Your search keyword '"Viral persistence"' showing total 6 results

1. The Brd4 acetyllysine-binding protein is involved in activation of polyomavirus JC.

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Author

Wollebo, Hassen, Bellizzi, Anna, Cossari, Dominique, Salkind, Julian, Safak, Mahmut, and White, Martyn

Subjects

*POLYOMAVIRUSES, *JOHN Cunningham virus, *PROGRESSIVE multifocal leukoencephalopathy, *NF-kappa B, *EPIGENETICS, *GENE expression

Abstract

Brd4 is an epigenetic reader protein and a member of the BET (bromodomain and extra terminal domain) family of proteins with two bromodomains that recognize acetylated lysine residues. Brd4 specifically binds to acetylated transcription factor NF-κB p65 and coactivates transcription. Polyomavirus JC (JCV) is regulated by a noncoding control region (NCCR) containing promoter/enhancer elements for viral gene expression including a binding site for NF-κB, which responds to proinflammatory cytokines such as TNF-α, the DNA damage response, calcium signaling and acetylation of the NF-κB p65 subunit on lysine residues K218 and K221. Earlier studies indicated that NF-κB is involved in the reactivation of persistent/latent JCV in glial cells to cause progressive multifocal leukoencephalopathy (PML), a severe demyelinating disease of the brain caused by replication of JCV in glial cells. To investigate the mechanism of action of NF-κB acetylation on JCV transcription, we examined Brd4 and found that JCV early transcription was stimulated by Brd4 via the JCV NF-κB site and that p65 K218 and K221 were involved. Treatment with the Brd4 inhibitor JQ1(+) or mutation of either K218 or K221 to glutamine (K218R or K221) inhibited this stimulation and decreased the proportion of p65 in the nucleus. We conclude that Brd4 is involved in the regulation of the activation status of JCV in glial cells. [ABSTRACT FROM AUTHOR] more...

Published

2016

2. Epigenetic regulation of polyomavirus JC involves acetylation of specific lysine residues in NF-κB p65.

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Author

Wollebo, Hassen, Bellizzi, Anna, Cossari, Dominique, Safak, Mahmut, Khalili, Kamel, and White, Martyn

Subjects

*JOHN Cunningham virus, *ACETYLATION, *EPIGENETICS, *NF-kappa B, *PROGRESSIVE multifocal leukoencephalopathy, *DEMYELINATION

Abstract

Progressive multifocal leukoencephalopathy (PML) is a fatal demyelinating disease caused by neurotropic polyomavirus, JC virus (JCV), a virus that causes lytic infection of CNS glial cells. After primary infection, JCV is controlled by the immune system but virus persists asymptomatically. Rarely, when immune function is impaired, it can reemerge to cause PML. The mechanisms of JCV persistence and reactivation are not well understood but our earlier work implicated epigenetic control by protein acetylation since histone deacetylase inhibitors such as trichostatin A (TSA) strongly stimulate JCV transcription. Since both TNF-α and TSA activate JCV transcription via the same unique NF-κB site in the JCV control region, we investigated a role for acetylation of NF-κB in JCV regulation. A site-directed mutagenesis strategy was employed targeting the known lysine acetylation sites of NF-κB p65: K218, K221, and K310. We individually mutated each lysine to arginine, which cannot be acetylated and retains a positive charge like lysine. K218R and K221R impaired transactivation of JCV early promoter transcription either alone or combined with TSA treatment or coexpression of acetyltransferase transcriptional coactivator p300 but K310R was largely without effect. Mutation of lysine to glutamine gives mutants with a negative charge like acetyllysine. However, K218Q and K221Q showed impaired activity and only K310Q showed enhanced transactivation. NF-κB acetylation can regulate several aspects of the process of activation including complex formation with IκB, translocation to the nucleus, and DNA binding and transcriptional activation. Cell fractionation studies revealed that the mutants had no defect in translocation to the nucleus whereas gel shift studies revealed reduced binding to the JCV NF-κB site. Thus, acetylation regulates NF-κB p65 activity toward JCV at the level of p65 binding to the JCV control region and activation of JCV transcription. [ABSTRACT FROM AUTHOR] more...

Published

2015

3. Cell-cell contact viral transfer contributes to HIV infection and persistence in astrocytes.

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Author

Luo, Xiaoyu and He, Johnny

Subjects

*CELL communication, *HIV infections, *ASTROCYTES, *ENDOCYTOSIS, *VIRAL receptors, *CD4 antigen

Abstract

Astrocytes are the most abundant cells in the central nervous system and play important roles in human immunodeficiency virus (HIV)/neuro-acquired immunodeficiency syndrome. Detection of HIV proviral DNA, RNA, and early gene products but not late structural gene products in astrocytes in vivo and in vitro indicates that astrocytes are susceptible to HIV infection albeit in a restricted manner. We as well as others have shown that cell-free HIV is capable of entering CD4− astrocytes through human mannose receptor-mediated endocytosis. In this study, we took advantage of several newly developed fluorescence protein-based HIV reporter viruses and further characterized HIV interaction with astrocytes. First, we found that HIV was successfully transferred to astrocytes from HIV-infected CD4+ T cells in a cell-cell contact- and gp120-dependent manner. In addition, we demonstrated that, compared to endocytosis-mediated cell-free HIV entry and subsequent degradation of endocytosed virions, the cell-cell contact between astrocytes and HIV-infected CD4+ T cells led to robust HIV infection of astrocytes but retained the restricted nature of viral gene expression. Furthermore, we showed that HIV latency was established in astrocytes. Lastly, we demonstrated that infectious progeny HIV was readily recovered from HIV latent astrocytes in a cell-cell contact-mediated manner. Taken together, our studies point to the importance of the cell-cell contact-mediated HIV interaction with astrocytes and provide direct evidence to support the notion that astrocytes are HIV latent reservoirs in the central nervous system. [ABSTRACT FROM AUTHOR] more...

Published

2015

4. Detection of the archetypal regulatory region of JC virus from the tonsil tissue of patients with tonsillitis and tonsilar hypertrophy.

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Author

Kato, Atsushi, Kitamura, Tadaichi, Takasaka, Tomokazu, Tominaga, Takashi, Ishikawa, Akira, Huai-Ying Zheng, and Yogo, Yoshiaki

Subjects

*DNA, *POLYMERASE chain reaction, *CENTRAL nervous system diseases, *TONSILLITIS, *HYPERTROPHY, *LYMPHOID tissue

Abstract

The regulatory regions of JC virus (JCV) DNAs in the brain of patients with progressive multifocal leukoencephalopathy (PML) (designated as PML-type regulatory regions) are hypervariable, whereas those in the urine and renal tissue of individuals without PML have the same basic structure, designated as the archetype. It is thought that JCV strains with the archetypal regulatory region circulate in the human population. Nevertheless, Monaco et al (J Virol 70: 7004–7012, 1996) reported that PML-type regulatory regions occur in human tonsil tissue. The purpose of this study is to confirm their findings. Using nested polymerase chain reaction (PCR), the authors detected the regulatory region of JCV DNA in the tonsil tissue from 14 (44%) of 32 donors with tonsillitis and tonsilar hypertrophy. Sequencing of the detected regulatory regions indicated that they were identical with the archetypal regulatory regions detected previously or, in a few cases, slightly deviated from the archetype. This finding suggests not only that tonsil tissue is the potential site of initial JCV infection but also that archetypal JCV strains circulate in the human population. [ABSTRACT FROM AUTHOR] more...

Published

2004

5. Eradication of HIV-1 from CNS reservoirs: current strategies and future priorities

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Author

Jeymohan Joseph

Subjects

business.industry, Research areas, Human immunodeficiency virus (HIV), Brain, Public relations, medicine.disease, medicine.disease_cause, Virus Latency, Novel gene, Cellular and Molecular Neuroscience, Animal model, Neurology, Acquired immunodeficiency syndrome (AIDS), Virology, Myeloid cells, medicine, HIV-1, Humans, Neurology (clinical), Business, Neurovirology, Viral persistence, Disease Reservoirs

Abstract

Eradication of HIV-1 and achieving a sterilizing or functional cure has become a priority area in the AIDS field. Large investments have been made by funding agencies, particularly NIH, in understanding the mechanisms of HIV persistence and approaches to target and eradicate latent reservoirs. The majority of the work that is ongoing has focused on studying resting CD4+ T cell reservoirs and developing strategies for reactivation and purging HIV from this cell type. However, it is becoming increasingly clear that other sites of HIV persistence exist including anatomic reservoirs such as the brain and gut. Also, myeloid cells residing in these anatomic compartments may harbor persistent HIV-1 that could potentially be a source of rebounding virus upon cessation of therapy. The brain is unique in terms of its immune privileged status and the presence of the blood-brain barrier which restricts entry of anti-retrovirals. HIV-1 seeds the brain early in infection and may reside in long-lived cells such as microglia and astrocytes and thus serve as a site of viral persistence. At an NIMH-sponsored meeting entitled “Eradication of HIV-CNS Reservoirs—Current and Future Strategies” held in Washington DC in conjunction with the 12th International Symposium on NeuroVirology (October 2013), many of the challenges in targeting brain HIV-1 reservoirs and the need to better understand the mechanisms of establishment of latency in this unique anatomic compartment were discussed. At that meeting, it was felt that the field would greatly benefit by the publication of a special issue of the Journal of NeuroVirology devoted to HIV-1 CNS reservoirs that would address the challenges and current knowledge in this area. This special issue represents work presented by many of the speakers at the NIMH-sponsored symposium. In addition, several other authors have contributed in order to provide a comprehensive review of the state of the field. The articles presented discuss current challenges in targeting CNS reservoirs as well as mechanisms of establishing persistence in CNS-derived cell populations such as microglia, macrophages, and astrocytes. Current approaches to target myeloid reservoirs as well as some novel gene editing strategies that may aid in HIV-1 eradication strategies are also discussed. I have provided below, for the reader of this special issue, a brief summary of each of the papers published in order to capture the flavor of the topic area covered. The summaries are by no means comprehensive but are illustrative of the research areas that these papers represent. An overview of the translational challenges in targeting latent HIV infection and the CNS reservoir problem was highlighted by Dr. David Margolis. Some of the challenges include the need for reliable, validated cell-based and animal model systems to test latency-reversing agents. He cautions that of several potential anatomic reservoirs, the central J. Joseph (*) Division of AIDS Research, National Institute of Mental Health, Room 9G20, MSC 9831 5601 Fishers Lane, Bethesda, MD 20892-9830, USA e-mail: jjeymoha@mail.nih.gov more...

Published

2015

6. 2002 Pioneer in NeuroVirology lecture

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Author

B. Wigdahl and V. ter Meulen

Subjects

Award Lecture, Measle Virus, business.industry, Virology, Cellular and Molecular Neuroscience, Neurology, Measle, Virus Persistence, Encephalitis, Medicine, Neurology (clinical), Viral persistence, Neurovirology, business

Abstract

(2002). 2002 Pioneer in NeuroVirology lecture. Journal of Neurovirology: Vol. 8, No. 3, pp. 34-34.

Published

2002