Ly6c+ “inflammatory monocytes” are microglial precursors recruited in a pathogenic manner in West Nile virus encephalitis

Getts, Daniel R.; Terry, Rachael; Getts, Meghann Teague; Müller, Marcus; Rana, Sabita; Shrestha, Bimmi; Radford, Jane; Rooijen, Nico van; Campbell, Iain L.; King, Nicholas J. C.

doi:10.1084/jem.20080421

Cited by 299 publications

(437 citation statements)

References 67 publications

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“…Increasing evidence suggests that WNV entry into the CNS is a multistep process that can occur through one of several routes (17,20,(31)(32)(33)(34)(35). WNV entry into the CNS has been shown to precede disruption of the BBB and leukocyte infiltration (32,33,36,37), suggesting that WNV utilizes a direct mechanism to initially invade the CNS, such as basolateral secretion of virus particles from infected brain endothelial cells or transcytosis. Thus, the brain endothelium likely constitutes a primary barrier to WNV neuroinvasion.…”

Section: Discussionmentioning

confidence: 99%

Differential Replication of Pathogenic and Nonpathogenic Strains of West Nile Virus within Astrocytes

Hussmann

Samuel

Kim

et al. 2013

J Virol

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The severity of West Nile virus (WNV) infection in immunocompetent animals is highly strain dependent, ranging from avirulent to highly neuropathogenic. Here, we investigate the nature of this strain-specific restriction by analyzing the replication of avirulent (WNV-MAD78) and highly virulent (WNV-NY) strains in neurons, astrocytes, and microvascular endothelial cells, which comprise the neurovascular unit within the central nervous system (CNS). We demonstrate that WNV-MAD78 replicated in and traversed brain microvascular endothelial cells as efficiently as WNV-NY. Likewise, similar levels of replication were detected in neurons. Thus, WNV-MAD78's nonneuropathogenic phenotype is not due to an intrinsic inability to replicate in key target cells within the CNS. In contrast, replication of WNV-MAD78 was delayed and reduced compared to that of WNV-NY in astrocytes. The reduced susceptibility of astrocytes to WNV-MAD78 was due to a delay in viral genome replication and an interferon-independent reduction in cell-to-cell spread. Together, our data suggest that astrocytes regulate WNV spread within the CNS and therefore are an attractive target for ameliorating WNV-induced neuropathology.

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Section: Discussionmentioning

confidence: 99%

Differential Replication of Pathogenic and Nonpathogenic Strains of West Nile Virus within Astrocytes

Hussmann

Samuel

Kim

et al. 2013

J Virol

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“…Work in many areas, including infectious disease, hypoxia, autoimmunity, and cancer, shows a definable wave of inflammatory monocyte recruitment into inflamed tissues expressing CCL2 and other chemokines. Once in the target tissue, these cells may differentiate into different effector cells, including DCs, macrophages, and even cells with a microglial phenotype [4,76], depending on the prevailing soluble factor milieu. In some cases these cells have important housekeeping functions (i.e., to digest and clear tissue debris before tissue remodelling); however, in many cases they express high levels of NO via induced NOS2 expression, as well as increased levels of NADPH oxidase, cathepsins, and myeloperoxidase, all of which may demonstrably contribute to further tissue damage in numerous conditions, including experimental autoimmune encephalomyelitis, myocardial infarction, and viral encephalitis [8,77,78].…”

Section: Targeting Inflammatory Myeloid Cellsmentioning

confidence: 99%

“…More recently, our increasing knowledge of the cellular subsets and regulatory roles of various members of immune system, combined with the emergence of safe, biocompatible nanoparticle platforms, is catalyzing the development of complex, highly adaptable, and programmable NP therapies that are predicted to revolutionize the standard of care of numerous disorders. For example, NPs may be engineered to specifically target cells of the mononuclear phagocyte system (MPS) for the purposes of restoring peripheral immune tolerance or to regulate aberrant monocyte activities during severe inflammation [2,[4][5][6][7]. Five-hundred-nanometer NPs with negative zeta potential can be harnessed to target circulating monocytes, reducing their potential for causing immune pathology in numerous experimental disease models including West Nile virus (WNV) encephalitis, myocardial infarction, and inflammatory bowel disease (IBD) [8].…”

Section: Introductionmentioning

confidence: 99%

Harnessing Nanoparticles for Immune Modulation

Getts¹,

Shea²,

Miller³

et al. 2016

Trends in Immunology

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Recent approaches using nanoparticles engineered for immune regulation have yielded promising results in preclinical models of disease. The number of nanoparticle therapies is growing, fueled by innovations in nanotechnology and advances in understanding of the underlying pathogenesis of immune-mediated diseases. In particular, recent mechanistic insight into the ways in which nanoparticles interact with the mononuclear phagocyte system and impact its function during homeostasis and inflammation have highlighted the potential of nanoparticle-based therapies for controlling severe inflammation while concurrently restoring peripheral immune tolerance in autoimmune disease. Here we review recent advances in nanoparticle-based approaches aimed at immune-modulation, and discuss these in the context of concepts in polymeric nanoparticle development, including particle modification, delivery and the factors associated with successful clinical deployment.

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“…These approaches are important when the aim is to gather data from large numbers of cells, and they have been successfully used with fluorescent polystyrene beads for tracking macrophage lineage (i.e. using their phagocytic function) cells in vivo (Getts et al 2008). …”

Section: Detection Imaging and Tracking In Vitromentioning

confidence: 99%

“…This approach, while obvious for cancer, could easily be adapted for various infectious diseases, particularly infections by extracellular organisms, those with extracellular phases, such as malaria, and/or those expressing pathogen-specific molecules on infected cell surfaces. Furthermore, specific cellular subsets in diseases characterised by over-exuberant pro-inflammatory immune responses could be targeted and inactivated or destroyed, for example, in autoimmune disease and even certain infectious diseases (Getts et al 2008;Getts et al 2011). Dually conjugated nanodiamonds could also be used to target cell subsets expressing a particular proinflammatory chemokine or cytokine receptor using the relevant chemokine or cytokine to deliver a behaviourmodifying signal to these cells .…”

Section: Nanodiamonds As Molecular Carriersmentioning

confidence: 99%

Luminescent nanodiamonds for biomedical applications

et al. 2011

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In recent years, nanodiamonds have emerged from primarily an industrial and mechanical applications base, to potentially underpinning sophisticated new technologies in biomedical and quantum science. Nanodiamonds are relatively inexpensive, biocompatible, easy to surface functionalise and optically stable. This combination of physical properties are ideally suited to biological applications, including intracellular labelling and tracking, extracellular drug delivery and adsorptive detection of bioactive molecules. Here we describe some of the methods and challenges for processing nanodiamond materials, detection schemes and some of the leading applications currently under investigation.

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Ly6c+ “inflammatory monocytes” are microglial precursors recruited in a pathogenic manner in West Nile virus encephalitis

Cited by 299 publications

References 67 publications

Differential Replication of Pathogenic and Nonpathogenic Strains of West Nile Virus within Astrocytes

Differential Replication of Pathogenic and Nonpathogenic Strains of West Nile Virus within Astrocytes

Harnessing Nanoparticles for Immune Modulation

Luminescent nanodiamonds for biomedical applications

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