Adenovirus Evasion of Interferon-Mediated Innate Immunity by Direct Antagonism of a Cellular Histone Posttranslational Modification

Fonseca, Greg J.; Thillainadesan, Gobi; Yousef, Ahmed F.; Ablack, Jailal; Mossman, Karen; Torchia, Joseph; Mymryk, Joe S.

doi:10.1016/j.chom.2012.05.005

Cited by 107 publications

(115 citation statements)

References 45 publications

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“…E1A suppresses signaling downstream of IFNR activation at STAT1 (51,81), compromises IFN-directed ISG activation by disrupting IFN-induced histone 2B monoubiquitination required for ISG induction (82), and blocks RNA activation of a TRIF/BS69 signalosome, which leads to NF-B and IRF3 activation (83). E1B functions to effectively repress IFN-induced antiviral strategies that impact replication (53,54).…”

Section: Discussionmentioning

confidence: 99%

Unabated Adenovirus Replication following Activation of the cGAS/STING-Dependent Antiviral Response in Human Cells

Lam

Falck-Pedersen

2014

J Virol

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Section: Discussionmentioning

confidence: 99%

Unabated Adenovirus Replication following Activation of the cGAS/STING-Dependent Antiviral Response in Human Cells

Lam

Falck-Pedersen

2014

J Virol

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“…Aberrant H2Bub1 levels can affect development (Wright et al 2011), apoptosis (Walter et al 2010), stem cell differentiation (Buszczak et al 2009;Fuchs et al 2012;Karpiuk et al 2012), viral infection outcome (Sarkari et al 2009;Fonseca et al 2012), and cell cycle progression (Hwang and Madhani 2009) and can promote cancer Blank et al 2012;Johnsen 2012;. Several mechanisms have been proposed to underlie the ability of H2Bub1 to exert those diverse effects, including impact on higher-order chromatin organization (Fierz et al 2011), altered nucleosome stability (Chandrasekharan et al 2009), regulation of H2A-H2B dimer displacement (Pavri et al 2006), and modulation of the recruitment of specific factors to chromatin (Shema-Yaacoby et al 2013).…”

Section: [Supplemental Materials Is Available For This Article]mentioning

confidence: 99%

Cotranscriptional histone H2B monoubiquitylation is tightly coupled with RNA polymerase II elongation rate

et al. 2014

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Various histone modifications decorate nucleosomes within transcribed genes. Among these, monoubiquitylation of histone H2B (H2Bub1) and methylation of histone H3 on lysines 36 (H3K36me2/3) and 79 (H3K79me2/3) correlate positively with gene expression. By measuring the progression of the transcriptional machinery along genes within live cells, we now report that H2B monoubiquitylation occurs cotranscriptionally and accurately reflects the advance of RNA polymerase II (Pol II). In contrast, H3K36me3 and H3K79me2 are less dynamic and represent Pol II movement less faithfully. High-resolution ChIP-seq reveals that H2Bub1 levels are selectively reduced at exons and decrease in an exon-dependent stepwise manner toward the 39 end of genes. Exonic depletion of H2Bub1 in gene bodies is highly correlated with Pol II pausing at exons, suggesting elongation rate changes associated with intron-exon structure. In support of this notion, H2Bub1 levels were found to be significantly correlated with transcription elongation rates measured in various cell lines. Overall, our data shed light on the organization of H2Bub1 within transcribed genes and single out H2Bub1 as a reliable marker for ongoing transcription elongation.

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“…Further complexities may be added to a mathematical model to explicitly account for the interplay between multiplicities of viral infection and the antiviral states mediated by interferon [119,122,123] as a cellular response to viral infection. Of course, the model would require additional distinction of antiviral and non-antiviral states [122] for uninfected cells (See [73] for example).…”

Section: Modeling Specific Mechanisms Of Actionmentioning

confidence: 99%

Fighting Cancer with Mathematics and Viruses

Santiago¹,

Heidbuechel²,

Kandell³

et al. 2017

Preprint

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After decades of research, oncolytic virotherapy has recently advanced to clinical application, and currently a multitude of novel agents and combination treatments are being evaluated for cancer therapy. Oncolytic agents preferentially replicate in tumor cells, inducing tumor cell lysis and complex anti-tumor effects, such as innate and adaptive immune responses and the destruction of tumor vasculature. With the availability of different vector platforms and the potential of both genetic engineering and combination regimens to enhance particular aspects of safety and efficacy, the identification of optimal treatments for patient subpopulations or even individual patients becomes a top priority. Mathematical modeling can provide support in this arena by making use of experimental and clinical data to generate hypotheses about the mechanisms underlying complex biology and, ultimately, predict optimal treatment protocols. Increasingly complex models can be applied to account for therapeutically relevant parameters such as components of the immune system. In this review, we describe current developments in oncolytic virotherapy and mathematical modeling to discuss the benefit of integrating different modeling approaches into biological and clinical experimentation. Conclusively, we propose a mutual combination of these fields of research for more efficient development and effective treatments.

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Adenovirus Evasion of Interferon-Mediated Innate Immunity by Direct Antagonism of a Cellular Histone Posttranslational Modification

Cited by 107 publications

References 45 publications

Unabated Adenovirus Replication following Activation of the cGAS/STING-Dependent Antiviral Response in Human Cells

Unabated Adenovirus Replication following Activation of the cGAS/STING-Dependent Antiviral Response in Human Cells

Cotranscriptional histone H2B monoubiquitylation is tightly coupled with RNA polymerase II elongation rate

Fighting Cancer with Mathematics and Viruses

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