SrasV1, PubMed, Curation, bibRecord, 002271

Enhancement of the infectivity of SARS-CoV in BALB/c mice by IMP dehydrogenase inhibitors, including ribavirin.

Identifieur interne : 002271 ( PubMed/Curation ); précédent : 002270; suivant : 002272

Enhancement of the infectivity of SARS-CoV in BALB/c mice by IMP dehydrogenase inhibitors, including ribavirin.

Auteurs : Dale L. Barnard [États-Unis] ; Craig W. Day ; Kevin Bailey ; Matthew Heiner ; Robert Montgomery ; Larry Lauridsen ; Scott Winslow ; Justin Hoopes ; Joseph K-K Li ; Jongdae Lee ; Dennis A. Carson ; Howard B. Cottam ; Robert W. Sidwell

Source :

Antiviral research [ 0166-3542 ] ; 2006.

RBID : pubmed:16621037

Descripteurs français

KwdFr :
- Acide mycophénolique (pharmacologie), Animaux, Antiviraux (pharmacologie), Cellules Caco-2, Cellules Vero, Cytokines (métabolisme), Effet cytopathogène viral (), Femelle, Humains, IMP dehydrogenase (antagonistes et inhibiteurs), Organismes exempts d'organismes pathogènes spécifiques, Poumon (anatomopathologie), Poumon (virologie), Ribavirine (pharmacologie), Ribonucléosides (pharmacologie), Réplication virale (), Souris, Souris de lignée BALB C, Survie cellulaire (), Syndrome respiratoire aigu sévère (traitement médicamenteux), Syndrome respiratoire aigu sévère (virologie), Séquençage par oligonucléotides en batterie, Virus du SRAS (), Virus du SRAS (enzymologie), Virus du SRAS (pathogénicité), Virus du SRAS (physiologie).
MESH :
- anatomopathologie : Poumon.
- antagonistes et inhibiteurs : IMP dehydrogenase.
- enzymologie : Virus du SRAS.
- métabolisme : Cytokines.
- pathogénicité : Virus du SRAS.
- pharmacologie : Acide mycophénolique, Antiviraux, Ribavirine, Ribonucléosides.
- physiologie : Virus du SRAS.
- traitement médicamenteux : Syndrome respiratoire aigu sévère.
- virologie : Poumon, Syndrome respiratoire aigu sévère.
- Animaux, Cellules Caco-2, Cellules Vero, Effet cytopathogène viral, Femelle, Humains, Organismes exempts d'organismes pathogènes spécifiques, Réplication virale, Souris, Souris de lignée BALB C, Survie cellulaire, Séquençage par oligonucléotides en batterie, Virus du SRAS.

English descriptors

KwdEn :
- Animals, Antiviral Agents (pharmacology), Caco-2 Cells, Cell Survival (drug effects), Chlorocebus aethiops, Cytokines (metabolism), Cytopathogenic Effect, Viral (drug effects), Female, Humans, IMP Dehydrogenase (antagonists & inhibitors), Lung (pathology), Lung (virology), Mice, Mice, Inbred BALB C, Mycophenolic Acid (pharmacology), Oligonucleotide Array Sequence Analysis, Ribavirin (pharmacology), Ribonucleosides (pharmacology), SARS Virus (drug effects), SARS Virus (enzymology), SARS Virus (pathogenicity), SARS Virus (physiology), Severe Acute Respiratory Syndrome (drug therapy), Severe Acute Respiratory Syndrome (virology), Specific Pathogen-Free Organisms, Vero Cells, Virus Replication (drug effects).
MESH :
- chemical , antagonists & inhibitors : IMP Dehydrogenase.
- chemical , metabolism : Cytokines.
- chemical , pharmacology : Antiviral Agents, Mycophenolic Acid, Ribavirin, Ribonucleosides.
- drug effects : Cell Survival, Cytopathogenic Effect, Viral, SARS Virus, Virus Replication.
- drug therapy : Severe Acute Respiratory Syndrome.
- enzymology : SARS Virus.
- pathogenicity : SARS Virus.
- pathology : Lung.
- physiology : SARS Virus.
- virology : Lung, Severe Acute Respiratory Syndrome.
- Animals, Caco-2 Cells, Chlorocebus aethiops, Female, Humans, Mice, Mice, Inbred BALB C, Oligonucleotide Array Sequence Analysis, Specific Pathogen-Free Organisms, Vero Cells.

Abstract

Because of the conflicting data concerning the SARS-CoV inhibitory efficacy of ribavirin, an inosine monophosphate (IMP) dehydrogenase inhibitor, studies were done to evaluate the efficacy of ribavirin and other IMP dehydrogenase inhibitors (5-ethynyl-1-beta-D-ribofuranosylimidazole-4-carboxamide (EICAR), mizoribine, and mycophenolic acid) in preventing viral replication in the lungs of BALB/c mice, a replication model for severe acute respiratory syndrome (SARS) infections (Subbarao, K., McAuliffe, J., Vogel, L., Fahle, G., Fischer, S., Tatti, K., Packard, M., Shieh, W.J., Zaki, S., Murphy, B., 2004. Prior infection and passive transfer of neutralizing antibody prevent replication of severe acute respiratory syndrome coronavirus (SARS-CoV) in the respiratory tract of mice. J. Virol. 78, 3572-3577). Ribavirin given at 75 mg/kg 4 h prior to virus exposure and then given twice daily for 3 days beginning at day 0 was found to increase virus lung titers and extend the length of time that virus could be detected in the lungs of mice. Other IMP dehydrogenase inhibitors administered near maximum tolerated doses using the same dosing regimen as for ribavirin were found to slightly enhance virus replication in the lungs. In addition, ribavirin treatment seemed also to promote the production of pro-inflammatory cytokines 4 days after cessation of treatment, although after 3 days of treatment ribavirin inhibited pro-inflammatory cytokine production in infected mice, significantly reducing the levels of the cytokines IL-1alpha, interleukin-5 (IL-5), monocyte chemotactic protein-1 (MCP-1), and granulocyte-macrophage colony stimulating factor (GM-CSF). These findings suggest that ribavirin may actually contribute to the pathogenesis of SARS-CoV by prolonging and/or enhancing viral replication in the lungs. By not inhibiting viral replication in the lungs of infected mice, ribavirin treatment may have provided a continual source of stimulation for the inflammatory response thought to contribute to the pathogenesis of the infection. Our data do not support the use of ribavirin or other IMP dehydrogenase inhibitors for treating SARS infections in humans.

DOI: 10.1016/j.antiviral.2006.03.001
PubMed: 16621037

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<term>Cellules Vero</term>
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<term>Effet cytopathogène viral ()</term>
<term>Femelle</term>
<term>Humains</term>
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<term>Organismes exempts d'organismes pathogènes spécifiques</term>
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<term>Virus du SRAS (pathogénicité)</term>
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<term>Severe Acute Respiratory Syndrome</term>
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<term>Caco-2 Cells</term>
<term>Chlorocebus aethiops</term>
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<term>Humans</term>
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<term>Specific Pathogen-Free Organisms</term>
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<term>Cellules Caco-2</term>
<term>Cellules Vero</term>
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<front><div type="abstract" xml:lang="en">Because of the conflicting data concerning the SARS-CoV inhibitory efficacy of ribavirin, an inosine monophosphate (IMP) dehydrogenase inhibitor, studies were done to evaluate the efficacy of ribavirin and other IMP dehydrogenase inhibitors (5-ethynyl-1-beta-D-ribofuranosylimidazole-4-carboxamide (EICAR), mizoribine, and mycophenolic acid) in preventing viral replication in the lungs of BALB/c mice, a replication model for severe acute respiratory syndrome (SARS) infections (Subbarao, K., McAuliffe, J., Vogel, L., Fahle, G., Fischer, S., Tatti, K., Packard, M., Shieh, W.J., Zaki, S., Murphy, B., 2004. Prior infection and passive transfer of neutralizing antibody prevent replication of severe acute respiratory syndrome coronavirus (SARS-CoV) in the respiratory tract of mice. J. Virol. 78, 3572-3577). Ribavirin given at 75 mg/kg 4 h prior to virus exposure and then given twice daily for 3 days beginning at day 0 was found to increase virus lung titers and extend the length of time that virus could be detected in the lungs of mice. Other IMP dehydrogenase inhibitors administered near maximum tolerated doses using the same dosing regimen as for ribavirin were found to slightly enhance virus replication in the lungs. In addition, ribavirin treatment seemed also to promote the production of pro-inflammatory cytokines 4 days after cessation of treatment, although after 3 days of treatment ribavirin inhibited pro-inflammatory cytokine production in infected mice, significantly reducing the levels of the cytokines IL-1alpha, interleukin-5 (IL-5), monocyte chemotactic protein-1 (MCP-1), and granulocyte-macrophage colony stimulating factor (GM-CSF). These findings suggest that ribavirin may actually contribute to the pathogenesis of SARS-CoV by prolonging and/or enhancing viral replication in the lungs. By not inhibiting viral replication in the lungs of infected mice, ribavirin treatment may have provided a continual source of stimulation for the inflammatory response thought to contribute to the pathogenesis of the infection. Our data do not support the use of ribavirin or other IMP dehydrogenase inhibitors for treating SARS infections in humans.</div>
</front>
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<DateCompleted><Year>2006</Year>
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<ArticleTitle>Enhancement of the infectivity of SARS-CoV in BALB/c mice by IMP dehydrogenase inhibitors, including ribavirin.</ArticleTitle>
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<Abstract><AbstractText>Because of the conflicting data concerning the SARS-CoV inhibitory efficacy of ribavirin, an inosine monophosphate (IMP) dehydrogenase inhibitor, studies were done to evaluate the efficacy of ribavirin and other IMP dehydrogenase inhibitors (5-ethynyl-1-beta-D-ribofuranosylimidazole-4-carboxamide (EICAR), mizoribine, and mycophenolic acid) in preventing viral replication in the lungs of BALB/c mice, a replication model for severe acute respiratory syndrome (SARS) infections (Subbarao, K., McAuliffe, J., Vogel, L., Fahle, G., Fischer, S., Tatti, K., Packard, M., Shieh, W.J., Zaki, S., Murphy, B., 2004. Prior infection and passive transfer of neutralizing antibody prevent replication of severe acute respiratory syndrome coronavirus (SARS-CoV) in the respiratory tract of mice. J. Virol. 78, 3572-3577). Ribavirin given at 75 mg/kg 4 h prior to virus exposure and then given twice daily for 3 days beginning at day 0 was found to increase virus lung titers and extend the length of time that virus could be detected in the lungs of mice. Other IMP dehydrogenase inhibitors administered near maximum tolerated doses using the same dosing regimen as for ribavirin were found to slightly enhance virus replication in the lungs. In addition, ribavirin treatment seemed also to promote the production of pro-inflammatory cytokines 4 days after cessation of treatment, although after 3 days of treatment ribavirin inhibited pro-inflammatory cytokine production in infected mice, significantly reducing the levels of the cytokines IL-1alpha, interleukin-5 (IL-5), monocyte chemotactic protein-1 (MCP-1), and granulocyte-macrophage colony stimulating factor (GM-CSF). These findings suggest that ribavirin may actually contribute to the pathogenesis of SARS-CoV by prolonging and/or enhancing viral replication in the lungs. By not inhibiting viral replication in the lungs of infected mice, ribavirin treatment may have provided a continual source of stimulation for the inflammatory response thought to contribute to the pathogenesis of the infection. Our data do not support the use of ribavirin or other IMP dehydrogenase inhibitors for treating SARS infections in humans.</AbstractText>
</Abstract>
<AuthorList CompleteYN="Y"><Author ValidYN="Y"><LastName>Barnard</LastName>
<ForeName>Dale L</ForeName>
<Initials>DL</Initials>
<AffiliationInfo><Affiliation>Institute for Antiviral Research, Utah State University, Logan, 84322-5600, USA. honery@usu.edu</Affiliation>
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<Initials>JK</Initials>
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<Author ValidYN="Y"><LastName>Lee</LastName>
<ForeName>Jongdae</ForeName>
<Initials>J</Initials>
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<Initials>DA</Initials>
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<Author ValidYN="Y"><LastName>Cottam</LastName>
<ForeName>Howard B</ForeName>
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<Author ValidYN="Y"><LastName>Sidwell</LastName>
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Enhancement of the infectivity of SARS-CoV in BALB/c mice by IMP dehydrogenase inhibitors, including ribavirin.

Enhancement of the infectivity of SARS-CoV in BALB/c mice by IMP dehydrogenase inhibitors, including ribavirin.

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