Virus Demyelination

Fazakerley, John K.; Walker, Robert

doi:10.1080/13550280390194046

Cited by 62 publications

(45 citation statements)

References 194 publications

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“…8 Several viruses can cause diseases involving demyelination, including measles, human immunodeficiency virus (HIV), and the human T-cell lymphotropic virus type I. 23 Therefore, it is biologically plausible for MS, as a demyelinating disease, to have a viral etiology. Viruses associated with MS have included measles, 3 Epstein-Barr virus (infectious mononucleosis), 4 human herpes virus 6, 5 and mumps.…”

Section: Discussionmentioning

confidence: 99%

Parental Age, Family Size, and Risk of Multiple Sclerosis

Montgomery¹,

Lambe²,

Olsson³

et al. 2004

Epidemiology

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Section: Discussionmentioning

confidence: 99%

Parental Age, Family Size, and Risk of Multiple Sclerosis

Montgomery¹,

Lambe²,

Olsson³

et al. 2004

Epidemiology

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“…Interestingly, these DEGs remained downregulated long after virus replication had ended, suggesting that SVV infection of the ganglia results in long-term changes in the ganglion transcriptome. Several of these genes were involved in myelination (MOBP, MAG, MBP, and PRG4), which suggested that SVV may lead to demyelination, as has been described for HSV-1 and -2 (149,150). Genes downregulated 14 dpi were involved in neuronal apoptosis, which may be another strategy that SVV utilizes to establish latency in the ganglia.…”

Section: Discussionmentioning

confidence: 99%

Acute Simian Varicella Virus Infection Causes Robust and Sustained Changes in Gene Expression in the Sensory Ganglia

Arnold

Girke

Sureshchandra

et al. 2016

J Virol

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Primary infection with varicella-zoster virus (VZV), a neurotropic alphaherpesvirus, results in varicella. VZV establishes latency in the sensory ganglia and can reactivate later in life to cause herpes zoster. The relationship between VZV and its host during acute infection in the sensory ganglia is not well understood due to limited access to clinical specimens. Intrabronchial inoculation of rhesus macaques with simian varicella virus (SVV) recapitulates the hallmarks of VZV infection in humans. We leveraged this animal model to characterize the host-pathogen interactions in the ganglia during both acute and latent infection by measuring both viral and host transcriptomes on days postinfection (dpi) 3, 7, 10, 14, and 100. SVV DNA and transcripts were detected in sensory ganglia 3 dpi, before the appearance of rash. CD4 and CD8 T cells were also detected in the sensory ganglia 3 dpi. Moreover, lung-resident T cells isolated from the same animals 3 dpi also harbored SVV DNA and transcripts, suggesting that T cells may be responsible for trafficking SVV to the ganglia. Transcriptome sequencing (RNA-Seq) analysis showed that cessation of viral transcription 7 dpi coincides with a robust antiviral innate immune response in the ganglia. Interestingly, a significant number of genes that play a critical role in nervous system development and function remained downregulated into latency. These studies provide novel insights into host-pathogen interactions in the sensory ganglia during acute varicella and demonstrate that SVV infection results in profound and sustained changes in neuronal gene expression. IMPORTANCEMany aspects of VZV infection of sensory ganglia remain poorly understood, due to limited access to human specimens and the fact that VZV is strictly a human virus. Infection of rhesus macaques with simian varicella virus (SVV), a homolog of VZV, provides a robust model of the human disease. Using this model, we show that SVV reaches the ganglia early after infection, most likely by T cells, and that the induction of a robust innate immune response correlates with cessation of virus transcription. We also report significant changes in the expression of genes that play an important role in neuronal function. Importantly, these changes persist long after viral replication ceases. Given the homology between SVV and VZV, and the genetic and physiological similarities between rhesus macaques and humans, our results provide novel insight into the interactions between VZV and its human host and explain some of the neurological consequences of VZV infection. V aricella-zoster virus (VZV) is a neurotropic alphaherpesvirus and the causative agent of varicella (chickenpox) (1). VZV establishes latency in the sensory ganglia and can reactivate later in life to cause herpes zoster (shingles), a painful disease that affects almost 1 million individuals in the United States alone (2). VZV is transmitted through the inhalation of virus-laden saliva droplets or by direct contact with the infectious fluid from vesicles...

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“…Immune mediators secreted by T cells and macrophages/microglia have been suggested to contribute to virally-induced demyelination due to dysregulation or death of oligodendrocyte lineage cells (Marro et al, 2014). These models are often considered alongside autoimmune-based models such as EAE, as they are useful for the characterization of infectious events leading to CNS immune responses (Baker and Amor, 2015; Fazakerley and Walker, 2003). Although EAE is powerful and remains most commonly used MS model, it is recognized that its limitations for MS therapy (Constantinescu et al, 2011) stem from a dependence on the artificial induction of the immune response (Mecha et al, 2013), unreliable predictability of treatments, a spinal cord preference over brain lesions, difficulty in analyzing remyelination of stochastic lesions and inconsistency of clinical functional progression (Ransohoff, 2012).…”

Section: Introductionmentioning

confidence: 99%

Pharmacological approaches to intervention in hypomyelinating and demyelinating white matter pathology

Chew

DeBoy

2016

Neuropharmacology

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White matter disease afflicts both developing and mature central nervous systems. Both cell intrinsic and extrinsic dysregulation result in profound changes in cell survival, axonal metabolism and functional performance. Experimental models of developmental white matter (WM) injury and demyelination have not only delineated mechanisms of signaling and inflammation, but have also paved the way for the discovery of pharmacological approaches to intervention. These reagents have been shown to enhance protection of the mature oligodendrocyte cell, accelerate progenitor cell recruitment and/or differentiation, or attenuate pathological stimuli arising from the inflammatory response to injury. Here we highlight reports of studies in the CNS in which compounds, namely peptides, hormones, and small molecule agonists/antagonists, have been used in experimental animal models of demyelination and neonatal brain injury that affect aspects of excitotoxicity, oligodendrocyte development and survival, and progenitor cell function, and which have been demonstrated to attenuate damage and improve WM protection in experimental models of injury. The molecular targets of these agents include growth factor and neurotransmitter receptors, morphogens and their signaling components, nuclear receptors, as well as the processes of iron transport and actin binding. By surveying the current evidence in non-immune targets of both the immature and mature WM, we aim to better understand pharmacological approaches modulating endogenous oligodendroglia that show potential for success in the contexts of developmental and adult WM pathology.

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Virus Demyelination

Cited by 62 publications

References 194 publications

Parental Age, Family Size, and Risk of Multiple Sclerosis

Parental Age, Family Size, and Risk of Multiple Sclerosis

Acute Simian Varicella Virus Infection Causes Robust and Sustained Changes in Gene Expression in the Sensory Ganglia

Pharmacological approaches to intervention in hypomyelinating and demyelinating white matter pathology

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