Your search keyword '"Orthobunyavirus drug effects"' showing total 14 results

1. Systemic Clodronate Liposome Treatment for Depletion of Blood-Contacting Phagocytes and Investigation of Their Role in the Control of Bunyavirus Viremia.

Author

Ander SE, Davenport BJ, Evans AB, and Morrison TE

Subjects

Animals, Orthobunyavirus immunology, Orthobunyavirus drug effects, Bunyaviridae Infections virology, Bunyaviridae Infections drug therapy, Disease Models, Animal, Liposomes, Clodronic Acid pharmacology, Clodronic Acid administration & dosage, Phagocytes drug effects, Phagocytes immunology, Phagocytes virology, Phagocytes metabolism, Viremia drug therapy, Viremia virology

Abstract

During viral infection, phagocytic cells participate in numerous immunological processes. A common approach to elucidate the specific contributions of phagocytic cells is through direct comparison of viral pathogenesis of phagocyte-depleted and phagocyte-intact animals. Clodronate liposomes are a versatile and simple means of depleting phagocytes in any animal model. Selection of clodronate liposome route of delivery can yield systemic or local phagocyte depletion as needed. Here we describe the application of clodronate liposome-mediated depletion of blood-contacting phagocytes to investigate their interactions with La Crosse virus (or other bunyaviruses) in a reductionist model of viremia., (© 2025. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2025

2. Identification of cap-dependent endonuclease inhibitors with broad-spectrum activity against bunyaviruses.

Author

Toba S, Sato A, Kawai M, Taoda Y, Unoh Y, Kusakabe S, Nobori H, Uehara S, Uemura K, Taniguchi K, Kobayashi M, Noshi T, Yoshida R, Naito A, Shishido T, Maruyama J, Paessler S, Carr MJ, Hall WW, Yoshimatsu K, Arikawa J, Matsuno K, Sakoda Y, Sasaki M, Orba Y, Sawa H, and Kida H

Subjects

Animals, Drug Evaluation, Preclinical, Drug Resistance, Viral drug effects, Drug Resistance, Viral genetics, Humans, Mice, Virus Replication drug effects, Antiviral Agents pharmacology, Endonucleases antagonists & inhibitors, Orthobunyavirus drug effects, Orthobunyavirus genetics, Orthobunyavirus metabolism

Abstract

Viral hemorrhagic fevers caused by members of the order Bunyavirales comprise endemic and emerging human infections that are significant public health concerns. Despite the disease severity, there are few therapeutic options available, and therefore effective antiviral drugs are urgently needed to reduce disease burdens. Bunyaviruses, like influenza viruses (IFVs), possess a cap-dependent endonuclease (CEN) that mediates the critical cap-snatching step of viral RNA transcription. We screened compounds from our CEN inhibitor (CENi) library and identified specific structural compounds that are 100 to 1,000 times more active in vitro than ribavirin against bunyaviruses, including Lassa virus, lymphocytic choriomeningitis virus (LCMV), and Junin virus. To investigate their inhibitory mechanism of action, drug-resistant viruses were selected in culture. Whole-genome sequencing revealed that amino acid substitutions in the CEN region of drug-resistant viruses were located in similar positions as those of the CEN α3-helix loop of IFVs derived under drug selection. Thus, our studies suggest that CENi compounds inhibit both bunyavirus and IFV replication in a mechanistically similar manner. Structural analysis revealed that the side chain of the carboxyl group at the seventh position of the main structure of the compound was essential for the high antiviral activity against bunyaviruses. In LCMV-infected mice, the compounds significantly decreased blood viral load, suppressed symptoms such as thrombocytopenia and hepatic dysfunction, and improved survival rates. These data suggest a potential broad-spectrum clinical utility of CENis for the treatment of both severe influenza and hemorrhagic diseases caused by bunyaviruses.

Published

2022

3. First report of antiviral activity of nordihydroguaiaretic acid against Fort Sherman virus (Orthobunyavirus).

Author

Martinez F, Mugas ML, Aguilar JJ, Marioni J, Contigiani MS, Núñez Montoya SC, and Konigheim BS

Subjects

Animals, Antiviral Agents pharmacology, Arachidonate 5-Lipoxygenase metabolism, Dose-Response Relationship, Drug, Haplorhini, Microbial Viability, Orthobunyavirus physiology, Sterol Regulatory Element Binding Protein 1 metabolism, Time Factors, Lipid Metabolism drug effects, Masoprocol pharmacology, Orthobunyavirus drug effects, Virus Replication drug effects

Abstract

The genus Orthobunyavirus are a group of viruses within arbovirus, with a zoonotic cycle, some of which could lead to human infection. A characteristic of these viruses is their lack of antiviral treatment or vaccine for its prevention. The objective of this work was to study the in vitro antiviral activity of nordihydroguaiaretic acid (NDGA), the most important active compound of Larrea divaricata Cav. (Zigophyllaceae), against Fort Sherman virus (FSV) as a model of Orthobunyavirus genus. At the same time, the effect of NDGA as a lipolytic agent on the cell cycle of this viral model was assessed. The method of reducing plaque forming units on LLC-MK2 cells was used to detect the action of NDGA on CbaAr426 and SFCrEq231 isolates of FSV. NDGA did not show virucidal effect, but it had antiviral activity with a similar inhibition in both isolates, which was dose dependent. It was established that the NDGA has a better inhibition 1-h post-internalization (p.i.), showing a different behavior in each isolate, which was dependent upon the time p.i. Since virus multiplication is dependent on host cell lipid metabolism, the antiviral effect of NDGA has been previously related to its ability to disturb the lipid metabolism, probably by interfering with the 5-lipoxigenase (5-LOX) and the sterol regulatory element-binding proteins (SREBP) pathway. We determined by using caffeic acid, a 5-LOX inhibitor, that the inhibition of this enzyme negatively affected the FSV replication; and by means of resveratrol, a SREBP1 inhibitor, it was showed that the negative regulation of this pathway only had action on the SFCrEq231 reduction. In addition, it was proved that the NDGA acts intracellularly, since it showed the ability to incorporate into LLC-MK2 cells. The information provided in this work converts the NDGA into a compound with antiviral activity in vitro against FSV (Orthobunyavirus), which can be subjected to structural modifications in the future to improve the activity., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2021

4. Novel Ionophores Active against La Crosse Virus Identified through Rapid Antiviral Screening.

Author

Sandler ZJ, Firpo MR, Omoba OS, Vu MN, Menachery VD, and Mounce BC

Subjects

Coronavirus drug effects, Dose-Response Relationship, Drug, Drug Evaluation, Preclinical, Encephalitis, California virology, Enterovirus drug effects, Flavivirus drug effects, Humans, Orthobunyavirus drug effects, United States, Antiviral Agents pharmacology, Encephalitis, California drug therapy, Ionophores pharmacology, La Crosse virus drug effects, Potassium metabolism, Valinomycin pharmacology, Virus Replication drug effects

Abstract

Bunyaviruses are significant human pathogens, causing diseases ranging from hemorrhagic fevers to encephalitis. Among these viruses, La Crosse virus (LACV), a member of the California serogroup, circulates in the eastern and midwestern United States. While LACV infection is often asymptomatic, dozens of cases of encephalitis are reported yearly. Unfortunately, no antivirals have been approved to treat LACV infection. Here, we developed a method to rapidly test potential antivirals against LACV infection. From this screen, we identified several potential antiviral molecules, including known antivirals. Additionally, we identified many novel antivirals that exhibited antiviral activity without affecting cellular viability. Valinomycin, a potassium ionophore, was among our top targets. We found that valinomycin exhibited potent anti-LACV activity in multiple cell types in a dose-dependent manner. Valinomycin did not affect particle stability or infectivity, suggesting that it may preclude virus replication by altering cellular potassium ions, a known determinant of LACV entry. We extended these results to other ionophores and found that the antiviral activity of valinomycin extended to other viral families, including bunyaviruses (Rift Valley fever virus, Keystone virus), enteroviruses (coxsackievirus, rhinovirus), flavirivuses (Zika virus), and coronaviruses (human coronavirus 229E [HCoV-229E] and Middle East respiratory syndrome CoV [MERS-CoV]). In all viral infections, we observed significant reductions in virus titer in valinomycin-treated cells. In sum, we demonstrate the importance of potassium ions to virus infection, suggesting a potential therapeutic target to disrupt virus replication., (Copyright © 2020 American Society for Microbiology.)

Published

2020

5. Antivirals in medical biodefense.

Author

Bugert JJ, Hucke F, Zanetta P, Bassetto M, and Brancale A

Subjects

Arboviruses pathogenicity, Filoviridae drug effects, Filoviridae pathogenicity, Humans, Orthobunyavirus drug effects, Orthobunyavirus pathogenicity, Orthomyxoviridae drug effects, Orthomyxoviridae pathogenicity, Paramyxovirinae drug effects, Paramyxovirinae pathogenicity, Poxviridae drug effects, Poxviridae pathogenicity, Virus Diseases virology, Antiviral Agents therapeutic use, Arboviruses drug effects, Bioterrorism prevention & control, Virus Diseases drug therapy

Abstract

The viruses historically implicated or currently considered as candidates for misuse in bioterrorist events are poxviruses, filoviruses, bunyaviruses, orthomyxoviruses, paramyxoviruses and a number of arboviruses causing encephalitis, including alpha- and flaviviruses. All these viruses are of concern for public health services when they occur in natural outbreaks or emerge in unvaccinated populations. Recent events and intelligence reports point to a growing risk of dangerous biological agents being used for nefarious purposes. Public health responses effective in natural outbreaks of infectious disease may not be sufficient to deal with the severe consequences of a deliberate release of such agents. One important aspect of countermeasures against viral biothreat agents are the antiviral treatment options available for use in post-exposure prophylaxis. These issues were adressed by the organizers of the 16th Medical Biodefense Conference, held in Munich in 2018, in a special session on the development of drugs to treat infections with viruses currently perceived as a threat to societies or associated with a potential for misuse as biothreat agents. This review will outline the state-of-the-art methods in antivirals research discussed and provide an overview of antiviral compounds in the pipeline that are already approved for use or still under development.

Published

2020

6. Potassium is a trigger for conformational change in the fusion spike of an enveloped RNA virus.

Author

Punch EK, Hover S, Blest HTW, Fuller J, Hewson R, Fontana J, Mankouri J, and Barr JN

Subjects

A549 Cells, Dose-Response Relationship, Drug, Humans, Orthobunyavirus metabolism, Potassium Channels metabolism, Protein Conformation drug effects, Viral Envelope Proteins chemistry, Viral Envelope Proteins metabolism, Orthobunyavirus drug effects, Orthobunyavirus physiology, Potassium pharmacology, Virus Internalization drug effects

Abstract

Many enveloped viruses enter cells through the endocytic network, from which they must subsequently escape through fusion of viral and endosomal membranes. This membrane fusion is mediated by virus-encoded spikes that respond to the dynamic endosomal environment, which triggers conformational changes in the spikes that initiate the fusion process. Several fusion triggers have been identified and include pH, membrane composition, and endosome-resident proteins, and these cues dictate when and where viral fusion occurs. We recently reported that infection with an enveloped bunyavirus requires elevated potassium ion concentrations [K + ], controlled by cellular K + channels, that are encountered during viral transit through maturing endosomes. Here we reveal the molecular basis for the K + requirement of bunyaviruses through the first direct visualization of a member of the Nairoviridae family, namely Hazara virus (HAZV), using cryo-EM. Using cryo-electron tomography, we observed HAZV spike glycoproteins within infectious HAZV particles exposed to both high and low [K + ], which showed that exposure to K + alone results in dramatic changes to the ultrastructural architecture of the virion surface. In low [K + ], the spikes adopted a compact conformation arranged in locally ordered arrays, whereas, following exposure to high [K + ], the spikes became extended, and spike-membrane interactions were observed. Viruses exposed to high [K + ] also displayed enhanced infectivity, thus identifying K + as a newly defined trigger that helps promote viral infection. Finally, we confirmed that K + channel blockers are inhibitory to HAZV infection, highlighting the potential of K + channels as anti-bunyavirus targets., (© 2018 Punch et al.)

Published

2018

7. Modulation of Potassium Channels Inhibits Bunyavirus Infection.

Author

Hover S, King B, Hall B, Loundras EA, Taqi H, Daly J, Dallas M, Peers C, Schnettler E, McKimmie C, Kohl A, Barr JN, and Mankouri J

Subjects

Aedes, Animals, Bunyamwera virus growth & development, Bunyamwera virus physiology, Bunyaviridae Infections metabolism, Bunyaviridae Infections virology, Cell Line, Chlorocebus aethiops, Gene Expression Regulation, Bacterial drug effects, Humans, Mesocricetus, Nairovirus drug effects, Nairovirus growth & development, Nairovirus physiology, Orthobunyavirus drug effects, Orthobunyavirus growth & development, Orthobunyavirus physiology, Potassium Channels, Tandem Pore Domain genetics, Potassium Channels, Tandem Pore Domain metabolism, Vero Cells, Antiviral Agents pharmacology, Bunyamwera virus drug effects, Bunyaviridae Infections drug therapy, Host-Pathogen Interactions drug effects, Potassium Channel Blockers pharmacology, Potassium Channels, Tandem Pore Domain antagonists & inhibitors, Virus Integration drug effects

Abstract

Bunyaviruses are considered to be emerging pathogens facilitated by the segmented nature of their genome that allows reassortment between different species to generate novel viruses with altered pathogenicity. Bunyaviruses are transmitted via a diverse range of arthropod vectors, as well as rodents, and have established a global disease range with massive importance in healthcare, animal welfare, and economics. There are no vaccines or anti-viral therapies available to treat human bunyavirus infections and so development of new anti-viral strategies is urgently required. Bunyamwera virus (BUNV; genus Orthobunyavirus) is the model bunyavirus, sharing aspects of its molecular and cellular biology with all Bunyaviridae family members. Here, we show for the first time that BUNV activates and requires cellular potassium (K(+)) channels to infect cells. Time of addition assays using K(+) channel modulating agents demonstrated that K(+) channel function is critical to events shortly after virus entry but prior to viral RNA synthesis/replication. A similar K(+) channel dependence was identified for other bunyaviruses namely Schmallenberg virus (Orthobunyavirus) as well as the more distantly related Hazara virus (Nairovirus). Using a rational pharmacological screening regimen, two-pore domain K(+) channels (K2P) were identified as the K(+) channel family mediating BUNV K(+) channel dependence. As several K2P channel modulators are currently in clinical use, our work suggests they may represent a new and safe drug class for the treatment of potentially lethal bunyavirus disease., (© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

8. Antiviral activity of type I interferons and interleukins 29 and 28a (type III interferons) against Apeu virus.

Author

Almeida GM, de Oliveira DB, Magalhães CL, Bonjardim CA, Ferreira PC, and Kroon EG

Subjects

Animals, Antiviral Agents pharmacology, Bunyaviridae Infections virology, Cells, Cultured, Chlorocebus aethiops, Dose-Response Relationship, Drug, Humans, Interferon Type I pharmacology, Interferons, Interleukins pharmacology, Leukocytes, Mononuclear drug effects, Orthobunyavirus drug effects, Orthobunyavirus immunology, Vero Cells, Antiviral Agents immunology, Bunyaviridae Infections drug therapy, Interferon Type I immunology, Interleukins immunology

Abstract

Interferons (IFNs) are cytokines with important immunomodulatory activity in vertebrates. Although type I IFNs and interleukins (IL) 29 and 28a (type III IFNs) bind to different cellular receptors and have distinct structures, most of their biological activities are redundant. Apeu virus (APEUV) is a member of the Bunyaviridae family isolated from the Brazilian rain forest. In this paper we evaluated the antiviral activity of type I and type III IFNs against APEUV. All tested IFNs were able to induce an antiviral state against the virus in a dose-dependent way. The activity of type III IFNs did not need the presence of type I IFNs. Mixing both types of IFNs did not improve the biological activity of each type alone. The tested IFNs were also able to protect human peripheral blood mononuclear cells from infection. IFN alpha2, IFN beta, IL-29 and IL-28a induced the expression of 2',5'-oligoadenylate synthetase (2'5'OAS) and 6-16 genes. Although MxA gene was related to antiviral activity against Bunyaviruses, there was no induction of MxA in our model. We were able to show activity of type I and type III IFNs against a RNA virus, and that this activity is not dependent on MxA gene.

Published

2008

9. In vitro and in vivo studies of the Interferon-alpha action on distinct Orthobunyavirus.

Author

Livonesi MC, de Sousa RL, Badra SJ, and Figueiredo LT

Subjects

Animals, Animals, Suckling, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Body Weight drug effects, Brain drug effects, Brain virology, Bunyaviridae Infections mortality, Bunyaviridae Infections prevention & control, Chlorocebus aethiops, Dose-Response Relationship, Drug, Interferon Type I pharmacology, Interferon Type I therapeutic use, Interferon alpha-2, Interferon-alpha pharmacology, Mice, Orthobunyavirus growth & development, Recombinant Proteins, Survival Rate, Time Factors, Vero Cells, Virus Replication drug effects, Bunyaviridae Infections drug therapy, Interferon-alpha therapeutic use, Orthobunyavirus drug effects

Abstract

Oropouche, Caraparu, Guama, Guaroa and Tacaiuma viruses (Orthobunyavirus genus) cause human febrile illnesses and/or encephalitis. To achieve a therapeutical agent to prevent and/or treat these diseases we evaluated the antiviral action of Interferon-alpha (IFN-alpha) on these orthobunyaviruses. In vitro results showed that all the studied orthobunyaviruses are susceptible to antiviral action of IFN-alpha, but this susceptibility is limited and dependent on both concentration of drug and treatment period. In vivo results demonstrated that IFN-alpha present antiviral action on Oropouche and Guaroa viruses when used as a prophylactic treatment. Moreover, a treatment initiated 3h after infection prevented the death of Guaroa virus infected-mice. Additionally, mortality of mice was related to the migration and replication of viruses in their brains. Our results suggest that IFN-alpha could be potentially useful in the prevention of diseases caused by Oropouche virus and in the prevention and/or treatment of diseases caused by Guaroa virus.

Published

2007

10. In vitro study of antiviral activity of mycophenolic acid on Brazilian orthobunyaviruses.

Author

Livonesi MC, Moro de Sousa RL, and Moraes Figueiredo LT

Subjects

Animals, Chlorocebus aethiops, Guanosine metabolism, Microbial Sensitivity Tests, Time Factors, Vero Cells, Viral Plaque Assay, Virus Replication drug effects, Antiviral Agents pharmacology, Mycophenolic Acid pharmacology, Orthobunyavirus drug effects

Abstract

Objective: Oropouche, Caraparu, Guama, Guaroa and Tacaiuma are ssRNA viruses that belong to the genus Orthobunyavirus and have been associated with human febrile illnesses and/or encephalitis. In this study, we evaluated the antiviral action of mycophenolic acid (MPA) on theseorthobunyaviruses to achieve a therapeutic agent to treat the diseases caused by these viruses., Methods: The in vitro antiviral evaluation to MPA was done by using plaque assay at different periods of treatment., Results: Results showed that MPA at a concentration of 10 microg/ml has significant antiviral activity on Tacaiuma virus when treatment was initiated either 24 h before or 2 h after viral infection. Moreover, MPA has an inhibitory effect on Guama virus replication, but only when treatment was initiated before cell infection. Addition of guanosine in the culture reverted the inhibitory effect of MPA on Tacaiuma and Guama viruses, suggesting that the antiviral activity of this substance was via depletion of the intracellular guanosine pool., Conclusion: Our results suggest that MPA would not be a good therapeutic agent to treat the diseases caused by Oropouche, Caraparu, Guama, Guaroa, and Tacaiuma viruses., ((c) 2007 S. Karger AG, Basel.)

Published

2007

11. In vitro and in vivo studies of ribavirin action on Brazilian Orthobunyavirus.

Author

Livonesi MC, De Sousa RL, Badra SJ, and Figueiredo LT

Subjects

Animals, Cell Line, Mice, Orthobunyavirus growth & development, Antiviral Agents pharmacology, Bunyaviridae Infections physiopathology, Orthobunyavirus drug effects, Ribavirin pharmacology

Abstract

Oropouche, Caraparu, Guama, Guaroa, and Tacaiuma are viruses (genus Orthobunyavirus) that cause human febrile illnesses and encephalitis. The goal of this study was to evaluate the antiviral action of ribavirin on these orthobunyaviruses to achieve a therapeutical agent to treat the diseases caused by these viruses. In vitro results showed that ribavirin (50 microg/mL) had antiviral activity only on the Tacaiuma virus. Addition of guanosine in the culture reversed the antiviral effect of ribavirin on Tacaiuma virus, suggesting that ribavirin inhibited this virus by reducing the intra-cellular guanosine pool. Moreover, ribavirin was not an effective drug in vivo because it was unable to inhibit the death of the mice or virus replication in the brain. The results suggest that ribavirin has no antiviral activity on the Oropouche, Caraparu, Guama, Guaroa, or Tacaiuma viruses; consequently, ribavirin would not be a good therapeutical agent to treat these arboviruses.

Published

2006

12. Virus inactivation by nucleic acid extraction reagents.

Author

Blow JA, Dohm DJ, Negley DL, and Mores CN

Subjects

Alphavirus drug effects, Flavivirus drug effects, Orthobunyavirus drug effects, DNA, Viral isolation & purification, Indicators and Reagents pharmacology, Reagent Kits, Diagnostic, Viruses drug effects

Abstract

Many assume that common methods to extract viral nucleic acids are able to render a sample non-infectious. It may be that inactivation of infectious virus is incomplete during viral nucleic acid extraction methods. Accordingly, two common viral nucleic acid extraction techniques were evaluated for the ability to inactivate high viral titer specimens. In particular, the potential for TRIzol LS Reagent (Invitrogen Corp., Carlsbad, CA) and AVL Buffer (Qiagen, Valencia, CA) were examined to render suspensions of alphaviruses, flaviviruses, filoviruses and a bunyavirus non-infectious to tissue culture assay. The dilution series for both extraction reagents consistently caused cell death through a 100-fold dilution. Except for the DEN subtype 4 positive control, all viruses had titers of at least 10(6)pfu/ml. No plaques were detected in any extraction reagent plus virus combination in this study, therefore, the extraction reagents appeared to inactivate completely each of the high-titer viruses used in this study. These results support the reliance upon either TRIzol LS Reagent or AVL Buffer to render clinical or environmental samples non-infectious, which has implications for the handling and processing of samples under austere field conditions and low level containment.

Published

2004

13. Effect of triethylamine on the recovery of selected South American alphaviruses, flaviviruses, and bunyaviruses from mosquito (Diptera: Culicidae) pools.

Author

O'Guinn ML and Turell MJ

Subjects

Animals, Encephalitis Virus, Eastern Equine isolation & purification, Encephalitis Virus, Venezuelan Equine isolation & purification, Female, Flavivirus isolation & purification, Orthobunyavirus drug effects, South America, Culicidae virology, Encephalitis Virus, Eastern Equine drug effects, Encephalitis Virus, Venezuelan Equine drug effects, Ethylamines pharmacology, Flavivirus drug effects, Orthobunyavirus isolation & purification

Abstract

We evaluated the effect of triethylamine (TEA) on the recovery of infectious virus from pools of mosquitoes for two South American alphaviruses (eastern equine encephalomyelitis and Venezuelan equine encephalomyelitis subtypes IIIC and ID), one flavivirus (Ilheus) and two bunyaviruses (Mirim [Guama group] and Itaqui [group C]). Mosquitoes were inoculated intrathoracically with virus, held for 7-10 d at 26 degrees C, and handled under one of four regimens before testing for the presence of virus by plaque assay. Mosquitoes were killed by freezing at - 70 degrees C for 3 min and tested immediately for the presence of virus; killed by freezing at -70 degrees C for 3 min and then held at room temperature for 1 h before testing for the presence of virus; anesthetized with TEA and assayed immediately for the presence of virus; or anesthetized with TEA and then held at room temperature for 1 h before being assayed for the presence of virus. For each of the viruses tested, viral titers in mosquitoes anesthetized with TEA were similar to those in mosquitoes killed by freezing at-70 degrees C. Likewise, there was no significant difference in viral titers in mosquitoes anesthetized with TEA and held at room temperature for 1 h or in mosquitoes frozen at -70 degrees C and held at room temperature for 1 h before being processed for virus by isolation. Triethylamine is advantageous for the handling of mosquitoes in a field environment. The elimination of the need for a cold chain, without compromising virus recovery, increases the feasibility of conducting research projects requiring the isolation of live virus from mosquitoes in remote tropical environments.

Published

2002

14. Characterization of murine Caraparu Bunyavirus liver infection and immunomodulator-mediated antiviral protection.

Author

Brinton MA, Gavin EI, Lo WK, Pinto AJ, and Morahan PS

Subjects

Adjuvants, Immunologic therapeutic use, Animals, Antiviral Agents therapeutic use, Bunyaviridae Infections microbiology, Female, Interferon-gamma pharmacology, Liver pathology, Liver Diseases microbiology, Liver Diseases pathology, Mice, Mice, Inbred Strains, Microscopy, Electron, Recombinant Proteins, Ribavirin pharmacology, Virus Replication drug effects, Adjuvants, Immunologic pharmacology, Antiviral Agents pharmacology, Bunyaviridae Infections drug therapy, Liver Diseases drug therapy, Orthobunyavirus drug effects

Abstract

A rapid, peripheral disease model utilizing the Bunyavirus, Caraparu, was established in mice for the evaluation of antiviral therapy with immunomodulators. 4-6-week-old B6C3F1 female mice, inoculated intraperitoneally with virus, developed coagulative liver necrosis and died between 4-6 days after infection. This Caraparu disease model was relatively resistant to treatment with immunomodulators, such as ABMP, Ampligen, alpha-interferon (IFN-alpha) or beta-interferon (IFN-beta). However, a significant increase in median survival time (MST) was consistently observed upon treatment with gamma-interferon (IFN-gamma). The nucleoside analog--ribavirin--was highly effective against Caraparu virus in repeated treatment schedules begun on either day -1, day 0, or day +1 of infection. Ribavirin gave little protection when initiation of treatment was delayed until day +2. However, combined treatment with IFN-gamma, starting on day 0 and ribavirin starting on day +2, significantly reduced mortality.

Published

1993