ABSTRACT
The European patents for epoetin alpha recently expired. Biosimilars (i.e. "a medicine which is similar to a biological medicine that has already been authorized" [EMEA 2007]) of epoetins have thus been released on the market in Europe. Because of the complexity of the processes that are required to produce medicinal products containing biotechnology-derived proteins as active substances and to characterize the physicochemical properties of these compounds, the guidelines that have been developed for generic drugs cannot be used for approval of biosimilar products. The EMEA guidelines do not answer all questions that have been raised for the development of biosimilars, and in some cases, decisions will have to be taken at a national level. This is why the Society of Nephrology (Société de néphrologie), the French-speaking Society of Dialysis (Société francophone de dialyse) and the Pediatric Society of Nephrology (Société de néphrologie pédiatrique) established guidelines for the usage of biosimilar epoetins concerning approval, identification, substitution of an innovator drug, post-marketing surveillance, extension of indication and pharmacovigilance plan.
Subject(s)
Erythropoietin/analogs & derivatives , Erythropoietin/therapeutic use , Drug Approval , Epoetin Alfa , Europe , Humans , Product Surveillance, Postmarketing , Recombinant ProteinsABSTRACT
Listeriosis is a rare but life-threatening infection. A favorable outcome is greatly aided by early administration of antibiotics with rapid bactericidal activity against Listeria monocytogenes. Moxifloxacin, a new-generation fluoroquinolone with extended activity against gram-positive bacteria, has proved its effectiveness in vitro against intracellular reservoirs of bacteria. The efficacies of moxifloxacin and amoxicillin were compared in vivo by survival curve assays and by studying the kinetics of bacterial growth in blood and organs in a murine model of central nervous system (CNS) listeriosis. We combined pharmacokinetic and pharmacodynamic approaches to correlate the observed efficacy in vivo with plasma and tissue moxifloxacin concentrations. Death was significantly delayed for animals treated with a single dose of moxifloxacin compared to a single dose of amoxicillin. We observed rapid bacterial clearance from blood and organs of animals treated with moxifloxacin. The decrease in the bacterial counts in blood and brain correlated with plasma and cerebral concentrations of antibiotic. Moxifloxacin peaked in the brain at 1.92 +/- 0.32 microg/g 1 hour after intraperitoneal injection. This suggests that moxifloxacin rapidly crosses the blood-brain barrier and diffuses into the cerebral parenchyma. Moreover, no resistant strains were selected during in vivo experiments. Our results indicate that moxifloxacin combines useful pharmacokinetic properties and rapid bactericidal activity and that it may be a valuable alternative for the treatment of CNS listeriosis.
Subject(s)
Anti-Infective Agents/therapeutic use , Aza Compounds/therapeutic use , Brain Diseases , Central Nervous System Bacterial Infections , Listeria monocytogenes/drug effects , Listeriosis , Quinolines/therapeutic use , Animals , Anti-Infective Agents/administration & dosage , Anti-Infective Agents/pharmacology , Aza Compounds/administration & dosage , Aza Compounds/pharmacology , Brain/microbiology , Brain Diseases/drug therapy , Brain Diseases/microbiology , Central Nervous System Bacterial Infections/drug therapy , Central Nervous System Bacterial Infections/microbiology , Disease Models, Animal , Fluoroquinolones , Listeriosis/drug therapy , Listeriosis/microbiology , Mice , Moxifloxacin , Quinolines/administration & dosage , Quinolines/pharmacology , Time Factors , Treatment OutcomeABSTRACT
OBJECTIVE: To investigate a potential pharmacokinetic interaction between mycophenolate mofetil (MMF) and aciclovir or valaciclovir. STUDY DESIGN AND PARTICIPANTS: Fifteen healthy subjects were enrolled in a prospective, randomised, open-label, single-dose, cross-over study conducted at a single centre. Subjects received each of the following five oral treatments: (i) aciclovir 800 mg alone; (ii) valaciclovir 2 g alone; (iii) MMF 1 g alone; (iv) valaciclovir 2 g + MMF 1 g; and (v) aciclovir 800 mg + MMF 1 g. The following pharmacokinetic parameters were estimated for aciclovir, mycophenolic acid (MPA) and its inactive glucuronide metabolite (MPAG) from the plasma concentration-time data using noncompartmental methods: area under the concentration-time curve from zero to infinity (AUC infinity), terminal elimination half-life (t1/2z), peak concentration (Cmax) and time to Cmax (tmax). The renal clearance (CLR) of aciclovir was also calculated. These parameters were compared when aciclovir or valaciclovir were coadministered with MMF relative to aciclovir, valaciclovir or MMF given alone. RESULTS AND DISCUSSION: Aciclovir Cmax, tmax and AUC infinity were significantly increased by 40%, 0.38 hour and 31%, respectively, following coadministration of aciclovir and MMF, whereas aciclovir t1/2z was significantly decreased by 11%. Following coadministration of valaciclovir and MMF, aciclovir pharmacokinetic parameters were not significantly modified except for tmax (about 0.5 hour shorter with MMF). MPA and MPAG pharmacokinetic parameters were not significantly modified following coadministration of MMF with valaciclovir or aciclovir except for MPAG AUC infinity, which was decreased by 12% with valaciclovir. Our results are similar to those reported in the literature, except for MPAG AUC. In urine, following coadministration of aciclovir and MMF, aciclovir CLR was significantly decreased by 19%. Competition between MPAG and aciclovir for renal tubular secretion could partly explain this phenomenon. Following coadministration of valaciclovir and MMF, aciclovir CLR was not significantly modified. CONCLUSION: In healthy subjects, interactions are observed after coadministration of MMF and aciclovir, but the extent of the interactions is unlikely to be of clinical significance. These interactions should be investigated in patients with abnormal renal function.
Subject(s)
Acyclovir/analogs & derivatives , Acyclovir/pharmacology , Acyclovir/pharmacokinetics , Antiviral Agents/pharmacology , Antiviral Agents/pharmacokinetics , Immunosuppressive Agents/pharmacology , Immunosuppressive Agents/pharmacokinetics , Mycophenolic Acid/analogs & derivatives , Mycophenolic Acid/pharmacology , Mycophenolic Acid/pharmacokinetics , Valine/analogs & derivatives , Valine/pharmacology , Valine/pharmacokinetics , Adult , Area Under Curve , Chromatography, Liquid , Cross-Over Studies , Drug Interactions , Glucuronides/metabolism , Half-Life , Humans , Male , Middle Aged , ValacyclovirABSTRACT
1. Mefloquine is a chiral neurotoxic antimalarial agent showing stereoselective brain uptake in humans and rats. It is a substrate and an inhibitor of the efflux protein P-glycoprotein. 2. We investigated the stereoselective uptake and efflux of mefloquine in mice, and the consequences of the combination with an efflux protein inhibitor, elacridar (GF120918) on its brain transport. 3. Racemic mefloquine (25 mg kg(-1)) was administered intraperitoneally with or without elacridar (10 mg kg(-1)). Six to seven mice were killed at each of 11 time-points between 30 min and 168 h after administration. Blood and brain concentrations of mefloquine enantiomers were determined using liquid chromatography. 4. A three-compartment model with zero-order absorption from the injection site was found to best represent the pharmacokinetics of both enantiomers in blood and brain. (-)Mefloquine had a lower blood and brain apparent volume of distribution and a lower efflux clearance from the brain, resulting in a larger brain/blood ratio compared to (+)mefloquine. Elacridar did not modify blood concentrations or the elimination rate from blood for either enantiomers. However, cerebral AUC(inf) of both enantiomers were increased, with a stronger effect on (+)mefloquine. The efflux clearance from the brain decreased for both enantiomers, with a larger decrease for (+)mefloquine. 5. After administration of racemic mefloquine in mice, blood and brain pharmacokinetics are stereoselective, (+)mefloquine being excreted from brain more rapidly than its antipode, showing that mefloquine is a substrate of efflux proteins and that mefloquine enantiomers undergo efflux in a stereoselective manner. Moreover, pretreatment with elacridar reduced the brain efflux clearances with a more pronounced effect on (+)mefloquine.
Subject(s)
ATP Binding Cassette Transporter, Subfamily B, Member 1/antagonists & inhibitors , ATP Binding Cassette Transporter, Subfamily B, Member 1/pharmacokinetics , Acridines/pharmacokinetics , Brain/metabolism , Mefloquine/pharmacokinetics , Stereoisomerism , Tetrahydroisoquinolines/pharmacokinetics , ATP Binding Cassette Transporter, Subfamily B, Member 1/administration & dosage , Acridines/administration & dosage , Acridines/chemistry , Animals , Area Under Curve , Blood-Brain Barrier/chemistry , Blood-Brain Barrier/drug effects , Blood-Brain Barrier/metabolism , Female , Injections, Intraperitoneal , Mefloquine/administration & dosage , Mefloquine/chemistry , Metabolic Clearance Rate/drug effects , Metabolic Clearance Rate/physiology , Mice , Tetrahydroisoquinolines/administration & dosage , Time FactorsABSTRACT
Moxifloxacin is a broad-spectrum antibacterial 8-methoxy-fluoroquinolone. In order to evaluate the pharmacokinetic properties of moxifloxacin in mouse plasma and brain tissue, we developed a high-performance liquid chromatography (HPLC) method. This study was based on single-drug delivery, intravenously dosed in a central listeriosis murine model. The method employed a reversed-phase Lichrospher RP-18 with a precolumn (250 × 4.6 mm) and a mobile phase composed of a mixture of acetonitrile, methanol, and citric buffer (pH = 3.5) with sodium dodecyl sulfate and tetrabutylammonium bromide. Fluorescence detection was performed at an excitation wavelength of 290 nm and an emission wavelength of 550 nm. The relative standard deviation of intra- and inter-day assays was <10%. This validated method led to a short retention time (8.0 min) for moxifloxacin. The standard curves were linear from 5-250 µg/L in plasma and from 0.1-2.5 µg/g of brain tissue. The limits of quantification were 5 µg/L in plasma and 0.1 µg/g in brain tissue. The method enabled the detection of systemic antimicrobial in plasma and in CNS in Listeria-infected mice. Injected moxifloxacin passed through the encephalic barrier within a 30 to 60 min after injection time frame. Moxifloxacin pharmacokinetics are modeled in an infected model compared to control mice.
ABSTRACT
Itraconazole is a fungistatic agent that, although highly lipophilic, shows poor transport through the blood brain barrier that may be due to efflux proteins. The combined administration of an efflux inhibitor with itraconazole should increase cerebral itraconazole concentrations and therefore, improve the treatment of Cryptococcus neoformans meningitis with this antifungal agent. To test this hypothesis, we have studied the influence of murine cerebral infection with C. neoformans and the inhibition of efflux by intraperitoneal injection of a P-glycoprotein inhibitor, GF120918 [N-(4-[2-(1,2,3,4-tetrahydro-6,7-dimethoxy-2-isoquinolinyl)-ethyl]-phenyl)9,10-dihydro-5-methoxy-9-oxo-4-acridine carboxamide], on the pharmacokinetics of itraconazole in plasma and brain after a single intraperitoneal itraconazole injection. We also investigated the influence of efflux inhibition on the efficacy of repeated doses of itraconazole in this murine model. The results showed that in healthy and infected mice pretreated or not with GF120918, plasma itraconazole values of area under the curve (AUC) were similar. In contrast, cerebral values of AUC were higher in infected mice compared with healthy mice. Moreover, the pretreatment of infected mice with GF120918 significantly increased cerebral itraconazole values of area under the curve and decreased weight loss in the treatment with itraconazole of a cerebral infection with C. neoformans.
Subject(s)
Antifungal Agents/metabolism , Brain/metabolism , Brain/microbiology , Cryptococcosis/metabolism , Cryptococcus neoformans , Itraconazole/metabolism , Tetrahydroisoquinolines , ATP Binding Cassette Transporter, Subfamily B, Member 1/antagonists & inhibitors , ATP Binding Cassette Transporter, Subfamily B, Member 1/metabolism , Acridines/pharmacology , Animals , Antifungal Agents/antagonists & inhibitors , Antifungal Agents/blood , Brain/drug effects , Cryptococcosis/drug therapy , Cryptococcus neoformans/drug effects , Isoquinolines/pharmacology , Itraconazole/antagonists & inhibitors , Itraconazole/blood , Mice , Mice, Inbred BALB C , Protein Transport/drug effectsABSTRACT
Long-term glucocorticoid treatment contributes to the growth retardation in children after renal transplantation. We investigated whether determination of prednisone (PN) and prednisolone (PL) in plasma and PN, PL, and 6-beta-hydroxyprednisolone (betaOH-PL) in urine could help to predict growth. PN and PL pharmacokinetics were studied in 36 children, from 5 to 15 years of age, receiving daily (D) or alternate-day (AD) oral PN treatment. Statural growth velocity was evaluated over a 1-year period. We compared three groups of children according to the growth kinetics during the study year (catch-up, stable, or decline) for clinical and pharmacokinetic parameters. A multiple linear regression analysis was performed in order to determine pharmacokinetic parameters able to explain height 1 year after inclusion. Height at the beginning of the study, creatinine clearance, and type of D or AD treatment explained 94.2% of height variance 1 year after inclusion. Only PL clearance was associated with growth evolution, but introduction of PL clearance in the multivariate model did not improve the variance of height accounted for by the previous model. We, therefore, do not recommend using glucocorticoid pharmacokinetics to predict growth retardation in children with renal transplantation.
Subject(s)
Glucocorticoids/adverse effects , Glucocorticoids/pharmacokinetics , Growth Disorders/chemically induced , Kidney Transplantation , Prednisolone/adverse effects , Prednisolone/pharmacokinetics , Prednisone/adverse effects , Prednisone/pharmacokinetics , Adolescent , Child , Child, Preschool , HumansABSTRACT
Um comprimido de nifedipina foi administrado a oito homens hipertensos hospitalizados (Estágio I ou II da WHO) com idades na faixa de 45 + ou - 10 anos. Após um teste inicial com placebo, 20, 40 e 60 mg de nifedipina foram administrados às 8:00 da manhä de modo randomizado em intervalos de 72 horas numa única administraçäo em estudo duplo-cego cruzado. A pressäo sangüínea e a freqüência cardíaca foram medidas duas vezes pelo mesmo observador a cada 20 minutos entre 7:00 e 8:00 da manhä e depois de intervalos horários até as 20:00 horas, as leituras sendo feitas primeiro com os pacientes deitados e depois de terem ficado em pé durante um minuto. Os níveis plasmáticos de nifedipina foram analisados em amostras retiradas de hora em hora das 8:00 às 12:00 horas e, a cada duas horas das 12:00 às 20:00 horas e 24 e 48 horas após a ingestäo da droga. Todas três doses reduziram de modo significativo a pressäo sangüínea. Esta reduçäo, na posiçäo deitada era significativamente maior (-18%) e durou mais tempo (12 horas) após a ingestäo de 60 mg do que após a ingestäo de 20 mg (-11% em 7 horas). As três doses causaram aumentos semelhantes na freqüência cardíaca (+29% a +38%), ocorrendo o aumento máximo em duas horas e durando 5 horas. O pico de concentraçöes plasmáticas e as áreas sob a curva de concentraçäo plasmática versus tempo foram dose-dependentes. A cinética foi linear entre 20 e 60 mg e a meia-vida dos comprimidos de nifedipina foi de cerca de 10 horas. A diminuiçäo da pressäo sangüínea arterial média apresentou forte correlaçäo com os níveis plasmáticos de nifedipina (r = 0,61; n = 190; p < 0,001). Quatro pacientes sentiram efeitos colaterais leves (cefaléias, rubores, sonolência ou fraqueza). A formulaçäo dos comprimidos de nifedipina apresentou potente açäo anti-hipertensiva que durou mais tempo que a formulaçäo em cápsulas