Publications by authors named "Beatrice Tyrrell"

Crimean-Congo haemorrhagic fever virus (CCHFV) is a pathogen of increasing public health concern, being a widely distributed arbovirus and the causative agent of the potentially fatal Crimean-Congo haemorrhagic fever. Hazara virus (HAZV) is a genetically and serologically related virus that has been proposed as a surrogate for antiviral and vaccine testing for CCHFV. Glycosylation analysis of HAZV has been limited; first, we confirmed for the first time the occupation of two N-glycosylation sites in the HAZV glycoprotein.

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Article Synopsis
  • Dendritic cells are key players in the immune response to dengue virus (DENV) and are significantly affected by the virus.
  • Research shows that specific deoxynojirimycin (DNJ) derivatives can provide antiviral effects against DENV in immature dendritic cells, mirroring results seen in macrophages.
  • The antiviral action of DNJ derivatives involves inhibiting an enzyme called ER α-glucosidase I, leading to decreased viral secretion and reduced inflammatory response in infected cells.
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Sepsis is a life-threatening condition involving a dysregulated immune response to infectious agents that cause injury to host tissues and organs. Current treatments are limited to early administration of antibiotics and supportive care. While appealing, the strategy of targeted inhibition of individual molecules in the inflammatory cascade has not proved beneficial.

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The antiviral mechanism of action of iminosugars against many enveloped viruses, including dengue virus (DENV), HIV, influenza and hepatitis C virus, is believed to be mediated by inducing misfolding of viral N-linked glycoproteins through inhibition of host endoplasmic reticulum-resident α-glucosidase enzymes. This leads to reduced secretion and/or infectivity of virions and hence lower viral titres, both in vitro and in vivo. Free oligosaccharide analysis from iminosugar-treated cells shows that antiviral activity correlates with production of mono- and tri-glucosylated sugars, indicative of inhibition of ER α-glucosidases.

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Sirtuin 2 (SIRT2) is one of the seven members of the family of NAD-dependent histone deacetylases. Sirtuins target histones and non-histone proteins according to their subcellular localization, influencing various biological processes. SIRT2 resides mainly in the cytoplasm and regulates cytoskeleton dynamics, cell cycle, and metabolic pathways.

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Influenza virus causes three to five million severe respiratory infections per year in seasonal epidemics, and sporadic pandemics, three of which occurred in the twentieth century and are a continuing global threat. Currently licensed antivirals exclusively target the viral neuraminidase or M2 ion channel, and emerging drug resistance necessitates the development of novel therapeutics. It is believed that a host-targeted strategy may combat the development of antiviral drug resistance.

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Protein kinase RNA activated (PKR) is a crucial mediator of anti-viral responses but is reported to be activated by multiple non-viral stimuli. However, mechanisms underlying PKR activation, particularly in response to bacterial infection, remain poorly understood. We have investigated mechanisms of PKR activation in human primary monocyte-derived dendritic cells in response to infection by Chlamydia trachomatis.

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Article Synopsis
  • Research indicates that iminosugars, previously thought to primarily inhibit α-glucosidases in the endoplasmic reticulum (ER), may have multiple antiviral mechanisms impacting various viral infections, including dengue virus (DENV).
  • Celgosivir, a type of bicyclic iminosugar, has shown promise as an antiviral agent in treating DENV in clinical models and has been confirmed to inhibit DENV secretion in human macrophages.
  • The study establishes that the antiviral effectiveness of iminosugars against DENV is more closely related to ER α-glucosidase inhibition rather than the processing of glycolipids, highlighting the need for further exploration of iminosugar mechanisms.
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The antiviral activity of UV-4 was previously demonstrated against dengue virus serotype 2 (DENV2) in multiple mouse models. Herein, step-wise minimal effective dose and therapeutic window of efficacy studies of UV-4B (UV-4 hydrochloride salt) were conducted in an antibody-dependent enhancement (ADE) mouse model of severe DENV2 infection in AG129 mice lacking types I and II interferon receptors. Significant survival benefit was demonstrated with 10-20 mg/kg of UV-4B administered thrice daily (TID) for seven days with initiation of treatment up to 48 h after infection.

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