Genome-wide analysis of regulatory G-quadruplexes affecting gene expression in human cytomegalovirus.

Genome-wide analysis of regulatory G-quadruplexes affecting gene expression in human cytomegalovirus.

G-quadruplex (G4), formed by repetitive guanosine-rich sequences, is known to play various key regulatory roles in cells. Herpesviruses containing a large double-stranded DNA genome show relatively higher density of G4-forming sequences in their genomes compared to human and mouse. However, it remai...

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Main Authors: Subramaniyam Ravichandran, Young-Eui Kim, Varun Bansal, Ambarnil Ghosh, Jeonghwan Hur, Vinod Kumar Subramani, Subhra Pradhan, Myoung Kyu Lee, Kyeong Kyu Kim, Jin-Hyun Ahn
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2018-09-01
Series:PLoS Pathogens
Online Access:http://europepmc.org/articles/PMC6179306?pdf=render
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spelling doaj-0b63aa024835454097eb0e788482643d2020-11-24T21:52:47ZengPublic Library of Science (PLoS)PLoS Pathogens1553-73661553-73742018-09-01149e100733410.1371/journal.ppat.1007334Genome-wide analysis of regulatory G-quadruplexes affecting gene expression in human cytomegalovirus.Subramaniyam RavichandranYoung-Eui KimVarun BansalAmbarnil GhoshJeonghwan HurVinod Kumar SubramaniSubhra PradhanMyoung Kyu LeeKyeong Kyu KimJin-Hyun AhnG-quadruplex (G4), formed by repetitive guanosine-rich sequences, is known to play various key regulatory roles in cells. Herpesviruses containing a large double-stranded DNA genome show relatively higher density of G4-forming sequences in their genomes compared to human and mouse. However, it remains poorly understood whether all of these sequences form G4 and how they play a role in the virus life cycle. In this study, we performed genome-wide analyses of G4s present in the putative promoter or gene regulatory regions of a 235-kb human cytomegalovirus (HCMV) genome and investigated their roles in viral gene expression. We evaluated 36 putative G4-forming sequences associated with 20 genes for their ability to form G4 and for the stability of G4s in the presence or absence of G4-stabilizing ligands, by circular dichroism and melting temperature analyses. Most identified sequences formed a stable G4; 28 sequences formed parallel G4s, one formed an antiparallel G4, and four showed mixed conformations. However, when we assessed the effect of G4 on viral promoters by cloning the 20 putative viral promoter regions containing 36 G4-forming sequences into the luciferase reporter and monitoring the expression of luciferase reporter gene in the presence of G4-stabilizing chemicals, we found that only 9 genes were affected by G4 formation. These results revealed promoter context-dependent gene suppression by G4 formation. Mutational analysis of two potential regulatory G4s also demonstrated gene suppression by the sequence-specific G4 formation. Furthermore, the analysis of a mutant virus incapable of G4 formation in the UL35 promoter confirmed promoter regulation by G4 in the context of virus infection. Our analyses provide a platform for assessing G4 functions at the genomic level and demonstrate the properties of the HCMV G4s and their regulatory roles in viral gene expression.http://europepmc.org/articles/PMC6179306?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Subramaniyam Ravichandran
Young-Eui Kim
Varun Bansal
Ambarnil Ghosh
Jeonghwan Hur
Vinod Kumar Subramani
Subhra Pradhan
Myoung Kyu Lee
Kyeong Kyu Kim
Jin-Hyun Ahn
spellingShingle Subramaniyam Ravichandran
Young-Eui Kim
Varun Bansal
Ambarnil Ghosh
Jeonghwan Hur
Vinod Kumar Subramani
Subhra Pradhan
Myoung Kyu Lee
Kyeong Kyu Kim
Jin-Hyun Ahn
Genome-wide analysis of regulatory G-quadruplexes affecting gene expression in human cytomegalovirus.
PLoS Pathogens
author_facet Subramaniyam Ravichandran
Young-Eui Kim
Varun Bansal
Ambarnil Ghosh
Jeonghwan Hur
Vinod Kumar Subramani
Subhra Pradhan
Myoung Kyu Lee
Kyeong Kyu Kim
Jin-Hyun Ahn
author_sort Subramaniyam Ravichandran
title Genome-wide analysis of regulatory G-quadruplexes affecting gene expression in human cytomegalovirus.
title_short Genome-wide analysis of regulatory G-quadruplexes affecting gene expression in human cytomegalovirus.
title_full Genome-wide analysis of regulatory G-quadruplexes affecting gene expression in human cytomegalovirus.
title_fullStr Genome-wide analysis of regulatory G-quadruplexes affecting gene expression in human cytomegalovirus.
title_full_unstemmed Genome-wide analysis of regulatory G-quadruplexes affecting gene expression in human cytomegalovirus.
title_sort genome-wide analysis of regulatory g-quadruplexes affecting gene expression in human cytomegalovirus.
publisher Public Library of Science (PLoS)
series PLoS Pathogens
issn 1553-7366
1553-7374
publishDate 2018-09-01
description G-quadruplex (G4), formed by repetitive guanosine-rich sequences, is known to play various key regulatory roles in cells. Herpesviruses containing a large double-stranded DNA genome show relatively higher density of G4-forming sequences in their genomes compared to human and mouse. However, it remains poorly understood whether all of these sequences form G4 and how they play a role in the virus life cycle. In this study, we performed genome-wide analyses of G4s present in the putative promoter or gene regulatory regions of a 235-kb human cytomegalovirus (HCMV) genome and investigated their roles in viral gene expression. We evaluated 36 putative G4-forming sequences associated with 20 genes for their ability to form G4 and for the stability of G4s in the presence or absence of G4-stabilizing ligands, by circular dichroism and melting temperature analyses. Most identified sequences formed a stable G4; 28 sequences formed parallel G4s, one formed an antiparallel G4, and four showed mixed conformations. However, when we assessed the effect of G4 on viral promoters by cloning the 20 putative viral promoter regions containing 36 G4-forming sequences into the luciferase reporter and monitoring the expression of luciferase reporter gene in the presence of G4-stabilizing chemicals, we found that only 9 genes were affected by G4 formation. These results revealed promoter context-dependent gene suppression by G4 formation. Mutational analysis of two potential regulatory G4s also demonstrated gene suppression by the sequence-specific G4 formation. Furthermore, the analysis of a mutant virus incapable of G4 formation in the UL35 promoter confirmed promoter regulation by G4 in the context of virus infection. Our analyses provide a platform for assessing G4 functions at the genomic level and demonstrate the properties of the HCMV G4s and their regulatory roles in viral gene expression.
url http://europepmc.org/articles/PMC6179306?pdf=render
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