Human cytomegalovirus tegument protein pp71 directs long-term gene expression from quiescent herpes simplex virus genomes. - Wikidata - awgldk - TriplyDB

Human cytomegalovirus tegument protein pp71 directs long-term gene expression from quiescent herpes simplex virus genomes.

Human cytomegalovirus tegument protein pp71 directs long-term gene expression from quiescent herpes simplex virus genomes.

http://www.wikidata.org/entity/Q40728386

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Antivirals reduce the formation of key Alzheimer's disease molecules in cell cultures acutely infected with herpes simplex virus type 1 Inactivating a cellular intrinsic immune defense mediated by Daxx is the mechanism through which the human cytomegalovirus pp71 protein stimulates viral immediate-early gene expression Functional inaccessibility of quiescent herpes simplex virus genomes Role of chromatin during herpesvirus infections.Comparison of the biological and biochemical activities of several members of the alphaherpesvirus ICP0 family of proteins.Herpes simplex viral-vector design for efficient transduction of nonneuronal cells without cytotoxicity.Latency Entry of Herpes Simplex Virus 1 Is Determined by the Interaction of Its Genome with the Nuclear Environment Epstein-Barr Virus (EBV) Tegument Protein BGLF2 Promotes EBV Reactivation through Activation of the p38 Mitogen-Activated Protein Kinase.The replication defect of ICP0-null mutant herpes simplex virus 1 can be largely complemented by the combined activities of human cytomegalovirus proteins IE1 and pp71 Human cytomegalovirus IE1 protein enhances herpes simplex virus type 1-induced syncytial formation in U373MG cells.Properties of virion transactivator proteins encoded by primate cytomegaloviruses Promyelocytic leukemia-nuclear body proteins: herpesvirus enemies, accomplices, or both?Tale of a tegument transactivator: the past, present and future of human CMV pp71 Virion factors that target Daxx to overcome intrinsic immunity.Components of promyelocytic leukemia nuclear bodies (ND10) act cooperatively to repress herpesvirus infection.Herpes simplex virus type 1 regulatory protein ICP0 aids infection in cells with a preinduced interferon response but does not impede interferon-induced gene induction.Regulation of ICP0-null mutant herpes simplex virus type 1 infection by ND10 components ATRX and hDaxx.Analysis of the functions of herpes simplex virus type 1 regulatory protein ICP0 that are critical for lytic infection and derepression of quiescent viral genomes.Human cytomegalovirus protein pp71 displaces the chromatin-associated factor ATRX from nuclear domain 10 at early stages of infection.Human cytomegalovirus gene expression is silenced by Daxx-mediated intrinsic immune defense in model latent infections established in vitro.Herpes simplex virus type 1 genomes are associated with ND10 nuclear substructures in quiescently infected human fibroblasts.The viral ubiquitin ligase ICP0 is neither sufficient nor necessary for degradation of the cellular DNA sensor IFI16 during herpes simplex virus 1 infection.Expression of herpes simplex virus 1 microRNAs in cell culture models of quiescent and latent infection.STAT-1- and IRF-3-dependent pathways are not essential for repression of ICP0-null mutant herpes simplex virus type 1 in human fibroblasts.Functional characterization of residues required for the herpes simplex virus 1 E3 ubiquitin ligase ICP0 to interact with the cellular E2 ubiquitin-conjugating enzyme UBE2D1 (UbcH5a)Induction of cellular stress overcomes the requirement of herpes simplex virus type 1 for immediate-early protein ICP0 and reactivates expression from quiescent viral genomes.Reactivation of expression from quiescent herpes simplex virus type 1 genomes in the absence of immediate-early protein ICP0.CD8(+) T-cell attenuation of cutaneous herpes simplex virus infection reduces the average viral copy number of the ensuing latent infection.Promyelocytic leukemia (PML) nuclear bodies (NBs) induce latent/quiescent HSV-1 genomes chromatinization through a PML NB/Histone H3.3/H3.3 Chaperone Axis

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P2860

Human cytomegalovirus tegument protein pp71 directs long-term gene expression from quiescent herpes simplex virus genomes.

http://www.wikidata.org/entity/Q40728386

description

2005 nî lūn-bûn

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2005年の論文

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2005年学术文章

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2005年学术文章

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2005年学术文章

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2005年学术文章

@zh-my

2005年学术文章

@zh-sg

2005年學術文章

@yue

2005年學術文章

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2005年學術文章

@zh-hant

name

Human cytomegalovirus tegument ...... herpes simplex virus genomes.

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type

label

Human cytomegalovirus tegument ...... herpes simplex virus genomes.

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prefLabel

Human cytomegalovirus tegument ...... herpes simplex virus genomes.

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P356

JVI.79.1.525-535.2005

P1433

Journal of Virology

P1476

Human cytomegalovirus tegument ...... herpes simplex virus genomes.

@en

P2093

Chris M Preston

http://www.w3.org/2001/XMLSchema#string

Mary Jane Nicholl

http://www.w3.org/2001/XMLSchema#string

P2860

A novel ubiquitin-specific protease is dynamically associated with the PML nuclear domain and binds to a herpesvirus regulatory protein

Association of herpes simplex virus type 1 ICP8 and ICP27 proteins with cellular RNA polymerase II holoenzyme

PML is critical for ND10 formation and recruits the PML-interacting protein daxx to this nuclear structure when modified by SUMO-1

ICP0, a regulator of herpes simplex virus during lytic and latent infection

The nuclear domain 10 (ND10) is disrupted by the human cytomegalovirus gene product IE1

Transcriptional regulation of the human cytomegalovirus US11 early gene.

Persistence and expression of the herpes simplex virus genome in the absence of immediate-early proteins.

Long-term transgene expression in mice infected with a herpes simplex virus type 1 mutant severely impaired for immediate-early gene expression.

Herpes simplex virus ICP0 mutants are hypersensitive to interferon

ICP22 and the UL13 protein kinase are both required for herpes simplex virus-induced modification of the large subunit of RNA polymerase II.

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525-535

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scholarly article

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10.1128/JVI.79.1.525-535.2005

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1

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2005-01-01T00:00:00Z

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Cytomegalovirus

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538741

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