PML/TRIM19-Dependent Inhibition of Retroviral Reverse-Transcription by Daxx.

PML/TRIM19-Dependent Inhibition of Retroviral Reverse-Transcription by Daxx.

PML (Promyelocytic Leukemia protein), also known as TRIM19, belongs to the family of tripartite motif (TRIM) proteins. PML is mainly expressed in the nucleus, where it forms dynamic structures known as PML nuclear bodies that recruit many other proteins, such as Sp100 and Daxx. While the role of PML...

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Main Authors: Jacques Dutrieux, Ghizlane Maarifi, Débora M Portilho, Nathalie J Arhel, Mounira K Chelbi-Alix, Sébastien Nisole
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-11-01
Series:PLoS Pathogens
Online Access:https://doi.org/10.1371/journal.ppat.1005280
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spelling doaj-998264145afb4631841b8a87e03ac4902021-04-21T17:38:43ZengPublic Library of Science (PLoS)PLoS Pathogens1553-73661553-73742015-11-011111e100528010.1371/journal.ppat.1005280PML/TRIM19-Dependent Inhibition of Retroviral Reverse-Transcription by Daxx.Jacques DutrieuxGhizlane MaarifiDébora M PortilhoNathalie J ArhelMounira K Chelbi-AlixSébastien NisolePML (Promyelocytic Leukemia protein), also known as TRIM19, belongs to the family of tripartite motif (TRIM) proteins. PML is mainly expressed in the nucleus, where it forms dynamic structures known as PML nuclear bodies that recruit many other proteins, such as Sp100 and Daxx. While the role of PML/TRIM19 in antiviral defense is well documented, its effect on HIV-1 infection remains unclear. Here we show that infection by HIV-1 and other retroviruses triggers the formation of PML cytoplasmic bodies, as early as 30 minutes post-infection. Quantification of the number and size of PML cytoplasmic bodies revealed that they last approximately 8 h, with a peak at 2 h post-infection. PML re-localization is blocked by reverse-transcription inhibitors and is not observed following infection with unrelated viruses, suggesting it is specifically triggered by retroviral reverse-transcription. Furthermore, we show that PML interferes with an early step of retroviral infection since PML knockdown dramatically increases reverse-transcription efficiency. We demonstrate that PML does not inhibit directly retroviral infection but acts through the stabilization of one of its well-characterized partners, Daxx. In the presence of PML, cytoplasmic Daxx is found in the vicinity of incoming HIV-1 capsids and inhibits reverse-transcription. Interestingly, Daxx not only interferes with exogenous retroviral infections but can also inhibit retrotransposition of endogenous retroviruses, thus identifying Daxx as a broad cellular inhibitor of reverse-transcription. Altogether, these findings unravel a novel antiviral function for PML and PML nuclear body-associated protein Daxx.https://doi.org/10.1371/journal.ppat.1005280
collection DOAJ
language English
format Article
sources DOAJ
author Jacques Dutrieux
Ghizlane Maarifi
Débora M Portilho
Nathalie J Arhel
Mounira K Chelbi-Alix
Sébastien Nisole
spellingShingle Jacques Dutrieux
Ghizlane Maarifi
Débora M Portilho
Nathalie J Arhel
Mounira K Chelbi-Alix
Sébastien Nisole
PML/TRIM19-Dependent Inhibition of Retroviral Reverse-Transcription by Daxx.
PLoS Pathogens
author_facet Jacques Dutrieux
Ghizlane Maarifi
Débora M Portilho
Nathalie J Arhel
Mounira K Chelbi-Alix
Sébastien Nisole
author_sort Jacques Dutrieux
title PML/TRIM19-Dependent Inhibition of Retroviral Reverse-Transcription by Daxx.
title_short PML/TRIM19-Dependent Inhibition of Retroviral Reverse-Transcription by Daxx.
title_full PML/TRIM19-Dependent Inhibition of Retroviral Reverse-Transcription by Daxx.
title_fullStr PML/TRIM19-Dependent Inhibition of Retroviral Reverse-Transcription by Daxx.
title_full_unstemmed PML/TRIM19-Dependent Inhibition of Retroviral Reverse-Transcription by Daxx.
title_sort pml/trim19-dependent inhibition of retroviral reverse-transcription by daxx.
publisher Public Library of Science (PLoS)
series PLoS Pathogens
issn 1553-7366
1553-7374
publishDate 2015-11-01
description PML (Promyelocytic Leukemia protein), also known as TRIM19, belongs to the family of tripartite motif (TRIM) proteins. PML is mainly expressed in the nucleus, where it forms dynamic structures known as PML nuclear bodies that recruit many other proteins, such as Sp100 and Daxx. While the role of PML/TRIM19 in antiviral defense is well documented, its effect on HIV-1 infection remains unclear. Here we show that infection by HIV-1 and other retroviruses triggers the formation of PML cytoplasmic bodies, as early as 30 minutes post-infection. Quantification of the number and size of PML cytoplasmic bodies revealed that they last approximately 8 h, with a peak at 2 h post-infection. PML re-localization is blocked by reverse-transcription inhibitors and is not observed following infection with unrelated viruses, suggesting it is specifically triggered by retroviral reverse-transcription. Furthermore, we show that PML interferes with an early step of retroviral infection since PML knockdown dramatically increases reverse-transcription efficiency. We demonstrate that PML does not inhibit directly retroviral infection but acts through the stabilization of one of its well-characterized partners, Daxx. In the presence of PML, cytoplasmic Daxx is found in the vicinity of incoming HIV-1 capsids and inhibits reverse-transcription. Interestingly, Daxx not only interferes with exogenous retroviral infections but can also inhibit retrotransposition of endogenous retroviruses, thus identifying Daxx as a broad cellular inhibitor of reverse-transcription. Altogether, these findings unravel a novel antiviral function for PML and PML nuclear body-associated protein Daxx.
url https://doi.org/10.1371/journal.ppat.1005280
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