Unknown

Dataset Information

0

KSHV RNA-binding protein ORF57 inhibits P-body formation to promote viral multiplication by interaction with Ago2 and GW182.

ABSTRACT: Cellular non-membranous RNA-granules, P-bodies (RNA processing bodies, PB) and stress granules (SG), are important components of the innate immune response to virus invasion. Mechanisms governing how a virus modulates PB formation remain elusive. Here, we report the important roles of GW182 and DDX6, but not Dicer, Ago2 and DCP1A, in PB formation, and that Kaposi's sarcoma-associated herpesvirus (KSHV) lytic infection reduces PB formation through several specific interactions with viral RNA-binding protein ORF57. The wild-type ORF57, but not its N-terminal dysfunctional mutant, inhibits PB formation by interacting with the N-terminal GW-domain of GW182 and the N-terminal domain of Ago2, two major components of PB. KSHV ORF57 also induces nuclear Ago2 speckles. Homologous HSV-1 ICP27, but not EBV EB2, shares this conserved inhibitory function with KSHV ORF57. By using time-lapse confocal microscopy of HeLa cells co-expressing GFP-tagged GW182, we demonstrated that viral ORF57 inhibits primarily the scaffolding of GW182 at the initial stage of PB formation. Consistently, KSHV-infected iSLK/Bac16 cells with reduced GW182 expression produced far fewer PB and SG, but 100-fold higher titer of infectious KSHV virions when compared to cells with normal GW182 expression. Altogether, our data provide the first evidence that a DNA virus evades host innate immunity by encoding an RNA-binding protein that promotes its replication by blocking PB formation.

SUBMITTER: Sharma NR 

PROVIDER: S-EPMC6755100 | biostudies-literature | 2019 Sep

REPOSITORIES: biostudies-literature

Json Xml
altmetric image

Publications

KSHV RNA-binding protein ORF57 inhibits P-body formation to promote viral multiplication by interaction with Ago2 and GW182.

Sharma Nishi R NR   Majerciak Vladimir V   Kruhlak Michael J MJ   Yu Lulu L   Kang Jeong Gu JG   Yang Acong A   Gu Shuo S   Fritzler Marvin J MJ   Zheng Zhi-Ming ZM  

Nucleic acids research 20190901 17

Cellular non-membranous RNA-granules, P-bodies (RNA processing bodies, PB) and stress granules (SG), are important components of the innate immune response to virus invasion. Mechanisms governing how a virus modulates PB formation remain elusive. Here, we report the important roles of GW182 and DDX6, but not Dicer, Ago2 and DCP1A, in PB formation, and that Kaposi's sarcoma-associated herpesvirus (KSHV) lytic infection reduces PB formation through several specific interactions with viral RNA-bind  ...[more]

Similar Datasets

Unknown KSHV inhibits stress granule formation by viral ORF57 blocking PKR activation.
| S-EPMC5679657 | biostudies-literature
Unknown Genome-wide regulation of KSHV RNA splicing by viral RNA-binding protein ORF57.
| S-EPMC9321434 | biostudies-literature
Transcriptomics Viral RNA-binding protein KSHV ORF57 and host transcriptome
2023-02-13 | GSE179728 | GEO
Unknown An interaction between KSHV ORF57 and UIF provides mRNA-adaptor redundancy in herpesvirus intronless mRNA export.
| S-EPMC3141038 | biostudies-literature
Unknown The C-terminal half of human Ago2 binds to multiple GW-rich regions of GW182 and requires GW182 to mediate silencing.
| S-EPMC2673069 | biostudies-literature
Transcriptomics Oncogenic Ras inhibits IRF1 to promote viral oncolysis
2014-11-13 | E-GEOD-49469 | biostudies-arrayexpress
Unknown CLIP-seq to Identify KSHV ORF57-Binding RNA in Host B Cells.
| S-EPMC6650155 | biostudies-literature
Unknown KSHV encoded ORF59 modulates histone arginine methylation of the viral genome to promote viral reactivation.
| S-EPMC5513536 | biostudies-literature
Unknown Interactions between KSHV ORF57 and the novel human TREX proteins, CHTOP and CIP29.
| S-EPMC5156329 | biostudies-literature
Unknown Identification of GW182 and its novel isoform TNGW1 as translational repressors in Ago2-mediated silencing.
| S-EPMC7695043 | biostudies-literature