The first days in the life of naïve human B-lymphocytes infected with Epstein-Barr virus

Pich, Dagmar; Mrozek-Górska, Paulina; Bouvet, Mickaël; Sugimoto, Atsuko; Akidil, Ezgi; Grundhoff, Adam; Hamperl, Stephan; Ling, Paul D.; Hammerschmidt, Wolfgang

doi:10.1101/666297

Cited by 22 publications

(44 citation statements)

References 85 publications

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“…Notably, the EBV tegument protein BNRF1 targets ATRX and DAXX for sequestration in promyelocytic leukemia (PML) bodies at this time point ( 24 ), suggesting that HIRA and newly induced CAF1 may be responsible. H3.1 and H3.3 levels remained stable at day 4 postinfection, a time point at which cells divide every 8 to 12 h ( 11 – 13 ). Interestingly, after the period of Burkitt-like hyperproliferation that extended roughly from day 3 to day 7 postinfection, H3.1 and H3.3 levels nearly doubled, even controlling for increases in EBV genome copy numbers over this interval.…”

Section: Resultsmentioning

confidence: 99%

“…Incoming EBV genomes are organized into nucleosomes, which must then be maintained or remodeled on newly synthesized, damaged, or transcribed regions of EBV genomes. Burkitt lymphoma cells are among the fastest growing human tumor cells, and newly EBV-infected B-cells undergo Burkitt-like hyperproliferation between day 3 and day 7 postinfection in cell culture ( 11 – 13 ). Host machinery must therefore propagate chromatin-encoded epigenetic information with each cell cycle, a process which begins with histone loading.…”

Section: Discussionmentioning

confidence: 99%

“…It is plausible that other histone chaperones, in particular, HIRA, may play key roles in H3/H4 loading onto incoming EBV genomes prior to mitosis in newly infected cells. CAF1 may then carry out DNA replication-dependent roles, beginning with entry of the newly infected cell into S-phase at approximately 72 h postinfection ( 11 – 13 ), and HIRA plays ongoing roles that remain to be defined. Notably, EBV tegument protein BNRF1 subverts DAXX/ATRX-mediated H3.3 loading on viral chromatin for the first several days postinfection and presumably also with lytic reactivation ( 23 , 24 ) ( Fig.…”

Section: Discussionmentioning

confidence: 99%

“…Multiple layers of epigenetic regulation enable EBV to establish latency in newly infected B-cells, in which a small number of virus-encoded proteins and viral noncoding RNAs (ncRNAs) reprogram the metabolism, growth, and survival pathways of infected cells ( 7 – 9 ). Within 3 days of infection, quiescent B-cells are reprogramed to become rapidly growing lymphoblasts that divide as frequently as every 8 h ( 10 – 13 ).…”

Section: Introductionmentioning

confidence: 99%

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Histone Loaders CAF1 and HIRA Restrict Epstein-Barr Virus B-Cell Lytic Reactivation

Zhang

Jiang

Trudeau

et al. 2020

mBio

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Epstein-Barr virus (EBV) infects 95% of adults worldwide and causes infectious mononucleosis. EBV is associated with endemic Burkitt lymphoma, Hodgkin lymphoma, posttransplant lymphomas, nasopharyngeal and gastric carcinomas. In these cancers and in most infected B-cells, EBV maintains a state of latency, where nearly 80 lytic cycle antigens are epigenetically suppressed. To gain insights into host epigenetic factors necessary for EBV latency, we recently performed a human genome-wide CRISPR screen that identified the chromatin assembly factor CAF1 as a putative Burkitt latency maintenance factor. CAF1 loads histones H3 and H4 onto newly synthesized host DNA, though its roles in EBV genome chromatin assembly are uncharacterized. Here, we found that CAF1 depletion triggered lytic reactivation and virion secretion from Burkitt cells, despite also strongly inducing interferon-stimulated genes. CAF1 perturbation diminished occupancy of histones 3.1 and 3.3 and of repressive histone 3 lysine 9 and 27 trimethyl (H3K9me3 and H3K27me3) marks at multiple viral genome lytic cycle regulatory elements. Suggestive of an early role in establishment of latency, EBV strongly upregulated CAF1 expression in newly infected primary human B-cells prior to the first mitosis, and histone 3.1 and 3.3 were loaded on the EBV genome by this time point. Knockout of CAF1 subunit CHAF1B impaired establishment of latency in newly EBV-infected Burkitt cells. A nonredundant latency maintenance role was also identified for the DNA synthesis-independent histone 3.3 loader histone regulatory homologue A (HIRA). Since EBV latency also requires histone chaperones alpha thalassemia/mental retardation syndrome X-linked chromatin remodeler (ATRX) and death domain-associated protein (DAXX), EBV coopts multiple host histone pathways to maintain latency, and these are potential targets for lytic induction therapeutic approaches. IMPORTANCE Epstein-Barr virus (EBV) was discovered as the first human tumor virus in endemic Burkitt lymphoma, the most common childhood cancer in sub-Saharan Africa. In Burkitt lymphoma and in 200,000 EBV-associated cancers per year, epigenetic mechanisms maintain viral latency, during which lytic cycle factors are silenced. This property complicated EBV’s discovery and facilitates tumor immunoevasion. DNA methylation and chromatin-based mechanisms contribute to lytic gene silencing. Here, we identified histone chaperones CAF1 and HIRA, which have key roles in host DNA replication-dependent and replication-independent pathways, respectively, as important for EBV latency. EBV strongly upregulates CAF1 in newly infected B-cells, where viral genomes acquire histone 3.1 and 3.3 variants prior to the first mitosis. Since histone chaperones ATRX and DAXX also function in maintenance of EBV latency, our results suggest that EBV coopts multiple histone pathways to reprogram viral genomes and highlight targets for lytic induction therapeutic strategies.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Histone Loaders CAF1 and HIRA Restrict Epstein-Barr Virus B-Cell Lytic Reactivation

Zhang

Jiang

Trudeau

et al. 2020

mBio

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“…Latency establishment is an intricately regulated process that allows viruses to temporarily adopt an alternative viral state. Taking EBV as an example, upon infection of B lymphocytes, the virus first activates all eight latency genes to aid in the activation of naive B cells (type III latency), and then certain genes are switched off (type I/II latency), to minimize the number of viral proteins that are detectable by the immune system, with different latency types utilizing distinct viral promoters that are associated with active chromatin marks only when needed [72][73][74] . Meanwhile, lytic viral genes remain transcriptionally silent and are associated with heterochromatic markers during latency 70,75 .…”

Section: Latent Viral Infections Upon Infection Of Certain Cellmentioning

confidence: 99%

Epigenetic and epitranscriptomic regulation of viral replication

2020

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Eukaryotic gene expression is regulated not only by genomic enhancers and promoters, but also by covalent modifications added to both chromatin and RNAs. Whereas cellular gene expression may be either enhanced or inhibited by specific epigenetic modifications deposited on histones (in particular, histone H3), these epigenetic modifications can also repress viral gene expression, potentially functioning as a potent antiviral innate immune response in DNA virus-infected cells. However, viruses have evolved countermeasures that prevent the epigenetic silencing of their genes during lytic replication, and they can also take advantage of epigenetic silencing to establish latent infections. By contrast, the various covalent modifications added to RNAs, termed epitranscriptomic modifications, can positively regulate mRNA translation and/or stability, and both DNA and RNA viruses have evolved to utilize epitranscriptomic modifications as a means to maximize viral gene expression. As a consequence, both chromatin and RNA modifications could serve as novel targets for the development of antivirals. In this Review, we discuss how host epigenetic and epitranscriptomic processes regulate viral gene expression at the levels of chromatin and RNA function, respectively, and explore how viruses modify, avoid or utilize these processes in order to regulate viral gene expression.

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Epstein-Barr virus BNRF1 destabilizes SMC5/6 cohesin complexes to evade its restriction of replication compartments

et al. 2022

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The first days in the life of naïve human B-lymphocytes infected with Epstein-Barr virus

Cited by 22 publications

References 85 publications

Histone Loaders CAF1 and HIRA Restrict Epstein-Barr Virus B-Cell Lytic Reactivation

Histone Loaders CAF1 and HIRA Restrict Epstein-Barr Virus B-Cell Lytic Reactivation

Epigenetic and epitranscriptomic regulation of viral replication

Epstein-Barr virus BNRF1 destabilizes SMC5/6 cohesin complexes to evade its restriction of replication compartments

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