelial cells demonstrated that infection of the human vaginal epithelial cell line (VK2) with HSV-2 resulted in increased expression of TRIM26, a negative regulator of the Type I interferon pathway. Given that upregulation of TRIM26 could negatively affect anti-viral pathways, we decided to further study the role of TRIM26 in HSV-2 infection and replication. To do this, we designed and generated two cell lines derived from VK2s with TRIM26 overexpressed (OE) and knocked out (KO). Both, along with wildtype (WT) VK2, were infected with HSV-2 and viral titres were measured in supernatants 24 h later. Our results showed significantly enhanced virus production by TRIM26 OE cells, but very little replication in TRIM26 KO cells. We next examined interferon-β production and expression of two distinct interferon stimulated genes (ISGs), MX1 and ISG15, in all three cell lines, prior to and following HSV-2 infection. The absence of TRIM26 (KO) significantly upregulated interferon-β production at baseline and even further after HSV-2 infection. TRIM26 KO cells also showed significant increase in the expression of MX1 and ISG15 before and after HSV-2 infection. Immunofluorescent staining indicated that overexpression of TRIM26 substantially decreased the nuclear localization of IRF3, the primary mediator of ISG activation, before and after HSV-2 infection. Taken together, our data indicate that HSV-2 utilizes host factor TRIM26 to evade anti-viral response and thereby increase its replication in vaginal epithelial cells.https://www.mdpi.com/1999-4915/13/1/70TRIM26intrinsic immunityinterferonISGHSV-2epithelial cell
collection DOAJ
language English
format Article
sources DOAJ
author Tushar Dhawan
Muhammad Atif Zahoor
Nishant Heryani
Samuel Tekeste Workenhe
Aisha Nazli
Charu Kaushic
spellingShingle Tushar Dhawan
Muhammad Atif Zahoor
Nishant Heryani
Samuel Tekeste Workenhe
Aisha Nazli
Charu Kaushic
TRIM26 Facilitates HSV-2 Infection by Downregulating Antiviral Responses through the IRF3 Pathway
Viruses
TRIM26
intrinsic immunity
interferon
ISG
HSV-2
epithelial cell
author_facet Tushar Dhawan
Muhammad Atif Zahoor
Nishant Heryani
Samuel Tekeste Workenhe
Aisha Nazli
Charu Kaushic
author_sort Tushar Dhawan
title TRIM26 Facilitates HSV-2 Infection by Downregulating Antiviral Responses through the IRF3 Pathway
title_short TRIM26 Facilitates HSV-2 Infection by Downregulating Antiviral Responses through the IRF3 Pathway
title_full TRIM26 Facilitates HSV-2 Infection by Downregulating Antiviral Responses through the IRF3 Pathway
title_fullStr TRIM26 Facilitates HSV-2 Infection by Downregulating Antiviral Responses through the IRF3 Pathway
title_full_unstemmed TRIM26 Facilitates HSV-2 Infection by Downregulating Antiviral Responses through the IRF3 Pathway
title_sort trim26 facilitates hsv-2 infection by downregulating antiviral responses through the irf3 pathway
publisher MDPI AG
series Viruses
issn 1999-4915
publishDate 2021-01-01
description Herpes simplex virus type 2 (HSV-2) is the primary cause of genital herpes which results in significant morbidity and mortality, especially in women, worldwide. HSV-2 is transmitted primarily through infection of epithelial cells at skin and mucosal surfaces. Our earlier work to examine interactions between HSV-2 and vaginal epithelial cells demonstrated that infection of the human vaginal epithelial cell line (VK2) with HSV-2 resulted in increased expression of TRIM26, a negative regulator of the Type I interferon pathway. Given that upregulation of TRIM26 could negatively affect anti-viral pathways, we decided to further study the role of TRIM26 in HSV-2 infection and replication. To do this, we designed and generated two cell lines derived from VK2s with TRIM26 overexpressed (OE) and knocked out (KO). Both, along with wildtype (WT) VK2, were infected with HSV-2 and viral titres were measured in supernatants 24 h later. Our results showed significantly enhanced virus production by TRIM26 OE cells, but very little replication in TRIM26 KO cells. We next examined interferon-β production and expression of two distinct interferon stimulated genes (ISGs), MX1 and ISG15, in all three cell lines, prior to and following HSV-2 infection. The absence of TRIM26 (KO) significantly upregulated interferon-β production at baseline and even further after HSV-2 infection. TRIM26 KO cells also showed significant increase in the expression of MX1 and ISG15 before and after HSV-2 infection. Immunofluorescent staining indicated that overexpression of TRIM26 substantially decreased the nuclear localization of IRF3, the primary mediator of ISG activation, before and after HSV-2 infection. Taken together, our data indicate that HSV-2 utilizes host factor TRIM26 to evade anti-viral response and thereby increase its replication in vaginal epithelial cells.
topic TRIM26
intrinsic immunity
interferon
ISG
HSV-2
epithelial cell
url https://www.mdpi.com/1999-4915/13/1/70
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AT nishantheryani trim26facilitateshsv2infectionbydownregulatingantiviralresponsesthroughtheirf3pathway
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