HCMV protein LUNA is required for viral reactivation from latently infected primary CD14⁺ cells.

HCMV protein LUNA is required for viral reactivation from latently infected primary CD14⁺ cells.

Human cytomegalovirus (HCMV) is a member of the Herpesviridae family that infects individuals throughout the world. Following an initial lytic stage, HCMV can persist in the individual for life in a non-active (or latent) form. During latency, the virus resides within cells of the myeloid lineage. T...

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Main Authors: Lisa R Keyes, Danna Hargett, Melisa Soland, Mariana G Bego, Cyprian C Rossetto, Graca Almeida-Porada, Stephen St Jeor
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3530514?pdf=render
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spelling doaj-c41526cc3514472a86e6953a8a7896492020-11-25T02:39:15ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-01712e5282710.1371/journal.pone.0052827HCMV protein LUNA is required for viral reactivation from latently infected primary CD14⁺ cells.Lisa R KeyesDanna HargettMelisa SolandMariana G BegoCyprian C RossettoGraca Almeida-PoradaStephen St JeorHuman cytomegalovirus (HCMV) is a member of the Herpesviridae family that infects individuals throughout the world. Following an initial lytic stage, HCMV can persist in the individual for life in a non-active (or latent) form. During latency, the virus resides within cells of the myeloid lineage. The mechanisms controlling HCMV latency are not completely understood. A latency associated transcript, UL81-82ast, encoding the protein LUNA (Latency Unique Natural Antigen) was identified from latently infected donors in vivo. To address the role of the UL81-82ast protein product LUNA, in the context of the viral genome, we developed a recombinant HCMV bacterial artificial chromosome (BAC) that does not express LUNA. This construct, LUNA knockout FIX virus (FIX-ΔLUNA), was used to evaluate LUNA's role in HCMV latency. The FIX-ΔLUNA virus was able to lytically infect Human Fibroblast (HF) cells, showing that LUNA is not required to establish a lytic infection. Interestingly, we observed significantly higher viral copy numbers in HF cells infected with FIX-ΔLUNA when compared to FIX-WT virus. Furthermore, FIX-WT and FIX-ΔLUNA genomic DNA and transcription of UL81-82ast persisted over time in primary monocytes. In contrast, the levels of UL138 transcript expression in FIX-ΔLUNA infected HF and CD14⁺ cells was 100 and 1000 fold lower (respectively) when compared to the levels observed for FIX-WT infection. Moreover, FIX-ΔLUNA virus failed to reactivate from infected CD14⁺ cells following differentiation. This lack of viral reactivation was accompanied by a lack of lytic gene expression, increase in viral copy numbers, and lack of the production of infectious units following differentiation of the cells. Our study suggests that the LUNA protein is involved in regulating HCMV reactivation, and that in the absence of LUNA, HCMV may not be able to enter a proper latent state and therefore cannot be rescued from the established persistent infection in CD14⁺ cells.http://europepmc.org/articles/PMC3530514?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Lisa R Keyes
Danna Hargett
Melisa Soland
Mariana G Bego
Cyprian C Rossetto
Graca Almeida-Porada
Stephen St Jeor
spellingShingle Lisa R Keyes
Danna Hargett
Melisa Soland
Mariana G Bego
Cyprian C Rossetto
Graca Almeida-Porada
Stephen St Jeor
HCMV protein LUNA is required for viral reactivation from latently infected primary CD14⁺ cells.
PLoS ONE
author_facet Lisa R Keyes
Danna Hargett
Melisa Soland
Mariana G Bego
Cyprian C Rossetto
Graca Almeida-Porada
Stephen St Jeor
author_sort Lisa R Keyes
title HCMV protein LUNA is required for viral reactivation from latently infected primary CD14⁺ cells.
title_short HCMV protein LUNA is required for viral reactivation from latently infected primary CD14⁺ cells.
title_full HCMV protein LUNA is required for viral reactivation from latently infected primary CD14⁺ cells.
title_fullStr HCMV protein LUNA is required for viral reactivation from latently infected primary CD14⁺ cells.
title_full_unstemmed HCMV protein LUNA is required for viral reactivation from latently infected primary CD14⁺ cells.
title_sort hcmv protein luna is required for viral reactivation from latently infected primary cd14⁺ cells.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Human cytomegalovirus (HCMV) is a member of the Herpesviridae family that infects individuals throughout the world. Following an initial lytic stage, HCMV can persist in the individual for life in a non-active (or latent) form. During latency, the virus resides within cells of the myeloid lineage. The mechanisms controlling HCMV latency are not completely understood. A latency associated transcript, UL81-82ast, encoding the protein LUNA (Latency Unique Natural Antigen) was identified from latently infected donors in vivo. To address the role of the UL81-82ast protein product LUNA, in the context of the viral genome, we developed a recombinant HCMV bacterial artificial chromosome (BAC) that does not express LUNA. This construct, LUNA knockout FIX virus (FIX-ΔLUNA), was used to evaluate LUNA's role in HCMV latency. The FIX-ΔLUNA virus was able to lytically infect Human Fibroblast (HF) cells, showing that LUNA is not required to establish a lytic infection. Interestingly, we observed significantly higher viral copy numbers in HF cells infected with FIX-ΔLUNA when compared to FIX-WT virus. Furthermore, FIX-WT and FIX-ΔLUNA genomic DNA and transcription of UL81-82ast persisted over time in primary monocytes. In contrast, the levels of UL138 transcript expression in FIX-ΔLUNA infected HF and CD14⁺ cells was 100 and 1000 fold lower (respectively) when compared to the levels observed for FIX-WT infection. Moreover, FIX-ΔLUNA virus failed to reactivate from infected CD14⁺ cells following differentiation. This lack of viral reactivation was accompanied by a lack of lytic gene expression, increase in viral copy numbers, and lack of the production of infectious units following differentiation of the cells. Our study suggests that the LUNA protein is involved in regulating HCMV reactivation, and that in the absence of LUNA, HCMV may not be able to enter a proper latent state and therefore cannot be rescued from the established persistent infection in CD14⁺ cells.
url http://europepmc.org/articles/PMC3530514?pdf=render
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