C3H/HeN mouse model for the evaluation of antiviral agents for the treatment of Venezuelan equine encephalitis virus infection

Julander, Justin G.; Skirpstunas, Ramona T.; Siddharthan, Venkatraman; Shafer, Kristiina; Hoopes, Justin D.; Smee, Donald F.; Morrey, John D.

doi:10.1016/j.antiviral.2008.01.007

Cited by 48 publications

(70 citation statements)

References 32 publications

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“…C3H/HeN and BALB/C mice vaccinated dermally with TC-83, the live attenuated vaccine strain, survive. However, aerosol or IN infection with TC83 results in 90-100% mortality in C3H/HeN animals unlike inbred counterparts BALB/C that respond with no evidence of mortality (Julander, et al, 2007;Julander, et al, 2008c;Steele, et al, 2007;Steele, et al, 1998;Steele, et al, 2006). Similar experiences have shown that route of administration can alter neuroinvasion with nonpathogenic viruses failing to enter the CNS by peripheral routes, but exhibiting the ability to enter the CNS by IC, IN, or aerosol administration.…”

Section: Mouse Modelmentioning

confidence: 84%

“…Direct invasion of the brain via the bloodstream does not seem to be significant in VEE infection. Neuroinvasion results in caudal spread of the virus, and ultimately, overwhelming disseminated brain infection (Julander, et al, 2007;Julander, et al, 2008b). Thus, all routes of infection in mice with virulent forms of the virus result in neuroinvasion.…”

Section: Mouse Modelmentioning

confidence: 99%

“…Animals genetically modified with deficiencies in type I IFN signaling are highly susceptible to VEE infection and, even attenuated strains are uniformly lethal in these animals (White, et al, 2001). Additionally, artificial induction of type I IFN or prophylactic administration of type I IFN delays or prevents death in animal models (Julander, et al, 2008b). In the case of IN or aerosol infection, the rapid entry of virus to the CNS results in earlier neuroinvasion and may limit or alter the effectiveness of early innate immune mechanisms such as IFN or other as yet other unexplored mechanisms.…”

Section: Innate Immune Response To Veementioning

confidence: 99%

See 2 more Smart Citations

Encephalitic Development in Alphaviral Infection

Paessler¹,

Taylor²

2011

Non-Flavivirus Encephalitis

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Section: Mouse Modelmentioning

confidence: 84%

Section: Mouse Modelmentioning

confidence: 99%

Section: Innate Immune Response To Veementioning

confidence: 99%

See 1 more Smart Citation

Encephalitic Development in Alphaviral Infection

Paessler¹,

Taylor²

2011

Non-Flavivirus Encephalitis

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“…Like most strains, the clinical features of disease in these mice include lethargy, hunched posture and weight loss. This commonly used model also exhibits a similar CNS disease to that seen in other animal models, such as the development of meningo-encephalitis, gliosis and multifocal neurophil vacuolation (Julander et al, 2008). Differences do exist, however.…”

Section: A Taylor and Othersmentioning

confidence: 86%

“…Breakthrough infections were more frequent with the highly virulent serogroup 1A/B viruses following aerosol challenge (Phillpotts & Wright, 1999). C3H/HeN mice are particularly sensitive to VEEV TC-83 infection when receiving the virus intranasally, intracranially or by aerosol exposure Julander et al, 2008;Ludwig et al, 2001). Like most strains, the clinical features of disease in these mice include lethargy, hunched posture and weight loss.…”

Section: A Taylor and Othersmentioning

confidence: 99%

Mouse models of alphavirus-induced inflammatory disease

Taylor

Herrero

Rudd

et al. 2015

Journal of General Virology

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Part of the Togaviridae family, alphaviruses are arthropod-borne viruses that are widely distributed throughout the globe. Alphaviruses are able to infect a variety of vertebrate hosts, but in humans, infection can result in extensive morbidity and mortality. Symptomatic infection can manifest as fever, an erythematous rash and/or significant inflammatory pathologies such as arthritis and encephalitis. Recent overwhelming outbreaks of alphaviral disease have highlighted the void in our understanding of alphavirus pathogenesis and the re-emergence of alphaviruses has given new impetus to anti-alphaviral drug design. In this review, the development of viable mouse models of Old Word and New World alphaviruses is examined. How mouse models that best replicate human disease have been used to elucidate the immunopathology of alphavirus pathogenesis and trial novel therapeutic discoveries is also discussed.

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Acute exposure to abuse‐like concentrations of toluene induces inflammation in mouse lungs and brain

Svenson

Davidson

Thakur

et al. 2022

J of Applied Toxicology

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Toluene is an aromatic hydrocarbon commonly abused by young adolescents for its central nervous system depressant effects. Although toluene's pharmacological effects at high concentrations are relatively well-known, few studies have assessed toluene's effects on lung and brain tissues. The present study characterized the pathological effects of acute inhaled toluene exposure in the lungs and brains of male Swiss-Webster mice (N = 68). Using a static vapor exposure chamber, mice (PND 28) received a single 30-min toluene administration (0, 1000, 2000, or 4000 ppm). Lung and brain tissues were extracted 24-h post-exposure. Histology results revealed significant changes in the morphology of lung tissue (e.g., irregular cellular architecture) with the 2000-and 4000-ppm exposures expressing greater signs of pathology than control 0-ppm exposure. Markers of immune system activity (F4/80 and Ly-6G) and cellular proliferation (Ki-67) in the lung revealed no significant differences. Additionally, brain tissues were analyzed for changes of astrogliosis (glial fibrillary acidic protein [GFAP]) and oxidative stress (glutathione peroxidase [GPx]). GFAP showed increased astrogliosis in the striatum with 2000-ppm toluene showing significantly higher expression than control (p < 0.05) and a marginal effect in the hippocampus.No other markers showed significant changes. The increased signs of inflammation and cellular damage suggest that exposure to a single high concentration of toluene, typical of abuse, is capable of producing pathology in both lung and brain tissue.

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C3H/HeN mouse model for the evaluation of antiviral agents for the treatment of Venezuelan equine encephalitis virus infection

Cited by 48 publications

References 32 publications

Encephalitic Development in Alphaviral Infection

Encephalitic Development in Alphaviral Infection

Mouse models of alphavirus-induced inflammatory disease

Acute exposure to abuse‐like concentrations of toluene induces inflammation in mouse lungs and brain

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