Your search keyword '"Quinolines pharmacokinetics"' showing total 80 results

1. Pharmacokinetics and safety of TBAJ-876, a novel antimycobacterial diarylquinoline, in healthy subjects.

Author

Lombardi A, Pappas F, Nedelman J, Hickman D, Jaw-Tsai S, Olugbosi M, Bruinenberg P, Beumont M, and Sun E

Subjects

Humans, Adult, Male, Female, Middle Aged, Young Adult, Drug Interactions, Healthy Volunteers, Adolescent, Cytochrome P-450 CYP3A metabolism, Biological Availability, Quinolines pharmacokinetics, Administration, Oral, Diarylquinolines pharmacokinetics, Diarylquinolines pharmacology, Antitubercular Agents pharmacokinetics, Antitubercular Agents adverse effects, Antitubercular Agents pharmacology

Abstract

TBAJ-876, a second-generation diarylquinoline with greater antimycobacterial activity and a potentially better safety profile compared with bedaquiline, is under development for the treatment of drug-susceptible and drug-resistant tuberculosis (TB). A phase 1, first-in-human study of TBAJ-876, comprising a single-ascending dose (SAD) part including a food effect cohort, a multiple-ascending dose (MAD) part, and a relative bioavailability part of tablets versus oral suspension, was conducted on 137 healthy adults. A drug-drug interaction study was conducted on 28 healthy adults to evaluate the effects of TBAJ-876 on a cytochrome P450 3A4 substrate (midazolam) and a P-glycoprotein substrate (digoxin). TBAJ-876 was well-tolerated at single doses up to 800 mg and multiple doses up to 200 mg for 14 days. No deaths or serious adverse events occurred. No episodes of clinically significant prolongation of the QTc interval were observed. TBAJ-876 exposures were dose proportional in the SAD and MAD studies. TBAJ-876 exhibited multicompartmental pharmacokinetics (PK) with a long terminal half-life yielding quantifiable concentrations up to the longest follow-up of 10 weeks after a single dose and resulting in accumulation with multiple dosing. In the fed state, TBAJ-876 exposures approximately doubled with the tablet formulation, whereas M3 metabolite exposures decreased by approximately 20%. The relative bioavailability of TBAJ-876 was similar between tablets and the oral suspension at 100-mg doses. With co-administration of TBAJ-876, the AUC 0-inf of midazolam was unchanged and the C max was reduced by 14%; the AUC 0-last of digoxin was increased by 51%, and the C max was increased by 18%. These results support further investigation of TBAJ-876 for the treatment of tuberculosis., Competing Interests: The authors declare no conflict of interest.

Published

2024

2. Comparison of lumefantrine, mefloquine, and piperaquine concentrations between capillary plasma and venous plasma samples in pregnant women with uncomplicated falciparum and vivax malaria.

Author

Saito M, Wilaisrisak P, Pimanpanarak M, Viladpai-Nguen J, Paw MK, Koesukwiwat U, Tarning J, White NJ, Nosten F, and McGready R

Subjects

Humans, Female, Pregnancy, Adult, Young Adult, Ethanolamines blood, Ethanolamines pharmacokinetics, Ethanolamines therapeutic use, Fluorenes blood, Fluorenes therapeutic use, Fluorenes pharmacokinetics, Adolescent, Mefloquine blood, Mefloquine therapeutic use, Mefloquine pharmacokinetics, Antimalarials blood, Antimalarials therapeutic use, Antimalarials pharmacokinetics, Quinolines blood, Quinolines pharmacokinetics, Quinolines therapeutic use, Lumefantrine therapeutic use, Lumefantrine blood, Malaria, Falciparum drug therapy, Malaria, Falciparum blood, Malaria, Vivax drug therapy, Malaria, Vivax blood, Piperazines

Abstract

Capillary samples offer practical benefits compared with venous samples for the measurement of drug concentrations, but the relationship between the two measures varies between different drugs. We measured the concentrations of lumefantrine, mefloquine, piperaquine in 270 pairs of venous plasma and concurrent capillary plasma samples collected from 270 pregnant women with uncomplicated falciparum or vivax malaria. The median and range of venous plasma concentrations included in this study were 447.5 ng/mL (8.81-3,370) for lumefantrine (day 7, n = 76, median total dose received 96.0 mg/kg), 17.9 ng/mL (1.72-181) for desbutyl-lumefantrine, 1,885 ng/mL (762-4,830) for mefloquine (days 3-21, n = 90, median total dose 24.9 mg/kg), 641 ng/mL (79.9-1,950) for carboxy-mefloquine, and 51.8 ng/mL (3.57-851) for piperaquine (days 3-21, n = 89, median total dose 52.2 mg/kg). Although venous and capillary plasma concentrations showed a high correlation (Pearson's correlation coefficient: 0.90-0.99) for all antimalarials and their primary metabolites, they were not directly interchangeable. Using the concurrent capillary plasma concentrations and other variables, the proportions of venous plasma samples predicted within a ±10% precision range was 34% (26/76) for lumefantrine, 36% (32/89) for desbutyl-lumefantrine, 74% (67/90) for mefloquine, 82% (74/90) for carboxy-mefloquine, and 24% (21/89) for piperaquine. Venous plasma concentrations of mefloquine, but not lumefantrine and piperaquine, could be predicted by capillary plasma samples with an acceptable level of agreement. Capillary plasma samples can be utilized for pharmacokinetic and clinical studies, but caution surrounding cut-off values is required at the individual level.CLINICAL TRIALSThis study is registered with ClinicalTrials.gov as NCT01054248., Competing Interests: The authors declare no conflict of interest.

Published

2024

3. Efavirenz-Based Antiretroviral Therapy but Not Pregnancy Increased Unbound Piperaquine Exposure in Women during Malaria Chemoprevention.

Author

Hong H, Aslam-Mir U, Kajubi R, Wallender E, Mwebaza N, Dorsey G, Rosenthal PJ, Aweeka FT, and Huang L

Subjects

Adult, Pregnancy, Humans, Female, Chemoprevention methods, Antimalarials pharmacokinetics, Malaria drug therapy, Malaria prevention & control, Quinolines pharmacokinetics, HIV Infections drug therapy, HIV Infections prevention & control

Abstract

Dihydroartemisinin-piperaquine (DP) is highly effective for malaria chemoprevention during pregnancy, but the standard dosing of DP that is used for nonpregnant adults may not be optimal for pregnant women. We previously reported that the pharmacokinetic exposure of total piperaquine (PQ; both bound and unbound to plasma proteins) is reduced significantly in the context of pregnancy or efavirenz (EFV)-based antiretroviral therapy (ART). However, as PQ is >99% protein-bound, reduced protein binding during pregnancy may lead to an increase in the pharmacologically active unbound drug fraction (f u ), relative to the total PQ. We investigated the impact of pregnancy and EFV use on the f u of PQ to inform the interpretation of pharmacokinetics. Plasma samples from 0 to 24 h after the third (final) DP dose were collected from pregnant women at 28 weeks gestation who were receiving or not receiving EFV-based ART as well as from women 34 to 54 weeks postpartum who were not receiving EFV-based ART, who served as controls. Unbound PQ was quantified via ultrafiltration and liquid chromatography-tandem mass spectrometry, with f u being calculated as PQ unbound /PQ total . The geometric mean f u did not differ between pregnant and postpartum women ( P = 0.66), but it was 23% ( P < 0.01) greater in pregnant women receiving EFV-based ART, compared to that in postpartum women who were not receiving EFV-based ART. The altered drug-protein binding, potentially due to the displacement of PQ from plasma proteins by EFV, resulted in only a 14% lower unbound PQ exposure ( P = 0.13) in the presence of a 31% lower total PQ exposure ( P < 0.01), as estimated by the area under the concentration time curve from 0 to 24 h post-last dose in pregnant women who were receiving EFV-based ART. The results suggest that the impact of pregnancy and EFV-based ART on the exposure and, in turn, the efficacy of PQ for malaria prevention may not be as significant as was suggested by the changes in the total PQ exposure. Further study during the terminal elimination phase (e.g., on day 28 post-dose) would help better characterize the unbound PQ exposure during the full dosing interval and, thus, the overall efficacy of PQ for malaria chemoprevention in this special population.

Published

2023

4. Piperaquine Pharmacokinetic and Pharmacodynamic Profiles in Healthy Volunteers of Papua New Guinea after Administration of Three-Monthly Doses of Dihydroartemisinin-Piperaquine.

Author

Millat-Martínez P, Salman S, Moore BR, Baro B, Page-Sharp M, Batty KT, Robinson LJ, Pomat W, Karunajeewa H, Laman M, Manning L, Mitjà O, and Bassat Q

Subjects

Adult, Artemisinins adverse effects, Artemisinins pharmacokinetics, Artemisinins pharmacology, Female, Healthy Volunteers, Humans, Long QT Syndrome chemically induced, Longitudinal Studies, Male, Papua New Guinea, Antimalarials adverse effects, Antimalarials pharmacokinetics, Antimalarials pharmacology, Malaria, Falciparum drug therapy, Piperazines adverse effects, Piperazines pharmacokinetics, Piperazines pharmacology, Quinolines adverse effects, Quinolines pharmacokinetics, Quinolines pharmacology

Abstract

Mass drug administration (MDA) with monthly dihydroartemisinin-piperaquine (DHA-PQP) appears useful in malaria control and elimination strategies. Determining the relationship between consecutive piperaquine phosphate (PQP) exposure and its impact on QT interval prolongation is a key safety consideration for MDA campaigns. Healthy volunteers from Papua New Guinea received a 3-day course of DHA-PQP (2.1/17.1 mg/kg) monthly for 3 consecutive months in a single arm longitudinal study. Plasma PQP concentrations were measured after the third dose of each course (at 52-54 h) and at 0 h of course 3. Twelve-lead electrocardiographic readings were conducted at 0 h, 48 h, 52 h, and day 7 of each course. QT interval corrected by Fridericia's formula (QTcF) was measured at each time point. A pharmacokinetic-pharmacodynamic model using nonlinear mixed effects models was developed to correlate PQP concentrations with QTcF. Ten thousand female and 10,000 male individuals were simulated at each treatment course. Eighty-two participants were included; mean age was 28.3 years (standard deviation [SD] ±12.3 years), and 36 (44%) were female. Pharmacokinetic-pharmacodynamic models were determined with 290 PQP concentrations and 868 QTcF observations. The average baseline QTcF was 392 ms with a between-subject variability SD ±14.4 ms and between-occasion variability SD ±3.64 ms. From the population modeled, only 0.08% of males and 0.45% of females would be at risk of an absolute QTcF of >500 ms. DHA-PQP is safe at standard doses in consecutive months, and the likelihood of severe cardiac events occurring during an MDA campaign is very low. This study has been registered at ClinicalTrials.gov under identifier NCT02605720.

Published

2022

5. Piperaquine Exposure Is Altered by Pregnancy, HIV, and Nutritional Status in Ugandan Women.

Author

Hughes E, Imperial M, Wallender E, Kajubi R, Huang L, Jagannathan P, Zhang N, Kakuru A, Natureeba P, Mwima MW, Muhindo M, Mwebaza N, Clark TD, Opira B, Nakalembe M, Havlir D, Kamya M, Rosenthal PJ, Dorsey G, Aweeka F, and Savic RM

Subjects

Drug Combinations, Female, Humans, Molecular Diagnostic Techniques, Nucleic Acid Amplification Techniques, Nutritional Status, Pregnancy, Uganda, Antimalarials pharmacokinetics, Antimalarials therapeutic use, HIV Infections drug therapy, HIV Infections prevention & control, Quinolines pharmacokinetics, Quinolines therapeutic use

Abstract

Dihydroartemisinin-piperaquine (DHA-PQ) provides highly effective therapy and chemoprevention for malaria in pregnant African women. PQ concentrations of >10.3 ng/ml have been associated with reduced maternal parasitemia, placental malaria, and improved birth outcomes. We characterized the population pharmacokinetics (PK) of PQ in a post hoc analysis of human immunodeficiency virus (HIV)-infected and -uninfected pregnant women receiving DHA-PQ as chemoprevention every 4 or 8 weeks. The effects of covariates such as pregnancy, nutritional status (body mass index [BMI]), and efavirenz (EFV)-based antiretroviral therapy were investigated. PQ concentrations from two chemoprevention trials were pooled to create a population PK database from 274 women and 2,218 PK observations. A three-compartment model with an absorption lag best fit the data. Consistent with our prior intensive PK evaluation, pregnancy and EFV use resulted in a 72% and 61% increased PQ clearance, compared to postpartum and HIV-uninfected pregnant women, respectively. Low BMI at 28 weeks of gestation was associated with increased clearance (2% increase per unit decrease in BMI). Low-BMI women given DHA-PQ every 8 weeks had a higher prevalence of parasitemia, malaria infection, and placental malaria compared to women with higher BMIs. The reduced piperaquine exposure in women with low BMI as well as during EFV coadministration, compared to pregnant women with higher BMIs and not taking EFV, suggests that these populations could benefit from weekly instead of monthly dosing for prevention of malaria parasitemia. Simulations indicated that because of the BMI-clearance relationship, weight-based regimens would not improve protection compared to a 2,880 mg fixed-dose regimen when provided monthly. (The clinical trials described in this paper have been registered at ClinicalTrials.gov under identifiers NCT02163447 and NCT02282293.)., (Copyright © 2020 American Society for Microbiology.)

Published

2020

6. Preclinical Antimalarial Combination Study of M5717, a Plasmodium falciparum Elongation Factor 2 Inhibitor, and Pyronaridine, a Hemozoin Formation Inhibitor.

Author

Rottmann M, Jonat B, Gumpp C, Dhingra SK, Giddins MJ, Yin X, Badolo L, Greco B, Fidock DA, Oeuvray C, and Spangenberg T

Subjects

Animals, Antimalarials pharmacokinetics, Drug Resistance physiology, Drug Therapy, Combination, Hemeproteins antagonists & inhibitors, Malaria, Falciparum prevention & control, Mice, Mice, SCID, Naphthyridines pharmacokinetics, Peptide Elongation Factor 2 antagonists & inhibitors, Quinolines chemistry, Quinolines pharmacokinetics, Antimalarials pharmacology, Malaria, Falciparum drug therapy, Naphthyridines pharmacology, Plasmodium falciparum drug effects, Quinolines pharmacology

Abstract

Antimalarial drug resistance in the Plasmodium falciparum parasite poses a constant challenge for drug development. To mitigate this risk, new antimalarial medicines should be developed as fixed-dose combinations. Assessing the pharmacodynamic interactions of potential antimalarial drug combination partners during early phases of development is essential in developing the targeted parasitological and clinical profile of the final drug product. Here, we have studied the combination of M5717, a P. falciparum translation elongation factor 2 inhibitor, and pyronaridine, an inhibitor of hemozoin formation. Our test cascade consisted of in vitro isobolograms as well as in vivo studies in the P. falciparum severe combined immunodeficient (SCID) mouse model. We also analyzed pharmacokinetic and pharmacodynamic parameters, including genomic sequencing of recrudescent parasites. We observed no pharmacokinetic interactions with the combination of M5717 and pyronaridine. M5717 did not negatively impact the rate of kill of the faster-acting pyronaridine, and the latter was able to suppress the selection of M5717-resistant mutants, as well as significantly delay the recrudescence of parasites both with suboptimal and optimal dosing regimens., (Copyright © 2020 Rottmann et al.)

Published

2020

7. Improving Methods for Analyzing Antimalarial Drug Efficacy Trials: Molecular Correction Based on Length-Polymorphic Markers msp-1 , msp-2 , and glurp .

Author

Jones S, Kay K, Hodel EM, Chy S, Mbituyumuremyi A, Uwimana A, Menard D, Felger I, and Hastings I

Subjects

Algorithms, Antigens, Protozoan metabolism, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Artemisinins pharmacology, Biomarkers metabolism, Clinical Trials as Topic, Gene Expression, Humans, Lumefantrine pharmacokinetics, Lumefantrine pharmacology, Malaria, Falciparum drug therapy, Malaria, Falciparum parasitology, Mefloquine pharmacokinetics, Mefloquine pharmacology, Merozoite Surface Protein 1 metabolism, Parasitic Sensitivity Tests, Plasmodium falciparum genetics, Plasmodium falciparum growth & development, Polymorphism, Restriction Fragment Length, Protozoan Proteins metabolism, Quinolines pharmacokinetics, Quinolines pharmacology, Time Factors, Treatment Outcome, Antigens, Protozoan genetics, Antimalarials pharmacology, Merozoite Surface Protein 1 genetics, Models, Statistical, Plasmodium falciparum drug effects, Protozoan Proteins genetics

Abstract

Drug efficacy trials monitor the continued efficacy of front-line drugs against falciparum malaria. Overestimating efficacy results in a country retaining a failing drug as first-line treatment with associated increases in morbidity and mortality, while underestimating drug effectiveness leads to removal of an effective treatment with substantial practical and economic implications. Trials are challenging: they require long durations of follow-up to detect drug failures, and patients are frequently reinfected during that period. Molecular correction based on parasite genotypes distinguishes reinfections from drug failures to ensure the accuracy of failure rate estimates. Several molecular correction "algorithms" have been proposed, but which is most accurate and/or robust remains unknown. We used pharmacological modeling to simulate parasite dynamics and genetic signals that occur in patients enrolled in malaria drug clinical trials. We compared estimates of treatment failure obtained from a selection of proposed molecular correction algorithms against the known "true" failure rate in the model. Our findings are as follows. (i) Molecular correction is essential to avoid substantial overestimates of drug failure rates. (ii) The current WHO-recommended algorithm consistently underestimates the true failure rate. (iii) Newly proposed algorithms produce more accurate failure rate estimates; the most accurate algorithm depends on the choice of drug, trial follow-up length, and transmission intensity. (iv) Long durations of patient follow-up may be counterproductive; large numbers of new infections accumulate and may be misclassified, overestimating drug failure rate. (v) Our model was highly consistent with existing in vivo data. The current WHO-recommended method for molecular correction and analysis of clinical trials should be reevaluated and updated., (Copyright © 2019 Jones et al.)

Published

2019

8. Sequential Open-Label Study of the Safety, Tolerability, and Pharmacokinetic Interactions between Dihydroartemisinin-Piperaquine and Mefloquine in Healthy Thai Adults.

Author

Hanboonkunupakarn B, van der Pluijm RW, Hoglund R, Pukrittayakamee S, Winterberg M, Mukaka M, Waithira N, Chotivanich K, Singhasivanon P, White NJ, Dondorp AM, Tarning J, and Jittamala P

Subjects

Adult, Antimalarials adverse effects, Artemisinins adverse effects, Cardiotoxicity etiology, Dizziness chemically induced, Female, Healthy Volunteers, Humans, Male, Mefloquine adverse effects, Middle Aged, Nausea chemically induced, Quinolines adverse effects, Thailand, Antimalarials pharmacology, Artemisinins pharmacokinetics, Mefloquine pharmacokinetics, Quinolines pharmacokinetics

Abstract

Artemisinin-based combination therapies (ACTs) have contributed substantially to the global decline in Plasmodium falciparum morbidity and mortality, but resistance to artemisinins and their partner drugs is increasing in Southeast Asia, threatening malaria control. New antimalarial compounds will not be generally available soon. Combining three existing antimalarials in the form of triple ACTs, including dihydroartemisinin (DHA)-piperaquine + mefloquine, is a potential treatment option for multidrug-resistant Plasmodium falciparum malaria. In a sequential open-label study, healthy Thai volunteers were treated with DHA-piperaquine (120 to 960 mg), mefloquine (500 mg), and DHA-piperaquine + mefloquine (120 to 960 mg + 500 mg), and serial symptom questionnaires, biochemistry, full blood counts, pharmacokinetic profiles, and electrocardiographic measurements were performed. Fifteen healthy subjects were enrolled. There was no difference in the incidence or severity of adverse events between the three treatment arms. The slight prolongation in QTc (QT interval corrected for heart rate) associated with DHA-piperaquine administration did not increase after administration of DHA-piperaquine + mefloquine. The addition of mefloquine had no significant effect on the pharmacokinetic properties of piperaquine. However, coadministration of mefloquine significantly reduced the exposures to dihydroartemisinin for area under the concentration-time curve (-22.6%; 90% confidence interval [CI], -33.1, -10.4; P  = 0.0039) and maximum concentration of drug in serum (-29.0%; 90% CI, -40.6, -15.1; P  = 0.0079). Mefloquine can be added safely to dihydroartemisinin-piperaquine in malaria treatment. (This study has been registered at ClinicalTrials.gov under identifier NCT02324738.)., (Copyright © 2019 Hanboonkunupakarn et al.)

Published

2019

9. Modeling Prevention of Malaria and Selection of Drug Resistance with Different Dosing Schedules of Dihydroartemisinin-Piperaquine Preventive Therapy during Pregnancy in Uganda.

Author

Wallender E, Zhang N, Conrad M, Kakuru A, Muhindo M, Tumwebaze P, Kajubi R, Mota D, Legac J, Jagannathan P, Havlir D, Kamya M, Dorsey G, Aweeka F, Rosenthal PJ, and Savic RM

Subjects

Artemisinins pharmacokinetics, Drug Resistance physiology, Drug Therapy, Combination, Female, Humans, Malaria drug therapy, Pregnancy, Pregnancy Complications, Parasitic drug therapy, Quinolines pharmacokinetics, Uganda, Young Adult, Antimalarials pharmacokinetics, Antimalarials therapeutic use, Artemisinins therapeutic use, Malaria prevention & control, Pregnancy Complications, Parasitic prevention & control, Quinolines therapeutic use

Abstract

Dihydroartemisinin-piperaquine (DHA-PQ) is under study for intermittent preventive treatment during pregnancy (IPTp), but it may accelerate selection for drug resistance. Understanding the relationships between piperaquine concentration, prevention of parasitemia, and selection for decreased drug sensitivity can inform control policies and optimization of DHA-PQ dosing. Piperaquine concentrations, measures of parasitemia, and Plasmodium falciparum genotypes associated with decreased aminoquinoline sensitivity in Africa ( pfmdr1 86Y, pfcrt 76T) were obtained from pregnant Ugandan women randomized to IPTp with sulfadoxine-pyrimethamine (SP) or DHA-PQ. Joint pharmacokinetic/pharmacodynamic models described relationships between piperaquine concentration and the probability of genotypes of interest using nonlinear mixed effects modeling. An increase in the piperaquine plasma concentration was associated with a log-linear decrease in risk of parasitemia. Our models predicted that higher median piperaquine concentrations would be required to provide 99% protection against mutant infections than against wild-type infections ( pfmdr1 : N86, 9.6 ng/ml; 86Y, 19.6 ng/ml; pfcrt : K76, 6.5 ng/ml; 76T, 19.6 ng/ml). Comparing monthly, weekly, and daily dosing, daily low-dose DHA-PQ was predicted to result in the fewest infections and the fewest mutant infections per 1,000 pregnancies (predicted mutant infections for pfmdr1 86Y: SP monthly, 607; DHA-PQ monthly, 198; DHA-PQ daily, 1; for pfcrt 76T: SP monthly, 1,564; DHA-PQ monthly, 283; DHA-PQ daily, 1). Our models predict that higher piperaquine concentrations are needed to prevent infections with the pfmdr1/pfcrt mutant compared to those with wild-type parasites and that, despite selection for mutants by DHA-PQ, the overall burden of mutant infections is lower for IPTp with DHA-PQ than for IPTp with SP. (This study has been registered at ClinicalTrials.gov under identifier NCT02282293.)., (Copyright © 2019 American Society for Microbiology.)

Published

2019

10. Metabolism of Piperaquine to Its Antiplasmodial Metabolites and Their Pharmacokinetic Profiles in Healthy Volunteers.

Author

Liu H, Zhou H, Cai T, Yang A, Zang M, and Xing J

Subjects

Animals, Antimalarials blood, Antimalarials pharmacology, Artemisinins pharmacology, Biotransformation, Drug Administration Schedule, Drug Dosage Calculations, Drug Therapy, Combination, Half-Life, Healthy Volunteers, Humans, Malaria metabolism, Malaria mortality, Malaria parasitology, Male, Mice, Mice, Inbred ICR, Oxides blood, Plasmodium falciparum growth & development, Plasmodium falciparum pathogenicity, Plasmodium yoelii growth & development, Plasmodium yoelii pathogenicity, Quinolines blood, Quinolines pharmacology, Rats, Wistar, Recurrence, Survival Analysis, Young Adult, Antimalarials pharmacokinetics, Malaria drug therapy, Plasmodium falciparum drug effects, Plasmodium yoelii drug effects, Quinolines pharmacokinetics

Abstract

As a partner antimalarial for artemisinin drug-based combination therapy (ACT), piperaquine (PQ) can be metabolized into two major metabolites, including piperaquine N -oxide (M1) and piperaquine N , N -dioxide (M2). To better understand the antimalarial potency of PQ, the antimalarial activity of the PQ metabolites (M1 and M2) was studied in vitro (in Plasmodium falciparum strains Pf 3D7 and Pf Dd2) and in vivo (in the murine species Plasmodium yoelii ) in this study. The recrudescence and survival time of infected mice were also recorded after drug treatment. The pharmacokinetic profiles of PQ and its two metabolites (M1 and M2) were investigated in healthy subjects after oral doses of two widely used ACT regimens, i.e., dihydroartemisinin plus piperaquine phosphate (Duo-Cotecxin) and artemisinin plus piperaquine (Artequick). Remarkable antiplasmodial activity was found for PQ (50% growth-inhibitory concentration [IC 50 ], 4.5 nM against Pf 3D7 and 6.9 nM against Pf Dd2; 90% effective dose [ED 90 ], 1.3 mg/kg of body weight), M1 (IC 50 , 25.5 nM against Pf 3D7 and 38.7 nM against Pf Dd2; ED 90 , 1.3 mg/kg), and M2 (IC 50 , 31.2 nM against Pf 3D7 and 33.8 nM against Pf Dd2; ED 90 , 2.9 mg/kg). Compared with PQ, M1 showed comparable efficacy in terms of recrudescence and survival time and M2 had relatively weaker antimalarial potency. PQ and its two metabolites displayed a long elimination half-life (∼11 days for PQ, ∼9 days for M1, and ∼4 days for M2), and they accumulated after repeated administrations. The contribution of the two PQ metabolites to the efficacy of piperaquine as a partner drug of ACT for the treatment of malaria should be considered for PQ dose optimization., (Copyright © 2018 American Society for Microbiology.)

Published

2018

11. Efficacy and Tolerability Outcomes of a Phase II, Randomized, Open-Label, Multicenter Study of a New Water-Dispersible Pediatric Formulation of Dihydroartemisinin-Piperaquine for the Treatment of Uncomplicated Plasmodium falciparum Malaria in African Infants.

Author

Gargano N, Madrid L, Valentini G, D'Alessandro U, Halidou T, Sirima S, Tshefu A, Mtoro A, Gesase S, and Bassat Q

Subjects

Africa, Antimalarials adverse effects, Artemisinins adverse effects, Artemisinins pharmacokinetics, Drug Combinations, Female, Humans, Infant, Kaplan-Meier Estimate, Malaria, Falciparum mortality, Male, Quinolines adverse effects, Quinolines pharmacokinetics, Treatment Outcome, Antimalarials therapeutic use, Artemisinins therapeutic use, Malaria, Falciparum drug therapy, Quinolines therapeutic use

Abstract

Artemisinin combination therapies are considered the mainstay of malaria treatment, but pediatric-friendly formulations for the treatment of infants are scarce. We sought to evaluate the efficacy and safety of a new dispersible-tablet formulation of dihydroartemisinin/piperaquine phosphate (DHA/PQP) in comparison to the marketed tablet (Eurartesim) in the treatment of infants with uncomplicated Plasmodium falciparum malaria. Reported here are the results of a large phase II, randomized, open-label, multicenter trial conducted in African infants (6 to 12 months of age) from Mozambique, Burkina Faso, The Gambia, the Democratic Republic of the Congo, and Tanzania. Primary efficacy endpoint was the PCR-corrected adequate clinical and parasitological response (ACPR) at day 28. Analysis was performed for the intention-to-treat (ITT) and per-protocol (PP) populations. A total of 201 patients received the dispersible-tablet formulation, and 99 received the conventional one administered as crushed tablets. At day 28, the PCR-corrected ACPRs were 86.9% (ITT) and 98.3% (PP) in the dispersible-tablet group and 84.9% (ITT) and 100% (PP) in the crushed-tablet group. At day 42, these values were 85.9% (ITT) and 96.5% (PP) in the dispersible-tablet group and 82.8% (ITT) and 96.4% (PP) in the crushed-tablet group. The comparison between survival curves for time to new infections showed no statistically significant differences ( P = 0.409). The safety and tolerability profile for the two groups was similar in terms of type and frequency of adverse events and was consistent with that expected in African infants with malaria. A standard 3-day treatment with the new dispersible DHA/PQP formulation is as efficacious as the currently used tablet in African infants and has a comparable safety profile. (This trial was registered at ClinicalTrials.gov under registration no. NCT01992900.)., (Copyright © 2017 Gargano et al.)

Published

2017

12. Safety, Pharmacokinetics, and Antiviral Activity of a Novel HIV Antiviral, ABX464, in Treatment-Naive HIV-Infected Subjects in a Phase 2 Randomized, Controlled Study.

Author

Steens JM, Scherrer D, Gineste P, Barrett PN, Khuanchai S, Winai R, Ruxrungtham K, Tazi J, Murphy R, and Ehrlich H

Subjects

Adolescent, Adult, Aged, Anti-HIV Agents adverse effects, Anti-HIV Agents pharmacokinetics, Double-Blind Method, Female, HIV Infections drug therapy, Humans, Male, Middle Aged, Quinolines adverse effects, Quinolines pharmacokinetics, Treatment Outcome, Viral Load drug effects, Virus Replication drug effects, Young Adult, Anti-HIV Agents therapeutic use, HIV-1 drug effects, HIV-1 pathogenicity, Quinolines therapeutic use

Abstract

We investigated the safety and antiviral effects of an anti-HIV compound (ABX464) with a unique mechanism of viral replication inhibition. This was a randomized, double-blind, placebo-controlled, dose-ranging study in treatment-naive HIV-infected patients. Participants were assigned to eight groups; each group included eight subjects receiving either the study compound, ABX464 ( n = 6), or the corresponding placebo ( n = 2), according to a randomization code. The first dose administered was 25 mg, given once or 3 times a day over a 2- to 3-week period. Ascending doses of up to 150 mg were delivered after review of the safety data. The primary objective of the study was to assess the safety and tolerability of ABX464 after repeated oral administrations in subjects infected by HIV. Sixty-six subjects were enrolled and were randomized. Sixty-three subjects completed the study according to the study protocol. Twenty-one adverse events (AEs) were reported by 7 subjects out of 16 (44%) who received placebo, and 158 AEs were reported by 39 subjects out of 50 (78%) who received the study drug. In the ABX464 treatment group, all of these adverse events were mild to moderate. No subjects discontinued treatment due to drug-related AEs. Administration of ABX464 at up to 150 mg once a day was safe and well tolerated in HIV-infected subjects. An efficacy signal with respect to a reduction of the viral load by ABX464 was detected, mainly in subjects treated at the highest dose. Further studies will be required to demonstrate antiviral effects in HIV-infected subjects in combination with other antiretroviral therapies. (This study is registered on the ClinicalTrials.gov website under registration no. NCT02452242.)., (Copyright © 2017 Steens et al.)

Published

2017

13. Prediction of Improved Antimalarial Chemoprevention with Weekly Dosing of Dihydroartemisinin-Piperaquine.

Author

Permala J, Tarning J, Nosten F, White NJ, Karlsson MO, and Bergstrand M

Subjects

Antimalarials administration & dosage, Antimalarials pharmacokinetics, Artemisinins administration & dosage, Chemoprevention methods, Computer Simulation, Drug Administration Schedule, Drug Therapy, Combination, Humans, Malaria, Falciparum drug therapy, Quinolines administration & dosage, Treatment Outcome, Antimalarials therapeutic use, Artemisinins pharmacokinetics, Artemisinins therapeutic use, Malaria, Falciparum prevention & control, Quinolines pharmacokinetics, Quinolines therapeutic use

Abstract

Intermittent preventive treatment (IPT) is used to reduce malaria morbidity and mortality, especially in vulnerable groups such as children and pregnant women. IPT with the fixed dose combination of piperaquine (PQ) and dihydroartemisinin (DHA) is being evaluated as a potential mass treatment to control and eliminate artemisinin-resistant falciparum malaria. This study explored alternative DHA-PQ adult dosing regimens compared to the monthly adult dosing regimen currently being studied in clinical trials. A time-to-event model describing the concentration-effect relationship of preventive DHA-PQ administration was used to explore the potential clinical efficacy of once-weekly adult dosing regimens. Loading dose strategies were evaluated and the advantage of weekly dosing regimen was tested against different degrees of adherence. Assuming perfect adherence, three tablets weekly dosing regimen scenarios maintained malaria incidence of 0.2 to 0.3% per year compared to 2.1 to 2.6% for all monthly dosing regimen scenarios and 52% for the placebo. The three tablets weekly dosing regimen was also more forgiving (i.e., less sensitive to poor adherence), resulting in a predicted ∼4% malaria incidence per year compared to ∼8% for dosing regimen of two tablets weekly and ∼10% for monthly regimens (assuming 60% adherence and 35% interindividual variability). These results suggest that weekly dosing of DHA-PQ for malaria chemoprevention would improve treatment outcomes compared to monthly administration by lowering the incidence of malaria infections, reducing safety concerns about high PQ peak plasma concentrations and being more forgiving. In addition, weekly dosing is expected to reduce the selection pressure for PQ resistance., (Copyright © 2017 Permala et al.)

Published

2017

14. Piperaquine Population Pharmacokinetics and Cardiac Safety in Cambodia.

Author

Vanachayangkul P, Lon C, Spring M, Sok S, Ta-Aksorn W, Kodchakorn C, Pann ST, Chann S, Ittiverakul M, Sriwichai S, Buathong N, Kuntawunginn W, So M, Youdaline T, Milner E, Wojnarski M, Lanteri C, Manning J, Prom S, Haigney M, Cantilena L, and Saunders D

Subjects

Antimalarials therapeutic use, Artemisinins adverse effects, Artemisinins therapeutic use, Cambodia, Cardiotoxicity, Drug Therapy, Combination, Female, Humans, Malaria, Falciparum parasitology, Male, Myocardial Contraction physiology, Plasmodium falciparum drug effects, Quinolines blood, Quinolines therapeutic use, Antimalarials adverse effects, Arrhythmias, Cardiac chemically induced, Artemisinins pharmacokinetics, Malaria, Falciparum drug therapy, Myocardial Contraction drug effects, Quinolines pharmacokinetics

Abstract

Despite the rising rates of resistance to dihydroartemisinin-piperaquine (DP), DP remains a first-line therapy for uncomplicated malaria in many parts of Cambodia. While DP is generally well tolerated as a 3-day DP (3DP) regimen, compressed 2-day DP (2DP) regimens were associated with treatment-limiting cardiac repolarization effects in a recent clinical trial. To better estimate the risks of piperaquine on QT interval prolongation, we pooled data from three randomized clinical trials conducted between 2010 and 2014 in northern Cambodia. A population pharmacokinetic model was developed to compare exposure-response relationships between the 2DP and 3DP regimens while accounting for differences in regimen and sample collection times between studies. A 2-compartment model with first-order absorption and elimination without covariates best fit the data. The linear slope-intercept model predicted a 0.05-ms QT prolongation per ng/ml of piperaquine (5 ms per 100 ng/ml) in this largely male population. Though the plasma half-life was similar in both regimens, peak and total piperaquine exposures were higher in those treated with the 2DP regimen. Furthermore, the correlation between the plasma piperaquine concentration and the QT interval prolongation was stronger in the population receiving the 2DP regimen. Neither the time since the previous meal nor the baseline serum magnesium or potassium levels had additive effects on QT interval prolongation. As electrocardiographic monitoring is often nonexistent in areas where malaria is endemic, 2DP regimens should be avoided and the 3DP regimen should be carefully considered in settings where viable alternative therapies exist. When DP is employed, the risk of cardiotoxicity can be mitigated by combining a 3-day regimen, enforcing a 3-h fast before and after administration, and avoiding the concomitant use of QT interval-prolonging medications. (This study used data from three clinical trials that are registered at ClinicalTrials.gov under identifiers NCT01280162, NCT01624337, and NCT01849640.)., (Copyright © 2017 American Society for Microbiology.)

Published

2017

15. Pharmacokinetic Interactions between Tafenoquine and Dihydroartemisinin-Piperaquine or Artemether-Lumefantrine in Healthy Adult Subjects.

Author

Green JA, Mohamed K, Goyal N, Bouhired S, Hussaini A, Jones SW, Koh GC, Kostov I, Taylor M, Wolstenholm A, and Duparc S

Subjects

Adolescent, Adult, Aged, Aminoquinolines adverse effects, Antimalarials adverse effects, Artemisinins adverse effects, Drug Interactions, Drug Therapy, Combination, Ethanolamines adverse effects, Female, Fluorenes adverse effects, Half-Life, Healthy Volunteers, Humans, Lumefantrine, Male, Middle Aged, Plasmodium vivax drug effects, Quinolines adverse effects, Young Adult, Aminoquinolines pharmacokinetics, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Ethanolamines pharmacokinetics, Fluorenes pharmacokinetics, Malaria, Vivax drug therapy, Quinolines pharmacokinetics

Abstract

Tafenoquine is in development as a single-dose treatment for relapse prevention in individuals with Plasmodium vivax malaria. Tafenoquine must be coadministered with a blood schizonticide, either chloroquine or artemisinin-based combination therapy (ACT). This open-label, randomized, parallel-group study evaluated potential drug interactions between tafenoquine and two ACTs: dihydroartemisinin-piperaquine and artemether-lumefantrine. Healthy volunteers of either sex aged 18 to 65 years without glucose-6-phosphate dehydrogenase deficiency were randomized into five cohorts (n = 24 per cohort) to receive tafenoquine on day 1 (300 mg) plus once-daily dihydroartemisinin-piperaquine on days 1, 2, and 3 (120 mg/960 mg for 36 to <75 kg of body weight and 160 mg/1,280 mg for ≥75 to 100 kg of body weight), or plus artemether-lumefantrine (80 mg/480 mg) in two doses 8 h apart on day 1 and then twice daily on days 2 and 3, or each drug alone. The pharmacokinetic parameters of tafenoquine, piperaquine, lumefantrine, artemether, and dihydroartemisinin were determined by using noncompartmental methods. Point estimates and 90% confidence intervals were calculated for area under the concentration-time curve (AUC) and maximum observed plasma concentration (C max ) comparisons of tafenoquine plus ACT versus tafenoquine or ACT. All subjects receiving dihydroartemisinin-piperaquine experienced QTc prolongation (a known risk with this drug), but tafenoquine coadministration had no clinically relevant additional effect. Tafenoquine coadministration had no clinically relevant effects on dihydroartemisinin, piperaquine, artemether, or lumefantrine pharmacokinetics. Dihydroartemisinin-piperaquine coadministration increased the tafenoquine C max by 38% (90% confidence interval, 25 to 52%), the AUC from time zero to infinity (AUC 0-∞ ) by 12% (1 to 26%), and the half-life (t 1/2 ) by 29% (19 to 40%), with no effect on the AUC from time zero to the time of the last nonzero concentration (AUC 0-last ). Artemether-lumefantrine coadministration had no effect on tafenoquine pharmacokinetics. Tafenoquine can be coadministered with dihydroartemisinin-piperaquine or artemether-lumefantrine without dose adjustment for any of these compounds. (This study has been registered at ClinicalTrials.gov under registration no. NCT02184637.)., (Copyright © 2016 Green et al.)

Published

2016

16. How Robust Are Malaria Parasite Clearance Rates as Indicators of Drug Effectiveness and Resistance?

Author

Hastings IM, Kay K, and Hodel EM

Subjects

Adult, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Artesunate, Child, Dose-Response Relationship, Drug, Drug Administration Schedule, Drug Combinations, Drug Dosage Calculations, Drug Resistance, Humans, Immunity, Innate, Malaria, Falciparum diagnosis, Malaria, Falciparum immunology, Malaria, Falciparum parasitology, Mefloquine pharmacokinetics, Mefloquine pharmacology, Parasitemia diagnosis, Parasitemia immunology, Parasitic Sensitivity Tests, Plasmodium falciparum physiology, Quinolines pharmacokinetics, Quinolines pharmacology, Treatment Outcome, Antimalarials pharmacology, Artemisinins pharmacology, Malaria, Falciparum drug therapy, Models, Statistical, Parasitemia drug therapy, Plasmodium falciparum drug effects

Abstract

Artemisinin-based combination therapies (ACTs) are currently the first-line drugs for treating uncomplicated falciparum malaria, the most deadly of the human malarias. Malaria parasite clearance rates estimated from patients' blood following ACT treatment have been widely adopted as a measure of drug effectiveness and as surveillance tools for detecting the presence of potential artemisinin resistance. This metric has not been investigated in detail, nor have its properties or potential shortcomings been identified. Herein, the pharmacology of drug treatment, parasite biology, and human immunity are combined to investigate the dynamics of parasite clearance following ACT. This approach parsimoniously recovers the principal clinical features and dynamics of clearance. Human immunity is the primary determinant of clearance rates, unless or until artemisinin killing has fallen to near-ineffective levels. Clearance rates are therefore highly insensitive metrics for surveillance that may lead to overconfidence, as even quite substantial reductions in drug sensitivity may not be detected as lower clearance rates. Equally serious is the use of clearance rates to quantify the impact of ACT regimen changes, as this strategy will plausibly miss even very substantial increases in drug effectiveness. In particular, the malaria community may be missing the opportunity to dramatically increase ACT effectiveness through regimen changes, particularly through a switch to twice-daily regimens and/or increases in artemisinin dosing levels. The malaria community therefore appears overreliant on a single metric of drug effectiveness, the parasite clearance rate, that has significant and serious shortcomings., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

17. Population pharmacokinetics, tolerability, and safety of dihydroartemisinin-piperaquine and sulfadoxine-pyrimethamine-piperaquine in pregnant and nonpregnant Papua New Guinean women.

Author

Benjamin JM, Moore BR, Salman S, Page-Sharp M, Tawat S, Yadi G, Lorry L, Siba PM, Batty KT, Robinson LJ, Mueller I, and Davis TM

Subjects

Adolescent, Adult, Antimalarials therapeutic use, Area Under Curve, Artemisinins adverse effects, Artemisinins therapeutic use, Biological Availability, Dietary Fats, Drug Combinations, Female, Follow-Up Studies, Food-Drug Interactions, Humans, Infant, Newborn, Malaria, Falciparum drug therapy, Malaria, Falciparum metabolism, Models, Statistical, Papua New Guinea epidemiology, Pregnancy, Pregnancy Outcome, Pyrimethamine therapeutic use, Quinolines therapeutic use, Sulfadoxine therapeutic use, Young Adult, Antimalarials adverse effects, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Pyrimethamine adverse effects, Pyrimethamine pharmacokinetics, Quinolines adverse effects, Quinolines pharmacokinetics, Sulfadoxine adverse effects, Sulfadoxine pharmacokinetics

Abstract

The tolerability, safety, and disposition of dihydroartemisinin (DHA) and piperaquine (PQ) were assessed in 32 pregnant (second/third trimester) and 33 nonpregnant Papua New Guinean women randomized to adult treatment courses of DHA-PQ (three daily doses) or sulfadoxine-pyrimethamine (SP)-PQ (three daily PQ doses, single dose of SP). All dose adminstrations were observed, and subjects fasted for 2 h postdose. Plasma PQ was assayed by using high-performance liquid chromatography, and DHA was assessed by using liquid chromatography-mass spectrometry. Compartmental pharmacokinetic models were developed using a population-based approach. Both regimens were well tolerated. There was an expected increase in the rate-corrected electrocardiographic QT interval which was independent of pregnancy and treatment. Two pregnant and two nonpregnant women had Plasmodium falciparum parasitemia which cleared within 48 h, and no other subject became slide positive for malaria during 42 days of follow-up. Of 30 pregnant women followed to delivery, 27 (90%) delivered healthy babies and 3 (10%) had stillbirths; these obstetric outcomes are consistent with those in the general population. The area under the plasma PQ concentration-time curve (AUC0-∞) was lower in the pregnant patients (median [interquartile range], 23,721 μg · h/liter [21,481 to 27,951 μg · h/liter] versus 35,644 μg · h/liter [29,546 to 39,541 μg · h/liter]; P < 0.001) in association with a greater clearance relative to bioavailability (73.5 liters/h [69.4 to 78.4] versus 53.8 liters/h [49.7 to 58.2]; P < 0.001), but pregnancy did not influence the pharmacokinetics of DHA. The apparent pharmacokinetic differences between the present study and results from other studies of women with uncomplicated malaria that showed no effect of pregnancy on the AUC0-∞ of PQ and greater bioavailability may reflect differences in postdose fat intake, proportions of women with malaria, and/or racial differences in drug disposition., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

18. Pharmacokinetics of piperaquine transfer into the breast milk of Melanesian mothers.

Author

Moore BR, Salman S, Benjamin J, Page-Sharp M, Yadi G, Batty KT, Siba PM, Mueller I, and Davis TM

Subjects

Adult, Aging metabolism, Antimalarials adverse effects, Chromatography, High Pressure Liquid, Computer Simulation, Female, Humans, Infant, Infant, Newborn, Melanesia, Models, Biological, Postpartum Period, Quinolines adverse effects, Young Adult, Antimalarials pharmacokinetics, Milk, Human metabolism, Quinolines pharmacokinetics

Abstract

Transfer of piperaquine (PQ) into breast milk was examined in 27 Papua New Guinean women given a 3-day course of dihydroartemisinin-PQ or sulfadoxine-pyrimethamine-PQ during the second/third trimester. Breast milk was sampled on days 1, 2, 3 to 5, 7 to 11, and 14 to 17 postdelivery, a median of 70 days postdose (range, 6 to 145 days). A blood sample was taken at delivery, and additional serial samples were available from 9 women who delivered within 42 days of dosing. Milk and plasma PQ were assayed by high-performance liquid chromatography. A population-based approach was used to model the loge(plasma) and milk concentration-time data. A sigmoid Emax model best described PQ breast milk transfer. The population average milk:plasma PQ ratio was 0.58, with a peak of 2.5 at delivery. The model-derived maximum milk intake (148 ml/kg of body weight/day) was similar to the accepted value of 150 ml/kg/day. The median estimated absolute and relative cumulative infant PQ doses were 22 μg and 0.07%, respectively, corresponding to absolute and relative daily doses of 0.41 μg/kg and 0.004%. Model-based simulations for PQ treatment regimens given at birth, 1 week postdelivery, and 6 weeks postdelivery showed that the highest median estimated relative total infant dose (0.36%; median absolute total dose of 101 μg/kg) was seen after maternal PQ treatment 6 weeks postpartum. The maximum simulated relative total and daily doses from any scenario were 4.3% and 2.5%, respectively, which were lower than the recommended 10% upper limit. Piperaquine is transferred into breast milk after maternal treatment doses, but PQ exposure for suckling infants appears safe., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

19. Open-label, single-dose, parallel-group study in healthy volunteers to determine the drug-drug interaction potential between KAE609 (cipargamin) and piperaquine.

Author

Stein DS, Jain JP, Kangas M, Lefèvre G, Machineni S, Griffin P, and Lickliter J

Subjects

Adolescent, Adult, Dose-Response Relationship, Drug, Drug Interactions, Female, Healthy Volunteers, Humans, Indoles administration & dosage, Male, Middle Aged, Quinolines administration & dosage, Spiro Compounds administration & dosage, Young Adult, Indoles pharmacokinetics, Indoles pharmacology, Quinolines pharmacokinetics, Quinolines pharmacology, Spiro Compounds pharmacokinetics, Spiro Compounds pharmacology

Abstract

KAE609 represents a new class of potent, fast-acting, schizonticidal antimalarials. This study investigated the safety and pharmacokinetics of KAE609 in combination with the long-acting antimalarial piperaquine (PPQ) in healthy volunteers. A two-way pharmacokinetic interaction was hypothesized for KAE609 and PPQ, as both drugs are CYP3A4 substrates and inhibitors. The potential for both agents to affect the QT interval was also assessed. This was an open-label, parallel-group, single-dose study with healthy volunteers. Subjects were randomized to four parallel dosing arms with five cohorts (2:2:2:2:1), receiving 75 mg KAE609 plus 320 mg PPQ, 25 mg KAE609 plus 1,280 mg PPQ, 25 mg KAE609 alone, 320 mg PPQ alone, or 1,280 mg PPQ alone. Triplicate electrocardiograms were performed over the first 24 h after dosing, with single electrocardiograms at other time points. Routine safety (up to 89 days) and pharmacokinetic (up to 61 days) assessments were performed. Of the 110 subjects recruited, 99 completed the study. Coadministration of PPQ had no overall effect on exposure to KAE609, although 1,280 mg PPQ decreased the KAE609 maximum concentration (Cmax) by 17%. The group that received 25 mg KAE609 plus 1,280 mg PPQ showed a 32% increase in the PPQ area under the concentration-time curve from 0 to infinity (AUCinf), while the group that received 75 mg KAE609 plus 320 mg PPQ showed a 14% reduction. Mean changes from baseline in the QT interval corrected by Fridericia's method (QTcF) and the QT interval corrected by Bazett's method (QTcB) with PPQ were consistent with its known effects. PPQ but not KAE609 exposure correlated with corrected QT interval (QTc) increases, and KAE609 did not affect the PPQ exposure-QTc relationship. The QTcF effect for PPQ (least-squares estimate of the difference in mean maximal changes from baseline of 7.47 ms [90% confidence interval, 3.55 to 11.4 ms]) was consistent with the criteria for a positive thorough QT study. No subject had QTcF or QTcB values of >500 ms. Both drugs given alone or in combination were well tolerated, with no deaths, serious adverse events (AEs), or severe AEs reported. Most AEs were mild; upper respiratory tract infections, headache, diarrhea, and oropharyngeal pain were most common. PPQ and KAE609 coadministration had no relevant effect on exposure to either agent, and KAE609 did not affect or potentiate the known effects of PPQ on cardiac conduction., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

20. Open-label crossover study of primaquine and dihydroartemisinin-piperaquine pharmacokinetics in healthy adult thai subjects.

Author

Hanboonkunupakarn B, Ashley EA, Jittamala P, Tarning J, Pukrittayakamee S, Hanpithakpong W, Chotsiri P, Wattanakul T, Panapipat S, Lee SJ, Day NP, and White NJ

Subjects

Administration, Oral, Adult, Alanine Transaminase blood, Antimalarials blood, Area Under Curve, Artemisinins blood, Aspartate Aminotransferases blood, Biological Availability, Cross-Over Studies, Drug Administration Schedule, Drug Therapy, Combination, Female, Humans, Male, Middle Aged, Primaquine blood, Quinolines blood, Thailand, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Primaquine pharmacokinetics, Quinolines pharmacokinetics

Abstract

Dihydroartemisinin-piperaquine is an artemisinin-based combination treatment (ACT) recommended by the WHO for uncomplicated Plasmodium falciparum malaria, and it is being used increasingly for resistant vivax malaria where combination with primaquine is required for radical cure. The WHO recently reinforced its recommendations to add a single dose of primaquine to ACTs to reduce P. falciparum transmission in low-transmission settings. The pharmacokinetics of primaquine and dihydroartemisinin-piperaquine were evaluated in 16 healthy Thai adult volunteers in a randomized crossover study. Volunteers were randomized to two groups of three sequential hospital admissions to receive 30 mg (base) primaquine, 3 tablets of dihydroartemisinin-piperaquine (120/960 mg), and the drugs together at the same doses. Blood sampling was performed over 3 days following primaquine and 36 days following dihydroartemisinin-piperaquine dosing. Pharmacokinetic assessment was done with a noncompartmental approach. The drugs were well tolerated. There were no statistically significant differences in dihydroartemisinin and piperaquine pharmacokinetics with or without primaquine. Dihydroartemisinin-piperaquine coadministration significantly increased plasma primaquine levels; geometric mean ratios (90% confidence interval [CI]) of primaquine combined versus primaquine alone for maximum concentration (Cmax), area under the concentration-time curve from 0 h to the end of the study (AUC0-last), and area under the concentration-time curve from 0 h to infinity (AUC0-∞) were 148% (117 to 187%), 129% (103 to 163%), and 128% (102 to 161%), respectively. This interaction is similar to that described recently with chloroquine and may result in an enhanced radical curative effect. (This study has been registered at ClinicalTrials.gov under registration no. NCT01525511.)., (Copyright © 2014 Hanboonkunupakarn et al.)

Published

2014

21. Improving the role and contribution of pharmacokinetic analyses in antimalarial drug clinical trials.

Author

Kay K, Hodel EM, and Hastings IM

Subjects

Antimalarials therapeutic use, Artemisinins pharmacokinetics, Artemisinins therapeutic use, Clinical Trials as Topic, Drug Evaluation, Humans, Quinolines pharmacokinetics, Quinolines therapeutic use, Antimalarials pharmacokinetics

Abstract

It is now World Health Organization (WHO) policy that drug concentrations on day 7 be measured as part of routine assessment in antimalarial drug efficacy trials. The rationale is that this single pharmacological measure serves as a simple and practical predictor of treatment outcome for antimalarial drugs with long half-lives. Herein we review theoretical data and field studies and conclude that the day 7 drug concentration (d7c) actually appears to be a poor predictor of therapeutic outcome. This poor predictive capability combined with the fact that many routine antimalarial trials will have few or no failures means that there appears to be little justification for this WHO recommendation. Pharmacological studies have a huge potential to improve antimalarial dosing, and we propose study designs that use more-focused, sophisticated, and cost-effective ways of generating these data than the mass collection of single d7c concentrations., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

22. Effect of coadministered fat on the tolerability, safety, and pharmacokinetic properties of dihydroartemisinin-piperaquine in Papua New Guinean children with uncomplicated malaria.

Author

Moore BR, Benjamin JM, Salman S, Griffin S, Ginny E, Page-Sharp M, Robinson LJ, Siba P, Batty KT, Mueller I, and Davis TM

Subjects

Antimalarials administration & dosage, Antimalarials therapeutic use, Artemisinins administration & dosage, Child, Female, Hemodynamics drug effects, Humans, Malaria drug therapy, Male, Quinolines administration & dosage, Antimalarials adverse effects, Antimalarials pharmacokinetics, Artemisinins adverse effects, Artemisinins pharmacokinetics, Malaria blood, Quinolines adverse effects, Quinolines pharmacokinetics

Abstract

Coadministration of dihydroartemisinin-piperaquine (DHA-PQ) with fat may improve bioavailability and antimalarial efficacy, but it might also increase toxicity. There have been no studies of these potential effects in the pediatric age group. The tolerability, safety, efficacy, and pharmacokinetics of DHA-PQ administered with or without 8.5 g fat were investigated in 30 Papua New Guinean children aged 5 to 10 years diagnosed with uncomplicated falciparum malaria. Three daily 2.5:11.5-mg-base/kg doses were given with water (n = 14, group A) or milk (n = 16, group B), with regular clinical/laboratory assessment and blood sampling over 42 days. Plasma PQ was assayed by high-performance liquid chromatography with UV detection, and DHA was assayed using liquid chromatography-mass spectrometry. Compartmental pharmacokinetic models for PQ and DHA were developed using a population-based approach. DHA-PQ was generally well tolerated, and initial fever and parasite clearance were prompt. There were no differences in the areas under the concentration-time curve (AUC0-∞) for PQ (median, 41,906 versus 36,752 μg · h/liter in groups A and B, respectively; P = 0.24) or DHA (4,047 versus 4,190 μg · h/liter; P = 0.67). There were also no significant between-group differences in prolongation of the corrected electrocardiographic QT interval (QTc) initially during follow-up, but the QTc tended to be higher in group B children at 24 h (mean ± standard deviation [SD], 15 ± 10 versus 6 ± 15 ms(0.5) in group A, P = 0.067) and 168 h (10 ± 18 versus 1 ± 23 ms(0.5), P = 0.24) when plasma PQ concentrations were relatively low. A small amount of fat does not change the bioavailability of DHA-PQ in children, but a delayed persistent effect on ventricular repolarization cannot be excluded., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

23. Population pharmacokinetic assessment of the effect of food on piperaquine bioavailability in patients with uncomplicated malaria.

Author

Tarning J, Lindegardh N, Lwin KM, Annerberg A, Kiricharoen L, Ashley E, White NJ, Nosten F, and Day NP

Subjects

Adolescent, Adult, Aged, Fasting blood, Humans, Malaria, Falciparum blood, Middle Aged, Monte Carlo Method, Quinolines therapeutic use, Young Adult, Antimalarials pharmacokinetics, Antimalarials therapeutic use, Malaria, Falciparum drug therapy, Quinolines pharmacokinetics

Abstract

Previously published literature reports various impacts of food on the oral bioavailability of piperaquine. The aim of this study was to use a population modeling approach to investigate the impact of concomitant intake of a small amount of food on piperaquine pharmacokinetics. This was an open, randomized comparison of piperaquine pharmacokinetics when administered as a fixed oral formulation once daily for 3 days with (n=15) and without (n=15) concomitant food to patients with uncomplicated Plasmodium falciparum malaria in Thailand. Nonlinear mixed-effects modeling was used to characterize the pharmacokinetics of piperaquine and the influence of concomitant food intake. A modified Monte Carlo mapped power approach was applied to evaluate the relationship between statistical power and various degrees of covariate effect sizes of the given study design. Piperaquine population pharmacokinetics were described well in fasting and fed patients by a three-compartment distribution model with flexible absorption. The final model showed a 25% increase in relative bioavailability per dose occasion during recovery from malaria but demonstrated no clinical impact of concomitant intake of a low-fat meal. Body weight and age were both significant covariates in the final model. The novel power approach concluded that the study was adequately powered to detect a food effect of at least 35%. This modified Monte Carlo mapped power approach may be a useful tool for evaluating the power to detect true covariate effects in mixed-effects modeling and a given study design. A small amount of food does not affect piperaquine absorption significantly in acute malaria.

Published

2014

24. Preclinical characterization of the novel hepatitis C virus NS3 protease inhibitor GS-9451.

Author

Yang H, Robinson M, Corsa AC, Peng B, Cheng G, Tian Y, Wang Y, Pakdaman R, Shen M, Qi X, Mo H, Tay C, Krawczyk S, Sheng XC, Kim CU, Yang C, and Delaney WE 4th

Subjects

Animals, Antiviral Agents pharmacokinetics, Benzimidazoles pharmacology, Dogs, Drug Evaluation, Preclinical, Drug Resistance, Viral drug effects, Drug Resistance, Viral genetics, Drug Synergism, Drug Therapy, Combination, Fluorenes pharmacology, Haplorhini, Hepacivirus physiology, Hepatitis C, Chronic pathology, Hepatitis C, Chronic virology, Hepatocytes drug effects, Hepatocytes virology, Humans, Inhibitory Concentration 50, Interferon-alpha pharmacology, Protease Inhibitors pharmacokinetics, Purines pharmacology, Pyridazines pharmacology, Quinolines pharmacokinetics, Rats, Replicon drug effects, Ribavirin pharmacology, Viral Nonstructural Proteins metabolism, Antiviral Agents pharmacology, Hepacivirus drug effects, Hepatitis C, Chronic drug therapy, Protease Inhibitors pharmacology, Quinolines pharmacology, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

GS-9451 is a selective hepatitis C virus (HCV) NS3 protease inhibitor in development for the treatment of genotype 1 (GT1) HCV infection. Key preclinical properties of GS-9451, including in vitro antiviral activity, selectivity, cross-resistance, and combination activity, as well as pharmacokinetic properties, were determined. In multiple GT1a and GT1b replicon cell lines, GS-9451 had mean 50% effective concentrations (EC50s) of 13 and 5.4 nM, respectively, with minimal cytotoxicity; similar potency was observed in chimeric replicons encoding the NS3 protease gene of GT1 clinical isolates. GS-9451 was less active in GT2a replicon cells (EC50 = 316 nM). Additive to synergistic in vitro antiviral activity was observed when GS-9451 was combined with other agents, including alpha interferon, ribavirin, and the polymerase inhibitors GS-6620 and tegobuvir (GS-9190), as well as the NS5A inhibitor ledipasvir (GS-5885). GS-9451 retained wild-type activity against multiple classes of NS5B and NS5A inhibitor resistance mutations. GS-9451 was stable in hepatic microsomes and hepatocytes from human and three other tested species. Systemic clearance was low in dogs and monkeys but high in rats. GS-9451 showed good oral bioavailability in all three species tested. In rats, GS-9451 levels were ∼40-fold higher in liver than plasma after intravenous dosing, and elimination of GS-9451 was primarily through biliary excretion. Together, these results are consistent with the antiviral activity observed in a recent phase 1b study. The results of in vitro cross-resistance and combination antiviral assays support the ongoing development of GS-9451 in combination with other agents for the treatment of chronic HCV infection.

Published

2014

25. Model-based estimates of the effects of efavirenz on bedaquiline pharmacokinetics and suggested dose adjustments for patients coinfected with HIV and tuberculosis.

Author

Svensson EM, Aweeka F, Park JG, Marzan F, Dooley KE, and Karlsson MO

Subjects

Adolescent, Adult, Aged, Alkynes, Anti-HIV Agents administration & dosage, Anti-HIV Agents therapeutic use, Antitubercular Agents administration & dosage, Antitubercular Agents therapeutic use, Benzoxazines administration & dosage, Benzoxazines therapeutic use, Cyclopropanes, Diarylquinolines, Dose-Response Relationship, Drug, Drug Interactions, Drug Therapy, Combination, HIV Infections complications, Humans, Middle Aged, Quinolines administration & dosage, Quinolines therapeutic use, Stochastic Processes, Treatment Outcome, Tuberculosis complications, Tuberculosis drug therapy, Young Adult, Anti-HIV Agents pharmacokinetics, Antitubercular Agents pharmacokinetics, Benzoxazines pharmacokinetics, HIV Infections drug therapy, Models, Biological, Quinolines pharmacokinetics

Abstract

Safe, effective concomitant treatment regimens for tuberculosis (TB) and HIV infection are urgently needed. Bedaquiline (BDQ) is a promising new anti-TB drug, and efavirenz (EFV) is a commonly used antiretroviral. Due to EFV's induction of cytochrome P450 3A4, the metabolic enzyme responsible for BDQ biotransformation, the drugs are expected to interact. Based on data from a phase I, single-dose pharmacokinetic study, a nonlinear mixed-effects model characterizing BDQ pharmacokinetics and interaction with multiple-dose EFV was developed. BDQ pharmacokinetics were best described by a 3-compartment disposition model with absorption through a dynamic transit compartment model. Metabolites M2 and M3 were described by 2-compartment models with clearance of BDQ and M2, respectively, as input. Impact of induction was described as an instantaneous change in clearance 1 week after initialization of EFV treatment and estimated for all compounds. The model predicts average steady-state concentrations of BDQ and M2 to be reduced by 52% (relative standard error [RSE], 3.7%) with chronic coadministration. A range of models with alternative structural assumptions regarding onset of induction effect and fraction metabolized resulted in similar estimates of the typical reduction and did not offer a markedly better fit to data. Simulations to investigate alternative regimens mitigating the estimated interaction effect were performed. The results suggest that simple adjustments of the standard regimen during EFV coadministration can prevent reduced exposure to BDQ without increasing exposures to M2. However, exposure to M3 would increase. Evaluation in clinical trials of adjusted regimens is necessary to ensure appropriate dosing for HIV-infected TB patients on an EFV-based regimen.

Published

2013

26. Activity of moxifloxacin, imipenem, and ertapenem against Escherichia coli, Enterobacter cloacae, Enterococcus faecalis, and Bacteroides fragilis in monocultures and mixed cultures in an in vitro pharmacokinetic/pharmacodynamic model simulating concentrations in the human pancreas.

Author

Schubert S and Dalhoff A

Subjects

Anti-Bacterial Agents pharmacokinetics, Aza Compounds pharmacokinetics, Bacterial Load, Colony Count, Microbial, Ertapenem, Fluoroquinolones, Humans, Imipenem pharmacokinetics, Microbial Sensitivity Tests, Models, Statistical, Moxifloxacin, Pancreatitis, Acute Necrotizing microbiology, Quinolines pharmacokinetics, Regression Analysis, beta-Lactams pharmacokinetics, Anti-Bacterial Agents pharmacology, Aza Compounds pharmacology, Bacteroides fragilis drug effects, Enterobacter cloacae drug effects, Enterococcus faecalis drug effects, Escherichia coli drug effects, Imipenem pharmacology, Pancreas metabolism, Quinolines pharmacology, beta-Lactams pharmacology

Abstract

The activities of moxifloxacin, imipenem, and ertapenem against pathogens causing severe necrotizing pancreatitis were studied in an in vitro pharmacokinetics/pharmacodynamics (PK/PD) model. Escherichia coli, Enterobacter cloacae, Enterococcus faecalis, and Bacteroides fragilis were exposed in monocultures and mixed cultures to concentrations of the three agents comparable to those in the human pancreas. Moxifloxacin was more active than the two carbapenems in monocultures and mixed cultures, reducing the numbers of CFU more drastically and more rapidly.

Published

2012

27. Moxifloxacin population pharmacokinetics in patients with pulmonary tuberculosis and the effect of intermittent high-dose rifapentine.

Author

Zvada SP, Denti P, Geldenhuys H, Meredith S, van As D, Hatherill M, Hanekom W, Wiesner L, Simonsson US, Jindani A, Harrison T, and McIlleron HM

Subjects

Adult, Antibiotics, Antitubercular therapeutic use, Antitubercular Agents blood, Antitubercular Agents therapeutic use, Aza Compounds therapeutic use, Drug Administration Schedule, Drug Therapy, Combination, Fluoroquinolones, Humans, Moxifloxacin, Mycobacterium tuberculosis drug effects, Quinolines therapeutic use, Rifampin administration & dosage, Rifampin therapeutic use, Tuberculosis, Pulmonary metabolism, Antibiotics, Antitubercular administration & dosage, Antitubercular Agents pharmacokinetics, Aza Compounds blood, Aza Compounds pharmacokinetics, Quinolines blood, Quinolines pharmacokinetics, Rifampin analogs & derivatives, Tuberculosis, Pulmonary drug therapy

Abstract

We described the population pharmacokinetics of moxifloxacin and the effect of high-dose intermittent rifapentine in patients with pulmonary tuberculosis who were randomized to a continuation-phase regimen of 400 mg moxifloxacin and 900 mg rifapentine twice weekly or 400 mg moxifloxacin and 1,200 mg rifapentine once weekly. A two-compartment model with transit absorption best described moxifloxacin pharmacokinetics. Although rifapentine increased the clearance of moxifloxacin by 8% during antituberculosis treatment compared to that after treatment completion without rifapentine, it did not result in a clinically significant change in moxifloxacin exposure.

Published

2012

28. Pharmacokinetic comparison of two piperaquine-containing artemisinin combination therapies in Papua New Guinean children with uncomplicated malaria.

Author

Salman S, Page-Sharp M, Batty KT, Kose K, Griffin S, Siba PM, Ilett KF, Mueller I, and Davis TM

Subjects

Antimalarials therapeutic use, Artemisinins therapeutic use, Child, Child, Preschool, Female, Humans, Malaria blood, Malaria metabolism, Male, Quinolines therapeutic use, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Malaria drug therapy, Quinolines pharmacokinetics

Abstract

Pharmacokinetic differences between piperaquine (PQ) base and PQ tetraphosphate were investigated in 34 Papua New Guinean children aged 5 to 10 years treated for uncomplicated malaria with artemisinin-PQ (ART-PQ) base or dihydroartemisinin-PQ (DHA-PQ) tetraphosphate. Twelve children received ART-PQ base (two daily doses of 3 mg of ART and 18 mg of PQ base as granules/kg of body weight) as recommended by the manufacturer, with regular clinical assessment and blood sampling over 56 days. PQ concentrations in plasma samples collected from 22 children of similar ages with malaria in a previously published pharmacokinetic study of DHA-PQ tetraphosphate (three daily doses of 2.5 mg of ART and 20 mg of PQ tetraphosphate as tablets/kg of body weight) were available for comparison. The disposition of ART was also assessed in the 12 children who received ART-PQ base. Plasma PQ was assayed by high-performance liquid chromatography with UV detection, and ART was assayed using liquid chromatography-mass spectrometry. Multicompartment pharmacokinetic models for PQ and ART were developed using a population-based approach. ART-PQ base was well tolerated, and initial fever abatement and parasite clearance were prompt. There were no differences between the two treatments in the values for the PQ area under the concentration-time curve from time zero to infinity (AUC(0-∞)), with medians of 49,451 (n = 12) and 44,556 (n = 22) μg · h/liter for ART-PQ base and DHA-PQ tetraphosphate, respectively. Recurrent parasitemia was associated with lower PQ exposure. Using a two-compartment ART model, the median AUC(0-∞) was 1,652 μg · h/liter. There was evidence of autoinduction of ART metabolism (relative bioavailability for the second dose, 0.27). These and previously published data suggest that a 3-day ART-PQ base regimen should be further evaluated, in line with World Health Organization recommendations for all artemisinin combination therapies.

Published

2012

29. Effect of coadministration of moxifloxacin and rifampin on Mycobacterium tuberculosis in a murine aerosol infection model.

Author

Balasubramanian V, Solapure S, Gaonkar S, Mahesh Kumar KN, Shandil RK, Deshpande A, Kumar N, Vishwas KG, Panduga V, Reddy J, Ganguly S, Louie A, and Drusano GL

Subjects

Animals, Antitubercular Agents administration & dosage, Antitubercular Agents pharmacokinetics, Aza Compounds administration & dosage, Aza Compounds pharmacokinetics, Fluoroquinolones, Mice, Mice, Inbred BALB C, Moxifloxacin, Quinolines administration & dosage, Quinolines pharmacokinetics, Rifampin administration & dosage, Rifampin pharmacokinetics, Tuberculosis, Pulmonary microbiology, Antitubercular Agents therapeutic use, Aza Compounds therapeutic use, Mycobacterium tuberculosis drug effects, Mycobacterium tuberculosis pathogenicity, Quinolines therapeutic use, Rifampin therapeutic use, Tuberculosis, Pulmonary drug therapy

Abstract

Coadministration of moxifloxacin and rifampin was evaluated in a murine model of Mycobacterium tuberculosis pulmonary infection to determine whether the finding of antagonism documented in a hollow-fiber infection model could be recapitulated in vivo. Colony counts were followed in a no-treatment control group, groups administered moxifloxacin or rifampin monotherapy, and a group administered a combination of the two agents. Following 18 days of once-daily oral administration to mice infected with M. tuberculosis, there was a reduction in the plasma exposure to rifampin that decreased further when rifampin was coadministered with moxifloxacin. Pharmacodynamic analysis demonstrated a mild antagonistic interaction between moxifloxacin and rifampin with respect to cell kill in the mouse model for tuberculosis (TB). No emergence of resistance was noted over 28 days of therapy, even with monotherapy. This was true even though one of the agents in the combination (moxifloxacin) induces error-prone replication. The previously noted antagonism with respect to cell kill shown in the hollow-fiber infection model was recapitulated in the murine TB lung model, although to a lesser extent.

Published

2012

30. No effect of a single supratherapeutic dose of lersivirine, a next-generation nonnucleoside reverse transcriptase inhibitor, on corrected QT interval in healthy subjects.

Author

Vourvahis M, Wang R, Ndongo MN, O'Gorman M, and Tawadrous M

Subjects

Adult, Anti-HIV Agents administration & dosage, Anti-HIV Agents blood, Anti-Infective Agents administration & dosage, Anti-Infective Agents blood, Anti-Infective Agents pharmacokinetics, Aza Compounds administration & dosage, Aza Compounds blood, Aza Compounds pharmacokinetics, Blood Pressure drug effects, Cross-Over Studies, Dose-Response Relationship, Drug, Electrocardiography, Fluoroquinolones, Heart physiology, Heart Rate drug effects, Humans, Male, Middle Aged, Moxifloxacin, Nitriles administration & dosage, Nitriles blood, Placebos, Pyrazoles administration & dosage, Pyrazoles blood, Quinolines administration & dosage, Quinolines blood, Quinolines pharmacokinetics, Reverse Transcriptase Inhibitors administration & dosage, Reverse Transcriptase Inhibitors blood, Anti-HIV Agents pharmacokinetics, Heart drug effects, Nitriles pharmacokinetics, Pyrazoles pharmacokinetics, Reverse Transcriptase Inhibitors pharmacokinetics

Abstract

The objective of this study was to investigate the effect of a supratherapeutic dose of lersivirine (LRV) on corrected QT (QTc) interval using Fridericia's equation (QTcF) in healthy subjects. In this randomized, single-dose, placebo- and active-controlled 3-way crossover study, healthy adult males (n = 48) were randomized to receive LRV (2,400 mg), moxifloxacin (400 mg), or placebo for each treatment period. Triplicate 12-lead electrocardiogram measurements were performed, PK samples were collected, and vital signs were measured. Adverse event monitoring and safety laboratory testing were performed. All subjects were white (mean age, 39 years; body mass index [BMI], 25.6 kg/m(2)) and completed the study. Following LRV administration, the upper bound of the 90% confidence interval (CI) for time-matched adjusted mean differences to placebo QTcF at each time point postdose was below the regulatory threshold of 10 ms, satisfying the criteria for a negative thorough QT/QTc study. The highest upper bound of QTcF 90% CI occurred at 6 h for LRV (3.32 ms; 90% CI, 1.47 to 5.17 ms). The study was deemed adequately sensitive as the lower bound of the 90% CI for the adjusted mean QTcF differences between moxifloxacin and placebo at the moxifloxacin historical T(max) of 3 h was >5 ms (15.29 ms; 90% CI, 13.44 to 17.14 ms). There was no statistically significant relationship between LRV exposure and placebo-adjusted change from baseline QTcF or clinically significant changes in QRS complex, pulse rate (PR) interval, heart rate, or blood pressure. LRV (2,400 mg) did not prolong the QTcF interval, and no clinically relevant electrocardiogram or vital sign changes were observed in healthy subjects.

Published

2012

31. Population pharmacokinetics of dihydroartemisinin and piperaquine in pregnant and nonpregnant women with uncomplicated malaria.

Author

Tarning J, Rijken MJ, McGready R, Phyo AP, Hanpithakpong W, Day NP, White NJ, Nosten F, and Lindegardh N

Subjects

Adolescent, Adult, Antimalarials administration & dosage, Area Under Curve, Artemisinins administration & dosage, Body Weight physiology, Chromatography, High Pressure Liquid, Female, Half-Life, Humans, Middle Aged, Myanmar, Nonlinear Dynamics, Population, Predictive Value of Tests, Pregnancy, Quinolines administration & dosage, Software, Tandem Mass Spectrometry, Thailand, Young Adult, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Malaria metabolism, Pregnancy Complications, Parasitic metabolism, Quinolines pharmacokinetics

Abstract

Pregnant women are particularly vulnerable to malaria. The pharmacokinetic properties of antimalarial drugs are often affected by pregnancy, resulting in lower drug concentrations and a consequently higher risk of treatment failure. The objective of this study was to evaluate the population pharmacokinetic properties of piperaquine and dihydroartemisinin in pregnant and nonpregnant women with uncomplicated malaria. Twenty-four pregnant and 24 matched nonpregnant women on the Thai-Myanmar boarder were treated with a standard fixed oral 3-day treatment, and venous plasma concentrations of both drugs were measured frequently for pharmacokinetic evaluation. Population pharmacokinetics were evaluated with nonlinear mixed-effects modeling. The main pharmacokinetic finding was an unaltered total exposure to piperaquine but reduced exposure to dihydroartemisinin in pregnant compared to nonpregnant women with uncomplicated malaria. Piperaquine was best described by a three-compartment disposition model with a 45% higher elimination clearance and a 47% increase in relative bioavailability in pregnant women compared with nonpregnant women. The resulting net effect of pregnancy was an unaltered total exposure to piperaquine but a shorter terminal elimination half-life. Dihydroartemisinin was best described by a one-compartment disposition model with a 38% lower relative bioavailability in pregnant women than nonpregnant women. The resulting net effect of pregnancy was a decreased total exposure to dihydroartemisinin. The shorter terminal elimination half-life of piperaquine and lower exposure to dihydroartemisinin will shorten the posttreatment prophylactic effect and might affect cure rates. The clinical impact of these pharmacokinetic findings in pregnant women with uncomplicated malaria needs to be evaluated in larger series.

Published

2012

32. Pharmacokinetics and pharmacodynamics of TMC207 and its N-desmethyl metabolite in a murine model of tuberculosis.

Author

Rouan MC, Lounis N, Gevers T, Dillen L, Gilissen R, Raoof A, and Andries K

Subjects

ATP Synthetase Complexes metabolism, Animals, Antitubercular Agents blood, Antitubercular Agents pharmacokinetics, Area Under Curve, Bacterial Proteins metabolism, Biotransformation, Colony Count, Microbial, Diarylquinolines, Disease Models, Animal, Drug Administration Routes, Drug Administration Schedule, Drug Dosage Calculations, Female, Half-Life, Humans, Lung microbiology, Male, Mice, Microbial Sensitivity Tests, Mycobacterium tuberculosis growth & development, Quinolines blood, Quinolines pharmacokinetics, Tuberculosis, Pulmonary microbiology, ATP Synthetase Complexes antagonists & inhibitors, Antitubercular Agents pharmacology, Bacterial Proteins antagonists & inhibitors, Lung drug effects, Mycobacterium tuberculosis drug effects, Quinolines pharmacology, Tuberculosis, Pulmonary drug therapy

Abstract

TMC207 is a first-in-class diarylquinoline with a new mode of action against mycobacteria targeting the ATP synthase. It is metabolized to an active derivative, N-desmethyl TMC207, and both compounds are eliminated with long terminal half-lives (50 to 60 h in mice) reflecting slow release from tissues such as lung and spleen. In vitro, TMC207 is 5-fold more potent against Mycobacterium tuberculosis than N-desmethyl TMC207, and the effects of the two compounds are additive. The pharmacokinetic and pharmacodynamic (PK-PD) response was investigated in the murine model of tuberculosis (TB) infection following oral administration of different doses of TMC207 or N-desmethyl TMC207 at 5 days per week for 4 weeks starting the day after intravenous infection with M. tuberculosis and following administration of different doses of TMC207 at various dosing frequencies for 6 weeks starting 2 weeks after infection. Upon administration of N-desmethyl TMC207, maximum plasma concentration (C(max)), area under the plasma concentration-time curve from time zero to 168 h postdose (AUC(168h)), and minimum plasma concentration (C(min)) were approximately dose proportional between 8 and 64 mg/kg, and the lung CFU counts were strongly correlated with these pharmacokinetic parameters using an inhibitory sigmoid maximum effect (E(max)) model. Administration of the highest dose (64 mg/kg) produced a 4.0-log(10) reduction of the bacillary load at an average exposure (average concentration [C(avg)] or AUC(168h) divided by 168) of 2.7 μg/ml. Upon administration of the highest dose of TMC207 (50 mg/kg) 5 days per week for 4 weeks, the total reduction of the bacillary load was 4.7 log(10). TMC207 was estimated to contribute to a 1.8-log(10) reduction and its corresponding exposure (C(avg)) was 0.5 μg/ml. Optimal bactericidal activity with N-desmethyl TMC207 was reached at a high exposure compared to that achieved in humans, suggesting a minor contribution of the metabolite to the overall bactericidal activity in TB-infected patients treated with TMC207. Following administration of TMC207 at a total weekly dose of 15, 30, or 60 mg/kg fractionated for either 5 days per week, twice weekly, or once weekly, the bactericidal activity was correlated to the total weekly dose and was not influenced by the frequency of administration. Exposures (AUC(168h)) to TMC207 and N-desmethyl TMC207 mirrored this dose response, indicating that the bactericidal activity of TMC207 is concentration dependent and that AUC is the main PK-PD driver on which dose optimization should be based for dosing frequencies up to once weekly. The PK-PD profile supports intermittent administration of TMC207, in agreement with its slow release from tissues.

Published

2012

33. Pharmacokinetic evaluation of the penetration of antituberculosis agents in rabbit pulmonary lesions.

Author

Kjellsson MC, Via LE, Goh A, Weiner D, Low KM, Kern S, Pillai G, Barry CE 3rd, and Dartois V

Subjects

Animals, Antitubercular Agents blood, Aza Compounds blood, Biological Availability, Disease Models, Animal, Drug Administration Schedule, Female, Fluoroquinolones, Granuloma microbiology, Humans, Isoniazid blood, Isoniazid pharmacokinetics, Lung chemistry, Lung microbiology, Moxifloxacin, Mycobacterium tuberculosis growth & development, Pyrazinamide blood, Pyrazinamide pharmacokinetics, Quinolines blood, Rabbits, Rifampin blood, Rifampin pharmacokinetics, Tissue Extracts chemistry, Tuberculosis, Pulmonary blood, Tuberculosis, Pulmonary microbiology, Antitubercular Agents pharmacokinetics, Aza Compounds pharmacokinetics, Lung drug effects, Mycobacterium tuberculosis drug effects, Quinolines pharmacokinetics, Tuberculosis, Pulmonary drug therapy

Abstract

Standard antituberculosis (anti-TB) therapy requires the use of multiple drugs for a minimum of 6 months, with variable outcomes that are influenced by a number of microbiological, pathological, and clinical factors. This is despite the availability of antibiotics that have good activity against Mycobacterium tuberculosis in vitro and favorable pharmacokinetic profiles in plasma. However, little is known about the distribution of widely used antituberculous agents in the pulmonary lesions where the pathogen resides. The rabbit model of TB infection was used to explore the hypothesis that standard drugs have various abilities to penetrate lung tissue and lesions and that adequate drug levels are not consistently reached at the site of infection. Using noncompartmental and population pharmacokinetic approaches, we modeled the rate and extent of distribution of isoniazid, rifampin, pyrazinamide, and moxifloxacin in rabbit lung and lesions. Moxifloxacin reproducibly showed favorable partitioning into lung and granulomas, while the exposure of isoniazid, rifampin, and pyrazinamide in lesions was markedly lower than in plasma. The extent of penetration in lung and lesions followed different trends for each drug. All four agents distributed rapidly from plasma to tissue with equilibration half-lives of less than 1 min to an hour. The models adequately described the plasma concentrations and reasonably captured actual lesion concentrations. Though further refinement is needed to accurately predict the behavior of these drugs in human subjects, our results enable the integration of lesion-specific pharmacokinetic-pharmacodynamic (PK-PD) indices in clinical trial simulations and in in vitro PK-PD studies with M. tuberculosis.

Published

2012

34. Pharmacokinetics of dihydroartemisinin and piperaquine in pregnant and nonpregnant women with uncomplicated falciparum malaria.

Author

Rijken MJ, McGready R, Phyo AP, Lindegardh N, Tarning J, Laochan N, Than HH, Mu O, Win AK, Singhasivanon P, White N, and Nosten F

Subjects

Adult, Antimalarials therapeutic use, Area Under Curve, Artemisinins therapeutic use, Drug Administration Schedule, Drug Therapy, Combination, Female, Half-Life, Humans, Pregnancy, Pregnancy Outcome, Quinolines therapeutic use, Thailand, Young Adult, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Malaria, Falciparum drug therapy, Pregnancy Complications, Parasitic drug therapy, Quinolines pharmacokinetics

Abstract

Dihydroartemisinin-piperaquine is a fixed-dose artemisinin-based combination treatment. Some antimalarials have altered pharmacokinetics in pregnancy. Pregnant women in the 2nd or 3rd trimester and matched nonpregnant women with uncomplicated falciparum malaria were treated with a total of 6.4 mg/kg of body weight dihydroartemisinin and 51.2 mg/kg piperaquine once daily for 3 days. Venous blood samples were drawn at prespecified time points over 9 weeks. Plasma dihydroartemisinin and piperaquine concentrations were analyzed by liquid chromatography-mass spectrometry. Piperaquine and dihydroartemisinin pharmacokinetics were well described. There were no significant differences in total piperaquine exposure (P = 0.80) or drug exposure during the terminal elimination phase (72 h to infinity) (P = 0.64) between the two groups. The apparent volume of distribution of piperaquine was significantly smaller (602 liters/kg versus 877 liters/kg) in pregnant women than in nonpregnant women (P = 0.0057), and the terminal elimination half-life was significantly shorter (17.8 days versus 25.6 days; P = 0.0023). Dihydroartemisinin exposure after the first dose was significantly lower (844 h × ng/ml versus 1,220 h × ng/ml, P = 0.0021) in pregnant women, but there were no significant differences in total dihydroartemisinin exposure or maximum concentrations between the two groups. There were no significant differences in any pharmacokinetic parameters between the second and third trimester. These results obtained through noncompartmental analysis suggest that in the treatment of falciparum malaria, there are no clinically important differences in the pharmacokinetics of dihydroartemisinin or piperaquine between pregnant and nonpregnant women. However, a more detailed analysis using population pharmacokinetic modeling is needed to fully investigate the differences found for some of the pharmacokinetic parameters, such as the terminal half-life.

Published

2011

35. Pharmacokinetic/pharmacodynamic (PK/PD) indices of antibiotics predicted by a semimechanistic PKPD model: a step toward model-based dose optimization.

Author

Nielsen EI, Cars O, and Friberg LE

Subjects

Anti-Bacterial Agents administration & dosage, Anti-Bacterial Agents therapeutic use, Area Under Curve, Aza Compounds pharmacokinetics, Aza Compounds pharmacology, Cefuroxime pharmacokinetics, Cefuroxime pharmacology, Computer Simulation, Erythromycin pharmacokinetics, Erythromycin pharmacology, Fluoroquinolones, Gentamicins pharmacokinetics, Gentamicins pharmacology, Humans, Microbial Sensitivity Tests, Moxifloxacin, Penicillin G pharmacokinetics, Penicillin G pharmacology, Quinolines pharmacokinetics, Quinolines pharmacology, Vancomycin pharmacokinetics, Vancomycin pharmacology, Anti-Bacterial Agents pharmacokinetics, Anti-Bacterial Agents pharmacology, Escherichia coli drug effects, Streptococcus pyogenes drug effects

Abstract

A pharmacokinetic-pharmacodynamic (PKPD) model that characterizes the full time course of in vitro time-kill curve experiments of antibacterial drugs was here evaluated in its capacity to predict the previously determined PK/PD indices. Six drugs (benzylpenicillin, cefuroxime, erythromycin, gentamicin, moxifloxacin, and vancomycin), representing a broad selection of mechanisms of action and PK and PD characteristics, were investigated. For each drug, a dose fractionation study was simulated, using a wide range of total daily doses given as intermittent doses (dosing intervals of 4, 8, 12, or 24 h) or as a constant drug exposure. The time course of the drug concentration (PK model) as well as the bacterial response to drug exposure (in vitro PKPD model) was predicted. Nonlinear least-squares regression analyses determined the PK/PD index (the maximal unbound drug concentration [fC(max)]/MIC, the area under the unbound drug concentration-time curve [fAUC]/MIC, or the percentage of a 24-h time period that the unbound drug concentration exceeds the MIC [fT(>MIC)]) that was most predictive of the effect. The in silico predictions based on the in vitro PKPD model identified the previously determined PK/PD indices, with fT(>MIC) being the best predictor of the effect for β-lactams and fAUC/MIC being the best predictor for the four remaining evaluated drugs. The selection and magnitude of the PK/PD index were, however, shown to be sensitive to differences in PK in subpopulations, uncertainty in MICs, and investigated dosing intervals. In comparison with the use of the PK/PD indices, a model-based approach, where the full time course of effect can be predicted, has a lower sensitivity to study design and allows for PK differences in subpopulations to be considered directly. This study supports the use of PKPD models built from in vitro time-kill curves in the development of optimal dosing regimens for antibacterial drugs.

Published

2011

36. A small amount of fat does not affect piperaquine exposure in patients with malaria.

Author

Annerberg A, Lwin KM, Lindegardh N, Khrutsawadchai S, Ashley E, Day NP, Singhasivanon P, Tarning J, White NJ, and Nosten F

Subjects

Adolescent, Adult, Aged, Artemisinins blood, Artemisinins pharmacokinetics, Chromatography, Liquid, Dietary Fats administration & dosage, Female, Humans, Malaria, Falciparum blood, Male, Middle Aged, Quinolines blood, Quinolines pharmacokinetics, Tandem Mass Spectrometry, Young Adult, Artemisinins therapeutic use, Dietary Fats adverse effects, Malaria, Falciparum drug therapy, Quinolines therapeutic use

Abstract

Dihydroartemisinin-piperaquine is a new, highly effective, and well-tolerated combination treatment for uncomplicated falciparum malaria. The lipophilic characteristic of piperaquine suggests that administration together with fat will increase the oral bioavailability of the drug, and this has been reported for healthy volunteers. This pharmacokinetic study monitored 30 adult patients with uncomplicated falciparum malaria for 4.5 months to evaluate the effects of the concomitant intake of fat on the total piperaquine exposure. The fixed-drug combination of dihydroartemisinin-piperaquine was given with water to fasting patients (n = 15) or was coadministered with 200 ml milk containing 6.4 g fat (n = 15). The drug combination was generally well tolerated, and there were no severe adverse effects reported for either group during the study. Total piperaquine exposure (area under the concentration-time curve from zero to infinity [AUC(0-∞)]; results are given as medians [ranges]) were not statistically different between fed (29.5 h · μg/ml [20.6 to 58.7 h · μg/ml]) and fasting (23.9 h · μg/ml [11.9 to 72.9 h · μg/ml]) patients, but the interindividual variation was reduced in the fed group. Overall, none of the pharmacokinetic parameters differed statistically between the groups. Total piperaquine exposure correlated well with the day 7 concentrations in the fasted group, but the fed group showed a poor correlation. In conclusion, the coadministration of 6.4 g fat did not have any significant effect on piperaquine pharmacokinetics in the treatment of uncomplicated malaria.

Published

2011

37. Effect of administration of moxifloxacin plus rifampin against Mycobacterium tuberculosis for 7 of 7 days versus 5 of 7 days in an in vitro pharmacodynamic system.

Author

Drusano GL, Sgambati N, Eichas A, Brown D, Kulawy R, and Louie A

Subjects

Antitubercular Agents pharmacokinetics, Antitubercular Agents pharmacology, Aza Compounds pharmacokinetics, Aza Compounds pharmacology, Colony Count, Microbial, Fluoroquinolones, Humans, Microbial Sensitivity Tests methods, Moxifloxacin, Mutation, Quinolines pharmacokinetics, Quinolines pharmacology, Rifampin pharmacokinetics, Rifampin pharmacology, Selection, Genetic, Time Factors, Antitubercular Agents administration & dosage, Aza Compounds administration & dosage, Drug Resistance, Bacterial drug effects, Mycobacterium tuberculosis drug effects, Quinolines administration & dosage, Rifampin administration & dosage

Abstract

Unlabelled: Some trials administered antituberculosis agents for 5 of 7 days (5/7-day regimen) to optimize adherence. Since moxifloxacin has a longer half-life than rifampin, rifampin concentrations are <1% of the maximum concentration in serum (C(max)) on day 6 and nondetectable on day 7, while concentrations of moxifloxacin remain and are able to induce error-prone replication. We determined if functional moxifloxacin monotherapy for 24 h/week caused resistance. In in vitro pharmacodynamic experiments, Mycobacterium tuberculosis was treated with mean area under the concentration-time curve (AUC) exposures for moxifloxacin and rifampin of 400 and 600 mg/kg/day and exposures equal to 1 standard deviation (SD) above and below the mean values. The drugs were administered on schedules of 7/7 days and 5/7 days. Over the 28-day experiments, bacteria were plated onto antibiotic-free agar to determine the effects of exposure and schedule on the total population. MICs were checked for emergence of resistance. At days 7 and 14, there was a 0.56- to 1.22-log(10)-CFU/ml greater cell kill with the 7/7-day regimen versus the 5/7-day regimen (low exposure). This difference was not seen for the larger exposures at day 21. At day 23, the low-exposure 5/7-day arm had breakthrough resistance, with the total count increasing to >2 log(10) CFU/ml above the low-exposure 7/7-day arm. Pharmacokinetic mismatching of drugs in the therapy of tuberculosis may result in emergence of resistance when a drug holiday is imposed during which there is functional monotherapy and where the remaining agent induces error-prone replication. This is particularly true for the portion of the population where the clearance is higher (1 SD above the mean)., Importance: Directly observed therapy is a cornerstone of treatment of Mycobacterium tuberculosis. Patients are often given a drug holiday to facilitate the direct observation of therapy. With rifampin and moxifloxacin, there is a discordance between the half-lives of these agents (1.9 versus 6.5 h when employed in combination). In addition, moxifloxacin induces error-prone replication in Mycobacterium tuberculosis. In this experiment, we demonstrate that the drug holiday (5 of 7 days of therapy [5/7-day regimen]) allows the emergence of resistance to moxifloxacin, which was not seen with 7/7-day therapy. If drug holidays are used, it is imperative to better match pharmacokinetics to minimize the risk of emergence of resistance.

Published

2011

38. Predicting in vitro antibacterial efficacy across experimental designs with a semimechanistic pharmacokinetic-pharmacodynamic model.

Author

Nielsen EI, Cars O, and Friberg LE

Subjects

Aza Compounds pharmacokinetics, Aza Compounds pharmacology, Cefuroxime pharmacokinetics, Cefuroxime pharmacology, Erythromycin pharmacokinetics, Erythromycin pharmacology, Fluoroquinolones, Microbial Sensitivity Tests, Moxifloxacin, Penicillin G pharmacokinetics, Penicillin G pharmacology, Quinolines pharmacokinetics, Quinolines pharmacology, Streptococcus pyogenes drug effects, Streptococcus pyogenes metabolism, Vancomycin pharmacokinetics, Vancomycin pharmacology, Anti-Bacterial Agents pharmacokinetics, Anti-Bacterial Agents pharmacology

Abstract

We have previously described a general semimechanistic pharmacokinetic-pharmacodynamic (PKPD) model that successfully characterized the time course of antibacterial effects seen in bacterial cultures when exposed to static concentrations of five antibacterial agents of different classes. In this PKPD model, the total bacterial population was divided into two subpopulations, one growing drug-susceptible population and one resting drug-insensitive population. The drug effect was included as an increase in the killing rate of the drug-susceptible bacteria with a maximum-effect (E(max)) model. The aim of the present study was to evaluate the ability of this PKPD model to describe and predict data from in vitro experiments with dynamic concentration-time profiles. Dynamic time-kill curve experiments were performed by using an in vitro kinetic system, where cultures of Streptococcus pyogenes were exposed to benzylpenicillin, cefuroxime, erythromycin, moxifloxacin, or vancomycin using different starting concentrations (2 and 16 times the MIC) and elimination conditions (human half-life, reduced half-life, and constant concentrations). The PKPD model was applied, and the observations for the static as well as dynamic experiments were compared to model predictions based on parameter estimation using (i) static data, (ii) dynamic data, and (iii) combined static and dynamic data. Differences in experimental settings between static and dynamic experiments did not affect the growth kinetics of the bacteria significantly. With parameter reestimation, the structure of our previously proposed PKPD model could well characterize the bacterial growth and killing kinetics when exposed to dynamic concentrations with different elimination rates of all five investigated antibiotics. Furthermore, the model with parameter estimates based on data from only the static time-kill curve experiments could predict the majority of the time-kill curves from the dynamic experiments reasonably well. Adding data from dynamic experiments in the estimation improved the model fit for cefuroxime and vancomycin, indicating some differences in sensitivity to experimental conditions among the antibiotics studied.

Published

2011

39. Contrasting effects of acidic pH on the extracellular and intracellular activities of the anti-gram-positive fluoroquinolones moxifloxacin and delafloxacin against Staphylococcus aureus.

Author

Lemaire S, Tulkens PM, and Van Bambeke F

Subjects

Animals, Anti-Infective Agents chemistry, Anti-Infective Agents pharmacokinetics, Aza Compounds chemistry, Aza Compounds pharmacokinetics, Cell Line, Culture Media chemistry, Fluoroquinolones chemistry, Fluoroquinolones pharmacokinetics, Humans, Hydrogen-Ion Concentration, Macrophages metabolism, Mice, Microbial Sensitivity Tests, Models, Biological, Monocytes microbiology, Moxifloxacin, Quinolines chemistry, Quinolines pharmacokinetics, Staphylococcal Infections microbiology, Staphylococcus aureus metabolism, Anti-Infective Agents pharmacology, Aza Compounds pharmacology, Fluoroquinolones pharmacology, Monocytes metabolism, Quinolines pharmacology, Staphylococcus aureus drug effects

Abstract

In contrast to currently marketed fluoroquinolones, which are zwitterionic, delafloxacin is an investigational fluoroquinolone with an anionic character that is highly active against Gram-positive bacteria. We have examined the effect of acidic pH on its accumulation in Staphylococcus aureus and in human THP-1 cells, in parallel with its activity against extracellular and intracellular S. aureus. Moxifloxacin was used as a comparator. Delafloxacin showed MICs 3 to 5 log(2) dilutions lower than those of moxifloxacin for a collection of 35 strains with relevant resistance mechanisms and also proved to be 10-fold more potent against intracellular S. aureus ATCC 25923. In medium at pH 5.5, this difference was further enhanced, with the MIC decreasing by 5 log(2) dilutions. In infected cells incubated in acidic medium, the relative potency was 10-fold higher than that at neutral pH and the maximal relative efficacy reached a bactericidal effect at 24 h. These results can be explained by a 10-fold increase in delafloxacin accumulation in both bacteria and cells at acidic pH, making delafloxacin one of the most efficient drugs tested in this model. Opposite effects were seen for moxifloxacin with respect to both activity and accumulation. As reported for zwitterionic fluoroquinolones, delafloxacin was found associated with the soluble fraction in homogenates of eukaryotic cells. Taken together, these properties may confer to delafloxacin an advantage for the eradication of S. aureus in acidic environments, including intracellular infections.

Published

2011

40. Should moxifloxacin be used for the treatment of extensively drug-resistant tuberculosis? An answer from a murine model.

Author

Poissy J, Aubry A, Fernandez C, Lott MC, Chauffour A, Jarlier V, Farinotti R, and Veziris N

Subjects

Animals, Antitubercular Agents pharmacokinetics, Aza Compounds pharmacokinetics, DNA Gyrase genetics, Enoxacin therapeutic use, Fluoroquinolones therapeutic use, Gatifloxacin, Mice, Microbial Sensitivity Tests, Moxifloxacin, Mutation, Mycobacterium tuberculosis genetics, Ofloxacin therapeutic use, Quinolines pharmacokinetics, Tuberculosis microbiology, Tuberculosis, Multidrug-Resistant genetics, Antitubercular Agents therapeutic use, Aza Compounds therapeutic use, Mycobacterium tuberculosis drug effects, Quinolines therapeutic use, Tuberculosis, Multidrug-Resistant drug therapy

Abstract

The prevalence of extensively drug-resistant tuberculosis (XDR-TB), defined as TB that is resistant to isoniazid, rifampin, fluoroquinolones, and aminoglycosides, is rising worldwide. The extent of Mycobacterium tuberculosis resistance to fluoroquinolones depends on the mutation in the DNA gyrase, the only target of fluoroquinolones. The MIC of moxifloxacin, the most active fluoroquinolone against M. tuberculosis, may be lower than its peak serum level for some ofloxacin-resistant strains of Mycobacterium tuberculosis. Therefore, if the MIC of moxifloxacin is lower than its peak serum level, it may be effective against XDR-TB. Our objective was to determine the efficacy of moxifloxacin in treating ofloxacin-resistant TB. We selected isogenic fluoroquinolone-resistant mutants of M. tuberculosis H37Rv in vivo. We infected Swiss mice with either wild-type H37Rv or one of three mutant strains with different MICs that are commonly seen in clinical practice. The MICs of the mutant strains ranged from below to above the peak moxifloxacin level seen in humans (3 μg/ml). Each mouse was treated with one of four moxifloxacin doses for 1 month. Moxifloxacin was effective against mutant strain GyrB D500N, with the lowest MIC (0.5 μg/ml), when the standard dose was doubled. Moxifloxacin reduced mortality in mice infected with mutant strain GyrA A90V with an intermediate MIC (2 μg/ml). However, it had no impact on the mutant strain GyrA D94G with the highest MIC (4 μg/ml). Our study underscores current WHO recommendations to use moxifloxacin when there is resistance to early-generation fluoroquinolones such as ofloxacin, restricting this recommendation to strains with moxifloxacin MICs of less than or equal to 2 μg/ml.

Published

2010

41. Activities of high-dose daptomycin, vancomycin, and moxifloxacin alone or in combination with clarithromycin or rifampin in a novel in vitro model of Staphylococcus aureus biofilm.

Author

Parra-Ruiz J, Vidaillac C, Rose WE, and Rybak MJ

Subjects

Anti-Bacterial Agents pharmacokinetics, Aza Compounds pharmacokinetics, Clarithromycin pharmacokinetics, Daptomycin pharmacokinetics, Fluoroquinolones, Microscopy, Electron, Scanning, Moxifloxacin, Quinolines pharmacokinetics, Rifampin pharmacokinetics, Staphylococcus aureus ultrastructure, Vancomycin pharmacokinetics, Anti-Bacterial Agents pharmacology, Aza Compounds pharmacology, Biofilms drug effects, Clarithromycin pharmacology, Daptomycin pharmacology, Quinolines pharmacology, Rifampin pharmacology, Staphylococcus aureus drug effects, Vancomycin pharmacology

Abstract

Biofilm formation is an important virulence factor that allows bacteria to resist host responses and antibacterial agents. The aim of the study was to assess the in vitro activities of several antimicrobials alone or in combination against two Staphylococcus aureus isolates in a novel pharmacokinetic/pharmacodynamic (PK/PD) model of biofilm for 3 days. One methicillin-susceptible S. aureus strain (SH1000) and one methicillin-resistant S. aureus strain (N315) were evaluated in a modified biofilm reactor with polystyrene coupons. Simulated regimens included vancomycin (VAN) plus rifampin (RIF), moxifloxacin (MOX), and high doses (10 mg/kg of body weight/day) of daptomycin (DAP) alone or combined with RIF or clarithromycin (CLA). Against viable planktonic bacteria (PB) and biofilm-embedded bacteria (BB) of SH1000, neither DAP nor MOX alone was bactericidal. In contrast, the combination of DAP or MOX with CLA significantly increased the activity of the two agents against both PB and BB (P < 0.01), and DAP plus CLA reached the limit of detection at 72 h. Against PB of N315, DAP alone briefly achieved bactericidal activity at 24 h, whereas sustained bactericidal activity was observed at 32 h with VAN plus RIF. Overall, only a minimal reduction was observed with both regimens against BB (<2.8 log(10) CFU/ml). Finally, the combination of DAP and RIF was bactericidal against both PB and BB, achieving the limit of detection at 72 h. In conclusion, we developed a novel in vitro PK/PD model to assess the activities of antimicrobials against mature bacterial biofilm. Combinations of DAP or MOX with CLA were the most effective regimens and may represent promising options to treat persistent infections caused by S. aureus biofilms.

Published

2010

42. Moxifloxacin pharmacokinetics/pharmacodynamics and optimal dose and susceptibility breakpoint identification for treatment of disseminated Mycobacterium avium infection.

Author

Deshpande D, Srivastava S, Meek C, Leff R, Hall GS, and Gumbo T

Subjects

Anti-Bacterial Agents administration & dosage, Area Under Curve, Aza Compounds administration & dosage, Cell Line, Colony Count, Microbial, Fluoroquinolones, Half-Life, Humans, In Vitro Techniques, Microbial Sensitivity Tests, Models, Biological, Monte Carlo Method, Moxifloxacin, Mycobacterium avium-intracellulare Infection metabolism, Mycobacterium avium-intracellulare Infection microbiology, Protein Binding, Quinolines administration & dosage, Anti-Bacterial Agents pharmacokinetics, Anti-Bacterial Agents pharmacology, Aza Compounds pharmacokinetics, Aza Compounds pharmacology, Mycobacterium avium Complex drug effects, Mycobacterium avium-intracellulare Infection drug therapy, Quinolines pharmacokinetics, Quinolines pharmacology

Abstract

Organisms of the Mycobacterium avium-intracellulare complex (MAC) have been demonstrated to be susceptible to moxifloxacin. However, clinical data on how to utilize moxifloxacin to treat disseminated MAC are scanty. In addition, there have been no moxifloxacin pharmacokinetic-pharmacodynamic (PK/PD) studies performed for MAC infection. We utilized an in vitro PK/PD model of intracellular MAC to study moxifloxacin PK/PD for disseminated disease. Moxifloxacin doses, based on a serum half-life of 12 h, were administered, and the 0- to 24-h area under the concentration-time curve (AUC(0-24)) to MIC ratios associated with 1.0 log(10) CFU/ml per week kill and 90% of maximal kill (EC(90)) were identified. The AUC(0-24)/MIC ratio associated with 1.0 log(10) CFU/ml kill was 17.12, and that with EC(90) was 391.56 (r(2) = 0.97). Next, the moxifloxacin MIC distribution in 102 clinical isolates of MAC was identified. The median MIC was 1 to 2 mg/liter. Monte Carlo simulations of 10,000 patients with disseminated MAC were performed to determine the probability that daily moxifloxacin doses of 400 and 800 mg/day would achieve or exceed 1.0 log(10) CFU/ml per week kill or EC(90). Doses of 400 and 800 mg/day achieved the AUC(0-24)/MIC ratio of 17.12 in 64% and 92% of patients, respectively. The critical concentration of moxifloxacin against MAC was identified as 0.25 mg/liter in Middlebrook media. The proposed susceptibility breakpoint means that a larger proportion of clinical isolates is resistant to moxifloxacin prior to therapy. For patients infected with susceptible isolates, however, 800 mg a day should be examined for safety and efficacy for disseminated M. avium disease.

Published

2010

43. Bacterial strain-to-strain variation in pharmacodynamic index magnitude, a hitherto unconsidered factor in establishing antibiotic clinical breakpoints.

Author

MacGowan AP, Reynolds R, Noel AR, and Bowker KE

Subjects

Anti-Bacterial Agents pharmacology, Area Under Curve, Aza Compounds pharmacology, Fluoroquinolones, Humans, Microbial Sensitivity Tests, Models, Theoretical, Moxifloxacin, Quinolines pharmacology, Staphylococcus aureus drug effects, Anti-Bacterial Agents pharmacokinetics, Aza Compounds pharmacokinetics, Quinolines pharmacokinetics

Abstract

Antibiotic pharmacodynamic modeling allows variations in pathogen susceptibility and human pharmacokinetics to be accounted for when considering antibiotic doses, potential bacterial pathogen targets for therapy, and clinical susceptibility breakpoints. Variation in the pharmacodynamic index (area-under-the-concentration curve to 24 h [AUC(24)]/MIC; maximum serum concentration of drug in the serum/MIC; time the serum concentration remains higher than the MIC [T > MIC]) is not usually considered. In an in vitro pharmacokinetic model of infection using a dose-ranging design, we established the relationship between AUC(24)/MIC and the antibacterial effect for moxifloxacin against 10 strains of Staphylococcus aureus. The distributions of AUC(24)/MIC targets for 24-h bacteriostatic effect and 1-log, 2-log, and 3-log drops in bacterial counts were used to calculate potential clinical breakpoint values, and these were compared with those obtained by the more conventional approach of taking a single AUC(24)/MIC target. Consideration of the AUC(24)/MIC as a distribution rather than a single value resulted in a lower clinical breakpoint.

Published

2009

44. ATP synthase inhibition of Mycobacterium avium is not bactericidal.

Author

Lounis N, Gevers T, Van den Berg J, Vranckx L, and Andries K

Subjects

Animals, Diarylquinolines, Female, Mice, Mice, Inbred C57BL, Microbial Sensitivity Tests, Quinolines pharmacokinetics, Antitubercular Agents pharmacology, Enzyme Inhibitors pharmacology, Mycobacterium avium drug effects, Quinolines pharmacology

Abstract

The efficacy of ATP synthase inhibitor TMC207 was assessed in early and late Mycobacterium avium infections in mice. In contrast to what was earlier observed for M. tuberculosis, a bacteriostatic effect was obtained. In vitro, the minimal bactericidal concentration (MBC)/MIC ratio was very high. The MBC was more relevant for assessment of pharmacokinetic/pharmacodynamic relationships than the MIC.

Published

2009

45. Pharmacokinetics and ex vivo pharmacodynamic antimalarial activity of dihydroartemisinin-piperaquine in patients with uncomplicated falciparum malaria in Vietnam.

Author

Nguyen DV, Nguyen QP, Nguyen ND, Le TT, Nguyen TD, Dinh DN, Nguyen TX, Bui D, Chavchich M, and Edstein MD

Subjects

Adolescent, Humans, Male, Middle Aged, Vietnam, Young Adult, Antimalarials pharmacokinetics, Antimalarials therapeutic use, Artemisinins pharmacokinetics, Artemisinins therapeutic use, Malaria, Falciparum drug therapy, Quinolines pharmacokinetics, Quinolines therapeutic use

Abstract

Compared to healthy subjects, malaria patients show a reduction in the mean oral clearance (1.19 versus 5.87 liters/h/kg of body weight) and apparent volume of distribution (1.47 versus 8.02 liters/kg) of dihydroartemisinin in Vietnamese patients following treatment with dihydroartemisinin-piperaquine (Artekin) for uncomplicated Plasmodium falciparum. Dihydroartemisinin is responsible for most of the ex vivo antimalarial activity of dihydroartemisinin-piperaquine.

Published

2009

46. Piperaquine pharmacodynamics and parasite viability in a murine malaria model.

Author

Moore BR, Ilett KF, Page-Sharp M, Jago JD, and Batty KT

Subjects

Animals, Antimalarials therapeutic use, Disease Models, Animal, Male, Mice, Mice, Inbred BALB C, Plasmodium berghei physiology, Quinolines therapeutic use, Antimalarials pharmacokinetics, Antimalarials pharmacology, Malaria drug therapy, Plasmodium berghei drug effects, Quinolines pharmacokinetics, Quinolines pharmacology

Abstract

Piperaquine (PQ) is an important partner drug in antimalarial combination treatments, but the long half-life of PQ raises concerns about drug resistance. Our aim was to investigate the extended antimalarial effect of PQ in a study of drug efficacy, reinoculation outcomes, and parasite viability after the administration of a single dose of PQ in the murine malaria model. Initially, male Swiss mice were inoculated with Plasmodium berghei and at 64 h after parasite inoculation were given PQ phosphate at 90 mg/kg of body weight intraperitoneally. Parasite viability, drug efficacy, reinoculation responses, and parasite resistance were determined at 25, 40, 60, 90, and 130 days after drug administration. At each time point, six mice were reinoculated with 10(7) P. berghei parasites and blood was harvested from another four mice for viability passage into naïve mice (n = 5 for each blood sample) and from another two mice for determination of the plasma PQ concentration. The efficacy study demonstrated that the residual PQ concentrations did not suppress the infection after 25 days. Viable parasites were present up to 90 days after PQ dosing, although only 50% and 25% of the passaged parasites remained viable at 60 and 90 days postdosing, respectively. Viable parasites passaged into the naïve hosts were generally resistant to PQ when they were exposed to the drug for a second time. PQ was found to have a substantial antimalarial effect in this model, and the effect appears to be sufficient for a host immunological response to be established, resulting in the long-term survival of P. berghei-infected mice.

Published

2009

47. Penetration of moxifloxacin into bone evaluated by Monte Carlo simulation.

Author

Landersdorfer CB, Kinzig M, Hennig FF, Bulitta JB, Holzgrabe U, Drusano GL, Sörgel F, and Gusinde J

Subjects

Aged, Anti-Bacterial Agents administration & dosage, Area Under Curve, Aza Compounds administration & dosage, Chromatography, High Pressure Liquid, Female, Femur surgery, Fluoroquinolones, Humans, Male, Microbial Sensitivity Tests, Middle Aged, Moxifloxacin, Quinolines administration & dosage, Staphylococcal Infections microbiology, Staphylococcal Infections prevention & control, Staphylococcus aureus drug effects, Treatment Outcome, Anti-Bacterial Agents pharmacokinetics, Arthroplasty, Replacement, Hip, Aza Compounds pharmacokinetics, Femur metabolism, Monte Carlo Method, Quinolines pharmacokinetics

Abstract

Moxifloxacin is a fluoroquinolone with a broad spectrum of activity and good penetration into many tissues, including bone. Penetration of moxifloxacin into bone has not yet been studied using compartmental modeling techniques. Therefore, we determined the rate and extent of bone penetration by moxifloxacin and evaluated its pharmacodynamic profile in bone via Monte Carlo simulation. Twenty-four patients (10 males, 14 females) undergoing total hip replacement received 400 mg moxifloxacin orally 2 to 7 h prior to surgery. Blood and bone specimens were collected. Bone samples were pulverized under liquid nitrogen by a cryogenic mill, including an internal standard. Drug concentrations were analyzed by high-performance liquid chromatography. We used ADAPT II (results reported), NONMEM, and WinBUGS for pharmacokinetic analysis. Monte Carlo simulation was performed to reverse engineer the necessary area under the free concentration-time curve fAUC(SERUM)/MIC in serum and total AUC(BONE)/MIC in bone for a successful clinical or microbiological outcome. The median (10% to 90% percentile for between-subject variability) of the AUC in bone divided by the AUC in serum (AUC(BONE)/AUC(SERUM)) was 80% (51 to 126%) for cortical bone and 78% (42 to 144%) for cancellous bone. Equilibration between serum and bone was rapid. Moxifloxacin achieved robust (> or = 90%) probabilities of target attainment (PTAs) in serum, cortical bone, and cancellous bone up to MICs of < or = 0.375 mg/liter based on the targets fAUC(SERUM)/MIC > or = 40 and AUC(BONE)/MIC > or = 33. Moxifloxacin showed high bone concentrations and a rapid equilibrium between bone and serum. The favorable PTAs compared to the 90%-inhibitory MIC of Staphylococcus aureus warrant future clinical trials on the effectiveness of moxifloxacin in the treatment of bone infections.

Published

2009

48. P-glycoprotein-mediated transport of moxifloxacin in a Calu-3 lung epithelial cell model.

Author

Brillault J, De Castro WV, Harnois T, Kitzis A, Olivier JC, and Couet W

Subjects

Biological Transport, Cells, Cultured, Dose-Response Relationship, Drug, Epithelial Cells metabolism, Fluoroquinolones, Humans, Moxifloxacin, Rifampin pharmacology, ATP Binding Cassette Transporter, Subfamily B, Member 1 physiology, Anti-Infective Agents pharmacokinetics, Aza Compounds pharmacokinetics, Lung metabolism, Quinolines pharmacokinetics

Abstract

Moxifloxacin (MXF) is a fluoroquinolone antibiotic that is effective against respiratory infections. However, the mechanisms of MXF lung diffusion are unknown. Active transport in other tissues has been suggested for several members of the fluoroquinolone family. In this study, transport of MXF was systematically investigated across a Calu-3 lung epithelial cell model. MXF showed polarized transport, with the secretory permeability being twice as high as the absorptive permeability. The secretory permeability was concentration dependent (apparent P(max) = 13.6 x 10(-6) cm x s(-1); apparent K(m) = 147 microM), suggesting saturated transport at concentrations higher than 350 microg/ml. The P-glycoprotein inhibitor PSC-833 inhibited MXF transport in both directions, whereas probenecid, a multidrug resistance-related protein inhibitor, appeared to have no effect in the Calu-3 model. Moreover, rifampin, a known inducer of efflux transport proteins, upregulated the expression of P-glycoprotein in Calu-3 cells and enhanced MXF active transport. In conclusion, this study clearly indicates that MXF is subject to P-glycoprotein-mediated active transport in the Calu-3 model. This P-glycoprotein-dependent secretion may lead to higher MXF epithelial lining fluid concentrations than those in plasma. Furthermore, drug-drug interactions may be expected when MXF is combined with other P-glycoprotein substrates or modulators.

Published

2009

49. Pharmacokinetics and bioequivalence evaluation of two fixed-dose tablet formulations of dihydroartemisinin and piperaquine in Vietnamese subjects.

Author

Chinh NT, Quang NN, Thanh NX, Dai B, Geue JP, Addison RS, Travers T, and Edstein MD

Subjects

Adult, Antimalarials analysis, Area Under Curve, Artemisinins analysis, Chemistry, Pharmaceutical, Chromatography, Liquid, Cross-Over Studies, Drug Combinations, Half-Life, Humans, Male, Quinolines analysis, Tandem Mass Spectrometry, Therapeutic Equivalency, Antimalarials pharmacokinetics, Artemisinins pharmacokinetics, Quinolines pharmacokinetics

Abstract

The two fixed-dose combinations of dihydroartemisinin and piperaquine (Artekin and Arterakine) were found to be bioinequivalent in healthy Vietnamese subjects. However, because the peak plasma concentrations and areas under the concentration-time curves of dihydroartemisinin and piperaquine were only marginally different between the two formulations, similar therapeutic efficacies are expected in the treatment of malaria infections.

Published

2009

50. Repeated administration of high-dose intermittent rifapentine reduces rifapentine and moxifloxacin plasma concentrations.

Author

Dooley K, Flexner C, Hackman J, Peloquin CA, Nuermberger E, Chaisson RE, and Dorman SE

Subjects

Adult, Antitubercular Agents adverse effects, Antitubercular Agents pharmacokinetics, Aza Compounds adverse effects, Aza Compounds pharmacokinetics, Drug Administration Schedule, Drug Interactions, Drug Therapy, Combination, Drug Tolerance, Female, Fluoroquinolones, Humans, Male, Middle Aged, Moxifloxacin, Quinolines adverse effects, Quinolines pharmacokinetics, Rifampin administration & dosage, Rifampin adverse effects, Rifampin blood, Rifampin pharmacokinetics, Safety, Tuberculosis, Pulmonary blood, Tuberculosis, Pulmonary drug therapy, Young Adult, Antitubercular Agents administration & dosage, Antitubercular Agents blood, Aza Compounds administration & dosage, Aza Compounds blood, Quinolines administration & dosage, Quinolines blood, Rifampin analogs & derivatives

Abstract

Moxifloxacin- and rifapentine-based regimens are under investigation for the treatment of tuberculosis. However, rifapentine may induce enzymes that metabolize moxifloxacin, resulting in decreased moxifloxacin concentrations. In this phase I, two-period, sequential-design study, 13 subjects received 400 mg moxifloxacin daily for 4 days followed by daily moxifloxacin coadministered with 900 mg rifapentine thrice weekly. Pharmacokinetic analyses were performed after the 4th and 19th doses of moxifloxacin and after the 1st and 7th doses of rifapentine. For moxifloxacin, the mean area under the concentration-time curve from 0 to 24 h (AUC(0-24)) decreased by 17.2% (P = 0.0006) when the drug was coadministered with rifapentine, and the mean half-life (t(1/2)) decreased from 11.1 to 8.9 h (P = 0.0033). For rifapentine, the mean AUC(0-48) after seven thrice-weekly doses decreased by 20.3% (P = 0.0035) compared to the AUC(0-48) after the first dose, and the mean t(1/2) decreased from 18.5 to 14.8 h (P = 0.0004). The AUC(0-48) for the 25-desacetyl-rifapentine metabolite diminished 21%. Two days after completing the study drugs, one subject developed a fever and hepatitis, and another developed a flu-like illness with a rash. In conclusion, rifapentine modestly reduced moxifloxacin concentrations. Changes consistent with rifapentine autoinduction of metabolism were seen. Adverse reactions in two subjects may have represented rifamycin hypersensitivity syndrome, although some features were atypical.

Published

2008