Inhibition of Human Cytomegalovirus Replication by Artemisinins: Effects Mediated through Cell Cycle Modulation

Roy, Suheeta; He, Ran; Kapoor, Arun; Forman, Michael; Mazzone, Jennifer R.; Posner, Gary H.; Arav‐Boger, Ravit

doi:10.1128/aac.00262-15

Cited by 37 publications

(29 citation statements)

References 34 publications

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“…Cdk2 inhibitors with high selectivity such as Alsterpaullone, Indirubin-3′-monoxime, Purvalanol A, and r-Roscovitine have previously been shown to inhibit the replication of other viruses including HIV-1, Hepatitis C Virus, Human Cytomegalovirus, Adenovirus, and Varicella-Zoster Virus (Bresnahan et al, 1997; Taylor et al, 2004; Guendel et al, 2010; Cheng et al, 2013; Munakata et al, 2014; Roy et al, 2015). We therefore investigated if any of these inhibitors could affect the phosphorylation of VP40 in vitro .…”

Section: Resultsmentioning

confidence: 99%

Ebola VP40 in Exosomes Can Cause Immune Cell Dysfunction

et al. 2016

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Ebola virus (EBOV) is an enveloped, ssRNA virus from the family Filoviridae capable of causing severe hemorrhagic fever with up to 80–90% mortality rates. The most recent outbreak of EBOV in West Africa starting in 2014 resulted in over 11,300 deaths; however, long-lasting persistence and recurrence in survivors has been documented, potentially leading to further transmission of the virus. We have previously shown that exosomes from cells infected with HIV-1, HTLV-1 and Rift Valley Fever virus are able to transfer viral proteins and non-coding RNAs to naïve recipient cells, resulting in an altered cellular activity. In the current manuscript, we examined the effect of Ebola structural proteins VP40, GP, NP and VLPs on recipient immune cells, as well as the effect of exosomes containing these proteins on naïve immune cells. We found that VP40-transfected cells packaged VP40 into exosomes, and that these exosomes were capable of inducing apoptosis in recipient immune cells. Additionally, we show that presence of VP40 within parental cells or in exosomes delivered to naïve cells could result in the regulation of RNAi machinery including Dicer, Drosha, and Ago 1, which may play a role in the induction of cell death in recipient immune cells. Exosome biogenesis was regulated by VP40 in transfected cells by increasing levels of ESCRT-II proteins EAP20 and EAP45, and exosomal marker proteins CD63 and Alix. VP40 was phosphorylated by Cdk2/Cyclin complexes at Serine 233 which could be reversed with r-Roscovitine treatment. The level of VP40-containing exosomes could also be regulated by treated cells with FDA-approved Oxytetracycline. Additionally, we utilized novel nanoparticles to safely capture VP40 and other viral proteins from Ebola VLPs spiked into human samples using SDS/reducing agents, thus minimizing the need for BSL-4 conditions for most downstream assays. Collectively, our data indicates that VP40 packaged into exosomes may be responsible for the deregulation and eventual destruction of the T-cell and myeloid arms of the immune system (bystander lymphocyte apoptosis), allowing the virus to replicate to high titers in the immunocompromised host. Moreover, our results suggest that the use of drugs such as Oxytetracycline to modulate the levels of exosomes exiting EBOV-infected cells may be able to prevent the devastation of the adaptive immune system and allow for an improved rate of survival.

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Section: Resultsmentioning

confidence: 99%

Ebola VP40 in Exosomes Can Cause Immune Cell Dysfunction

et al. 2016

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“…It is an artemisinin-derived monomer able to inhibit in vitro CMV replication in human foreskin fibroblasts at micromolar concentrations through cell cycle modulation with an early arrest in G1 phase [55]. Cell cycle modulation via cyclin-dependent kinases and retinoblastoma protein appears to play an important role in artemisinins activities [56].…”

Section: Artesunate -The Antimalarialmentioning

confidence: 99%

Treatment of CMV infection after allogeneic hematopoietic stem cell transplantation

Madon

Giaccone

Festuccia

et al. 2016

Expert Review of Hematology

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“…Example strategies that attract cells in the mitotic state include the inhibition on anaphase-promoting complex (APC) by the apoptin protein of chicken anemia virus (CAV) [105], interference with kinetochores by HSV-1 ICP0 protein, and sustained CDK1-cyclin B1 activity by the non-degradable cyclin B analog EC27 protein of baculovirus [106]. Human CMV arrests cells in the S stage by preventing them from genome replication through the IE2 viral protein [107]. HBV triggers hepatocytes exist G0 but stall in G1 through the HBx viral protein that takes advantage of mitochondrialdependent calcium signaling [108].…”

Section: Cell Cycle Arrestmentioning

confidence: 99%

Orchestrated efforts on host network hijacking: Processes governing virus replication

et al. 2020

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With the high pervasiveness of viral diseases, the battle against viruses has never ceased. Here we discuss five cellular processes, namely "autophagy", "programmed cell death", "immune response", "cell cycle alteration", and "lipid metabolic reprogramming", that considerably guide viral replication after host infection in an orchestrated manner. On viral infection, "autophagy" and "programmed cell death" are two dynamically synchronized cell survival programs; "immune response" is a cell defense program typically suppressed by viruses; "cell cycle alteration" and "lipid metabolic reprogramming" are two altered cell housekeeping programs tunable in both directions. We emphasize on their functionalities in modulating viral replication, strategies viruses have evolved to tune these processes for their benefit, and how these processes orchestrate and govern cell fate upon viral infection. Understanding how viruses hijack host networks has both academic and industrial values in providing insights toward therapeutic strategy design for viral disease control, offering useful information in applications that aim to use viral vectors to improve human health such as gene therapy, and providing guidelines to maximize viral particle yield for improved vaccine production at a reduced cost. ARTICLE HISTORY

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Inhibition of Human Cytomegalovirus Replication by Artemisinins: Effects Mediated through Cell Cycle Modulation

Cited by 37 publications

References 34 publications

Ebola VP40 in Exosomes Can Cause Immune Cell Dysfunction

Ebola VP40 in Exosomes Can Cause Immune Cell Dysfunction

Treatment of CMV infection after allogeneic hematopoietic stem cell transplantation

Orchestrated efforts on host network hijacking: Processes governing virus replication

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