Your search keyword '"Naphthoquinones pharmacokinetics"' showing total 10 results

1. Artemisinin-naphthoquine combination therapy for uncomplicated pediatric malaria: a pharmacokinetic study.

Author

Batty KT, Salman S, Moore BR, Benjamin J, Lee ST, Page-Sharp M, Pitus N, Ilett KF, Mueller I, Hombhanje FW, Siba P, and Davis TM

Subjects

Antimalarials administration & dosage, Antimalarials blood, Artemisinins administration & dosage, Artemisinins blood, Biological Availability, Child, Chromatography, High Pressure Liquid, Chromatography, Liquid, Drug Administration Schedule, Female, Follow-Up Studies, Half-Life, Humans, Malaria, Falciparum blood, Malaria, Falciparum parasitology, Malaria, Vivax blood, Malaria, Vivax parasitology, Male, Mass Spectrometry, Naphthoquinones administration & dosage, Naphthoquinones blood, Papua New Guinea, Plasmodium falciparum physiology, Plasmodium vivax physiology, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Malaria, Falciparum drug therapy, Malaria, Vivax drug therapy, Naphthoquinones pharmacokinetics, Plasmodium falciparum drug effects, Plasmodium vivax drug effects

Abstract

Artemisinin-naphthoquine (ART-NQ) is a coformulated antimalarial therapy marketed as a single-dose treatment in Papua New Guinea and other tropical countries. To build on limited knowledge of the pharmacokinetic properties of the components, especially the tetra-aminoquinoline NQ, we studied ART-NQ disposition in Papua New Guinea children aged 5 to 12 years with uncomplicated malaria, comparing a single dose (15 and 6 mg/kg of body weight) administered with water (group 1; n = 13), a single dose (22 and 9 mg/kg) with milk (group 2) (n = 17), and two daily doses of 22 and 9 mg/kg with water (group 3; n = 16). The plasma NQ concentration was assayed by high-performance liquid chromatography, and the plasma ART concentration was assayed using liquid chromatography-mass spectrometry. Population-based multicompartment pharmacokinetic models for NQ and ART were developed. NQ disposition was best characterized by a three-compartment model with a mean absorption half-life (t(1/2)) of 1.0 h and predicted median maximum plasma concentrations that ranged as high as 57 μg/liter after the second dose in group 3. The mean NQ elimination t(1/2) was 22.8 days; clearance relative to bioavailability (CL/F) was 1.1 liters/h/kg; and volume at steady state relative to bioavailability (V(ss)/F) was 710 liters/kg. Administration of NQ with fat (8.5 g; 615 kJ) versus water was associated with 25% increased bioavailability. ART disposition was best characterized by a two-compartment model with a mean CL/F (4.1 liters/h/kg) and V/F (21 liters/kg) similar to those of previous studies. There was a 77% reduction in the bioavailability of the second ART dose (group 3). NQ has pharmacokinetic properties that confirm its potential as an artemisinin partner drug for treatment of uncomplicated pediatric malaria.

Published

2012

2. Lengthy antimalarial activity of atovaquone in human plasma following atovaquone-proguanil administration.

Author

Edstein MD, Kotecka BM, Anderson KL, Pombo DJ, Kyle DE, Rieckmann KH, and Good MF

Subjects

Animals, Antimalarials pharmacokinetics, Antimalarials pharmacology, Atovaquone, Biological Assay, Chromatography, High Pressure Liquid, Drug Therapy, Combination, Half-Life, Humans, Malaria, Falciparum drug therapy, Naphthoquinones pharmacokinetics, Naphthoquinones pharmacology, Plasmodium falciparum drug effects, Plasmodium falciparum genetics, Proguanil pharmacokinetics, Proguanil pharmacology, Antimalarials administration & dosage, Antimalarials blood, Naphthoquinones administration & dosage, Naphthoquinones blood, Proguanil administration & dosage

Published

2005

3. Atovaquone maintenance therapy prevents reactivation of toxoplasmic encephalitis in a murine model of reactivated toxoplasmosis.

Author

Dunay IR, Heimesaat MM, Bushrab FN, Müller RH, Stocker H, Arasteh K, Kurowski M, Fitzner R, Borner K, and Liesenfeld O

Subjects

Animals, Antiprotozoal Agents administration & dosage, Antiprotozoal Agents pharmacokinetics, Atovaquone, Brain pathology, Brain Chemistry drug effects, Chromatography, High Pressure Liquid, Female, Injections, Intravenous, Liver pathology, Lung pathology, Mass Spectrometry, Meninges pathology, Mice, Mice, Inbred C57BL, Naphthoquinones administration & dosage, Naphthoquinones pharmacokinetics, Pyrimethamine therapeutic use, Sulfadiazine therapeutic use, Survival Analysis, Toxoplasmosis, Cerebral pathology, Antiprotozoal Agents therapeutic use, Naphthoquinones therapeutic use, Toxoplasmosis, Cerebral drug therapy

Abstract

Acute therapy with pyrimethamine plus sulfadiazine is the treatment of choice for reactivated toxoplasmic encephalitis (TE). Acute therapy is followed by lifelong maintenance therapy (secondary prophylaxis) with the same drugs at lower dosages. The use of pyrimethamine plus sulfadiazine is hampered by severe side effects including allergic reactions and hematotoxicity. Alternative treatment regimens with pyrimethamine plus clindamycin or other antiparasitic drugs are less efficacious. Atovaquone nanosuspensions show excellent therapeutic effects for "acute" intravenous (i.v.) treatment of reactivated TE in a murine model. In the present study, the therapeutic efficacy of atovaquone for oral "maintenance" therapy was investigated. Mice with a targeted mutation in the interferon regulatory factor 8 gene were latently infected with Toxoplasma gondii, developed reactivated TE, and received acute i.v. therapy with atovaquone nanosuspensions. Mice were then treated orally with atovaquone suspension or other antiparasitic drugs to prevent relapse of TE. Maintenance therapy with atovaquone at daily doses of 50 or 100 mg/kg (body weight) protected mice against reactivated TE and death. This maintenance treatment was superior to standard therapy with pyrimethamine plus sulfadiazine. The latter combination was superior to the combination of pyrimethamine plus clindamycin. Inflammatory changes in the brain parenchyma and meninges, as well as parasite numbers, in the brains of mice confirmed the therapeutic efficacy of atovaquone for maintenance therapy. Atovaquone was detectable in sera, brains, livers, and lungs of infected mice by high-performance liquid chromatography and/or mass spectrometry. In conclusion, atovaquone appears to be superior to the standard maintenance therapy regimens in a murine model of reactivated TE. The therapeutic efficacy of atovaquone for maintenance therapy against TE should be further investigated in clinical trials.

Published

2004

4. Atovaquone nanosuspensions show excellent therapeutic effect in a new murine model of reactivated toxoplasmosis.

Author

Schöler N, Krause K, Kayser O, Müller RH, Borner K, Hahn H, and Liesenfeld O

Subjects

Animals, Antiprotozoal Agents pharmacokinetics, Atovaquone, Brain pathology, Chromatography, High Pressure Liquid, Injections, Intravenous, Macrophages, Peritoneal drug effects, Macrophages, Peritoneal parasitology, Male, Mice, Naphthoquinones pharmacokinetics, Sulfadiazine therapeutic use, Suspensions, Tissue Distribution, Toxoplasma drug effects, Antiprotozoal Agents therapeutic use, Naphthoquinones therapeutic use, Toxoplasmosis, Animal drug therapy

Abstract

Immunocompromised patients are at risk of developing toxoplasma encephalitis (TE). Standard therapy regimens (including sulfadiazine plus pyrimethamine) are hampered by severe side effects. While atovaquone has potent in vitro activity against Toxoplasma gondii, it is poorly absorbed after oral administration and shows poor therapeutic efficacy against TE. To overcome the low absorption of atovaquone, we prepared atovaquone nanosuspensions (ANSs) for intravenous (i.v.) administration. At concentrations higher than 1.0 microg/ml, ANS did not exert cytotoxicity and was as effective as free atovaquone (i.e., atovaquone suspended in medium) against T. gondii in freshly isolated peritoneal macrophages. In a new murine model of TE that closely mimics reactivated toxoplasmosis in immunocompromised hosts, using mice with a targeted mutation in the gene encoding the interferon consensus sequence binding protein, i.v.-administered ANS doses of 10.0 mg/kg of body weight protected the animals against development of TE and death. Atovaquone was detectable in the sera, brains, livers, and lungs of mice by high-performance liquid chromatography. Development of TE and mortality in mice treated with 1.0- or 0.1-mg/kg i.v. doses of ANS did not differ from that in mice treated orally with 100 mg of atovaquone/kg. In conclusion, i.v. ANSs may prove to be an effective treatment alternative for patients with TE.

Published

2001

5. Phase I safety and pharmacokinetics study of micronized atovaquone in human immunodeficiency virus-infected infants and children. Pediatric AIDS Clinical Trials Group.

Author

Hughes W, Dorenbaum A, Yogev R, Beauchamp B, Xu J, McNamara J, Moye J, Purdue L, van Dyke R, Rogers M, and Sadler B

Subjects

AIDS-Related Opportunistic Infections metabolism, AIDS-Related Opportunistic Infections microbiology, Antifungal Agents administration & dosage, Antifungal Agents pharmacokinetics, Atovaquone, Child, Child, Preschool, Humans, Infant, Naphthoquinones administration & dosage, Naphthoquinones pharmacokinetics, Pneumonia, Pneumocystis drug therapy, Pneumonia, Pneumocystis metabolism, AIDS-Related Opportunistic Infections drug therapy, Antifungal Agents adverse effects, Naphthoquinones adverse effects

Abstract

A phase I dose-escalating safety and pharmacokinetic study evaluated an oral suspension of micronized atovaquone (m-atovaquone) in infants and children stratified into age groups from 1 month to 12 years of age. Dosages of 10, 30, and 45 mg/kg of body weight/day were evaluated as single daily doses over a period of 12 days. Steady-state concentrations in plasma were determined on day 12, and single postdose concentrations were measured on days 1, 3, 5, 7, 9, 13, 15, 18, 21, and 24. Prior studies with adults suggest that the average plasma atovaquone concentration of 15 micrograms/ml is associated with therapeutic success in more than 95% of patients with Pneumocystis carinii pneumonitis. The results showed m-atovaquone to be safe and well tolerated. Dosages of 30 mg/kg/day were adequate to achieve an average steady-state concentration of greater than 15 micrograms/ml in children ages 1 to 3 months and 2 to 12 years, but a dosage of 45 mg/kg/day was needed to reach this concentration in infants 3 to 24 months of age. The oral suspension of atovaquone is safe and well tolerated in children. A single daily dose of 30 mg/kg provides bioavailability considered adequate for therapy of P. carinii pneumonia, but infants between 3 and 24 months of age may require a dosage of 45 mg/kg/day.

Published

1998

6. Disposition of atovaquone in humans.

Author

Rolan PE, Mercer AJ, Tate E, Benjamin I, and Posner J

Subjects

Adult, Atovaquone, Bile metabolism, Biliary Tract metabolism, Biliary Tract Surgical Procedures, Carbon Radioisotopes, Feces, Humans, Male, Middle Aged, Antiprotozoal Agents pharmacokinetics, Naphthoquinones pharmacokinetics

Abstract

Atovaquone is an antiprotozoal compound with good in vitro stability against metabolic inactivation. Previous human studies which did not involve radiolabelling had not accounted for a substantial proportion of the dose. The possible metabolism of atovaquone in men was examined in a radiolabelling study involving four healthy male volunteers. Radioactivity was eliminated almost exclusively via the feces. All radioactivity in plasma, urine, and feces was accounted for by atovaquone, with no evidence of metabolites. Radiolabelled atovaquone was administered to a patient with an indwelling biliary tube after surgery. Biliary radioactivity was approximately 10- to 40-fold higher than that in plasma and was accounted for by atovaquone. Atovaquone is not significantly metabolized in humans but is excreted into bile against a high concentration gradient.

Published

1997

7. In vitro and in vivo effects of rifabutin alone or combined with atovaquone against Toxoplasma gondii.

Author

Romand S, Della Bruna C, Farinotti R, and Derouin F

Subjects

Animals, Anti-Bacterial Agents pharmacokinetics, Anti-Bacterial Agents therapeutic use, Antiprotozoal Agents pharmacokinetics, Antiprotozoal Agents therapeutic use, Atovaquone, Brain parasitology, Drug Synergism, Enzyme-Linked Immunosorbent Assay, Female, Mice, Naphthoquinones pharmacokinetics, Naphthoquinones therapeutic use, Rifabutin pharmacokinetics, Rifabutin therapeutic use, Survival Analysis, Toxoplasmosis, Animal drug therapy, Toxoplasmosis, Animal parasitology, Anti-Bacterial Agents pharmacology, Antiprotozoal Agents pharmacology, Naphthoquinones pharmacology, Rifabutin pharmacology, Toxoplasma drug effects

Abstract

The efficacy of rifabutin (RIFA) alone or in combination with atovaquone (ATO) was examined in vitro and in a murine model of acute toxoplasmosis. In vitro studies were performed with MRC5 fibroblast tissue cultures, with quantification of Toxoplasma growth by enzyme-linked immunosorbent assay. For in vivo studies, mice were acutely infected with 10(4) tachyzoites of the virulent RH strain and were then treated perorally for 10 days from day 1 or day 4 postinfection. The efficacy of each drug regimen was assessed by determination of survival rates and sequential titration of parasites in blood, brain, and lungs by a tissue culture method. In vitro, RIFA was inhibitory for Toxoplasma growth at concentrations between 0.5 and 20 micrograms/ml; the 50% inhibitory concentration was estimated to be 1.68 micrograms/ml. When RIFA and ATO were combined, synergistic effects were noted for RIFA at 20 micrograms/ml combined with ATO at 0.01 or 0.02 microgram/ml and RIFA at 1, 2, or 5 micrograms/ml combined with ATO at 0.02 microgram/ml. In vivo, administration of RIFA at 200 mg/kg of body weight per day from day 1 to day 10 resulted in a 100% protection during treatment, with clearance of parasites from the blood, brain, and lungs. After the cessation of therapy, relapses occurred in the brain and lungs; the mortality was 46% at the end of the experiment (day 30). Among the mice treated with RIFA at 200 mg/kg/day from day 4 to day 14, no death was recorded during the treatment period and a marked reduction in parasite burdens was observed in blood and tissues; however, relapses occurred and 10% of mice survived until day 30. Administration of RIFA at 200 mg/kg/day in combination with ATO at 100 mg/kg/day resulted in a marked prolongation of survival compared with that for mice that received ATO or RIFA alone. However, in mice receiving the combination, parasite burdens in blood and organs were similar to those in mice treated with RIFA alone. These results confirmed the activity of RIFA in the treatment of acute toxoplasmosis and the potential of the combination of RIFA-ATO since the two drugs act synergistically against Toxoplasma gondii.

Published

1996

8. Single-dose and steady-state pharmacokinetics of a novel microfluidized suspension of atovaquone in human immunodeficiency virus-seropositive patients.

Author

Dixon R, Pozniak AL, Watt HM, Rolan P, and Posner J

Subjects

Adult, Antifungal Agents administration & dosage, Antifungal Agents adverse effects, Atovaquone, Biological Availability, Food-Drug Interactions, Humans, Male, Naphthoquinones administration & dosage, Naphthoquinones adverse effects, Suspensions, Antifungal Agents pharmacokinetics, HIV Seropositivity metabolism, Naphthoquinones pharmacokinetics

Abstract

The single- and multiple-dose pharmacokinetics of and tolerability to a new microfluidized suspension of atovaquone were studied in human immunodeficiency virus-seropositive patients with CD4 counts of < or = 200 cells per mm3 in order to define a dosing regimen for the treatment of Pneumocystis carinii pneumonia. This was an open study with groups of six patients each. In the first part of the study, six subjects received escalating single doses of 500, 1,000, and 1,500 mg after an overnight fast at weekly intervals. In the second part of the study, groups of six subjects were dosed for 14 days according to three regimens: 1,000 mg twice daily fasting, twice daily with a high-fat meal, or once daily with a high-fat meal. Plasma atovaquone levels were assayed by high-performance liquid chromatography. Pharmacokinetic parameters were determined by noncompartmental methods, and statistical comparison of parameters for single doses was performed by analysis of variance. Plasma drug concentrations increased with single doses from 500 to 1,000 mg but were no higher with a dose of 1,500 mg. Thus, 1,000 mg was selected for multiple administration. A regimen of 1,000 mg twice daily with food resulted in a 93% increase in the average trough steady-state concentration compared with 1,000 mg once daily with food. Food increased the bioavailability of atovaquone 1.4-fold over that in the fasting state. All patients who received 1,000 mg twice daily with food achieved target steady-state concentrations in plasma of 15 to 25 micrograms/ml. Multiple-dose regimens were generally well tolerated, but the higher levels in plasma achieved by 1,000 mg twice daily with food were associated with an increased incidence of rash. In conclusion, target plasma atovaquone concentrations for the treatment of P. carinii pneumonia can be achieved in most patients with 1,000 mg twice daily in a fasting state and in all patients with 1,000 mg twice daily administered with food, but at higher concentrations in plasma, there may be an increased risk of rash.

Published

1996

9. Antipneumocystis activity of 17C91, a prodrug of atovaquone.

Author

Comley JC, Yeates CL, and Frend TJ

Subjects

Animals, Atovaquone, Female, Mice, Mice, SCID, Naphthoquinones pharmacokinetics, Antifungal Agents therapeutic use, Carbamates pharmacology, Naphthoquinones pharmacology, Naphthoquinones therapeutic use, Pneumonia, Pneumocystis prevention & control, Prodrugs therapeutic use

Abstract

The prophylactic efficacy of 17C91, a carbamate prodrug of atovaquone (ATQ), was investigated in a severe combined immunodeficient mouse model of Pneumocystis carinii pneumonia (PCP). At an oral dosage equivalent to 100 mg of ATQ per kg of body weight per day, 17C91 protected 9 of 10 mice from PCP and had a prophylactic efficacy comparable to that of co-trimoxazole (at 250 mg of sulfamethoxazole plus 50 mg of trimethoprim per kg per day orally). The intensity of P. carinii infection (infection score) of mice treated with 17C91 correlated with the concentration of ATQ in the plasma, with clearance of the infection associated with plasma ATQ levels of >35 micrograms/ml. 17C91 given orally provided enhanced levels of ATQ in the plasma compared with the conventional ATQ formulation. Additional studies reported in this paper demonstrate that the prophylactic activity of 17C91 against PCP in severe combined immunodeficient mice is comparable to that of a new oral microparticulate formulation of ATQ.

Published

1995

10. Efficacy of a hydroxynaphthoquinone, 566C80, in experimental Pneumocystis carinii pneumonitis.

Author

Hughes WT, Gray VL, Gutteridge WE, Latter VS, and Pudney M

Subjects

Animals, Anti-Infective Agents pharmacokinetics, Atovaquone, Dexamethasone therapeutic use, Lung pathology, Male, Naphthoquinones pharmacokinetics, Pneumonia, Pneumocystis microbiology, Pneumonia, Pneumocystis pathology, Rats, Rats, Inbred Strains, Tetracyclines therapeutic use, Trimethoprim, Sulfamethoxazole Drug Combination therapeutic use, Anti-Infective Agents therapeutic use, Naphthoquinones therapeutic use, Pneumonia, Pneumocystis drug therapy

Abstract

The efficacy of a new class of drugs for Pneumocystis carinii pneumonitis was demonstrated. 566C80, a hydroxynaphthoquinone, administered orally in a dose of greater than or equal to 100 mg/kg of body weight per day prophylactically prevented P. carinii pneumonitis in 90% or more of rats, while all untreated control animals developed pneumonitis. When 566C80 (100 mg/kg per day) was administered for 3 weeks after P. carinii pneumonitis was established, therapy was totally effective and all of the untreated controls had progressive P. carinii pneumonitis. A dose of 566C80 of between 25 and 50 mg/kg per day protected 50% of the rats from P. carinii pneumonitis, and a dose of between 50 and 100 mg/kg per day cured 50% of those treated for P. carinii pneumonitis. Both prophylaxis and treatment with 566C80 were at least as effective as with trimethoprim-sulfamethoxazole. Animals maintained on immunosuppression after completion of treatment remained free of P. carinii, suggesting a killing effect. Clearance of P. carinii was associated with levels of 60 micrograms or more of 566C80 per ml of plasma. This hydroxynaphthoquinone offers promise as an anti-P. carinii drug.

Published

1990