Your search keyword '"Bailey KW"' showing total 9 results

1. Topical treatment of cutaneous vaccinia virus infections in immunosuppressed hairless mice with selected antiviral substances.

Author

Smee DF, Bailey KW, Wong MH, and Tarbet EB

Subjects

Administration, Topical, Animals, Antiviral Agents chemistry, Cidofovir, Cyclophosphamide chemistry, Cytosine chemistry, Cytosine pharmacology, Female, Immune Tolerance, Immunosuppression Therapy, Mice, Mice, Hairless, Microbial Sensitivity Tests, Organophosphonates chemistry, Purines chemistry, Skin Diseases, Viral immunology, Skin Diseases, Viral virology, Vaccinia immunology, Vaccinia virology, Vaccinia virus immunology, Vaccinia virus isolation & purification, Antiviral Agents pharmacology, Cyclophosphamide pharmacology, Cytosine analogs & derivatives, Organophosphonates pharmacology, Purines pharmacology, Skin Diseases, Viral drug therapy, Vaccinia drug therapy, Vaccinia virus drug effects

Abstract

Background: Certain nucleoside, nucleotide and pyrophosphate analogues may be useful for treating severe complications arising as a result of virus dissemination following smallpox (live vaccinia virus) vaccinations, especially in immunocompromised individuals. We used an immunosuppressed hairless mouse model to study the effects of 10 antiviral agents on progressive vaccinia infections., Methods: Hairless mice were immunosuppressed by treatment with cyclophosphamide (100 mg/kg) every 4 days starting 1 day prior to vaccinia virus (WR strain) infection of wounded skin. Topical treatments with antiviral agents were applied twice a day for 7 days starting 5 days after virus exposure., Results: Topical 1% cidofovir cream treatment was effective in significantly reducing primary lesion severity and decreasing the number of satellite lesions. Topical 1% cyclic HPMPC and 1% phosphonoacetic acid were not quite as active as cidofovir. Ribavirin (5%) treatment reduced lesion severity and diminished the numbers of satellite lesions, but the mice died significantly sooner than placebos. 2-Amino-7-[(1,3,-dihydroxy-2-propoxy)methyl]purine (compound S2242; 1%) moderately reduced primary lesion sizes. Ineffective treatments included 5% arabinosyladenine, 1% arabinosylcytosine, 1% 5-chloro-arabinosylcytosine, 5% arabinosylhypoxanthine 5-monophosphate and 5% viramidine., Conclusions: Of the compounds tested, topically applied cidofovir was the most effective treatment of cutaneous vaccinia virus infections in immunosuppressed mice. Topical treatment with cidofovir could be considered as an adjunct to intravenous drug therapy for serious infections.

Published

2011

2. Characterization and treatment of cidofovir-resistant vaccinia (WR strain) virus infections in cell culture and in mice.

Author

Smee DF, Wandersee MK, Bailey KW, Hostetler KY, Holy A, and Sidwell RW

Subjects

Animals, Cells, Cultured, Cidofovir, Cytosine pharmacology, Mice, Mice, Inbred BALB C, Mice, SCID, Mutation, Vaccinia virus drug effects, Vaccinia virus genetics, Vaccinia virus pathogenicity, Virus Replication, Cytosine analogs & derivatives, Disease Models, Animal, Drug Resistance genetics, Organophosphonates pharmacology, Vaccinia virology

Abstract

The wild-type (WT) vaccinia (WR strain) virus is highly virulent to mice by intranasal inoculation, yet death can be prevented by cidofovir treatment. A cidofovir-resistant (CDV-R) mutant of the virus was developed by 15 Vero cell culture passages in order to determine cross-resistance to other inhibitors, growth characteristics, virulence in infected mice, and suitability of the animal model for studying antiviral therapies. Comparisons were made to the original WT virus and to a WT virus passaged 15 times in culture (WTp15 virus). Cidofovir inhibited WT, WTp15, and CDV-R viruses by 50% at 61, 56 and 790 microM, respectively, in plaque reduction assays, with similar inhibition seen in virus yield studies. Cross-resistance occurred with compounds related to cidofovir, but not with unrelated nucleosides. The resistant virus produced 300-fold fewer infectious particles (PFU) than WT and WTp15 viruses in mouse C1271 cells, yet replicated similarly in Vero (monkey) cells. The CDV-R virus was completely attenuated for virulence at 10(7) PFU per mouse in normal BALB/c mice and in severe combined immunodeficient (SCID) mice. The WTp15 virus was 100-fold less virulent than WT virus in BALB/c mice. Thus, the lack of virulence of the resistant virus in the animal model is explained partly by its reduced ability to replicate in mouse cells and by attenuation occurring as a result of extensive cell culturing (inferred from what occurred with the WTp15 virus). Lung and snout virus titre reduction parameters were used to assess antiviral activity of compounds in BALB/c mice infected intranasally with the CDV-R virus. Cidofovir, HDP-cidofovir and arabinofuranosyladenine treatments reduced lung virus titres or = eight-fold. The animal model appears to have limited utility in drug efficacy testing.

Published

2005

3. Topical cidofovir is more effective than is parenteral therapy for treatment of progressive vaccinia in immunocompromised mice.

Author

Smee DF, Bailey KW, Wong MH, Wandersee MK, and Sidwell RW

Subjects

Administration, Topical, Animals, Antiviral Agents therapeutic use, Antiviral Agents toxicity, Brain virology, Cidofovir, Cyclophosphamide pharmacology, Cyclophosphamide toxicity, Cytosine therapeutic use, Cytosine toxicity, Disease Models, Animal, Female, Immunosuppressive Agents pharmacology, Immunosuppressive Agents toxicity, Injections, Intraperitoneal, Kidney virology, Liver virology, Lung virology, Mice, Mice, Hairless, Organophosphorus Compounds therapeutic use, Organophosphorus Compounds toxicity, Skin virology, Specific Pathogen-Free Organisms, Spleen virology, Survival Analysis, Time Factors, Vaccinia pathology, Viral Plaque Assay, Antiviral Agents administration & dosage, Cytosine administration & dosage, Cytosine analogs & derivatives, Immunocompromised Host, Organophosphonates, Organophosphorus Compounds administration & dosage, Vaccinia drug therapy

Abstract

Background: Severe complications may arise as a result of virus dissemination after smallpox (live vaccinia virus) vaccination, particularly in immunocompromised individuals. We developed a new mouse model for studying the effects of antiviral agents on progressive vaccinia virus infections., Methods: Hairless mice were treated with cyclophosphamide (100 mg/kg/day) every 4 days starting 1 day before vaccinia virus exposure to wounded skin. Primary lesions progressed in severity, satellite lesions developed, and the infection eventually killed the mice., Results: Topical treatment with 1%-cidofovir cream (twice daily for 7 days) was much more effective in reducing the severity of primary lesions and the number of satellite lesions than was parenteral cidofovir treatment (100 mg/kg/day, given every 3 days). Both forms of treatment delayed death. Topical drug treatment markedly reduced virus titers in the skin and snout, whereas parenteral treatment did not, suggesting that the latter treatment resulted in lower drug exposure to skin. Topical treatment starting 9 days after infection delayed death by 10 days, compared with treatment with placebo. Combining topical and parenteral cidofovir treatments provided the greatest reduction in lesion severity and prolongation of life., Conclusions: Topical cidofovir treatment was superior to parenteral treatment. This new animal model may be useful in evaluation of the efficacy of treatment regimens against complications from smallpox vaccination.

Published

2004

4. Comparative effects of cidofovir and cyclic HPMPC on lethal cowpox and vaccinia virus respiratory infections in mice.

Author

Smee DF, Bailey KW, and Sidwell RW

Subjects

Administration, Intranasal, Animals, Antiviral Agents administration & dosage, Cidofovir, Cowpox veterinary, Cytosine administration & dosage, Female, Infusions, Parenteral, Liver drug effects, Liver pathology, Lung Diseases veterinary, Lung Diseases virology, Mice, Mice, Inbred BALB C, Organophosphorus Compounds administration & dosage, Vaccinia veterinary, Antiviral Agents pharmacology, Cowpox drug therapy, Cytosine analogs & derivatives, Cytosine pharmacology, Lung Diseases drug therapy, Organophosphonates, Organophosphorus Compounds pharmacology, Vaccinia drug therapy

Abstract

Background: Cidofovir is approved for the treatment of cytomegalovirus retinitis in humans. Although highly effective, the drug can cause renal toxicity in patients. There is much interest in cidofovir as a potential treatment for smallpox, monkeypox and other orthopoxvirus infections. A cyclic phosphonate form of cidofovir, 1-[((S)-2-hydroxy-2-oxo-1,4,2-dioxaphosphorinan-5-yl)methyl]cytosine (cyclic HPMPC), was reported to be less nephrotoxic than cidofovir in animals. Thus, it was deemed important to directly compare the activities of cidofovir and cyclic HPMPC against poxvirus infections in mouse models., Methods: The compounds were evaluated by intraperitoneal and intranasal infection routes using multiple doses of each agent, with single doses of compound given 24 h after virus challenge., Results: By intraperitoneal route, cidofovir protected mice from mortality at 40, 80 and 160 mg/kg, whereas cyclic HPMPC was similarly protective only at 160 mg/kg. By intranasal route, cidofovir was active down to 5 mg/kg, compared to cyclic HPMPC efficacy at 20 and 40 mg/kg. Intraperitoneal doses of 40, 80 and 160 mg/kg cidofovir significantly reduced mortality from vaccinia virus infections, compared to doses of 80 and 160 mg/kg cyclic HPMPC. Intranasal treatment with cidofovir at 5-40 mg/kg was comparably effective to cyclic HPMPC doses of 20 and 40 mg/kg in vaccinia virus infections. Active doses significantly reduced lung virus titers and lung consolidation. Overall, the potency of cyclic HPMPC was about 4 times less than that of cidofovir., Conclusions: Although cyclic HPMPC is reported to exhibit reduced nephrotoxicity in vivo, it is also less potent than cidofovir against orthopoxvirus infections. For this reason, cyclic HPMPC may not offer any advantage over cidofovir in treating these infections in humans., (Copyright 2003 S. Karger AG, Basel)

Published

2003

5. Treatment of lethal cowpox virus respiratory infections in mice with 2-amino-7-[(1,3-dihydroxy-2-propoxy)methyl]purine and its orally active diacetate ester prodrug.

Author

Smee DF, Bailey KW, and Sidwell RW

Subjects

Animals, Area Under Curve, Body Weight, Chlorocebus aethiops, Cidofovir, Cowpox virus metabolism, Cytosine analogs & derivatives, Cytosine pharmacology, Disease Models, Animal, Female, Lung virology, Mice, Mice, Inbred BALB C, Nasal Mucosa virology, Organophosphorus Compounds pharmacology, Statistics, Nonparametric, Vero Cells, Antiviral Agents pharmacology, Cowpox drug therapy, Cowpox virus growth & development, Organophosphonates, Prodrugs pharmacology, Purines pharmacology

Abstract

The acyclic purine nucleoside analog, 2-amino-7-[(1,3-dihydroxy-2-propoxy)methyl]purine (S2242) and its orally active diacetate ester prodrug (HOE961) were reported to be potent inhibitors of vaccinia virus replication in cell culture and in infected mice. These compounds were evaluated further, using infections with the related cowpox virus. Against a wild-type (WT) cowpox virus strain in mouse C127I cell culture, 50% effective concentrations (EC(50), determined by plaque reduction assays) of S2242 and cidofovir (a positive control) were 3.5 and 1.0 microM, respectively. EC(50) values obtained against a cidofovir-resistant strain of the virus were 33 and 230 microM, respectively. Compounds were at least ten-fold less potent against WT virus in Vero cells than C127I cells. S2242 and cidofovir were 50% inhibitory to the proliferation of uninfected C127I cells at 340 and 180 microM, respectively, but neither compound inhibited Vero cell growth at 1000 microM. Mice were lethally infected with cowpox virus by intranasal inoculation, followed 24 h later by antiviral treatment for 5 consecutive days. Once or twice daily intraperitoneal (i.p.) treatments with either S2242 or HOE961 at 100 mg/kg per day resulted in > or = 70 survival compared with no survivors in the placebo group. Lower doses of these compounds (10 and 30 mg/kg per day) were not protective, however. Cidofovir was 100% protective at 30 mg/kg per day. A 10-day course of treatment gave comparable survival results and demonstrated the oral efficacy of HOE961. Treatments with S2242 (100 mg/kg per day) and cidofovir (30 mg/kg per day) each reduced lung and nasal virus titers by approximately ten-fold, whereas, HOE961 (100 mg/kg per day) was less active. Overall, S2242 and HOE961 were found to be effective against cowpox virus infections in mice but were less potent than cidofovir. Since, HOE961 was orally active, it may have advantages over the other parenterally administered compounds for treating orthopoxvirus infections.

Published

2002

6. Effects of cidofovir on the pathogenesis of a lethal vaccinia virus respiratory infection in mice.

Author

Smee DF, Bailey KW, Wong MH, and Sidwell RW

Subjects

Administration, Intranasal, Animals, Blood Gas Monitoring, Transcutaneous, Body Weight, Cells, Cultured, Chlorocebus aethiops, Cidofovir, Cytosine administration & dosage, Cytosine therapeutic use, Injections, Intraperitoneal, Lung drug effects, Lung pathology, Lung virology, Mice, Mice, Inbred BALB C, Organ Size drug effects, Organophosphorus Compounds administration & dosage, Organophosphorus Compounds therapeutic use, Respiratory System drug effects, Respiratory System virology, Respiratory Tract Infections mortality, Respiratory Tract Infections virology, Time Factors, Vaccinia blood, Vaccinia virus growth & development, Vaccinia virus pathogenicity, Vero Cells, Viral Plaque Assay, Virus Replication drug effects, Antiviral Agents therapeutic use, Cytosine analogs & derivatives, Cytosine pharmacology, Organophosphonates, Organophosphorus Compounds pharmacology, Respiratory Tract Infections drug therapy, Vaccinia drug therapy, Vaccinia virus drug effects

Abstract

Intranasal infection of BALB/c mice with the WR strain of vaccinia virus leads to pneumonia, profound weight loss, and death. Although the major sites of virus replication are in the lungs and nasal tissue, dissemination of the virus to other visceral organs and brain occurs via the blood. In this report the effects of cidofovir on the pathogenesis of the infection was studied. Mice were infected intranasally with virus followed 1 day later by a single intraperitoneal treatment with cidofovir (100 mg/kg) or placebo. Placebo-treated mice were dead by day 8, whereas all cidofovir-treated animals survived through 21 days. Cidofovir treatment did not prevent profound weight loss from occurring during the acute phase of the infection, but the mice gained weight quickly after the 8th day. Significantly higher arterial oxygen saturation levels, as determined by pulse oximetry, were seen in cidofovir-treated animals compared to placebos on days 4-7. Cidofovir treatment markedly improved lung consolidation scores and prevented lung weights from increasing during the infection. Virus titers in lungs and nasal tissue were high starting from the first day of the infection, whereas the titers in liver, spleen, brain, and blood was low for 3 days then markedly rose between days 4 and 6. Lung and nasal virus titers were reduced 10-30-fold by cidofovir treatment on days 2, 4 and 6. Virus titers in the other tissues and blood at their peak (day 6) were 30- to >1000-fold less than in tissues of placebos. These results illustrate the ability of a single cidofovir treatment to control the pathogenesis of an acute lethal infection in various tissues during the vaccinia virus infection in mice.

Published

2001

7. Treatment of lethal vaccinia virus respiratory infections in mice with cidofovir.

Author

Smee DF, Bailey KW, and Sidwell RW

Subjects

Administration, Intranasal, Animals, Antiviral Agents administration & dosage, Cidofovir, Cowpox virus isolation & purification, Cytosine administration & dosage, Disease Models, Animal, Drug Evaluation, Preclinical, Injections, Intraperitoneal, Injections, Subcutaneous, Lung virology, Mice, Mice, Inbred BALB C, Nose virology, Organ Specificity, Organophosphorus Compounds administration & dosage, Paranasal Sinuses virology, Pneumonia, Viral virology, Spleen virology, Vaccinia virology, Vaccinia virus isolation & purification, Viral Load, Viremia virology, Antiviral Agents therapeutic use, Cytosine analogs & derivatives, Cytosine therapeutic use, Organophosphonates, Organophosphorus Compounds therapeutic use, Pneumonia, Viral drug therapy, Vaccinia drug therapy, Vaccinia virus drug effects

Abstract

Intranasal infection of BALB/c mice with the WR strain of vaccinia virus leads to pneumonia, profound weight loss and death. Five days after intranasal inoculation, virus from untreated mice was recovered from 11 organs, tissues and whole blood. The highest titres [>10(8) plaque forming units (pfu)/g] were in lungs and nose/sinus tissue, with about 10(7) pfu/g in spleen and blood. Seven other organs contained 30- to > or = 50-fold lower amounts of virus. Mice infected with the related cowpox virus (for comparative purposes) had the majority of virus located in the respiratory tract. The vaccinia mouse model was used to study the efficacy of cidofovir treatments on the infection. Subcutaneous injections of 30 or 100 mg/kg/day, given on days 1 and 4 after virus challenge, reduced mortality by 60-100%. However, lung virus titres on days 2-5 were reduced no more than 10-fold by these treatments. A moderate improvement in drug efficacy occurred with daily treatments for 5 days. The efficacy of cidofovir also increased as the virus challenge dose decreased, where subcutaneous or intraperitoneal treatment routes showed similar degrees of protection. Although it has been known for many years that the WR strain of vaccinia virus can cause lethal infections by intranasal route, its application to antiviral therapy represents a new model for studying anti-orthopoxvirus agents.

Published

2001

8. Intranasal treatment of cowpox virus respiratory infections in mice with cidofovir.

Author

Smee DF, Bailey KW, Wong M, and Sidwell RW

Subjects

Administration, Intranasal, Animals, Antiviral Agents administration & dosage, Antiviral Agents therapeutic use, Chlorocebus aethiops, Cidofovir, Cowpox mortality, Cowpox virology, Cowpox virus growth & development, Cytosine administration & dosage, Cytosine pharmacology, Cytosine therapeutic use, Female, Mice, Mice, Inbred BALB C, Organophosphorus Compounds administration & dosage, Organophosphorus Compounds therapeutic use, Respiratory System drug effects, Respiratory System virology, Respiratory Tract Infections mortality, Respiratory Tract Infections virology, Vero Cells, Viral Plaque Assay, Antiviral Agents pharmacology, Cowpox drug therapy, Cowpox virus drug effects, Cytosine analogs & derivatives, Organophosphonates, Organophosphorus Compounds pharmacology, Respiratory Tract Infections drug therapy

Abstract

Orthopoxvirus infections in mice have been effectively treated with cidofovir, a clinically approved drug given by intravenous infusion to treat cytomegalovirus infections. In a bioterrorist scenario it would be technically difficult to give this drug to a large number of exposed individuals. New treatment approaches are being sought, which include giving cidofovir by alternative routes or designing oral prodrugs of cidofovir. In this report, intranasal cidofovir was investigated as a treatment of pulmonary cowpox virus infections in BALB/c mice. Ninety to 100% of animals given a single intranasal drug treatment (10, 20 or 40 mg/kg) 24 h after virus challenge survived the infection, whereas all placebo-treated mice died. Doses of 2.5 and 5 mg/kg resulted in 60 and 80% survival, respectively. Single treatments of 20 and 40 mg/kg could be given up to 3 days after virus inoculation and still be 80-90% protective. A single 40 mg/kg treatment of infected mice given 1 or 2 days after infection also resulted in statistically significant decreases in virus titer in lungs and nose/sinus compared to the placebo group. Drug efficacy was found to be contingent upon treatment volume. A 10 mg/kg intranasal dose given 24 h after virus challenge was 100 and 50% effective in volumes of 40 and 20 microl, respectively. The same dose in 5 and 10 microl volumes caused no decrease in mortality. The results of these studies establish the utility of cidofovir treatment of poxvirus infections in mice by intranasal route. The data suggest the possibility that aerosol delivery of cidofovir to human lungs may be a viable alternative to intravenous dosing.

Published

2000

9. Treatment of cowpox virus respiratory infections in mice with ribavirin as a single agent or followed sequentially by cidofovir.

Author

Smee DF, Bailey KW, and Sidwell RW

Subjects

Animals, Body Weight, Cell Line, Chlorocebus aethiops, Cidofovir, Cowpox veterinary, Cowpox virus growth & development, Cytosine analogs & derivatives, Dose-Response Relationship, Drug, Drug Therapy, Combination, Humans, Lung pathology, Lung virology, Mice, Mice, Inbred BALB C, Respiratory Tract Infections mortality, Respiratory Tract Infections virology, Vero Cells, Viral Plaque Assay, Antiviral Agents therapeutic use, Cowpox drug therapy, Cowpox virus drug effects, Cytosine therapeutic use, Organophosphonates, Organophosphorus Compounds therapeutic use, Respiratory Tract Infections drug therapy, Ribavirin therapeutic use

Abstract

To better understand the potential of ribavirin in the treatment of orthopoxvirus infections (such as those acquired through bioterrorist activities), the efficacy of the drug was studied in a cowpox respiratory infection model in mice under varying disease severity. Mice did not survive a high intranasal cowpox virus challenge [3 x 10(6) plaque forming units (pfu)/animal] treated with subcutaneous ribavirin (100 mg/kg/day for 5 days), but lived 3.9 days longer than placebos. In contrast, 100% of animals receiving the same dose of drug survived a 3 x 10(5) pfu challenge compared with 0% survival of those that received placebo. Survival rates of 50 and 30% occurred with ribavirin doses of 50 and 25 mg/kg/day, respectively. At the 100 mg/kg/day dose, ribavirin reduced lung virus titres 40-fold on day 6 of the infection relative to titres in the placebo group. Weight loss resulting from illness and mean lung weights of mice treated with ribavirin were also significantly reduced. Mice were infected intranasally with the high 3 x 10(6) pfu virus challenge dose and treated with 100 mg/kg/day ribavirin for 5 days, followed by single injections of 75 mg/kg cidofovir on day 6, 7, 8 or 9. Cidofovir alone (without ribavirin) administered on day 6 had no beneficial effect on disease outcome. Ribavirin alone increased the mean time to death by 3.7 days. Ribavirin treatment for 5 days followed by cidofovir treatment on days 6 and 7 significantly increased the mean time to death beyond that achieved with ribavirin alone by 8.2 and 4.4 days, respectively, with 30 and 40% of mice surviving the infection. These results suggest that many individuals infected with an orthopoxvirus by aerosol route would benefit by a course of ribavirin therapy. Later, the fewer number of very sick individuals could be treated with intravenous cidofovir.

Published

2000