Epstein-Barr Virus Rta-Mediated Accumulation of DNA Methylation Interferes with CTCF Binding in both Host and Viral Genomes

Chen, Yen–Ju; Chen, Yulian; Chang, Yao; Wu, Chung-Chun; Ko, Ying-Chieh; Tsao, Sai Wah; Chen, Jen‐Yang; Lin, Su‐Fang

doi:10.1128/jvi.00736-17

Cited by 7 publications

(4 citation statements)

References 83 publications

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“…Entry of EBV into cells does not use xCT. A small upregulation of SLC7A11 occurred in EBV-negative 293 cells exogenously expressing the EBV lytic transactivator protein RTA [ 39 ]. Changes in SLC7A11 gene expression occur during primary EBV infection when B cells are reprogrammed and thousands of genes are regulated [ 40 , 41 ].…”

Section: Discussionmentioning

confidence: 99%

Transcriptome analysis of Burkitt lymphoma cells treated with anti-convulsant drugs that are inhibitors of Epstein–Barr virus lytic reactivation

Gorres,

Reineke,

Miller

2024

PLoS ONE

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Herpesviruses have two distinct life cycle stages, latency and lytic replication. Epstein-Barr virus (EBV), a gamma-herpesvirus, establishes latency in vivo and in cultured cells. Cell lines harboring latent EBV can be induced into the lytic cycle by treatment with chemical inducing agents. In the Burkitt lymphoma cell line HH514-16 the viral lytic cycle is triggered by butyrate, a histone deacetylase (HDAC) inhibitor. Butyrate also alters expression of thousands of cellular genes. However, valproic acid (VPA), another HDAC inhibitor with global effects on cellular gene expression blocks EBV lytic gene expression in Burkitt lymphoma cell lines. Valpromide (VPM), an amide derivative of VPA, is not an HDAC inhibitor, but like VPA blocks induction of the EBV lytic cycle. VPA and VPM are the first examples of inhibitors of initial stages of lytic reactivation. We compared the effects of VPA and VPM, alone and in combination with butyrate, on host cellular gene expression using whole transcriptome analysis (RNA-seq). Gene expression was analyzed 6 h after addition of the compounds, a time before the first EBV lytic transcripts are detected. The results address two alternative, yet possibly complementary, mechanisms for regulation of EBV lytic reactivation. First, cellular genes that were up- or down-regulated by butyrate, but no longer altered in the presence of VPA or VPM, represent genes that correlated with EBV lytic reactivation. Second, genes regulated similarly by VPA and VPM in the absence and presence of butyrate are candidates for suppressors of EBV reactivation. Two genes upregulated by the lytic cycle inhibitors, CHAC1 and SLC7A11, are related to redox status and the iron-dependent cell death pathway ferroptosis. This study generates new hypotheses for control of the latency to lytic cycle switch of EBV and provides the first description of effects of the anti-convulsant drug VPM on global human cellular gene expression.

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Section: Discussionmentioning

confidence: 99%

Transcriptome analysis of Burkitt lymphoma cells treated with anti-convulsant drugs that are inhibitors of Epstein–Barr virus lytic reactivation

Gorres,

Reineke,

Miller

2024

PLoS ONE

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“…Consequently, it is speculated that the absence of SLC5A8 expression is largely influenced by dense methylation in this block of 20 CpG dinucleotides. Along these CpGs, a computational prediction using the Genomatix software (https://genomatix.de/) identified the consensus binding sites for the methylation-sensitive transcription factor E2F and transcriptional repressor CTCF (34,35); however, further experiments are required to determine the role of these transcription factors in the regulation of SLC5A8 expression.…”

Section: Discussionmentioning

confidence: 99%

Sodium-coupled monocarboxylate transporter is a target of epigenetic repression in cervical cancer

et al. 2019

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The SLC5A8 gene encodes Na monocarboxylate transporter 1, which is epigenetically inactivated in various tumour types. This has been attributed to the fact that it prevents the entry of histone deacetylase (HDAC) inhibitors and favours the metabolic reprogramming of neoplastic cells. Nevertheless, its expression and regulation in cervical cancer (CC) have not been elucidated to date. The aim of the present study was to investigate whether SLC5A8 expression is silenced in CC and if epigenetic mechanisms are involved in its regulation. Using RNA and DNA from human CC cell lines and tumour tissues from patients with CC, the expression of SLC5A8 was analysed by reverse transcription polymerase chain reaction and the methylation status of its CpG island (CGI) by bisulphite-modified sequencing. Additionally, SLC5A8 reactivation was examined in the CC cell lines following treatment with DNA methylation (5-aza-2′-deoxycytidine) and HDAC inhibitors (trichostatin A and pyruvate). All the CC cell lines and a range of tumour tissues (65.5%) exhibited complete or partial loss of SLC5A8 transcription. The bisulphite-sequencing revealed that hypermethylation of the CGI within SLC5A8 first exon was associated with its downregulation in the majority of cases. The transporter expression was restored in the CC cell lines following exposure to 5-aza-2′-deoxycytidine alone, or in combination with trichostatin A or pyruvate, suggesting that DNA methylation and histone deacetylation contribute to its inhibition in a cell line-dependent manner. Together, the results of the present study demonstrate the key role of DNA hypermethylation in the repression of SLC5A8 in CC, as well as the involvement of histone deacetylation, at least partially. This allows for research focused on the potential function of SLC5A8 as a tumour suppressor in CC, and as a biomarker or therapeutic target in this malignancy.

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“…Furthermore, several studies have revealed that CTCF can regulate viral gene expression in other double-stranded DNA viruses. For instance, in Kaposi’s sarcoma herpesvirus (KSHV) [ 74 , 75 , 76 , 77 , 78 , 79 , 80 , 81 , 82 ], herpes simplex virus (HSV) [ 83 , 84 , 85 , 86 , 87 , 88 , 89 ] and human cytomegalovirus (CMV) [ 90 ], CTCF has been shown to bind to the viral genome and regulate viral gene expression by modulating the accessibility of the viral genome to transcription factors. Finally, it has also been suggested that viruses can modulate CTCF activity to promote viral replication.…”

Section: Ebv and Ctcfmentioning

confidence: 99%

Three-Dimensional Chromatin Structure of the EBV Genome: A Crucial Factor in Viral Infection

Caruso

Maestri

Tempera

2023

Viruses

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Epstein–Barr Virus (EBV) is a human gamma-herpesvirus that is widespread worldwide. To this day, about 200,000 cancer cases per year are attributed to EBV infection. EBV is capable of infecting both B cells and epithelial cells. Upon entry, viral DNA reaches the nucleus and undergoes a process of circularization and chromatinization and establishes a latent lifelong infection in host cells. There are different types of latency all characterized by different expressions of latent viral genes correlated with a different three-dimensional architecture of the viral genome. There are multiple factors involved in the regulation and maintenance of this three-dimensional organization, such as CTCF, PARP1, MYC and Nuclear Lamina, emphasizing its central role in latency maintenance.

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Epstein-Barr Virus Rta-Mediated Accumulation of DNA Methylation Interferes with CTCF Binding in both Host and Viral Genomes

Cited by 7 publications

References 83 publications

Transcriptome analysis of Burkitt lymphoma cells treated with anti-convulsant drugs that are inhibitors of Epstein–Barr virus lytic reactivation

Transcriptome analysis of Burkitt lymphoma cells treated with anti-convulsant drugs that are inhibitors of Epstein–Barr virus lytic reactivation

Sodium-coupled monocarboxylate transporter is a target of epigenetic repression in cervical cancer

Three-Dimensional Chromatin Structure of the EBV Genome: A Crucial Factor in Viral Infection

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