Host-viral effects of chromatin assembly factor 1 interaction with HCMV IE2

Lee, Sung Bau; Lee, Chung-Fan; Ou, Derick S. C.; Dulal, Kalpana; Chang, Liang-Hao; Ma, Chen-Han; Huang, Chun-Ming; Zhu, Hua; Lin, Yu-Chi; Juan, Li‐Jung

doi:10.1038/cr.2011.53

Cited by 13 publications

(6 citation statements)

References 72 publications

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“…et al , reported that histone H1.4 phosphorylation at S35, a variant of H1.2, seems to be necessary for maintaining proper mitotic chromatin structure such as chromatin decondensation [49]. Viruses have been shown to increase nuclear size and result in chromatin decondensation [50,51], these effects are consistent with the changes in H1 phosphorylation induced by adenovirus we observe here.…”

Section: Insight Into Histone Phosphorylation Sitessupporting

confidence: 90%

Characterization of histone post-translational modifications during virus infection using mass spectrometry-based proteomics

Kulej

Avgousti

Weitzman

et al. 2015

Methods

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Viruses are obligate intracellular parasites that necessarily rely on hijacking cellular resources to produce viral progeny. The success of viral infection requires manipulation of host chromatin in order to activate genes useful for production of viral proteins as well as suppress antiviral responses. Host chromatin manipulation on a global level is likely reliant on modulation of post-translational modifications (PTMs) on histone proteins. Mass spectrometry (MS) is a powerful tool to quantify and identify novel histone PTMs, beyond the limitations of site-specific antibodies. Here, we employ MS to investigate global changes in histone PTM relative abundance in human cells during infection with adenovirus. Our method reveals several changes in histone PTM patterns during infection. We propose that this method can be used to uncover global changes in histone PTM patterns that are universally modulated by viruses to take over the cell.

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Section: Insight Into Histone Phosphorylation Sitessupporting

confidence: 90%

Characterization of histone post-translational modifications during virus infection using mass spectrometry-based proteomics

Kulej

Avgousti

Weitzman

et al. 2015

Methods

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“…compared to WT and Rev-Q548R IE2 genome replication ( Fig. 2A), which could possibly be explained by the recent transfection-based evidence that Q548R IE2 86 cannot bind to the chromatin assembly factor 1 protein p150 (16). However, the large increases in viral DNA levels between 24, 72, and 96 h p.i.…”

Section: Discussionmentioning

confidence: 58%

Mutation of Glutamine to Arginine at Position 548 of IE2 86 in Human Cytomegalovirus Leads to Decreased Expression of IE2 40, IE2 60, UL83, and UL84 and Increased Transcription of US8-9 and US29-32

Burgdorf

Clark

Burgdorf

et al. 2011

J Virol

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The IE2 86 protein of human cytomegalovirus (HCMV) is essential for productive infection. The mutation of glutamine to arginine at position 548 of IE2 86 causes the virus to grow both slowly and to very low titers, making it difficult to study this mutant via infection. In this study, Q548R IE2 86 HCMV was produced on the complementing cell line 86F/40HA, which allowed faster and higher-titer production of mutant virus. The main defects observed in this mutant were greatly decreased expression of IE2 40, IE2 60, UL83, and UL84. Genome replication and the induction of cell cycle arrest were found to proceed at or near wild-type levels, and there was no defect in transitioning to early or late protein expression. Q548R IE2 86 was still able to interact with UL84. Furthermore, Q548R IE2 40 maintained the ability to enhance UL84 expression in a cotransfection assay. Microarray analysis of Q548R IE2 HCMV revealed that the US8, US9, and US29-32 transcripts were all significantly upregulated. These results further confirm the importance of IE2 in UL83 and UL84 expression as well as pointing to several previously unknown regions of the HCMV genome that may be regulated by IE2.

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“…This indicates that other variables, such as high levels of transcription or blockage of sites by other proteins or complexes, influence IE2 occupancy. Previous immunofluorescence studies of IE2 in HCMV-infected cells suggested that IE2 predominantly localizes to the viral replication compartment in late infection and is enriched near viral genomes at PML bodies even prior to replication onset ( 37 , 77 , 78 ). This localization was also dependent on the ability of IE2 to bind DNA ( 37 ).…”

Section: Discussionmentioning

confidence: 99%

Human Cytomegalovirus IE2 Both Activates and Represses Initiation and Modulates Elongation in a Context-Dependent Manner

Ball

Parida

et al. 2022

mBio

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Host-viral effects of chromatin assembly factor 1 interaction with HCMV IE2

Cited by 13 publications

References 72 publications

Characterization of histone post-translational modifications during virus infection using mass spectrometry-based proteomics

Characterization of histone post-translational modifications during virus infection using mass spectrometry-based proteomics

Mutation of Glutamine to Arginine at Position 548 of IE2 86 in Human Cytomegalovirus Leads to Decreased Expression of IE2 40, IE2 60, UL83, and UL84 and Increased Transcription of US8-9 and US29-32

Human Cytomegalovirus IE2 Both Activates and Represses Initiation and Modulates Elongation in a Context-Dependent Manner

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