2018
DOI: 10.1371/journal.ppat.1007221
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An EBNA3C-deleted Epstein-Barr virus (EBV) mutant causes B-cell lymphomas with delayed onset in a cord blood-humanized mouse model

Abstract: EBV causes human B-cell lymphomas and transforms B cells in vitro. EBNA3C, an EBV protein expressed in latently-infected cells, is required for EBV transformation of B cells in vitro. While EBNA3C undoubtedly plays a key role in allowing EBV to successfully infect B cells, many EBV+ lymphomas do not express this protein, suggesting that cellular mutations and/or signaling pathways may obviate the need for EBNA3C in vivo under certain conditions. EBNA3C collaborates with EBNA3A to repress expression of the CDKN… Show more

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Cited by 25 publications
(59 citation statements)
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“…This persistence was associated with EBNA2-driven proliferation during the first month of infection, which then, switched to EBV latency 0 persistence with only non-translated EBER expression after three months 22 . The observed absence of EBV latency III seems to be caused by a combination of EBNA3A or EBNA3C deficiency and immune control of rare completely virus transformed B cells, because in a HIS mouse model with less immunocompetence, LMPexpressing EBNA3C-negative lymphomas can be observed at lower frequency compared to wild-type EBV infection 59 . These findings suggest that EBV persistence might be achieved with minimal or no EBV latency III infection.…”
Section: Persistence Without Transformationmentioning
confidence: 95%
“…This persistence was associated with EBNA2-driven proliferation during the first month of infection, which then, switched to EBV latency 0 persistence with only non-translated EBER expression after three months 22 . The observed absence of EBV latency III seems to be caused by a combination of EBNA3A or EBNA3C deficiency and immune control of rare completely virus transformed B cells, because in a HIS mouse model with less immunocompetence, LMPexpressing EBNA3C-negative lymphomas can be observed at lower frequency compared to wild-type EBV infection 59 . These findings suggest that EBV persistence might be achieved with minimal or no EBV latency III infection.…”
Section: Persistence Without Transformationmentioning
confidence: 95%
“…In mice reconstituted with functional components of a human immune system it is possible to study EBV's biology in vivo (Münz, 2015), but steps early after infection are difficult to investigate in this tractable model. To our knowledge, an EBNA2-deleted virus has not been studied in this animal model, yet, but, unexpectedly, EBV strains incapable of expressing EBNA3C were found to establish latency and cause B cell lymphomas albeit at a reduced frequency compared with wild-type EBV (Murer et al, 2018;Romero-Masters et al, 2018). EBNA3C is a transcriptional repressor and has been found to abrogate the expression of cell cycle inhibitors such as p16 INK4A encoded by CDKN2A, which is a prerequisite to establish lymphoblastoid cell lines with EBNA3C-deleted EBVs in vitro (Skalska et al, 2013).…”
Section: The Limitations Of the In Vitro B Cell Infection Modelmentioning
confidence: 99%
“…B cells infected with EBNA3C deleted mutant EBVs ceased to proliferate about two weeks post infection(Skalska et al, 2013) very much in contrast to the situation in vivo. In hu-mice EBNA3C deleted viruses established latent infection in B cells while the cells expressed appreciable levels of p16(Romero-Masters et al, 2018). Possibly, there are several reasons that may lead to the observed differences, but the comparison demonstrates the limitations of the experimental models with which we can study the biology of EBV infection in vitro.Some of these limitations also became obvious in our experiments.…”
mentioning
confidence: 98%
“…Thus, the ability of EBV to transform B cells into long-term LCLs in vitro may not adequately model certain aspects of EBV-associated B-cell lymphomas in humans. We have recently established a humanized mouse model that better models many aspects of the human disease, including a role for lytic infection [4], and the development of EBV-induced lymphomas in the absence of LMP1 or EBNA3C [5,6].…”
Section: Introductionmentioning
confidence: 99%