Revisiting promyelocytic leukemia protein targeting by human cytomegalovirus immediate-early protein 1

Promyelocytic leukemia (PML) bodies are nuclear organelles implicated in intrinsic and innate antiviral defense. The eponymous PML proteins, central to the self-organization of PML bodies, and other restriction factors found in these organelles are common targets of viral antagonism. The 72-kDa imme...

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Autores principales: Paulus, Christina, Harwardt, Thomas, Walter, Bernadette, Marxreiter, Andrea, Zenger, Marion, Reuschel, Edith, Nevels, Michael M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2020
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7224577/
https://www.ncbi.nlm.nih.gov/pubmed/32365141
http://dx.doi.org/10.1371/journal.ppat.1008537
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author Paulus, Christina
Harwardt, Thomas
Walter, Bernadette
Marxreiter, Andrea
Zenger, Marion
Reuschel, Edith
Nevels, Michael M.
author_facet Paulus, Christina
Harwardt, Thomas
Walter, Bernadette
Marxreiter, Andrea
Zenger, Marion
Reuschel, Edith
Nevels, Michael M.
author_sort Paulus, Christina
collection PubMed
description Promyelocytic leukemia (PML) bodies are nuclear organelles implicated in intrinsic and innate antiviral defense. The eponymous PML proteins, central to the self-organization of PML bodies, and other restriction factors found in these organelles are common targets of viral antagonism. The 72-kDa immediate-early protein 1 (IE1) is the principal antagonist of PML bodies encoded by the human cytomegalovirus (hCMV). IE1 is believed to disrupt PML bodies by inhibiting PML SUMOylation, while PML was proposed to act as an E3 ligase for IE1 SUMOylation. PML targeting by IE1 is considered to be crucial for hCMV replication at low multiplicities of infection, in part via counteracting antiviral gene induction linked to the cellular interferon (IFN) response. However, current concepts of IE1-PML interaction are largely derived from mutant IE1 proteins known or predicted to be metabolically unstable and globally misfolded. We performed systematic clustered charge-to-alanine scanning mutagenesis and identified a stable IE1 mutant protein (IE1cc172-176) with wild-type characteristics except for neither interacting with PML proteins nor inhibiting PML SUMOylation. Consequently, IE1cc172-176 does not associate with PML bodies and is selectively impaired for disrupting these organelles. Surprisingly, functional analysis of IE1cc172-176 revealed that the protein is hypermodified by mixed SUMO chains and that IE1 SUMOylation depends on nucleosome rather than PML binding. Furthermore, a mutant hCMV expressing IE1cc172-176 was only slightly attenuated compared to an IE1-null virus even at low multiplicities of infection. Finally, hCMV-induced expression of cytokine and IFN-stimulated genes turned out to be reduced rather than increased in the presence of IE1cc172-176 relative to wild-type IE1. Our findings challenge present views on the relationship of IE1 with PML and the role of PML in hCMV replication. This study also provides initial evidence for the idea that disruption of PML bodies upon viral infection is linked to activation rather than inhibition of innate immunity.
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spelling pubmed-72245772020-06-01 Revisiting promyelocytic leukemia protein targeting by human cytomegalovirus immediate-early protein 1 Paulus, Christina Harwardt, Thomas Walter, Bernadette Marxreiter, Andrea Zenger, Marion Reuschel, Edith Nevels, Michael M. PLoS Pathog Research Article Promyelocytic leukemia (PML) bodies are nuclear organelles implicated in intrinsic and innate antiviral defense. The eponymous PML proteins, central to the self-organization of PML bodies, and other restriction factors found in these organelles are common targets of viral antagonism. The 72-kDa immediate-early protein 1 (IE1) is the principal antagonist of PML bodies encoded by the human cytomegalovirus (hCMV). IE1 is believed to disrupt PML bodies by inhibiting PML SUMOylation, while PML was proposed to act as an E3 ligase for IE1 SUMOylation. PML targeting by IE1 is considered to be crucial for hCMV replication at low multiplicities of infection, in part via counteracting antiviral gene induction linked to the cellular interferon (IFN) response. However, current concepts of IE1-PML interaction are largely derived from mutant IE1 proteins known or predicted to be metabolically unstable and globally misfolded. We performed systematic clustered charge-to-alanine scanning mutagenesis and identified a stable IE1 mutant protein (IE1cc172-176) with wild-type characteristics except for neither interacting with PML proteins nor inhibiting PML SUMOylation. Consequently, IE1cc172-176 does not associate with PML bodies and is selectively impaired for disrupting these organelles. Surprisingly, functional analysis of IE1cc172-176 revealed that the protein is hypermodified by mixed SUMO chains and that IE1 SUMOylation depends on nucleosome rather than PML binding. Furthermore, a mutant hCMV expressing IE1cc172-176 was only slightly attenuated compared to an IE1-null virus even at low multiplicities of infection. Finally, hCMV-induced expression of cytokine and IFN-stimulated genes turned out to be reduced rather than increased in the presence of IE1cc172-176 relative to wild-type IE1. Our findings challenge present views on the relationship of IE1 with PML and the role of PML in hCMV replication. This study also provides initial evidence for the idea that disruption of PML bodies upon viral infection is linked to activation rather than inhibition of innate immunity. Public Library of Science 2020-05-04 /pmc/articles/PMC7224577/ /pubmed/32365141 http://dx.doi.org/10.1371/journal.ppat.1008537 Text en © 2020 Paulus et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Paulus, Christina
Harwardt, Thomas
Walter, Bernadette
Marxreiter, Andrea
Zenger, Marion
Reuschel, Edith
Nevels, Michael M.
Revisiting promyelocytic leukemia protein targeting by human cytomegalovirus immediate-early protein 1
title Revisiting promyelocytic leukemia protein targeting by human cytomegalovirus immediate-early protein 1
title_full Revisiting promyelocytic leukemia protein targeting by human cytomegalovirus immediate-early protein 1
title_fullStr Revisiting promyelocytic leukemia protein targeting by human cytomegalovirus immediate-early protein 1
title_full_unstemmed Revisiting promyelocytic leukemia protein targeting by human cytomegalovirus immediate-early protein 1
title_short Revisiting promyelocytic leukemia protein targeting by human cytomegalovirus immediate-early protein 1
title_sort revisiting promyelocytic leukemia protein targeting by human cytomegalovirus immediate-early protein 1
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7224577/
https://www.ncbi.nlm.nih.gov/pubmed/32365141
http://dx.doi.org/10.1371/journal.ppat.1008537
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