Mutational Analysis of the Repeated Open Reading Frames, ORFs 63 and 70 and ORFs 64 and 69, of Varicella-Zoster Virus

Sommer, Marvin; Zagha, Edward; Serrano, Oscar K.; Ku, Chia-Chi; Zerboni, Leigh; Baiker, Armin; Santos, Richard A.; Spengler, Mary L.; Lynch, Jennifer M.; Grose, Charles; Ruyechan, William T.; Hay, John; Arvin, Ann M.

doi:10.1128/jvi.75.17.8224-8239.2001

Cited by 68 publications

(98 citation statements)

References 52 publications

(50 reference statements)

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“…These experiments demonstrated that VZV spreads efficiently between neural cells in vivo, without changing cellular morphology or expression of neural cell proteins, including hNCAM, hGFAP, and ␤-tubulin III. VZV gene expression in neural cells differed dramatically from VZV infection of epidermal and dermal cells in human skin in vivo, which is associated with cell destruction and release of infectious virions (20)(21)(22)(23)(24). IE62, the major viral transactivating protein and an important component of the virion tegument (38,39), was restricted to the nuclei of neurons and glial cells, whereas IE62 localized to the cytoplasm of infected skin cells.…”

Section: Discussionmentioning

confidence: 99%

“…NOD-SCID mice transplanted with human neurosphere cells (StemCells Inc.) were inoculated with VZV-infected human melanoma cells at 4-6 months after transplant. Viruses tested were pOka, live attenuated vOka (Merck), and rOka⌬70, a deletion mutant with only one copy of the gene encoding IE63 (24). Melanoma cells were grown in tissue culture medium (DMEM, GIBCO) supplemented with heat-inactivated FCS.…”

Section: Methodsmentioning

confidence: 99%

“…VZV causes lytic infection of human dermal and epidermal cells in skin xenografts in vivo (20)(21)(22)(23)(24)38). To compare VZV protein expression in human neural and skin cells in vivo, skin xenografts were collected 3 weeks after VZV infection, and alternate sections were examined for IE62, IE63, ORF47 kinase, or gE synthesis (Fig.…”

Section: Vzv Protein Expression In Infected Skinmentioning

confidence: 99%

“…The expanding populations migrate throughout the brain from the SVZ to the olfactory bulb, express human neuronal and glial cell markers, and develop axonal processes. Skin and thymus͞liver xenografts in SCID mice permit analysis of VZV tropism for human epidermal and dermal cells and T cells within their intact tissue microenvironments in vivo (20)(21)(22)(23)(24). Therefore, we used the chimeric NOD-SCID mouse-human neural cell model to investigate VZV infection of differentiated neural cells in vivo.…”

mentioning

confidence: 99%

“…We also evaluated a VZV deletion mutant, rOka⌬70, that lacks one copy of the gene encoding IE63, because neural cell expression of IE63 has been prominent in autopsy and animal studies (9,13,15). This mutant, and two other single-copy ORF63͞70 variants, exhibits no deficiencies in cell culture and is as virulent as the parent virus in human skin xenografts in SCID mice (24), These experiments in the NOD-SCID mouse-human neural cell model showed that VZV infection with pOka, vOka, and rOka⌬70 was characterized by efficient spread in human neurons and glial cells, without disrupting cell morphology or expression of neural cell adhesion molecules (hNCAMs), glial fibrillary acidic protein (hGFAP), or neuron-specific class III ␤-tubulin in vivo. VZV infection of human neural cells exhibited a distinctive intracellular distribution of the IE regulatory proteins and a block in synthesis of the major envelope glycoprotein, gE, compared to lytic VZV infection of epidermal and dermal cells in vivo.…”

mentioning

confidence: 99%

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Varicella-zoster virus infection of human neural cells in vivo

Baiker

Fabel

Cozzio

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

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Varicella-zoster virus (VZV) establishes latency in sensory ganglia and causes herpes zoster upon reactivation. These investigations in a nonobese diabetic severe combined immunodeficient mousehuman neural cell model showed that VZV infected both neurons and glial cells and spread efficiently from cell to cell in vivo. Neural cell morphology and protein synthesis were preserved, in contrast to destruction of epithelial cells by VZV. Expression of VZV genes in neural cells was characterized by nuclear retention of the major viral transactivating protein and a block in synthesis of the predominant envelope glycoprotein. The attenuated VZV vaccine strain retained infectivity for neurons and glial cells in vivo. VZV gene expression in differentiated human neural cells in vivo differs from neural infection by herpes simplex virus, which is characterized by latency-associated transcripts, and from lytic VZV replication in skin. The chimeric nonobese diabetic severe combined immunodeficient mouse model may be useful for investigating other neurotropic human viruses.

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Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Vzv Protein Expression In Infected Skinmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Varicella-zoster virus infection of human neural cells in vivo

Baiker

Fabel

Cozzio

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

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Interaction of allergy history and antibodies to specific varicella‐zoster virus proteins on glioma risk

Lee

Bracci

Zhou

et al. 2013

Intl Journal of Cancer

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Glioma is the most common cancer of the central nervous system but with few confirmed risk factors. Glioma has been inversely associated with chicken pox, shingles, and seroreactivity to varicella virus (VZV), as well as to allergies and allergy-associated IgE. The role of antibody reactivity against individual VZV antigens has not been assessed. Ten VZV-related proteins, selected for high immunogenicity or known function, were synthesized and used as targets for antibody measurements in the sera of 143 glioma cases and 131 healthy controls selected from the San Francisco Bay Area Adult Glioma Study. Glioma cases exhibited significantly reduced seroreactivity compared to controls for six antigens, including proteins IE63 (OR = 0.26, 95%CI:0.12-0.58, comparing lowest quartile to highest), and the VZV-unique protein ORF2p (OR = 0.44, 95%CI:0.21-0.96, lowest quartile to highest). When stratifying the study population into those with low and high self-reported allergy history, VZV protein seroreactivity was only associated inversely with glioma among individuals self-reporting more than two allergies. The data provide insight into both allergy and VZV effects on glioma: strong anti-VZV reactions in highly allergic individuals is associated with reduced occurrence of glioma. This result suggests a role for specificity in the anti-VZV immunity in brain tumor suppression for both individual VZV antigens and in the fine-tuning of the immune response by allergy. Anti-VZV reactions may also be a biomarker of effective CNS immunosurveillance due to the tropism of the virus.

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Molecular studies of Varicella zoster virus

Quinlivan

Breuer²

2006

Rev. Med. Virol.

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VZV is a highly cell-associated member of the Herpesviridae family and one of the eight herpesviruses to infect humans. The virus is ubiquitous in most populations worldwide, primary infection with which causes varicella, more commonly known as chickenpox. Characteristic of members of the alphaherpesvirus sub-family, VZV is neurotropic and establishes latency in sensory neurones. Reactivation from latency, usually during periods of impaired cellular immunity, causes herpes zoster (shingles). Despite being one of the most genetically stable human herpesviruses, nucleotide alterations in the virus genome have been used to classify VZV strains from different geographical regions into distinct clades. Such studies have also provided evidence that, despite pre-existing immunity to VZV, subclinical reinfection and reactivation of reinfecting strains to cause zoster is also occurring. During both primary infection and reactivation, VZV infects several PBMC and skin cell lineages. Difficulties in studying the pathogenesis of VZV because of its high cell association and narrow host range have been overcome through the development of the VZV severe combined immunodeficient mouse model carrying human tissue implants. This model has provided a valuable tool for studying the importance of individual viral proteins during both the complex intracellular replication and assembly of new virions and for understanding the underlying mechanism of attenuation of the live varicella vaccine. In addition, a rat model has been developed and successfully used to uncover which viral proteins are important for both the establishment and maintenance of latent VZV infection.

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Mutational Analysis of the Repeated Open Reading Frames, ORFs 63 and 70 and ORFs 64 and 69, of Varicella-Zoster Virus

Cited by 68 publications

References 52 publications

Varicella-zoster virus infection of human neural cells in vivo

Varicella-zoster virus infection of human neural cells in vivo

Interaction of allergy history and antibodies to specific varicella‐zoster virus proteins on glioma risk

Molecular studies of Varicella zoster virus

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