Histone Hyperacetylation Occurs on Promoters of Lytic Cycle Regulatory Genes in Epstein-Barr Virus-Infected Cell Lines Which Are Refractory to Disruption of Latency by Histone Deacetylase Inhibitors

Countryman, Jill; Gradoville, Lyndle; Miller, George

doi:10.1128/jvi.00116-08

Cited by 85 publications

(113 citation statements)

References 84 publications

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“…Recently, studies of these histone marks in specific promoter regions in the EBV genome have yielded some interesting results from an analysis of the epigenetic patterns of viral genes, such as Cp, LMP2A and BZLF1, which code for essential latent proteins. As these histone marks are associated with open and accessible chromatin, these results suggested that, in coordination with DNA methylation, they have a major role in the modulation (activation or repression) of specific viral genes (Gerle et al, 2007;Countryman et al, 2008;Fejer et al, 2008).…”

Section: Epstein-barr Virusmentioning

confidence: 94%

“…This reactivation is initiated by the expression of the immediate-early gene BZLF1, which encodes the transcriptional activator Zta, probably by stimuli such as plasma cell differentiation, and has been found to be unmethylated (Fernandez et al, 2009). This protein, apart from affecting the expression of host genes (Chang et al, 2006), has the ability to bind to methylated sites and activate the expression of BRLF1, another of this virus's immediate-early genes, and both together then activate the expression of the remaining lytic genes, thereby inducing a lytic infection (Bhende et al, 2005;Countryman et al, 2008;Dickerson et al, 2009;Heather et al, 2009). …”

Section: Epstein-barr Virusmentioning

confidence: 99%

“…During latency, episomal DNA is associated with nucleosomes in arrays that are indistinguishable from bulk cellular DNA (Shaw et al, 1979;Dyson and Farrell, 1985) and, not surprisingly, the histone marks associated with particular nucleosome positioning affect the expression patterns of viral genes. Several studies have been published in relation to this that identify specific associations between the expression of viral genes and patterns of histone modification (Gerle et al, 2007;Countryman et al, 2008;Fejer et al, 2008).…”

Section: Epstein-barr Virusmentioning

confidence: 99%

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Viral epigenomes in human tumorigenesis

Fernández

Esteller

2010

Oncogene

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Viruses are associated with 15-20% of human cancers worldwide. In the last century, many studies were directed towards elucidating the molecular mechanisms and genetic alterations by which viruses cause cancer. The importance of epigenetics in the regulation of gene expression has prompted the investigation of virus and host interactions not only at the genetic level but also at the epigenetic level. In this study, we summarize the published epigenetic information relating to the genomes of viruses directly or indirectly associated with the establishment of tumorigenic processes. We also review aspects such as viral replication and latency associated with epigenetic changes and summarize what is known about epigenetic alterations in host genomes and the implications of these for the tumoral process. The advances made in characterizing epigenetic features in cancer-causing viruses have improved our understanding of their functional mechanisms. Knowledge of the epigenetic changes that occur in the genome of these viruses should provide us with markers for following cancer progression, as well as new tools for cancer therapy.

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Section: Epstein-barr Virusmentioning

confidence: 94%

Section: Epstein-barr Virusmentioning

confidence: 99%

Section: Epstein-barr Virusmentioning

confidence: 99%

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Viral epigenomes in human tumorigenesis

Fernández

Esteller

2010

Oncogene

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“…As a first step, we used the TPA þ NaB combination as the most commonly used treatment to trigger EBV lytic reactivation (2,21). Healthy donor-derived LCLs treated for 48 hours with TPA þ NaB showed significantly increased BARF1 mRNA expression (2.5 mean fold-increase, P 0.05; Fig.…”

Section: Doxorubicin Upregulates Barf1 Mrna Expressionmentioning

confidence: 99%

Broadening Specificity and Enhancing Cytotoxicity of Adoptive T Cells for Nasopharyngeal Carcinoma Immunotherapy

Faè

Martorelli

Mastorci

et al. 2016

Cancer Immunology Research

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Although promising, clinical responses to adoptive immunotherapy for nasopharyngeal carcinoma (NPC) are still limited by the restricted number of Epstein-Barr virus (EBV) antigens that can be targeted and their poor immunogenicity. Our previous work indicated that the immunogenic features of the NPCassociated viral antigen BARF1 may be exploited for immunotherapeutic purposes. Nevertheless, T-cell lines obtained with current protocols include only negligible numbers of BARF1-specific cytotoxic T lymphocytes, pointing to the need to enrich these effectors in BARF1 specificities. Considering that in B lymphocytes BARF1 is mainly a lytic EBV antigen, we tested different EBV lytic-cycle inducers (TPA/butyric acid, doxorubicin, and cisplatin) used at suboptimal concentrations for their ability to upregulate BARF1 expression in lymphoblastoid B-cell lines (LCL), the commonly used antigen-presenting cells, without compromising their survival. The LCLs treated with doxorubicin (DX-LCL) can reproducibly and efficiently generate EBV-specific effectors enriched in BARF1 specificities from both healthy donors and NPC patients. These DX-LCLs also had more pronounced immunogenic properties, including HLA class I upregulation and expression of immunogenic cell death markers, such as enhanced calreticulin exposure and HMGB1 release. In particular, doxorubicin triggers an HMGB1 autocrine/ paracrine loop with its receptor, TLR4, which is also upregulated in DX-LCLs and is responsible for NF-kB activation and a delayed apoptosis that allows a prolonged stimulation of EBV-specific T-cell precursors. This protocol may thus constitute a valid alternative to the use of engineered LCLs to generate EBV-specific T-cell lines for adoptive immunotherapy, being relatively simple, easily upgradable to Good Manufacturing Practice standards, and therefore more broadly applicable.

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“…Changes in histone acetylation in the BZLF1 promoter region results in activation of BZLF1 gene expression leading to reactivation from latency, as treatment with histone deacetylase (HDAC) inhibitors can activate viral lytic gene expression (7)(8)(9). It is reported that, in latently infected cells, the silent state of the virus genome is maintained, at least in part, by MEF2-mediated recruitment of HDAC proteins to the BZLF1 promoter region (10).…”

mentioning

confidence: 99%

Transcriptional Repression by Sumoylation of Epstein-Barr Virus BZLF1 Protein Correlates with Association of Histone Deacetylase

Murata

Hotta

Toyama

et al. 2010

Journal of Biological Chemistry

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The transition from latent to lytic phases of the Epstein-Barr virus life cycle is triggered by expression of a viral transactivator, BZLF1, that then induces expression of the viral immediateearly and early genes. The BZLF1 protein is post-translationally modified by a small ubiquitin-related modifier-1 (SUMO-1). Here we found that BZLF1 is conjugated at lysine 12 not only by SUMO-1 but also by SUMO-2 and 3. The K12R mutant of BZLF1, which no longer becomes sumoylated, exhibits stronger transactivation than the wild-type BZLF1 in a reporter assay system as well as in the context of virus genome with nucleosomal structures. Furthermore, exogenous supply of a SUMO-specific protease, SENP, caused de-sumoylation of BZLF1 and enhanced BZLF1-mediated transactivation. Immunoprecipitation experiments proved that histone deacetylase 3 preferentially associated with the sumoylated form of BZLF1. Levels of the sumoylated BZLF1 increased as lytic replication progressed. Based on these observations, we conclude that sumoylation of BZLF1 regulates its transcriptional activity through histone modification during Epstein-Barr virus productive replication.

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Histone Hyperacetylation Occurs on Promoters of Lytic Cycle Regulatory Genes in Epstein-Barr Virus-Infected Cell Lines Which Are Refractory to Disruption of Latency by Histone Deacetylase Inhibitors

Cited by 85 publications

References 84 publications

Viral epigenomes in human tumorigenesis

Viral epigenomes in human tumorigenesis

Broadening Specificity and Enhancing Cytotoxicity of Adoptive T Cells for Nasopharyngeal Carcinoma Immunotherapy

Transcriptional Repression by Sumoylation of Epstein-Barr Virus BZLF1 Protein Correlates with Association of Histone Deacetylase

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