Your search keyword '"Cytosine administration & dosage"' showing total 25 results

1. Combination therapy with brincidofovir and valganciclovir against species C adenovirus infection in the immunosuppressed Syrian hamster model allows for substantial reduction of dose for both compounds.

Author

Toth K, Tollefson AE, Spencer JF, Ying B, and Wold WSM

Subjects

Adenoviridae Infections virology, Adenoviruses, Human physiology, Animals, Antiviral Agents administration & dosage, Antiviral Agents pharmacology, Cytosine administration & dosage, Cytosine pharmacology, Cytosine therapeutic use, Disease Models, Animal, Drug Therapy, Combination, Ganciclovir administration & dosage, Ganciclovir pharmacology, Ganciclovir therapeutic use, HEK293 Cells, Humans, Immunocompromised Host, Mesocricetus, Organophosphonates administration & dosage, Organophosphonates pharmacology, Valganciclovir, Viral Load drug effects, Virus Replication drug effects, Adenoviridae Infections drug therapy, Adenoviruses, Human drug effects, Antiviral Agents therapeutic use, Cytosine analogs & derivatives, Ganciclovir analogs & derivatives, Organophosphonates therapeutic use

Abstract

Adenovirus infections of immunocompetent adults are usually mild and resolve without serious sequelae. However, adenovirus infections of immunocompromised patients often develop into life-threatening multi-organ disease. Pediatric hematopoietic transplant patients are especially threatened, with high incidence of infection and high mortality rates. Presently, there is no drug specifically approved by the FDA to treat adenovirus infections; thus there is an urgent need to develop effective antivirals against the virus. Previously, we demonstrated that brincidofovir and valganciclovir were efficacious against lethal intravenous challenge with human type 5 adenovirus in the Syrian hamster model. Here, we tested the in vivo efficacy of the combination of these two drugs and showed that the combination of brincidofovir and valganciclovir is more efficacious than either drug alone, thus potentially allowing decreased patient exposure to the drugs while maintaining antiviral efficacy. As antiviral compounds often have toxic side effects, a decrease in dose or duration of therapy allowed by the combination could also improve tolerability., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

2. Short-term clinical safety profile of brincidofovir: A favorable benefit-risk proposition in the treatment of smallpox.

Author

Chittick G, Morrison M, Brundage T, and Nichols WG

Subjects

Adenoviridae drug effects, Adolescent, Adult, Animals, Antiviral Agents administration & dosage, Antiviral Agents pharmacology, Cytomegalovirus drug effects, Cytosine administration & dosage, Cytosine pharmacology, Disease Models, Animal, Double-Blind Method, Drug Administration Schedule, Humans, Middle Aged, Orthopoxvirus drug effects, Safety, Young Adult, Cytosine analogs & derivatives, Organophosphonates administration & dosage, Organophosphonates pharmacology, Smallpox drug therapy

Abstract

Brincidofovir (BCV, CMX001) is an orally available, long-acting, broad-spectrum antiviral that has been evaluated in healthy subjects in Phase I studies and in hematopoietic cell transplant recipients and other immunocompromised patients in Phase II/III clinical trials for the prevention and treatment of cytomegalovirus and adenovirus infections. BCV has also shown in vitro activity against orthopoxviruses such as variola (smallpox) virus, and is under advanced development as a treatment for smallpox under the US FDA's 'Animal Rule'. The anticipated treatment regimen for smallpox is a total weekly dose of 200 mg administered orally for 3 consecutive weeks. To assess the benefit-to-risk profile of BCV for the treatment of smallpox, we evaluated short-term safety data associated with comparable doses from Phase I studies and from adult and pediatric subjects in the cytomegalovirus and adenovirus clinical programs. When administered at doses and durations similar to that proposed for the treatment of smallpox, BCV was generally well tolerated in both adults and pediatric subjects. The most common adverse events were mild gastrointestinal events and asymptomatic, transient, and reversible elevations in serum transaminases. The data presented herein indicate a favorable safety profile for BCV for the treatment of smallpox, and support its continued development for this indication., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

3. Efficacy of delayed brincidofovir treatment against a lethal rabbitpox virus challenge in New Zealand White rabbits.

Author

Grossi IM, Foster SA, Gainey MR, Krile RT, Dunn JA, Brundage T, and Khouri JM

Subjects

Animals, Antibodies, Neutralizing, Antibodies, Viral, Antiviral Agents therapeutic use, Body Temperature, Body Weight, Cytosine administration & dosage, Cytosine therapeutic use, Disease Models, Animal, Double-Blind Method, Organophosphonates administration & dosage, Poxviridae Infections drug therapy, Rabbits, Survival Rate, Treatment Outcome, Vaccination, Vaccinia mortality, Vaccinia physiopathology, Vaccinia virology, Variola virus, Viral Load drug effects, Cytosine analogs & derivatives, Organophosphonates therapeutic use, Smallpox drug therapy, Vaccinia drug therapy, Vaccinia virus drug effects

Abstract

In the event of a bioterror attack with variola virus (smallpox), exposure may only be identified following onset of fever. To determine if antiviral therapy with brincidofovir (BCV; CMX001) initiated at, or following, onset of fever could prevent severe illness and death, a lethal rabbitpox model was used. BCV is in advanced development as an antiviral for the treatment of smallpox under the US Food and Drug Administration's 'Animal Rule'. This pivotal study assessed the efficacy of immediate versus delayed treatment with BCV following onset of symptomatic disease in New Zealand White rabbits intradermally inoculated with a lethal rabbitpox virus (RPXV), strain Utrecht. Infected rabbits with confirmed fever were randomized to blinded treatment with placebo, BCV, or BCV delayed by 24, 48, or 72 h. The primary objective evaluated the survival benefit with BCV treatment. The assessment of reduction in the severity and progression of clinical events associated with RPXV were secondary objectives. Clinically and statistically significant reductions in mortality were observed when BCV was initiated up to 48 h following the onset of fever; survival rates were 100%, 93%, and 93% in the immediate treatment, 24-h, and 48-h delayed treatment groups, respectively, versus 48% in the placebo group (p < 0.05 for each vs. placebo). Significant improvements in clinical and virologic parameters were also observed. These findings provide a scientific rationale for therapeutic intervention with BCV in the event of a smallpox outbreak when vaccination is contraindicated or when diagnosis follows the appearance of clinical signs and symptoms., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

4. Buccal viral DNA as a trigger for brincidofovir therapy in the mousepox model of smallpox.

Author

Crump R, Korom M, Buller RM, and Parker S

Subjects

Animals, Antiviral Agents administration & dosage, Cytosine administration & dosage, Cytosine therapeutic use, DNA, Viral isolation & purification, Disease Models, Animal, Ectromelia, Infectious virology, Mice, Organophosphonates administration & dosage, Orthopoxvirus drug effects, Smallpox drug therapy, Smallpox virology, Antiviral Agents therapeutic use, Cytosine analogs & derivatives, DNA, Viral drug effects, Ectromelia virus drug effects, Ectromelia, Infectious drug therapy, Mouth Mucosa virology, Organophosphonates therapeutic use

Abstract

Orthopoxviruses continue to pose a significant threat to the population as potential agents of bioterrorism. An intentional release of natural or engineered variola virus (VARV) or monkeypox viruses would cause mortality and morbidity in the target population. To address this, antivirals have been developed and evaluated in animal models of smallpox and monkeypox. One such antiviral, brincidofovir (BCV, previously CMX001), has demonstrated high levels of efficacy against orthopoxviruses in animal models and is currently under clinical evaluation for prevention and treatment of diseases caused by cytomegaloviruses and adenoviruses. In this study we use the mousepox model of smallpox to evaluate the relationship between the magnitude of the infectious virus dose and an efficacious BCV therapy outcome when treatment is initiated concomitant with detection of ectromelia virus viral DNA (vDNA) in mouse buccal swabs. We found that vDNA could be detected in buccal swabs of some, but not all infected mice over a range of challenge doses by day 3 or 4 postexposure, when initiation of BCV treatment was efficacious, suggesting that detection of vDNA in buccal swabs could be used as a trigger to initiate BCV treatment of an entire potentially exposed population. However, buccal swabs of some mice did not become positive until 5 days postexposure, when initiation of BCV therapy failed to protect mice that received high doses of virus. And finally, the data suggest that the therapeutic window for efficacious BCV treatment decreases as the virus infectious dose increases. Extrapolating these findings to VARV, the data suggest that treatment should be initiated as soon as possible after exposure and not rely on a diagnostic tool such as the measurement of vDNA in buccal cavity swabs; however, consideration should be given to the fact that the behavior/disease-course of VARV in humans is different from that of ectromelia virus in the mouse., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2017

5. The efficacy and pharmacokinetics of brincidofovir for the treatment of lethal rabbitpox virus infection: a model of smallpox disease.

Author

Trost LC, Rose ML, Khouri J, Keilholz L, Long J, Godin SJ, and Foster SA

Subjects

Animals, Antibodies, Neutralizing blood, Antibodies, Viral blood, Antiviral Agents pharmacokinetics, Antiviral Agents therapeutic use, Cidofovir, Cytosine administration & dosage, Cytosine pharmacokinetics, Cytosine pharmacology, Cytosine therapeutic use, Humans, Injections, Intradermal, Organophosphonates administration & dosage, Organophosphonates pharmacology, Random Allocation, Vaccinia virology, Vaccinia virus growth & development, Variola virus drug effects, Variola virus growth & development, Cytosine analogs & derivatives, Disease Models, Animal, Organophosphonates pharmacokinetics, Organophosphonates therapeutic use, Rabbits, Smallpox drug therapy, Vaccinia drug therapy, Vaccinia virus drug effects

Abstract

Brincidofovir (BCV) has broad-spectrum in vitro activity against dsDNA viruses, including smallpox, and is being developed as a treatment for smallpox as well as infections caused by other dsDNA viruses. BCV has previously been shown to be active in multiple animal models of smallpox. Here we present the results of a randomized, blinded, placebo-controlled study of the efficacy and pharmacokinetics of a novel, "humanized" regimen of BCV for treatment of New Zealand White rabbits infected with a highly lethal inoculum of rabbitpox virus, a well characterized model of smallpox. Compared with placebo, a dose-dependent increase in survival was observed in all BCV-treatment groups. Concentrations of cidofovir diphosphate (CDV-PP), the active antiviral, in rabbit peripheral blood mononuclear cells (PBMCs) were determined for comparison to those produced in humans at the dose proposed for treatment of smallpox. CDV-PP exposure in PBMCs from rabbits given BCV scaled to human exposures at the dose proposed for treatment of smallpox, which is also currently under evaluation for other indications. The results of this study demonstrate the activity of BCV in the rabbitpox model of smallpox and the feasibility of scaling doses efficacious in the model to a proposed human dose and regimen for treatment of smallpox., (Copyright © 2015 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2015

6. Co-administration of the broad-spectrum antiviral, brincidofovir (CMX001), with smallpox vaccine does not compromise vaccine protection in mice challenged with ectromelia virus.

Author

Parker S, Crump R, Foster S, Hartzler H, Hembrador E, Lanier ER, Painter G, Schriewer J, Trost LC, and Buller RM

Subjects

Animals, Cytosine administration & dosage, Ectromelia virus immunology, Ectromelia, Infectious immunology, Ectromelia, Infectious virology, Female, Humans, Immunity, Mice, Mice, Inbred C57BL, Smallpox Vaccine immunology, Vaccination, Virus Replication, Antiviral Agents administration & dosage, Cytosine analogs & derivatives, Ectromelia virus physiology, Ectromelia, Infectious prevention & control, Organophosphonates administration & dosage, Smallpox Vaccine administration & dosage

Abstract

Natural orthopoxvirus outbreaks such as vaccinia, cowpox, cattlepox and buffalopox continue to cause morbidity in the human population. Monkeypox virus remains a significant agent of morbidity and mortality in Africa. Furthermore, monkeypox virus's broad host-range and expanding environs make it of particular concern as an emerging human pathogen. Monkeypox virus and variola virus (the etiological agent of smallpox) are both potential agents of bioterrorism. The first line response to orthopoxvirus disease is through vaccination with first-generation and second-generation vaccines, such as Dryvax and ACAM2000. Although these vaccines provide excellent protection, their widespread use is impeded by the high level of adverse events associated with vaccination using live, attenuated virus. It is possible that vaccines could be used in combination with antiviral drugs to reduce the incidence and severity of vaccine-associated adverse events, or as a preventive in individuals with uncertain exposure status or contraindication to vaccination. We have used the intranasal mousepox (ectromelia) model to evaluate the efficacy of vaccination with Dryvax or ACAM2000 in conjunction with treatment using the broad spectrum antiviral, brincidofovir (BCV, CMX001). We found that co-treatment with BCV reduced the severity of vaccination-associated lesion development. Although the immune response to vaccination was quantifiably attenuated, vaccination combined with BCV treatment did not alter the development of full protective immunity, even when administered two days following ectromelia challenge. Studies with a non-replicating vaccine, ACAM3000 (MVA), confirmed that BCV's mechanism of attenuating the immune response following vaccination with live virus was, as expected, by limiting viral replication and not through inhibition of the immune system. These studies suggest that, in the setting of post-exposure prophylaxis, co-administration of BCV with vaccination should be considered a first response to a smallpox emergency in subjects of uncertain exposure status or as a means of reduction of the incidence and severity of vaccine-associated adverse events., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2014

7. Evaluation of disease and viral biomarkers as triggers for therapeutic intervention in respiratory mousepox - an animal model of smallpox.

Author

Parker S, Chen NG, Foster S, Hartzler H, Hembrador E, Hruby D, Jordan R, Lanier R, Painter G, Painter W, Sagartz JE, Schriewer J, and Mark Buller R

Subjects

Animals, Cell Line, Cytosine administration & dosage, Disease Models, Animal, Drug Evaluation, Preclinical, Ectromelia virus drug effects, Ectromelia virus physiology, Ectromelia, Infectious genetics, Ectromelia, Infectious virology, Female, Humans, Mice, Mice, Hairless, Mice, Inbred C57BL, Monkeypox virus physiology, Smallpox virology, Variola virus drug effects, Variola virus genetics, Variola virus physiology, Virus Replication drug effects, Benzamides administration & dosage, Biomarkers, Pharmacological analysis, Cytosine analogs & derivatives, Ectromelia, Infectious drug therapy, Isoindoles administration & dosage, Monkeypox virus drug effects, Organophosphonates administration & dosage, Smallpox drug therapy

Abstract

The human population is currently faced with the potential use of natural or recombinant variola and monkeypox viruses as biological weapons. Furthermore, the emergence of human monkeypox in Africa and its expanding environs poses a significant natural threat. Such occurrences would require therapeutic and prophylactic intervention with antivirals to minimize morbidity and mortality of exposed populations. Two orally-bioavailable antivirals are currently in clinical trials; namely CMX001, an ether-lipid analog of cidofovir with activity at the DNA replication stage and ST-246, a novel viral egress inhibitor. Both of these drugs have previously been evaluated in the ectromelia/mousepox system; however, the trigger for intervention was not linked to a disease biomarker or a specific marker of virus replication. In this study we used lethal, intranasal, ectromelia virus infections of C57BL/6 and hairless SKH1 mice to model human disease and evaluate exanthematous rash (rash) as an indicator to initiate antiviral treatment. We show that significant protection can be provided to C57BL/6 mice by CMX001 or ST-246 when therapy is initiated on day 6 post infection or earlier. We also show that significant protection can be provided to SKH1 mice treated with CMX001 at day 3 post infection or earlier, but this is four or more days before detection of rash (ST-246 not tested). Although in this model rash could not be used as a treatment trigger, viral DNA was detected in blood by day 4 post infection and in the oropharyngeal secretions (saliva) by day 2-3 post infection - thus providing robust and specific markers of virus replication for therapy initiation. These findings are discussed in the context of current respiratory challenge animal models in use for the evaluation of poxvirus antivirals., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

8. Evaluation of inhaled cidofovir as postexposure prophylactic in an aerosol rabbitpox model.

Author

Verreault D, Sivasubramani SK, Talton JD, Doyle LA, Reddy JD, Killeen SZ, Didier PJ, Marx PA, and Roy CJ

Subjects

Administration, Inhalation, Animals, Cell Line, Cidofovir, Cytosine administration & dosage, Disease Models, Animal, Female, Lung pathology, Lung virology, Male, Rabbits, Vaccinia mortality, Vaccinia virology, Antiviral Agents administration & dosage, Cytosine analogs & derivatives, Organophosphonates administration & dosage, Post-Exposure Prophylaxis, Vaccinia prevention & control, Vaccinia virus

Abstract

Smallpox is considered a biological threat based upon the possibility of deliberate reintroduction into the population, creating an urgent need for effective antivirals. The antiviral drug cidofovir (Cr) has shown to be effective against poxviruses, although route-specific nephrotoxicity has hampered its development for emergency post-exposure prophylaxis (PEP). In this study, we use a micronized dry powder formulation of pharmaceutical-grade Cr (NanoFOVIRTM; Nf) to treat rabbits exposed to aerosolized rabbitpox virus (RPXV) to further evaluate the effectiveness of direct drug delivery to the lung. Naïve rabbits were infected with RPXV by aerosol; three subsets received aerosolized Nf at 0.5, 1.0 or 1.75mg/kg daily for 3days post-exposure, positive and negative control groups received intravenous (IV) Cr treatments and no treatment, respectively. Nf groups showed an antiviral-dose associated survival of 50% (0.5mg/kg), 80% (1.0mg/kg) and 100% (1.75mg/kg). All animals (100%) from the IV-Cr treatment group and none (0%) from the untreated controls survived. Nf (1.75) protected rabbits from RPX at approximately 10% of the equivalent IV-Cr dose. A dose-related effect was observed in clinical development of RPX disease in Nf groups. Significant reduction of RPX-induced pathological changes was observed in Nf (1.75) and IV-Cr groups. Results suggest that Nf may be a viable antiviral for emergency post-exposure prophylaxis and should be evaluated in other models of poxviral disease., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2012

9. Virological failure of intralesional cidofovir therapy in recurrent respiratory papillomatosis is not associated with genetic or epigenetic changes of HPV11: complete genome comparison of sequential isolates.

Author

Gáll T, Kis A, Fehér E, Gergely L, and Szarka K

Subjects

Cidofovir, Cytosine administration & dosage, DNA Methylation, DNA, Viral chemistry, DNA, Viral genetics, Epigenesis, Genetic, Human papillomavirus 11 isolation & purification, Humans, Molecular Sequence Data, Mutation, Polymorphism, Single-Stranded Conformational, Sequence Analysis, DNA, Treatment Failure, Antiviral Agents administration & dosage, Cytosine analogs & derivatives, Genome, Viral, Human papillomavirus 11 genetics, Organophosphonates administration & dosage, Papillomavirus Infections drug therapy, Papillomavirus Infections virology, Respiratory Tract Infections drug therapy, Respiratory Tract Infections virology

Abstract

Five sequential human papillomavirus type 11 (HPV11) positive samples collected from an aggressive juvenile onset recurrent respiratory papillomatosis before, during and after intralesional cidofovir therapy leading to virological failure after initial response were analyzed. Sequencing of the complete genome as well as methylation analysis by bisulfate modification and sequencing of the long control region (LCR) were performed to seek for genetic and epigenetic changes as a possible background for therapy failure. Single-strand conformation polymorphism of E1, E2, E6, E7 and LCR was used to exclude the presence of multiple HPV11 infection. All five complete genomes were identical and all four E2 binding sites in the LCR were uniformly unmethylated in all five genomes. Thus the virological failure was not due to virological factors suggesting that cidofovir action may depend more heavily on the host., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2011

10. Effect of oral treatment with (S)-HPMPA, HDP-(S)-HPMPA or ODE-(S)-HPMPA on replication of murine cytomegalovirus (MCMV) or human cytomegalovirus (HCMV) in animal models.

Author

Quenelle DC, Collins DJ, Pettway LR, Hartline CB, Beadle JR, Wan WB, Hostetler KY, and Kern ER

Subjects

Adenine administration & dosage, Adenine pharmacology, Adenine therapeutic use, Administration, Oral, Animals, Antiviral Agents administration & dosage, Antiviral Agents pharmacology, Cidofovir, Cytomegalovirus drug effects, Cytosine administration & dosage, Cytosine analogs & derivatives, Cytosine therapeutic use, Liver virology, Mice, Mice, Inbred BALB C, Mice, SCID, Muromegalovirus drug effects, Organophosphonates administration & dosage, Organophosphonates pharmacology, Survival Analysis, Adenine analogs & derivatives, Antiviral Agents therapeutic use, Cytomegalovirus Infections drug therapy, Herpesviridae Infections drug therapy, Organophosphonates therapeutic use

Abstract

We utilized BALB/c mice infected with murine CMV (MCMV) or severe combined immunodeficient (SCID) mice implanted with human fetal tissue and infected with HCMV to determine the efficacy of (S)-9-[3-hydroxy-2-(phophonomethoxy)propyl]adenine ((S)-HPMPA), hexadecyloxypropyl-(S)-HPMPA (HDP-(S)-HPMPA) or octadecyloxyethyl-(S)-HPMPA (ODE-(S)-HPMPA). In MCMV-infected BALB/c mice, oral HDP-(S)-HPMPA at 30 mg/kg significantly reduced mortality when started 24-48 h post inoculation. In the experimental HCMV infection, oral administration of vehicle or 10mg/kg of (S)-HPMPA, HDP-(S)-HPMPA or ODE-(S)-HPMPA was initiated 24h after infection and continued for 28 consecutive days. Cidofovir (CDV), at 20mg/kg given i.p., was used as a positive control. HDP-(S)-HPMPA or ODE-(S)-HPMPA significantly reduced viral replication compared to vehicle-treated mice, while oral (S)-HPMPA was ineffective.

Published

2008

11. Efficacy of therapeutic intervention with an oral ether-lipid analogue of cidofovir (CMX001) in a lethal mousepox model.

Author

Parker S, Touchette E, Oberle C, Almond M, Robertson A, Trost LC, Lampert B, Painter G, and Buller RM

Subjects

Administration, Oral, Animals, Antiviral Agents administration & dosage, Cidofovir, Cytosine administration & dosage, Cytosine metabolism, Cytosine therapeutic use, Ectromelia, Infectious prevention & control, Ectromelia, Infectious virology, Ether, Female, Hepatocytes metabolism, Humans, Mice, Mice, Inbred A, Organophosphonates administration & dosage, Organophosphonates metabolism, Antiviral Agents therapeutic use, Cytosine analogs & derivatives, Ectromelia virus drug effects, Ectromelia, Infectious drug therapy, Organophosphonates therapeutic use

Abstract

In the 21st century we are faced with the potential use of natural or recombinant VARV and MPXV as biological weapons, and the emergence of human MPXV. Such an occurrences would require therapeutic and prophylactic intervention with antivirals. Cidofovir, an antiviral approved for the treatment of cytomegalovirus retinitis in AIDS patients, has activity against poxviruses, but must be administered intravenously and is associated with nephrotoxicity. An ether-lipid analogue of CDV, CMX001 (HDP-CDV), has potent antiviral activity against a range of DNA viruses including poxviruses, excellent oral bioavailability and minimal nephrotoxicity. CMX001 and CDV are equally efficacious at protecting mice from mortality following high ectromelia virus doses (10,000 x LD(50)) introduced by the intra-nasal route or small particle aerosol. Using CMX001 at a 10mg/kg dose followed by 2.5mg/kg doses every other-day for 14 days provided solid protection against mortality and weight loss following an intra-nasal challenge of (100-200) x LD(50) of ectromelia virus. Furthermore, complete protection against mortality was achieved when administration was delayed until as late as 5 days post-infection, which is 3-4 days prior to the death of the untreated controls. This therapeutic window would be equivalent to intervening during the rash stage of ordinary smallpox.

Published

2008

12. Efficacy of N-methanocarbathymidine in treating mice infected intranasally with the IHD and WR strains of vaccinia virus.

Author

Smee DF, Hurst BL, Wong MH, Glazer RI, Rahman A, and Sidwell RW

Subjects

Administration, Oral, Animals, Cidofovir, Cytosine administration & dosage, Cytosine analogs & derivatives, Cytosine therapeutic use, Injections, Intraperitoneal, Mice, Organophosphonates administration & dosage, Organophosphonates therapeutic use, Survival Analysis, Thymidine administration & dosage, Thymidine therapeutic use, Thymidine toxicity, Viral Plaque Assay, Antiviral Agents therapeutic use, Thymidine analogs & derivatives, Vaccinia drug therapy, Vaccinia virus drug effects

Abstract

N-Methanocarbathymidine [(N)-MCT] is a newly identified inhibitor of orthopoxvirus replication in cell culture and in mice. Limited published animal studies indicated the compound is effective by intraperitoneal (i.p.) route at 10-100 mg/(kg day). More extensive studies using different treatment regimens in intranasally infected mice were conducted in order to further explore the potential of this compound compared to cidofovir in treating vaccinia virus infections. (N)-MCT was given twice a day for 7 days, whereas cidofovir was administered once a day for 2 days, each starting 24h after virus exposure for most experiments. (N)-MCT was not toxic up to 1000 mg/(kg day) by the i.p. treatment route. Oral and i.p. treatment regimens with (N)-MCT were directly compared during a vaccinia virus (IHD strain) infection, indicating that the nucleoside has good oral bioavailability in mice. Treatments by i.p. route with (N)-MCT (100 mg/(kg day)) reduced lung, nasal, and brain virus titers during an IHD virus infection, but not nearly to the same extent as i.p. cidofovir (100 mg/(kg day)). Treatment with both compounds decreased liver, spleen, and kidney virus titers, as well as reduced lung consolidation scores and lung weights. Onset of treatment could be delayed by 2 days with (N)-MCT and by 3 days with cidofovir, providing significant survival benefit during the IHD virus infection. Against a vaccinia virus (WR strain) infection in mice, i.p. (N)-MCT treatment prevented death at 500 mg/(kg day), which was comparable in activity to i.p. cidofovir (100 mg/(kg day)). Significant reductions in tissue virus titers occurred with both treatment regimens. (N)-MCT could be further pursued for its potential to treat orthopoxvirus infections in humans.

Published

2007

13. Cidofovir is effective against caprine herpesvirus 1 infection in goats.

Author

Tempesta M, Camero M, Bellacicco AL, Thiry J, Crescenzo G, Neyts J, Thiry E, and Buonavoglia C

Subjects

Animals, Cidofovir, Cytosine administration & dosage, Cytosine therapeutic use, Disease Models, Animal, Goats, Herpesviridae Infections virology, Organophosphonates administration & dosage, Varicellovirus isolation & purification, Virus Shedding drug effects, Cytosine analogs & derivatives, Herpesviridae Infections drug therapy, Organophosphonates therapeutic use, Varicellovirus drug effects

Abstract

Caprine herpesvirus 1 (CpHV-1) is a virus able to cause genital infection leading to vulvovaginitis or balanoposthitis in adult goats. CpHV-1 shares several biological similarities with herpes simplex type 2 (HSV-2) infection in man, such as genital tropism, type and site of typical lesions and it might provide an animal model for studies on antiviral drugs for HSV-2 infection in man. In this view the efficacy of cidofovir (CDV) drug was tested in six goats intravaginally infected with BA.1 strain of CpHV-1. Three goats received an intravaginal application of 3 ml of a 1% CDV preparation at 4h post infection and then every 12 h for five consecutive days. Three goats were kept as untreated controls. The goats were daily examined for clinical evidence of the infection and viral shedding. CDV was able to protect against disease progression and inhibited the onset of the local lesions due to the CpHV-1 replication. Treated animals shed virus for a shorter period (3 days less) and at lower titres than the control animals. CpHV-1 infection in goats may represent an excellent animal model for the study of novel strategies for the treatment of primary genital HSV-2 infection in man.

Published

2007

14. Antiviral activity of HPMPC (cidofovir) against orf virus infected lambs.

Author

Scagliarini A, McInnes CJ, Gallina L, Dal Pozzo F, Scagliarini L, Snoeck R, Prosperi S, Sales J, Gilray JA, and Nettleton PF

Subjects

Administration, Topical, Animals, Cidofovir, Cytosine administration & dosage, Ecthyma, Contagious virology, Paraffin administration & dosage, Sheep, Silicic Acid administration & dosage, Antiviral Agents administration & dosage, Cytosine analogs & derivatives, Ecthyma, Contagious drug therapy, Orf virus growth & development, Organophosphonates administration & dosage

Abstract

(S)-1-[3-hydroxy-2-(phosphonomethoxy)propyl]cytosine [corrected] (HPMPC, cidofovir, CDV, Vistide) is an acyclic nucleoside analogue with a potent and selective activity against a broad spectrum of DNA viruses including the poxviruses. In this study we present the results of different treatment regimens in lambs experimentally infected with orf virus with different cidofovir formulations prepared in Beeler basis and Unguentum M. Our results show that choice of excipient, concentration of codofovir [corrected] and treatment regimen were all important to the clinical outcome of the therapy. Whilst one particular regimen appeared to exacerbate the lesion, treatment with 1% (w/v) cidofovir cream, prepared in Beeler basis, for 4 consecutive days did result in milder lesions that resolved in milder lesions that resolved [corrected] more quickly than untreated lesions. Furthermore the scabs of the treated animals contained significantly lower amounts of viable virus meaning there should be less contamination of the environment with virus than would normally occur.

Published

2007

15. Papillomavirus and treatment.

Author

Snoeck R

Subjects

Antiviral Agents administration & dosage, Antiviral Agents therapeutic use, Carcinoma surgery, Carcinoma therapy, Carcinoma virology, Chemotherapy, Adjuvant, Cidofovir, Cytosine administration & dosage, Cytosine analogs & derivatives, Cytosine therapeutic use, Female, Humans, Organophosphonates administration & dosage, Organophosphonates therapeutic use, Papillomavirus Infections virology, Uterine Cervical Neoplasms surgery, Uterine Cervical Neoplasms therapy, Uterine Cervical Neoplasms virology, Viral Vaccines administration & dosage, Viral Vaccines therapeutic use, Warts surgery, Warts therapy, Warts virology, Papillomaviridae, Papillomavirus Infections surgery, Papillomavirus Infections therapy

Abstract

Human papillomaviruses (HPVs) are small DNA viruses responsible for a broad range of clinical presentations, characterized histologically by the proliferation of epithelial cells. HPVs are responsible for benign as well as malignant lesions, the most frequent of the latter being cervical carcinoma. A better knowledge of the immunobiology of these lesions allowed the development of prophylactic vaccines (for the most frequent genital types) that are presently under evaluation. The present paper describes different approaches for the treatment of HPV lesions, still mostly based on surgery, and underlines the importance of developing adjuvant therapies.

Published

2006

16. The efficacy of cidofovir treatment of mice infected with ectromelia (mousepox) virus encoding interleukin-4.

Author

Robbins SJ, Jackson RJ, Fenner F, Beaton S, Medveczky J, Ramshaw IA, and Ramsay AJ

Subjects

Animals, Antiviral Agents administration & dosage, Cidofovir, Cytosine administration & dosage, Ectromelia virus drug effects, Ectromelia, Infectious drug therapy, Ectromelia, Infectious genetics, Ectromelia, Infectious mortality, Mice, Mice, Inbred C57BL, Organophosphonates administration & dosage, Antiviral Agents therapeutic use, Cytosine analogs & derivatives, Cytosine therapeutic use, Ectromelia virus immunology, Ectromelia, Infectious immunology, Interleukin-4 physiology, Organophosphonates therapeutic use

Abstract

Improved vaccines and therapies for virulent poxvirus infection are required, particularly in the light of recent threats of bioterrorism. Cidofovir (HPMPC) is an acyclic nucleoside analog with proven efficacy against poxviruses. Here, we evaluated HPMPC in mice given a recombinant ectromelia virus (ECTV) encoding interleukin-4 (ECTV-IL-4) that is highly immune suppressive. Mousepox-sensitive BALB/c mice given HPMPC for five consecutive days after infection were protected against the lethal effects of a control ECTV recombinant, although they suffered a chronic form of mousepox disease. High doses of the drug resulted in a milder localized disease. In contrast, HPMPC failed to protect mousepox-resistant C57BL/6 mice against ECTV-IL-4, although its lethal effects were delayed by five daily doses of 20 mg/kg or a single dose of 100 mg/kg. Higher daily doses further delayed mortality, although the majority of animals eventually succumbed to infection. It appears that HPMPC inhibited ECTV-IL-4 replication without clearance, with the virus having a lethal effect when the drug was removed. Resistance of ECTV-IL-4 to HPMPC treatment may relate to the virus's ability to inhibit antiviral cell-mediated immunity. Interestingly, ECTV-IL-4-mediated immune suppression was not accompanied by a reduction in systemic IFN-gamma expression, suggestive of an alternative or highly localized suppressive mechanism.

Published

2005

17. The cotton rat model for adenovirus ocular infection: antiviral activity of cidofovir.

Author

Kaneko H, Mori S, Suzuki O, Iida T, Shigeta S, Abe M, Ohno S, Aoki K, and Suzutani T

Subjects

Adenoviridae Infections virology, Adenoviruses, Human growth & development, Administration, Topical, Animals, Antigens, Viral analysis, Antiviral Agents pharmacology, Cidofovir, Conjunctivitis, Viral drug therapy, Cornea virology, Cytosine administration & dosage, Cytosine pharmacology, Disease Models, Animal, Drug Evaluation, Preclinical, Female, Organophosphorus Compounds administration & dosage, Organophosphorus Compounds pharmacology, Rats, Sigmodontinae, Viral Plaque Assay, Virus Replication drug effects, Virus Shedding drug effects, Adenoviridae Infections drug therapy, Adenoviruses, Human drug effects, Antiviral Agents therapeutic use, Cytosine analogs & derivatives, Cytosine therapeutic use, Eye Infections, Viral drug therapy, Organophosphonates, Organophosphorus Compounds therapeutic use

Abstract

To determine the antiviral effects of compounds against ocular adenovirus (AdV) infection, we established an animal model of AdV infection in cotton rat eyes. Cotton rat eyes were inoculated intrastromally and topically with four AdV serotypes 4, 5, 8, and 37, and treated topically with 1% HPMPC (cidofovir) eye drops twice a day. The infected corneas were extracted and homogenized, and virus titers in the cornea specimens were determined by a plaque assay. The virus titer in AdV type 5-inoculated eyes peaked on days 0 through 3 after inoculation and virus shedding was detected for 18.0+/-2.8 days. AdV 5 antigen in the infected corneas was demonstrated in the corneal epithelial cells by immunofluorescence stain. However, for AdV serotypes 4, 8, and 37, no evidence of continued virus replication in cotton rat eyes was noted. Specimens from cidofovir-treated eyes infected with AdV 5 demonstrated a statistically significant reduction in the mean virus titer (days 3-15) (P=0.028) and virus shedding duration (P=0.0014), as compared with those of the control group.

Published

2004

18. HPMPC therapy of MCMV-induced retinal disease in the SCID mouse measured by electroretinography, a non-invasive technique.

Author

Garneau M, Bolger GT, Bousquet C, Kibler P, Tremblay F, and Cordingley MG

Subjects

Animals, Antiviral Agents administration & dosage, Cidofovir, Cytomegalovirus Retinitis virology, Cytosine administration & dosage, Disease Models, Animal, Electroretinography methods, Eye Infections, Viral drug therapy, Eye Infections, Viral virology, Female, Herpesviridae Infections drug therapy, Herpesviridae Infections virology, Humans, Mice, Mice, SCID, Organophosphorus Compounds administration & dosage, Retina virology, Treatment Outcome, Virus Replication, Antiviral Agents therapeutic use, Cytomegalovirus Retinitis drug therapy, Cytosine analogs & derivatives, Cytosine therapeutic use, Muromegalovirus pathogenicity, Organophosphonates, Organophosphorus Compounds therapeutic use

Abstract

The purpose of these studies was to investigate the use of non-invasive electroretinography for the evaluation of retinal disease and its treatment in an ocular murine cytomegalovirus (MCMV) disease model. While under anesthesia, 10(2.6)plaque forming units (pfu) of salivary gland passaged, Smith strain MCMV was injected in the anterior chamber of 6- to 8-week-old severe combined immunodeficiency (SCID) mice. At various times post-inoculation, bright-flash scotopic electroretinogram, viral titer, and histology were obtained from the injected eye. Antiviral therapy was tested using 0.1 and 5mg/kg/day subcutaneous injections of HPMPC (Cidofovir) once daily for 5 consecutive days. In infected animals, the a- and b-waves of the electroretinographic (ERG) signal were significantly reduced as of 10 days post-inoculation when compared to control animals. Therapy with HPMPC 0.1mg/kg/day subcutaneously (s.c.) once daily for 5 consecutive days was able to delay the decrease in ERG wave amplitude and inhibit viral replication, whereas 5mg/kg/day s.c. significantly protected the ERG, completely inhibited viral replication, and maintained ocular viral titer below the limit of detection for up to 17 days post-infection. The reduction of ERG activity during progression of retinal disease correlated well with reduction of disease pathology. ERG recording represents a valuable non-invasive technique to measure the progression of the retinal disease induced by MCMV and the efficacy of antiviral treatment in the ocular MCMV disease model.

Published

2003

19. Esterification of cidofovir with alkoxyalkanols increases oral bioavailability and diminishes drug accumulation in kidney.

Author

Ciesla SL, Trahan J, Wan WB, Beadle JR, Aldern KA, Painter GR, and Hostetler KY

Subjects

Administration, Oral, Animals, Antiviral Agents administration & dosage, Carbon Radioisotopes pharmacokinetics, Cidofovir, Cytosine administration & dosage, Esterification, Esters chemistry, Female, Mice, Organophosphorus Compounds administration & dosage, Radiopharmaceuticals pharmacokinetics, Tissue Distribution, Antiviral Agents chemistry, Antiviral Agents pharmacokinetics, Biological Availability, Cytosine analogs & derivatives, Cytosine chemistry, Cytosine pharmacokinetics, Kidney chemistry, Organophosphonates, Organophosphorus Compounds chemistry, Organophosphorus Compounds pharmacokinetics

Abstract

Smallpox was eradicated by vaccination in the 1970s. However, concerns have arisen about the potential use of variola virus as a biological weapon. Most of the world's population has little residual immunity because systematic vaccination against smallpox ceased in the early 1970s. Vaccination of key elements of the population against smallpox is again being considered. However, there are now large numbers of persons who cannot be safely vaccinated with the current vaccine because of AIDS, immunosuppressive drugs, and certain common skin disorders. It would be useful to have a potent orally active drug as an alternative for these persons in case of an outbreak of smallpox. Alkoxyalkyl esters of cidofovir (CDV) have been shown to be highly active and selective against poxviruses in vitro with activities several logs greater than the activity of unmodified CDV. This is due in large part to increased cellular penetration and conversion to CDV-diphosphate, the active antiviral. In this paper, the oral pharmacokinetics of 14C-labeled hexadecyloxypropyl-cidofir (HDP-CDV), octadecyloxyethyl-cidofir (ODP-CDV), and oleyloxypropyl-cidofir (OLP-CDV) are examined and oral bioavailability and tissue distribution assessed and compared with parenteral CDV. The alkoxyalkyl CDVs are highly orally bioavailable and do not concentrate in kidney, the site of the dose-limiting toxicity of CDV. Plasma and tissue drug levels are many times greater than the in vitro EC(50s) for variola, cowpox, and vaccinia viruses. Thus, the compounds are good candidates for further development for prevention and treatment of smallpox infection and the complications of vaccination.

Published

2003

20. Treatment of aerosolized cowpox virus infection in mice with aerosolized cidofovir.

Author

Bray M, Martinez M, Kefauver D, West M, and Roy C

Subjects

Administration, Inhalation, Aerosols, Animals, Antiviral Agents administration & dosage, Body Weight, Bronchopneumonia drug therapy, Bronchopneumonia prevention & control, Bronchopneumonia virology, Cidofovir, Cowpox prevention & control, Cowpox virology, Cowpox virus metabolism, Cytosine administration & dosage, Cytosine analogs & derivatives, Female, Injections, Subcutaneous, Lung pathology, Lung virology, Mice, Mice, Inbred BALB C, Organ Size, Organophosphorus Compounds administration & dosage, Statistics, Nonparametric, Antiviral Agents pharmacology, Cowpox drug therapy, Cowpox virus growth & development, Cytosine pharmacology, Organophosphonates, Organophosphorus Compounds pharmacology

Abstract

The Brighton strain of cowpox virus causes lethal bronchopneumonia when delivered as a small-particle (1 microm) aerosol to weanling BALB/c mice. We showed previously that this disease can be prevented or cured with one subcutaneous injection of cidofovir (HPMPC, Vistide). To determine whether even better results could be obtained by delivering the drug directly to the respiratory tract, we administered cidofovir by small-particle aqueous aerosol before or after aerosolized cowpox infection. In a series of five experiments, aerosol doses of 0.5-5 mg/kg were always more effective than 25 mg/kg and sometimes more effective than 100 mg/kg injected subcutaneously, as measured by changes in body and lung weight, lung viral titers, pulmonary pathology and survival. A cyclic analog ((1-[(S)-2-hydroxy-2-oxo-1,4,2-dioxaphosphorinan-5-yl)methyl] cytosine) (cHPMPC) was less protective. The results suggest that aerosolized cidofovir would be effective for prophylaxis or early post-exposure therapy of human smallpox or monkeypox virus infection.

Published

2002

21. 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

22. 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

23. Topical effects of cidofovir on cutaneous rabbit warts: treatment regimen and inoculum dependence.

Author

Duan J, Paris W, De Marte J, Roopchand D, Fleet TL, and Cordingley MG

Subjects

Administration, Topical, Animals, Cidofovir, Cytosine administration & dosage, Disease Models, Animal, Drug Evaluation, Preclinical, Female, Rabbits, Time Factors, Warts pathology, Warts virology, Antiviral Agents administration & dosage, Cottontail rabbit papillomavirus drug effects, Cottontail rabbit papillomavirus isolation & purification, Cytosine analogs & derivatives, Organophosphonates, Organophosphorus Compounds administration & dosage, Warts drug therapy

Abstract

The present study examined topical effects of cidofovir on cutaneous rabbit warts. Based on an inoculum-dependency study, each New Zealand White rabbit was inoculated with a high and low titer of cottontail rabbit papillomavirus (CRPV) at four sites on each dorsolateral area. Inoculation with 50 ID(50) induced papillomas at 100% of the inoculation sites within 16+/-1 days, and the wart growth curve plateaued within approximately 7 weeks. With an inoculum of 5 ID(50), 80% of the inoculated sites developed papillomas within 21+/-1 days and their size plateaued at a later time. Cidofovir was applied topically twice daily on the inoculated sites at a concentration of 1% for 18 days, starting at three different time points. In the first experiment, treatment was initiated 7 days post-inoculation. One of the inoculated sides received cidofovir or the vehicle, PBS, while the other side was left untreated. With this treatment regimen, cidofovir significantly delayed the time of onset and the growth rate of papillomas induced with the high titer of inoculum. It completely prevented papilloma-induction on the sites inoculated with the low titer of CRPV. Reversible side-effects of cidofovir were observed on the directly treated area including erythema, necrosis, and flaking. Both therapeutic and side-effects were limited to the sites of direct exposure. In the second experiment, one of the two sides in each group of rabbits received cidofovir or vehicle starting on day 29 post-inoculation. With this treatment regimen, cidofovir significantly reduced wart growth against the low titer only. Topical treatment initiated on day 49 post-inoculation was not effective on warts initiated with either viral titer. These results demonstrated that topical cidofovir could be very effective against papillomavirus-induced wart growth if it is initiated early during the infection, especially against low titers of inoculum.

Published

2000

24. Evaluation of infrequent dosing regimens with (S)-1-[3-hydroxy-2-(phosphonylmethoxy)propyl]-cytosine (S-HPMPC) on simian varicella infection in monkeys.

Author

Soike KF, Huang JL, Zhang JY, Bohm R, Hitchcock MJ, and Martin JC

Subjects

Administration, Oral, Animals, Antibodies, Viral blood, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Chlorocebus aethiops, Cidofovir, Cytosine administration & dosage, Cytosine pharmacology, Cytosine therapeutic use, Herpesvirus 3, Human immunology, Injections, Intravenous, Organophosphorus Compounds pharmacology, Organophosphorus Compounds therapeutic use, Viremia drug therapy, Antiviral Agents administration & dosage, Chickenpox drug therapy, Cytosine analogs & derivatives, Herpesvirus 3, Human drug effects, Organophosphonates, Organophosphorus Compounds administration & dosage

Abstract

(S)-1-[3-Hydroxy-2-(phosphonylmethoxy)propyl]cytosine (S-HPMPC) was able to prevent simian varicella infection in African green monkeys inoculated intratracheally with virus. A dose of 50 mg/S-HPMPC/kg administered intravenously was shown to prevent the development of rash, reduce viremia and protect the monkeys from death. The 50 mg/kg dose was effective when treatments initiated on day 2 post-infection (p.i.) was given as ten daily doses of 5 mg/kg, as 10 mg/kg administered on five days on an alternate-day schedule, as two 25 mg/kg doses given on day 2 and on day 7 p.i., or as a single injection of 50 mg/kg on day 2. The single 50 mg/kg dose was also effective when treatment was delayed until four days p.i., but was ineffective when treatment was delayed until six days p.i. The 50 mg/kg dose was not effective when given orally by gavage. No evidence of toxicity was noted in daily clinical examinations, or in frequent hematology and clinical chemistry tests performed during the clinical evaluation of the infection.

Published

1991

25. Effects of phosphonylmethoxyalkyl-purine and -pyrimidine derivatives on TK+ and TK- HSV-1 keratitis in rabbits.

Author

Maudgal PC and De Clercq E

Subjects

Adenine administration & dosage, Adenine therapeutic use, Animals, Bromodeoxyuridine administration & dosage, Bromodeoxyuridine analogs & derivatives, Bromodeoxyuridine therapeutic use, Cidofovir, Cytosine administration & dosage, Cytosine therapeutic use, Hempa administration & dosage, Keratitis, Herpetic microbiology, Ophthalmic Solutions, Organophosphorus Compounds administration & dosage, Rabbits, Simplexvirus drug effects, Simplexvirus enzymology, Thymidine Kinase metabolism, Adenine analogs & derivatives, Antiviral Agents therapeutic use, Cytosine analogs & derivatives, Hempa therapeutic use, Keratitis, Herpetic drug therapy, Organophosphonates, Organophosphorus Compounds therapeutic use

Abstract

The phosphonylmethoxyalkyl derivatives HPMPA [(S)-9-(3-hydroxy-2-phosphonylmethoxypropyl)adenine], HPMPC [(S)-1-(3-hydroxy-2-phosphonylmethoxypropyl)cytosine] and PMEA [9-(2-phosphonylmethoxyethyl)adenine] were evaluated as 0.2% eyedrops for their efficacy in the treatment of experimental herpes simplex virus type 1 (HSV-1) keratitis in the rabbit model. BVDU 0.2% eyedrops were used as the reference treatment. HPMPA, HPMPC, PMEA and BVDU eyedrops showed a rapid and highly significant healing effect (P less than 0.005) on keratitis caused by TK+ HSV-1 (McIntyre strain) when compared with placebo eyedrops, whereas BVDU treatment did not affect the course of TK- HSV-1 (VMW-1837) keratitis. HPMPA and HPMPC treatment again caused a highly significant healing (P less than 0.005, compared with placebo eyedrops). Although PMEA eyedrops were less effective than HPMPA or HPMPC eyedrops, the effect of PMEA eyedrops was significantly (P less than 0.05) different from the effect of either BVDU or placebo eyedrops.

Published

1991