Please use this identifier to cite or link to this item: https://accedacris.ulpgc.es/jspui/handle/10553/156450
Title: Human Cytomegalovirus RNA2.7 Is Required for Upregulating Multiple Cellular Genes To Promote Cell Motility and Viral Spread Late in Lytic Infection
Authors: Lau, Betty
Kerr, Karen
Camiolo, Salvatore
Nightingale, Katie
Gu, Quan
Antrobus, Robin
Martel Suárez, Nicolás Alfonso 
Loney, Colin
Stanton, Richard J.
Weekes, Michael P.
Davison, Andrew J.
Editors: Longnecker, Richard M.
UNESCO Clasification: 32 Ciencias médicas
2420 Virología
Keywords: Cell motility
Human cytomegalovirus
lncRNA
Regulation of gene expression
Issue Date: 2021
Journal: Journal of Virology 
Abstract: Long noncoding RNAs (lncRNAs) are frequently associated with broad modulation of gene expression and thus provide the cell with the ability to synchronize entire metabolic processes. We used transcriptomic approaches to investigate whether the most abundant human cytomegalovirus-encoded lncRNA, RNA2.7, has this characteristic. By comparing cells infected with wild-type virus (WT) to cells infected with RNA2.7 deletion mutants, RNA2.7 was implicated in regulating a large number of cellular genes late in lytic infection. Pathway analysis indicated that >100 of these genes are associated with promoting cell movement, and the 10 most highly regulated of these were validated in further experiments. Morphological analysis and live cell tracking of WT- and RNA2.7 mutant-infected cells indicated that RNA2.7 is involved in promoting the movement and detachment of infected cells late in infection, and plaque assays using sparse cell monolayers indicated that RNA2.7 is also involved in promoting cell-to-cell spread of virus. Consistent with the observation that upregulated mRNAs are relatively A+U-rich, which is a trait associated with transcript instability, and that they are also enriched in motifs associated with mRNA instability, transcriptional inhibition experiments on WT- and RNA2.7 mutant-infected cells showed that four upregulated transcripts lived longer in the presence of RNA2.7. These findings demonstrate that RNA2.7 is required for promoting cell movement and viral spread late in infection and suggest that this may be due to general stabilization of A+U-rich transcripts.
URI: https://accedacris.ulpgc.es/jspui/handle/10553/156450
ISSN: 0022-538X
DOI: 10.1128/JVI.00698-21
Source: Journal of Virology [eISSN 0022-538X], v. 95 (20) (Septiembre 2021)
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