A Refined Guinea Pig Model of Foot-and-Mouth Disease Virus Infection for Assessing the Efficacy of Antiviral Compounds

Vleeschauwer, Annebel R. De; Lefebvre, David; Willems, Tom; Paul, G.; Billiet, A.; Murao, Lyre Espada; Neyts, Johan; Goris, Nesya; Clercq, Kris De

doi:10.1111/tbed.12255

Cited by 15 publications

(10 citation statements)

References 25 publications

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“…GPID 50 of the virus was recorded as 10 5.3 /ml. The results are in agreement with the findings of De Vleeschauwer et al, (2016) who used guinea pigs to access antiviral compound activity against FMD.…”

Section: Calculation Of Guinea Pigs Infectious Dose 50 (Gpid 50 )supporting

confidence: 91%

In vitro Adaptation, Molecular Characterization and Tissue Tropism of Foot-and-mouth Disease Virus in Guinea Pigs

Mubarak¹,

Tipu²,

Aslam³

et al. 2022

IJAR

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Background: Foot-and-mouth disease is a highly contagious disease in cloven-footed animals. It is reported to be endemic in Pakistan. Methods: Molecular characterization of FMD virus field isolate was carried out, followed by an investigation of the tissue tropism in guinea pigs’ heart and respiratory organs. After calculating the biological titer of the virus and guinea pigs infectious dose50, the virus was injected into the hind metatarsal feet pads of 30 guinea pigs to study the pathogenesis of the disease at different day intervals from day 1 to 28. Result: Phylogenetic analysis showed that the isolate belonged to ME-SA topotype of serotype “O” with lineage Pan-Asia II. In pathological findings, hemorrhages and congestion in the heart and trachea and edema in the lungs were observed. Histopathological examination showed myocardial necrosis and tracheal epithelium sloughing along with bronchial edema. In Immunohistochemical studies, antigen load was detected in the heart, trachea and lungs up to 14 days post-inoculation. The study suggested that small experimental animals would be a better cost-effective replacement for large animals to study the pathogenesis of the disease as the virus did not change its behavior in these laboratory animals.

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Section: Calculation Of Guinea Pigs Infectious Dose 50 (Gpid 50 )supporting

confidence: 91%

In vitro Adaptation, Molecular Characterization and Tissue Tropism of Foot-and-mouth Disease Virus in Guinea Pigs

Mubarak¹,

Tipu²,

Aslam³

et al. 2022

IJAR

View full text Add to dashboard Cite

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“…The efficacy of 3-hydroxypyrazine-2-carboxamide and the prophylactic O1 Manisa vaccine against the foot-and-mouth disease virus was also compared in a guinea pig model. The efficacy of prophylactic therapy with T-1105 (guinea pigs, 400 mg/kg/day orally for 5 days) was shown to be comparable to that of animal vaccination [ 57 ].…”

Section: Structural Analogs Of Favipiravir Exhibiting Antiviral Activitymentioning

confidence: 99%

Favipiravir and Its Structural Analogs: Antiviral Activity and Synthesis Methods

et al. 2022

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1,4-Pyrazine-3-carboxamide-based antiviral compounds have been under intensive study for the last 20 years. One of these compounds, favipiravir (6-fluoro-3-hydroxypyrazine-2-carboxamide, T-705), is approved for use against the influenza infection in a number of countries. Now, favipiravir is being actively used against COVID-19. This review describes the in vivo metabolism of favipiravir, the mechanism of its antiviral activity, clinical findings, toxic properties, and the chemical synthesis routes for its production. We provide data on the synthesis and antiviral activity of structural analogs of favipiravir, including nucleosides and nucleotides based on them.

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“…In another study, the nucleoside analogue 2 0 -C-methylcytidine (2 0 CMC) prevented the establishment of FMDV infection in severe combined immunodeficient mice (Lefebvre et al, 2014a). Seeking improved models for in vivo assessment of candidate molecules, the same group have developed a refined approach in guinea pigs for assessing anti-FMDV biotherapeutics and shown promising preliminary results (De Vleeschauwer et al, 2016).…”

Section: Antiviral Interventionsmentioning

confidence: 99%

Global Foot-and-Mouth Disease Research Update and Gap Analysis: 5 - Biotherapeutics and Disinfectants

Robinson

Knight-Jones

Charleston

et al. 2016

Transbound Emerg Dis

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SummaryWe assessed knowledge gaps in foot-and-mouth disease (FMD) research. Findings are reported in a series of papers, and in this article, we consider biotherapeutics and disinfectants. The study took the form of a literature review (2011)(2012)(2013)(2014)(2015) combined with research updates collected in 2014 from 33 institutes from across the world. Findings were used to identify priority areas for future FMD research. While vaccines will remain the key immunological intervention used against FMD virus (FMDV) for the foreseeable future, it takes a few days for the immune system to respond to vaccination. In an outbreak situation, protection could potentially be provided during this period by the application of rapid, short-acting biotherapeutics, aiming either to stimulate a non-specific antiviral state in the animal or to specifically inhibit a part of the viral life cycle. Certain antiviral cytokines have been shown to promote rapid protection against FMD; however, the effects of different immune-modulators appear to vary across species in ways and for reasons that are not yet understood. Major barriers to the effective incorporation of biotherapeutics into control strategies are cost, limited understanding of their effect on subsequent immune responses to vaccines and uncertainty about their potential impact if used for disease containment. Recent research has highlighted the importance of environmental contamination in FMDV transmission. Effective disinfectants for FMDV have long been available, but research is being conducted to further develop methods for quantitatively evaluating their performance under field, or near-field, conditions. During outbreaks in South Korea in 2010 there was public concern about potential environmental contamination after the mass use of disinfectant and mass burial of culled stock; this should be considered during outbreak contingency planning.

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A Refined Guinea Pig Model of Foot-and-Mouth Disease Virus Infection for Assessing the Efficacy of Antiviral Compounds

Cited by 15 publications

References 25 publications

In vitro Adaptation, Molecular Characterization and Tissue Tropism of Foot-and-mouth Disease Virus in Guinea Pigs

In vitro Adaptation, Molecular Characterization and Tissue Tropism of Foot-and-mouth Disease Virus in Guinea Pigs

Favipiravir and Its Structural Analogs: Antiviral Activity and Synthesis Methods

Global Foot-and-Mouth Disease Research Update and Gap Analysis: 5 - Biotherapeutics and Disinfectants

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