Your search keyword '"Farinotti, R."' showing total 598 results

251. Chronic administration of verapamil, ketoconazole and carbamazepine: impact on immunological parameters.

Author

Bonhomme-Faivre L, Forestier F, Auchère D, Soursac M, Orbach-Arbouys S, and Farinotti R

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Animals, Blood Cell Count, Body Weight drug effects, Cytochrome P-450 Enzyme System metabolism, Immunity, Cellular drug effects, Male, Mice, Monocytes drug effects, Anticonvulsants pharmacology, Antifungal Agents pharmacology, Calcium Channel Blockers pharmacology, Carbamazepine pharmacology, Immunity drug effects, Ketoconazole pharmacology, Verapamil pharmacology

Abstract

Inhibitors of P-glycoprotein (P-gp) (verapamil) or cytochrome P-450 (ketoconazole) may reduce IL2 production and T lymphocyte proliferation in vitro. We have examined the effects of chronic oral administration of these drugs and of the cytochrome P450 inductor, carbamazepine, on the hematological and immunological parameters of mice. We found no changes after giving the mice 0.12 mg verapamil, 0.85 mg ketoconazole, or 0.514 mg carbamazepine per mouse for 4 weeks (5 days/week). But giving the drugs for an additional 7 weeks at 0.6 mg (verapamil), 4.25 mg (ketoconazole) or 2.57 mg/mouse (carbamazepine), resulted in significant decreases in monocytes in the verapamil treated group (-51%) and in CD4+ cells in the carbamazepine group (-35%). Chronic oral administration of these drugs reduced the lymphocyte counts of mice by 10-18% and their NK counts by 10-16%. These changes could be due to changes in P-gp function in the transport of IL2, with decreases caused by verapamil and ketoconazole.

Published

2002

252. Stereoselective distribution and stereoconversion of zopiclone enantiomers in plasma and brain tissues in rats.

Author

Fernandez C, Alet P, Davrinche C, Adrien J, Thuillier A, Farinotti R, and Gimenez F

Subjects

Administration, Oral, Animals, Area Under Curve, Azabicyclo Compounds, Chromatography, High Pressure Liquid, Hypnotics and Sedatives blood, Male, Piperazines blood, Rats, Rats, Sprague-Dawley, Stereoisomerism, Tissue Distribution, Brain metabolism, Hypnotics and Sedatives pharmacokinetics, Piperazines pharmacokinetics

Abstract

Concentrations of (-)-zopiclone and (+)-zopiclone were determined in plasma and brain after oral administration, to investigate the stereoselectivity of distribution in rats. Zopiclone enantiomers were administered separately to rats and concentrations were determined by chiral HPLC in plasma and brain. In initial experiments, rats were treated with urethane before cannulation for blood sampling but as this drug modified zopiclone pharmacokinetics, it was not used in subsequent studies. This study showed that zopiclone pharmacokinetics after oral gavage in rats are stereoselective. After oral administration of (+)-zopiclone, no stereoconversion was observed in plasma. Conversely, after administration of (-)-zopiclone, both enantiomers were found in plasma and brain with (+)-zopiclone/(-)-zopiclone ratios of 1 and 8.4 in plasma and brain, respectively. Our findings suggest that zopiclone undergoes stereoconversion and that it is stereospecifically distributed to the brain.

Published

2002

253. Recombinant interleukin-2 treatment decreases P-glycoprotein activity and paclitaxel metabolism in mice.

Author

Bonhomme-Faivre L, Pelloquin A, Tardivel S, Urien S, Mathieu MC, Castagne V, Lacour B, and Farinotti R

Subjects

Animals, Blotting, Western, Digoxin pharmacokinetics, Down-Regulation, Humans, Immunotherapy, Injections, Intraperitoneal, Male, Mice, Recombinant Proteins pharmacology, Tissue Distribution, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Antineoplastic Agents, Phytogenic pharmacokinetics, Interleukin-2 pharmacology, Paclitaxel pharmacokinetics

Abstract

Recombinant rIL-2 was reported to be able to decrease P-glycoprotein (P-gp) expression in cultured cells from human colon carcinoma. P-gp is considered an important factor in the control of Taxol efflux from tumor cells. Based on the premise that Taxol pharmacokinetic parameters could be modified as a result of diminished P-gp expression induced by recombinant interleukin (rIL)-2 and that this might elicit an interaction between the two drugs, we evaluated the pharmacokinetics of a novel strategy combining i.p. immunotherapy with rIL-2 and a cytotoxic agent, Taxol. Mice were allocated to two groups treated with rIL-2 (15 microg x 2/day from day 1 to 4) then Taxol (10 mg/kg i.p. day 5) or Taxol (10 mg/kg i.p.) alone (control group). The Taxol + rIL-2 combination provoked the development of ascites, presumably due to the presence of Cremophor EL in the Taxol preparation. Paclitaxel was measured in plasma and ascites by HPLC with UV detection. Paclitaxel pharmacokinetics were strongly modified by rIL-2 pretreatment. Compared to that observed in control mice, the apparent volume of distribution increased dramatically (Vd/F = 18.2 versus 4.1 l/kg) and the apparent plasma clearance decreased (Cl/F = 1.12 versus 1.66 l/h/kg). P-gp expression was determined in the liver, lung, intestine, brain and kidney in the two groups by immunodetection with the C219 anti-P-gp monoclonal antibody. A significant decrease in P-gp expression was observed in the intestine and in the brain in the rIL-2-pretreated mice as compared to controls. To study the functionality of P-gp, we compared digoxin (a model P-gp substrate) pharmacokinetics before and after pretreatment with rIL-2 (10 microg x 2/day from day 1 to 4), after a single 1 microg oral dose of digoxin used to quantify P-gp activity. Results showed a decrease in oral digoxin clearance after rIL-2 pretreatment indicating modified P-gp activity. We conclude that rIL-2 pretreatment is able to decrease P-gp activity and paclitaxel metabolism in vivo. This is the first study to demonstrate a decrease in P-gp activity and expression in organs such as the brain in vivo. A novel strategy combining immunotherapy with rIL-2 and a cytotoxic agent could potentially improve clinical results, particularly in brain cancer.

Published

2002

254. Determination of N-acetylation phenotype using caffeine as a metabolic probe and high-performance liquid chromatography with either ultraviolet detection or electrospray mass spectrometry.

Author

Baud-Camus F, Marquet P, Soursac M, Davrinche C, and Farinotti R

Subjects

Acetylation, HIV Infections metabolism, Humans, Phenotype, Reproducibility of Results, Caffeine urine, Chromatography, High Pressure Liquid methods, Spectrometry, Mass, Electrospray Ionization methods, Spectrophotometry, Ultraviolet methods

Abstract

A rapid, sensitive method using liquid chromatography-electrospray mass spectrometry (LC-ES-MS) was developed and evaluated for the simultaneous quantitative determination of caffeine metabolites 1U, 1X and AAMU in human urine. This method involved a simple dilution of urine samples. The chromatographic separation was achieved on a C18 reversed-phase column using a gradient of acetonitrile in 2 mM, pH 3.0 ammonium formate as mobile phase. After ionisation in an electrospray source, mass spectrometric detection was performed in the negative ion, selected ion monitoring mode. This method yielded acceptable accuracy and precision within the range 0.25-50 microg/ml. This analytical method was applied to investigate the N-acetylator phenotype of HIV-infected patients and compared with high-performance liquid chromatography with UV detection. Its specificity was better, which appeared to be absolutely necessary to prevent errors in metabolic ratios and phenotype interpretation.

Published

2001

255. Maternal-fetal transfer of saquinavir studied in the ex vivo placental perfusion model.

Author

Forestier F, de Renty P, Peytavin G, Dohin E, Farinotti R, and Mandelbrot L

Subjects

Female, Humans, In Vitro Techniques, Kinetics, Pregnancy, HIV Protease Inhibitors metabolism, Maternal-Fetal Exchange, Placenta metabolism, Saquinavir metabolism

Abstract

Objective: This study was undertaken to determine the placental transfer of the human immunodeficiency virus protease inhibitor saquinavir., Study Design: An ex vivo perfused human placental cotyledon model was used. Ten placental perfusion studies were performed, with concentrations of saquinavir in the maternal compartment ranging from 322 to 2197 ng/mL (within reference therapeutic ranges). Drug concentrations were determined by high-performance liquid chromatography., Results: The mean (+/- SD) fetal transfer rate of saquinavir was 1.8% +/- 1.6%, and the mean (+/- SD) clearance index was 0.05 +/- 0.05. A mean (+/- SD) of 1.6% +/- 3.1% of the perfused saquinavir was retained by the cotyledon. The small amount of saquinavir that crossed the placenta corresponded to the fraction not bound to human serum albumin., Conclusion: The low rate of placental transfer of saquinavir suggests that use of this antiretroviral drug by pregnant women may not lead to significant exposure of the fetus.

Published

2001

256. Intestinal absorption and metabolism of chlorpheniramine enantiomers in rat.

Author

Hiep BT, Fernandez C, Tod M, Banide H, Thuillier A, Lacour B, Farinotti R, and Gimenez F

Subjects

Animals, Chlorpheniramine chemistry, Cyclosporine pharmacology, Histamine H1 Antagonists chemistry, Histamine H1 Antagonists metabolism, Histamine H1 Antagonists pharmacokinetics, In Vitro Techniques, Intestinal Absorption drug effects, Male, Rats, Rats, Wistar, Stereoisomerism, Chlorpheniramine metabolism, Chlorpheniramine pharmacokinetics

Abstract

Chlorpheniramine (CPAM) is a chiral antihistaminic drug commercialized as a racemic mixture. The intestinal absorption and metabolism of CPAM have been investigated in rat using in vivo (oral and IV administration), in situ (intestinal loop model), and in vitro (everted sac model) experiments. Oral and IV administrations of 20 mg/kg of the racemic mixture show that the pharmacokinetics of CPAM are stereoselective, with higher AUCs for the (+)-S-enantiomer compared to its antipode. The monodesmethyl metabolite (DCPM) was quantifiable in blood and its pharmacokinetics are stereoselective after oral but not after IV administration. Experiments using intestinal loops and everted sacs showed that the absorption is not stereoselective and that in vivo stereoselective formation of DCPM is presumably due to stereoselective hepatic metabolism. Moreover, the in vitro and in situ absorption of CPAM are not modified by modulators of P-glycoprotein and cytochromes P450 (cyclosporin A, ketoconazole).

Published

2001

257. Maternal-fetal transfer and amniotic fluid accumulation of lamivudine in human immunodeficiency virus-infected pregnant women.

Author

Mandelbrot L, Peytavin G, Firtion G, and Farinotti R

Subjects

Adult, Anti-HIV Agents therapeutic use, Diffusion, Female, Fetal Blood metabolism, Humans, Kinetics, Lamivudine blood, Lamivudine therapeutic use, Pregnancy, Acquired Immunodeficiency Syndrome drug therapy, Amniotic Fluid metabolism, Anti-HIV Agents pharmacokinetics, Lamivudine pharmacokinetics, Maternal-Fetal Exchange, Pregnancy Complications, Infectious virology

Abstract

Objective: The purpose of this study was to investigate placental transfer and amniotic fluid concentrations of lamivudine in human immunodeficiency virus-infected women who received the agent during pregnancy., Study Design: Mothers in the study were receiving antiretroviral therapy that included lamivudine in a clinical setting. Maternal blood, cord blood, and amniotic fluid samples were obtained simultaneously at the time of delivery from 57 mother-infant pairs., Results: At a median of 8.5 hours after the last maternal oral 150-mg dose of lamivudine, median maternal and fetal plasma concentrations were 302 and 240 ng/mL, respectively. Individual maternal and fetal concentrations were strongly correlated (r2 = 0.36; P < 10(-4)), and their median ratio was about 1. The median concentration in the amniotic fluid was 5 times higher than that in maternal plasma (upper range of ratio, 133)., Conclusion: Lamivudine appeared to cross the placenta by simple diffusion and is concentrated in the amniotic fluid. High amniotic fluid levels of lamivudine may carry both benefits and risks for the child.

Published

2001

258. Interactions of racemic mefloquine and its enantiomers with P-glycoprotein in an immortalised rat brain capillary endothelial cell line, GPNT.

Author

Pham YT, Régina A, Farinotti R, Couraud P, Wainer IW, Roux F, and Gimenez F

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 chemistry, Animals, Caco-2 Cells, Cell Line, Cerebrovascular Circulation, Cyclosporine pharmacology, Endothelium, Vascular metabolism, Gene Expression Regulation drug effects, Humans, Rats, Stereoisomerism, Substrate Specificity, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Antimalarials pharmacology, Brain Chemistry, Endothelium, Vascular drug effects, Mefloquine pharmacology

Abstract

The brain distribution of the enantiomers of the antimalarial drug mefloquine is stereoselective according to the species. This stereoselectivity may be related to species-specific differences in the properties of some membrane-bound transport proteins, such as P-glycoprotein (P-gp). The interactions of racemic mefloquine and its individual enantiomers with the P-glycoprotein efflux transport system have been analysed in immortalised rat brain capillary endothelial GPNT cells. Parallel studies were carried out for comparison in human colon carcinoma Caco-2 cells. The cellular accumulation of the P-glycoprotein substrate, [(3)H]vinblastine, was significantly increased both in GPNT cells and in Caco-2 cells when treated with racemic mefloquine and the individual enantiomers. In GPNT cells, the (+)-stereoisomer of mefloquine was up to 8-fold more effective than its antipode in increasing cellular accumulation of [(3)H]vinblastine, while in Caco-2 cells, both enantiomers were equally effective. These results suggest that racemic mefloquine and its enantiomers are effective inhibitors of P-gp. Furthermore, a stereoselective P-glycoprotein inhibition is observed in rat cells but not in human cells. The efflux of [(14)C]mefloquine from GPNT cells was decreased when the cells were incubated with the P-gp modulators, verapamil, cyclosporin A or chlorpromazine, suggesting that MQ could be a P-gp substrate.

Published

2000

259. Chronic nifedipine dosing enhances cephalexin bioavailability and intestinal absorption in conscious rats.

Author

Berlioz F, Lepére-Prevot B, Julien S, Tsocas A, Carbon C, Rozé C, and Farinotti R

Subjects

Animals, Area Under Curve, Biological Availability, Drug Synergism, Half-Life, Intestinal Absorption, Male, Rats, Rats, Wistar, Cephalexin pharmacokinetics, Nifedipine pharmacology

Abstract

Cephalexin, a beta-lactam antibiotic, is rapidly absorbed via the di-and tripeptide intestinal transporters, as for many peptidomimetic drugs. Acute nifedipine has been shown to increase intestinal absorption of several beta-lactams: amoxicillin and cefixime in humans, and cephalexin in the rat. We showed previously that the nervous system was involved in the increasing effect of nifedipine on cephalexin intestinal absorption in anesthetized rats. The aim of the present study was 2-fold: 1) to investigate whether the effect of nifedipine is maintained in conscious rats, and 2) to determine whether the nifedipine effect will persist during chronic nifedipine administration. Acute and chronic oral administration of nifedipine significantly increased oral cephalexin area under the plasma concentration-time curve (34 and 25%, respectively) and maximum concentration in plasma (57 and 51%, respectively), while the distribution and elimination parameters of intra-arterial cephalexin were not affected by acute or chronic nifedipine administration. In conclusion, acute nifedipine effect on intestinal absorption of cephalexin is independent of anesthesia in rats. Since nifedipine could still enhance cephalexin intestinal absorption after a 7-day b.i.d. treatment, it can be envisaged to apply this effect to increase bioavailability of poorly absorbed peptidomimetic drugs in man.

Published

2000

260. Efavirenz-induced decrease in plasma amprenavir levels in human immunodeficiency virus-infected patients and correction by ritonavir.

Author

Duval X, Le Moing V, Longuet C, Leport C, Vildé JL, Lamotte C, Peytavin G, and Farinotti R

Subjects

Alkynes, Anti-HIV Agents pharmacology, Anti-HIV Agents therapeutic use, Benzoxazines, Carbamates, Cyclopropanes, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme Inhibitors, Drug Interactions, Drug Therapy, Combination, Furans, HIV Infections drug therapy, Humans, Oxazines therapeutic use, Oxidoreductases, N-Demethylating antagonists & inhibitors, Ritonavir therapeutic use, Sulfonamides therapeutic use, Anti-HIV Agents blood, Aryl Hydrocarbon Hydroxylases, HIV Infections blood, Oxazines pharmacology, Ritonavir pharmacology, Sulfonamides blood

Published

2000

261. Stereospecific versus nonstereospecific assessments for the bioequivalence of two formulations of racemic chlorpheniramine.

Author

Bui TH, Fernandez C, Vu K, Nguyen KH, Thuillier A, Farinotti R, Arnaud P, and Gimenez F

Subjects

Adult, Chlorpheniramine chemistry, Chlorpheniramine standards, Chromatography, High Pressure Liquid, Cross-Over Studies, Drug Compounding, Histamine H1 Antagonists chemistry, Histamine H1 Antagonists standards, Humans, Male, Reference Standards, Stereoisomerism, Therapeutic Equivalency, Chlorpheniramine pharmacokinetics, Histamine H1 Antagonists pharmacokinetics

Abstract

Chlorpheniramine (chlorphenamine, CPAM) is a racemic antihistaminic H1 drug containing two enantiomers. The aim of this study was to assess the bioequivalence of two formulations (reference and Vietnamese-tested formulation) of racemic chlorpheniramine combined with phenylpropanolamine in an open-labeled, randomized, crossover two-period study, after administration of 8 mg of racemic chlorpheniramine in 12 healthy Vietnamese subjects. First, dissolution of both formulations was tested in vitro according to USP requirements. Then the 12 subjects received both formulations after an overnight fast and a 7-day wash-out period. Plasma samples were collected up to 168 h. Plasma concentrations of total chlorpheniramine and its individual enantiomers were determined with a validated chiral HPLC method and pharmacokinetic parameters were estimated using model-independent analysis. For the reference formulation, Cmax and AUC values were higher for (+)S-chlorpheniramine ((+)S-CPAM) compared to (-)R-chlorpheniramine ((-)R-CPAM) (13.3 vs. 6.8 ng/ml and 409 vs. 222 ng/ml/h, respectively) while Clt/F and Vd/F were lower (9.8 vs. 17.6 l/h and 321 vs. 627 l, respectively). No difference was observed for Tmax, t(1/2), and MRT. Pharmacokinetic parameters were similar for the reference and the Vietnamese-tested formulation. Bioequivalence was assessed by Schuirmann test, as recommended by the current FDA and European Community criteria. Dissolution tests showed that both formulations were equivalent. A nonstereospecific, but not a stereospecific, approach indicated bioequivalence between the formulations., (Copyright 2000 Wiley-Liss, Inc.)

Published

2000

262. alpha(2)-adrenergic receptors stimulate oligopeptide transport in a human intestinal cell line.

Author

Berlioz F, Maoret JJ, Paris H, Laburthe M, Farinotti R, and Rozé C

Subjects

Adrenergic alpha-2 Receptor Agonists, Adrenergic alpha-Agonists pharmacology, Caco-2 Cells drug effects, Cephalexin pharmacokinetics, Cephalosporins pharmacokinetics, Clonidine pharmacology, HT29 Cells drug effects, HT29 Cells metabolism, Humans, Intestinal Absorption drug effects, Intestinal Absorption physiology, Intestinal Mucosa metabolism, Peptide Transporter 1, Transfection, Caco-2 Cells metabolism, Carrier Proteins metabolism, Receptors, Adrenergic, alpha-2 metabolism, Symporters

Abstract

Di- and tripeptides, as well as peptidomimetic drugs such as cephalexin (CFX), are absorbed by enterocytes via the oligopeptide transporter PepT1. We recently showed that the alpha(2)-adrenergic agonist clonidine increases CFX absorption in anaesthetized rats. Herein, we investigated whether alpha(2)-adrenergic receptors can directly affect PepT1 activity in a clone of the differentiated human intestinal cell line Caco-2 (Caco-2 3B) engineered to stably express alpha(2A)-adrenergic receptors at a density similar to that found in normal mucosa. Measurement of CFX fluxes across cell monolayers cultured on transwell filters demonstrated that the alpha(2)-agonists clonidine and UK14304 caused a 2-fold increase of CFX transport in Caco-2 3B cells, but not in Caco-2 (expressing PepT1 but not alpha(2)-adrenergic receptors) or in the HT29 19A clone (expressing alpha(2)-adrenergic receptors but not PepT1). The stimulatory effect of clonidine was abolished by glycyl-sarcosine (a competitor for the transporter) and blocked by yohimbine or RX821002 (alpha(2)-antagonists). Analysis of the kinetics of CFX transport in control and clonidine-treated Caco-2 3B cells showed that clonidine increased V(max) of CFX transport without changing K(m). Clonidine action was abolished by colchicine but not altered by amiloride, demonstrating that microtubule integrity but not Na(+)/H(+) exchanger activity is necessary for the effect of alpha(2)-agonists to occur. In conclusion, clonidine can directly activate alpha(2)-adrenergic receptors located on epithelial cells. The precise molecular mechanisms whereby these receptors modulate PepT1 activity remain to be elucidated but an increased translocation to the apical membrane of preformed cytoplasmic transporter molecules is likely to be involved.

Published

2000

263. Placental transfer of pyrimethamine studied in an ex vivo placental perfusion model.

Author

Peytavin G, Leng JJ, Forestier F, Saux M, Hohlfeld P, and Farinotti R

Subjects

Female, Humans, In Vitro Techniques, Kinetics, Perfusion, Pregnancy, Folic Acid Antagonists metabolism, Maternal-Fetal Exchange, Placenta metabolism, Pyrimethamine metabolism

Abstract

Pyrimethamine is used as and anti-infectious agent because of its antifolate properties. Its action is synergistic with that of dapsone and sulfamides on Toxoplasma gondii. The goal of the present study was to evaluate the placental transfer of pyrimethamine in an ex vivo model of perfused human placental cotyledon at term. Human placentas were perfused according to the slightly modified method of Schneider. The pyrimethamine fetal transfer rate was approximately 30%, while cotyledon clearance was about 1.8 ml/min. The placental transfer of pyrimethamine seems to be independent of the maternal concentrations of pyrimethamine, suggesting passive diffusion mechanisms or a nonsaturable active transport at the tested concentrations., (Copyright 2000 S. Karger AG, Basel)

Published

2000

264. Kinetics of antiviral activity and intracellular pharmacokinetics of human immunodeficiency virus type 1 protease inhibitors in tissue culture.

Author

Nascimbeni M, Lamotte C, Peytavin G, Farinotti R, and Clavel F

Subjects

HIV-1 drug effects, HIV-1 pathogenicity, HeLa Cells, Humans, Monocytes virology, Antiviral Agents pharmacokinetics, Antiviral Agents pharmacology, HIV Protease Inhibitors pharmacokinetics, HIV Protease Inhibitors pharmacology, HIV-1 enzymology

Abstract

We have examined the kinetics of the inhibition of human immunodeficiency virus type 1 (HIV-1) particle infectivity by protease inhibitors (PIs) in cell culture, using either transfected HeLa cells or infected peripheral blood mononuclear cells (PBMCs) as producers of infectious virions. Both the kinetics of the initiation of antiviral activity after addition of the PIs to these cultures and the kinetics of restoration of virion infectivity after removal of the PIs from the treated cultures were examined. We found that the kinetics of initiation of particle infectivity inhibition produced by a high extracellular concentration (5 microM) of the inhibitors were similar for all five inhibitors tested: loss of particle infectivity was perceptible as early as 1 h after the initiation of PI treatment and increased gradually thereafter. By contrast, the durability of this antiviral effect following removal of the drug from the culture varied dramatically according to the drug studied. In transfected HeLa cells, saquinavir and nelfinavir exerted the most prolonged inhibition, with the half-lives of their antiviral activities being greater than 24 h, while ritonavir exerted an intermediate length of inhibition (18 h) and indinavir and amprenavir exerted a reproducibly shorter length of inhibition (5 h). For all five tested PIs, these kinetics were significantly faster in PBMCs than in HeLa cells. The striking differences in antiviral kinetics observed among the different PIs appear mostly due to differences in their intracellular concentrations and/or rates of cellular clearance. Our observations, although limited to tissue culture conditions, may help delineate the cellular parameters of the antiviral activities of HIV-1 PIs and further optimize the efficiencies of these antiretrovirals in vivo.

Published

1999

265. Active intestinal elimination of ciprofloxacin in rats: modulation by different substrates.

Author

Dautrey S, Felice K, Petiet A, Lacour B, Carbon C, and Farinotti R

Subjects

Animals, Area Under Curve, Biological Transport, Active, Chemical Phenomena, Chemistry, Physical, Intestinal Absorption physiology, Male, Rats, Rats, Sprague-Dawley, Anti-Infective Agents pharmacokinetics, Ciprofloxacin pharmacokinetics, Intestinal Mucosa metabolism

Abstract

1. Two in vivo models, in the rat, were used to investigate, in the presence of different substrates, the overall and net intestinal elimination of ciprofloxacin: an open-intestinal perfusion model and an intestinal loop model respectively. 2. In the presence of quinidine, verapamil and cyclosporin (substrates of the P-glycoprotein (P-gp)), plasma AUCs of ciprofloxacin were 1.5 - 2 fold increased, while biliary clearance (1.5 - 2 fold), intestinal overall and net clearances (2 - 4 fold and 1.5 - 8 fold respectively) decreased. The weak effect obtained with cyclosporin as compared to verapamil and especially quinidine, suggests, for ciprofloxacin, the existence of transport systems distinct from the P-gp, as the OCT1 transporter which could be inhibited by quinidine. 3. With cephalexin and azlocillin, two beta-lactam antibiotics, plasma AUCs of ciprofloxacin increased and biliary and intestinal overall clearances decreased in a similar fashion (1.3 - 2 fold), suggesting the involvement of organic anion and/or cation transporters. 4. In the presence of structural analogues, the effect was dependent on the compound administered: Sparfloxacin had no effect on intestinal clearance of ciprofloxacin. In contrast, with pefloxacin, overall intestinal clearance of ciprofloxacin was decreased and net intestinal clearance increased. 5. The specificity of ciprofloxacin intestinal transport appears to be different from P-gp as outlined by the lack of competition with sparfloxacin, a P-gp substrate. Ciprofloxacin intestinal elimination seems to be mediated by organic anion and/or cation transporters and a mechanism sensitive to quinidine and verapamil.

Published

1999

266. In vivo efficacies of combinations of beta-lactams, beta-lactamase inhibitors, and rifampin against Acinetobacter baumannii in a mouse pneumonia model.

Author

Wolff M, Joly-Guillou ML, Farinotti R, and Carbon C

Subjects

Acinetobacter drug effects, Animals, Anti-Bacterial Agents pharmacokinetics, Female, Mice, Mice, Inbred C3H, Microbial Sensitivity Tests, Rifampin pharmacokinetics, beta-Lactams, Acinetobacter Infections drug therapy, Anti-Bacterial Agents therapeutic use, Drug Therapy, Combination therapeutic use, Enzyme Inhibitors therapeutic use, Pneumonia, Bacterial drug therapy, Rifampin therapeutic use, beta-Lactamase Inhibitors

Abstract

The effects of various regimens containing combinations of beta-lactams, beta-lactam inhibitor(s), and rifampin were assessed in a recently described mouse model of Acinetobacter baumannii pneumonia (M. L. Joly-Guillou, M. Wolff, J. J. Pocidalo, F. Walker, and C. Carbon, Antimicrob. Agents Chemother. 41:345-351, 1997). Two aspects of the therapeutic response were studied: the kinetics of the bactericidal effect (treatment was initiated 3 h after intratracheal inoculation, and bacterial counts were determined over a 24-h period) and survival (treatment was initiated 8 h after inoculation, and the cumulative mortality rate was assessed on day 5). Two clinical strains were used: a cephalosporinase-producing strain (SAN-94040) and a multiresistant strain (RCH-69). For SAN-94040 and RCH-69, MICs and MBCs (milligrams per liter) were as follows: ticarcillin, 32, 64, 256, and >256, respectively; ticarcillin-clavulanate, 32, 64, and 512, and >512, respectively; imipenem, 0.5, 0.5, 8, and 32, respectively; sulbactam, 0.5, 0.5, 8, and 8, respectively; and rifampin, 8, 8, 4, and 4, respectively. Against SAN-94040, four regimens, i.e., imipenem, sulbactam, imipenem-rifampin, and ticarcillin-clavulanate (at a 25/1 ratio)-sulbactam produced a true bactericidal effect (>/=3-log10 reduction of CFU/g of lung). The best survival rate (i.e., 93%) was obtained with the combination of ticarcillin-clavulanate-sulbactam, and regimens containing rifampin provided a survival rate of >/=65%. Against RCH-69, only regimens containing rifampin and the combination of imipenem-sulbactam had a true bactericidal effect. The best survival rates (>/=80%) were obtained with regimens containing rifampin and sulbactam. These results suggest that nonclassical combinations of beta-lactams, beta-lactamase inhibitors, and rifampin should be considered for the treatment of nosocomial pneumonia due to A. baumannii.

Published

1999

267. In vitro effects of racemates, separate enantiomers and major metabolites of mefloquine and halofantrine on metoprolol biotransformation by rat liver microsomes.

Author

Baune B, Furlan V, Taburet AM, and Farinotti R

Subjects

Animals, Antimalarials chemistry, Biotransformation drug effects, Male, Mefloquine chemistry, Metoprolol antagonists & inhibitors, Microsomes, Liver drug effects, Phenanthrenes chemistry, Rats, Rats, Sprague-Dawley, Stereoisomerism, Antimalarials pharmacology, Mefloquine pharmacology, Metoprolol pharmacokinetics, Microsomes, Liver metabolism, Phenanthrenes pharmacology

Abstract

1. The effects of the anti-malarial drugs mefloquine and halofantrine and of their major metabolites on metoprolol metabolism by rat liver microsomes have been investigated. 2. The observed Km and Vmax, and the formation kinetics of alpha-hydroxymetoprolol and O-demethylmetoprolol, two major metoprolol metabolites, were in keeping with published data. 3. In vitro, mefloquine competitively inhibited metoprolol biotransformation, whereas halofantrine did so in a mixed fashion. The mefloquine Ki of metoprolol alpha-hydroxylation and O-demethylation were 3.4 and 5.8 microM respectively, whereas those of halofantrine were 0.15 and 0.32 microM respectively. 4. The main metabolites, N-debutylhalofantrine and carboxymefloquine, were 4-10-fold less inhibitory than the parent drugs. The difference in inhibitory potency of parent drugs and metabolites was higher for halofantrine than for mefloquine. The potency order for metoprolol metabolism inhibition was halofantrine >> mefloquine = N-debutylhalofantrine > carboxymefloquine. 5. A preliminary study with anti-malarial enantiomers showed a weak difference, in metoprolol metabolism inhibition between the enantiomers of halofantrine or mefloquine. 6. It is concluded that halofantrine is a potent inhibitor of metoprolol metabolism and that halofantrine metabolites or its enantiomers may have a different inhibitor potency than the parent drug: (1) the inhibition potency of these compounds should be studied in vitro and (2) their in vivo elimination half-life and plasma concentrations should be taken into be account to extrapolate this experimental results to in vivo.

Published

1999

268. Drug interactions with diosmectite: a study using the artificial stomach-duodenum model.

Author

Castela-Papin N, Cai S, Vatier J, Keller F, Souleau CH, and Farinotti R

Subjects

Adsorption, Animals, Anti-Infective Agents pharmacokinetics, Cimetidine pharmacokinetics, Dapsone pharmacokinetics, Digoxin pharmacokinetics, Drug Interactions, Duodenum metabolism, Fluoroquinolones, Gastric Mucosa metabolism, Hydrogen-Ion Concentration, Intestinal Absorption drug effects, Metronidazole pharmacokinetics, Swine, Valproic Acid pharmacokinetics, Duodenum physiology, Gastrointestinal Agents pharmacology, Models, Biological, Pharmacokinetics, Silicates, Stomach physiology

Abstract

Drug interactions with diosmectite, a gastric-protective drug, were studied in vitro using an artificial stomach-duodenum model. The behavior of neutral and ionisable drugs with pKa values ranging between 2 and 8 was monitored to determine the physicochemical characteristics of the interactions. The main neutral (digoxin) and acid (valproic acid) drug substances were moderately fixed by clay (<27%), in a pH-independent manner. Basic compounds with a pKa<7 (dapsone, metronidazole, cimetidine) were strongly fixed in acid medium (?62%), and fully released under neutral conditions. Amphoteric (fluoroquinolones) and basic compounds with a pKa>/=7 (ranitidine, pyrimethamine) were adsorbed by more than 81% by diosmectite in gastric and duodenal compartments. In the part of the model representing the distal duodenum, the potential site for drug absorption, only the active substances which remained positively charged (amphoteric and basic compounds) showed a large reduction (>/=80%) in their available free fraction. Ionisation of drug substances administered per os concomitantly with diosmectite plays a crucial role in these interactions., (Copyright.)

Published

1999

269. Effect of selected antimalarial drugs and inhibitors of cytochrome P-450 3A4 on halofantrine metabolism by human liver microsomes.

Author

Baune B, Furlan V, Taburet AM, and Farinotti R

Subjects

Adolescent, Adult, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme System metabolism, Drug Interactions, Humans, Male, Middle Aged, Mixed Function Oxygenases metabolism, Antifungal Agents pharmacology, Antimalarials pharmacology, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Ketoconazole pharmacology, Microsomes, Liver drug effects, Microsomes, Liver metabolism, Mixed Function Oxygenases antagonists & inhibitors, Phenanthrenes metabolism

Abstract

Halofantrine (HF) is used in the treatment of uncomplicated multidrug-resistant Plasmodium falciparum malaria. Severe cardiotoxicity has been reported to be correlated with high plasma concentrations of HF but not with that of its metabolite N-debutylhalofantrine. The aim of this study was to investigate the effects of other antimalarial drugs and of ketoconazole, a typical cytochrome P-450 3A4 inhibitor, on HF metabolism by human liver microsomes. Antimalarial drug inhibitory effects were ranked as follows: primaquine > proguanil > mefloquine > quinine > quinidine > artemether > amodiaquine. Artemisine, doxycycline, sulfadoxine, and pyrimethamine showed little or no inhibition of HF metabolism. Mefloquine, quinine, quinidine, and ketoconazole used at maximal plasma concentrations inhibited N-debutylhalofantrine formation noncompetitively with Ki values of 70 microM, 49 microM, 62 microM, and 0.05 microM resulting in 7%, 49%, 26%, and 99% inhibition, respectively, in HF metabolism. In conclusion, we showed that quinine and quinidine coadministered with HF might inhibit its metabolism resulting in the potentiation of HF-induced cardiotoxicity in patients. This requires a close monitoring of ECG. For the same reasons, the concomitant administration of HF and ketoconazole must be avoided. By contrast, none of the other antimalarials studied inhibited HF metabolism and, by extrapolation, cytochrome P-450 3A4 activity.

Published

1999

270. Cerium-doped diosmectite for topical application studies of the cerium-clay interaction.

Author

Papin-Castéla N, Prognon P, Keller F, Bénazeth S, Farinotti R, Mahuzier G, and Souleau C

Subjects

Administration, Topical, Adsorption, Electrolytes chemistry, Fluorometry, Hydrogen-Ion Concentration, Kinetics, Sodium Chloride chemistry, Solutions, Anti-Infective Agents, Local administration & dosage, Anti-Infective Agents, Local chemistry, Cerium administration & dosage, Cerium chemistry, Gastrointestinal Agents chemistry, Silicates

Abstract

Cerium is used for its antiseptic and immunomodulatory properties in burn injury. We have developed a cerium-doped clay to replace existing ointments. Adsorption and release of cerium (Ce3+) by diosmectite were studied at 22+/-2 degrees C, in the presence of various other cationic species. Simple spectrofluorimetric determination of cerium was used (lambdaexc=240 nm/lambdaem=360 nm). Cerium binding reached a plateau within 2 min and was a function of the electrolyte content of the solution in contact with the clay. Langmuir isotherm treatment led to a maximal binding capacity of 66 mg of Ce3+ per gram of clay. Partial release occurred within 2 min (19% in the presence of isotonic NaCl solution). The ionic strength of the solution, and the ionic radius and charge of the electrolytes present in the bathing solution significantly influenced cerium release, in contrast to pH and temperature changes. These results strongly point to a cationic exchange mechanism between diosmectite and cerium solution., (Copyright.)

Published

1999

271. Halofantrine metabolism in microsomes in man: major role of CYP 3A4 and CYP 3A5.

Author

Baune B, Flinois JP, Furlan V, Gimenez F, Taburet AM, Becquemont L, and Farinotti R

Subjects

Benzoflavones pharmacology, Cytochrome P-450 CYP2C19, Cytochrome P-450 CYP2D6 metabolism, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme Inhibitors, Cytochrome P-450 Enzyme System metabolism, Cytochrome P-450 Enzyme System physiology, Enzyme Activation drug effects, Humans, Isoenzymes metabolism, Ketoconazole pharmacology, Kinetics, Microsomes enzymology, Microsomes metabolism, Microsomes, Liver enzymology, Mixed Function Oxygenases antagonists & inhibitors, Mixed Function Oxygenases metabolism, Mixed Function Oxygenases physiology, Saccharomyces cerevisiae, Substrate Specificity, Aryl Hydrocarbon Hydroxylases, Microsomes, Liver metabolism, Phenanthrenes metabolism

Abstract

We have clarified the contribution of the different enzymes involved in the N-debutylation of halofantrine in liver microsomes in man. The effect of ketoconazole and cytochrome P450 (CYP) 3A substrates on halofantrine metabolism has also been studied. The antimalarial drug halofantrine is metabolized into one major metabolite, N-debutylhalofantrine. In microsomes from nine livers from man, N-debutylation of halofantrine was highly variable with apparent Michaelis-Menten constant V(max) and K(m) values of 215+/-172 pmol min(-1) mg(-1) and 48+/-26 micromol L(-1), respectively, (mean+/-standard deviation). Formation of N-debutylhalofantrine was cytochrome P450 (CYP)-mediated. Studies using selective inhibitors of individual CYPs revealed the role of CYP 3As in the formation of N-debutylhalofantrine. alpha-Naphthoflavone, a CYP 3A activator, increased metabolite formation. In microsomes from 12 livers from man the rate of N-debutylation of halofantrine correlated strongly with CYP 3A4 relative levels (P = 0.002) and less strongly, but significantly, with CYP 2C8 levels (P = 0.025). To characterize CYP-mediated metabolism of halofantrine further, incubations were performed with yeast microsomes expressing specific CYP 3A4, CYP 3A5, CYP 2D6, CYP 2C8 and CYP 2C19 from man. The rate of formation of N-debutylhalofantrine was six- and twelvefold with CYP 3A4 than with CYP 3A5 and CYP 2C8, respectively. CYP 2D6 and CYP 2C19 did not mediate the N-debutylation of halofantrine, but, because in-vivo CYP 2C8 is present at lower concentrations than CYP 3A in the liver in man, the involvement of CYP 3As would be predominant. Diltiazem, erythromycin, nifedipine and cyclosporin (CYP 3A substrates) inhibited halofantrine metabolism. Similarly, ketoconazole inhibited, non-competitively, formation of N-debutylhalofantrine with an inhibition constant, K(i), of 0.05 microM. The theoretical percentage inhibition of halofantrine metabolism in-vivo by ketoconazole was estimated to be 99%. These results indicate that both CYP 3A4 and CYP 3A5 metabolize halofantrine, with major involvement of CYP 3A4. In-vivo, the other CYPs have a minor role only. Moreover, strong inhibition, and consequently increased halofantrine cardiotoxicity, might occur with the association of ketoconazole or other CYP 3A4 substrates.

Published

1999

272. Neural modulation of cephalexin intestinal absorption through the di- and tripeptide brush border transporter of rat jejunum in vivo.

Author

Berlioz F, Julien S, Tsocas A, Chariot J, Carbon C, Farinotti R, and Rozé C

Subjects

Adrenergic Antagonists pharmacology, Animals, Cephalexin blood, Hexamethonium pharmacology, Jejunum innervation, Lidocaine pharmacology, Male, Microvilli metabolism, Nifedipine pharmacology, Prazosin pharmacology, Rats, Rats, Wistar, Yohimbine pharmacology, ATP-Binding Cassette Transporters metabolism, Bacterial Proteins, Cephalexin metabolism, Cephalosporins metabolism, Intestinal Absorption, Jejunum physiology, Membrane Transport Proteins metabolism

Abstract

Intestinal absorption of beta-lactamine antibiotics (e.g., cefixime and cephalexin) has been shown to proceed through the dipeptide carrier system. In a previous study, nifedipine (NFP), an L-type calcium channel blocker, enhanced the absorption of cefixime in vivo but not in vitro, and it was suggested that neural mechanisms might be involved in the effect of NFP. The aim of the present study was to assess the involvement of the nervous system on the intestinal absorption of cephalexin (CFX). To investigate this, we used a single-pass jejunal perfusion technique in rats. NFP and diltiazem enhanced approximately 2-fold the plasma levels of CFX in treated rats versus untreated controls. NFP also increased approximately 2-fold the CFX level in portal plasma and increased urinary excretion of CFX, thus indicating that CFX did effectively increase CFX intestinal absorption. Perfusing high concentrations of dipeptides in the jejunal lumen competitively reduced CFX absorption and inhibited the enhancement of CFX absorption produced by NFP. Hexamethonium and lidocaine inhibited the effect of NFP, whereas atropine, capsaicin, clonidine, and isoproterenol enhanced CFX absorption by the same order of magnitude as NFP. Thus, complex neural networks can modulate the function of the intestinal di- and tripeptide transporter. Sympathetic noradrenergic fibers, intestinal sensory neurons, and nicotinic synapses are involved in the increase of CFX absorption produced by NFP.

Published

1999

273. Influence of renal failure on intestinal clearance of ciprofloxacin in rats.

Author

Dautrey S, Rabbaa L, Laouari D, Lacour B, Carbon C, and Farinotti R

Subjects

Animals, Area Under Curve, Bile metabolism, Chromatography, High Pressure Liquid, Creatinine blood, Male, Nephrectomy, Perfusion, Rats, Rats, Sprague-Dawley, Anti-Infective Agents pharmacokinetics, Ciprofloxacin pharmacokinetics, Intestinal Mucosa metabolism, Renal Insufficiency metabolism

Abstract

Following intravenous doses, ciprofloxacin pharmacokinetics in control and nephrectomized rats were studied. There were no differences between control and nephrectomized rats for area under the concentration-time curve in plasma or biliary clearance. The intestinal clearance of ciprofloxacin was increased in nephrectomized rats. Intestinal elimination seems to compensate partially for the decrease in urinary excretion of ciprofloxacin in nephrectomized rats.

Published

1999

274. Binding of chlorpheniramine enantiomers to human plasma proteins.

Author

Hiep BT, Gimenez F, Khanh VU, Hung NK, Thuillier A, Farinotti R, and Fernandez C

Subjects

Chlorpheniramine chemistry, Chlorpheniramine pharmacokinetics, Humans, In Vitro Techniques, Orosomucoid metabolism, Protein Binding, Serum Albumin metabolism, Stereoisomerism, Blood Proteins metabolism, Chlorpheniramine blood

Abstract

The in vitro binding of RS-chlorpheniramine to human proteins was studied by equilibrium dialysis. The binding to total plasma proteins and to individual albumin and alpha-glycoprotein acid is stereoselective. (+)S-chlorpheniramine is more extensively bound than its antipode to total plasma proteins (38% vs. 23%), to albumin (20% vs. 15%) and to alpha-glycoprotein acid (23% vs. 5%).

Published

1999

275. Cerebral uptake of mefloquine enantiomers in fatal cerebral malaria.

Author

Pham YT, Nosten F, Farinotti R, White NJ, and Gimenez F

Subjects

Autopsy, Fatal Outcome, Female, Humans, Male, Mefloquine blood, Stereoisomerism, Brain metabolism, Malaria, Cerebral metabolism, Mefloquine pharmacokinetics

Abstract

Patients and Methods: The brain disposition of the enantiomers of the antimalarial mefloquine was studied in two post-mortem human cerebral biopsies after oral administration of the racemic mixture., Background: Mefloquine (MQ) is an effective antimalarial drug used both for prophylaxis and treatment of chloroquine resistant Plasmodium falciparum. MQ is generally well tolerated in treatment. Minor side-effects have been described. Potentially serious neuropsychiatric reactions occur. The mechanism underlying the neurotoxicity is unknown, although a dose relationship is evidently involved., Results: Mefloquine enantiomer concentrations were determined using a chiral liquid chromatographic method. Mefloquine concentrations were higher in brain compared to plasma. Studied in one patient, white matter concentrations were higher compared to grey matter concentrations., Conclusion: Based on the ratios brain concentration/plasma concentration, the brain penetration of the (+) enantiomer is much higher than that of the (-) enantiomer.

Published

1999

276. Stereoselective binding of zopiclone to human plasma proteins.

Author

Fernandez C, Gimenez F, Thuillier A, and Farinotti R

Subjects

Azabicyclo Compounds, Humans, Orosomucoid metabolism, Protein Binding, Serum Albumin metabolism, Stereoisomerism, Substrate Specificity, Blood Proteins metabolism, Hypnotics and Sedatives blood, Piperazines blood

Abstract

The binding of racemic zopiclone (ZOP) and of its two enantiomers to plasma proteins, albumin and alpha 1-acid glycoprotein were compared. Our work shows that the binding of ZOP to human plasma proteins is stereoselective. The total plasma protein binding percentages were 79.3 +/- 5.5%, 83.8 +/- 5.2%, and 75.1 +/- 2.1%, for racemic zopiclone, (-)zopiclone and (+)zopiclone, respectively. These results were confirmed by the analysis of samples obtained from healthy volunteers after the oral administration of ZOP. The anticoagulant used for sampling was also shown to have an influence on the percentage binding and on its stereoselectivity. Considering albumin and alpha 1-acid glycoprotein separately, stereoselectivity was also observed.

Published

1999

277. Effects of Salmonella typhimurium infection and ofloxacin treatment on glucose and glutamine metabolism in Caco-2/TC-7 cells.

Author

Posho L, Delbos-Bocage L, Gueylard D, Farinotti R, and Carbon C

Subjects

Caco-2 Cells, Carbon Dioxide metabolism, Glycolysis, Humans, Salmonella typhimurium physiology, Anti-Infective Agents pharmacology, Glucose metabolism, Glutamine metabolism, Ofloxacin pharmacology, Salmonella typhimurium drug effects

Abstract

The effects of both Salmonella typhimurium infection and 5 mM ofloxacin treatment on 2 mM glutamine and 5 mM glucose metabolism in the enterocyte-like Caco-2/TC-7 cell line were studied. These cells utilized glutamine (212.07 +/- 16.75 [mean +/- standard deviation] nmol per h per 10(6) viable cells) and, to a lesser extent, glucose (139.63 +/- 11.52 nmol per h per 10(6) viable cells). Metabolism of these substrates in Caco-2/TC-7 cells resembled that in rat, pig, or human enterocytes. Infection by S. typhimurium C53-enhanced glucose and glutamine substrate utilization by 32 and 22%, respectively and enhanced glucose and glutamine substrate oxidation by eight- and twofold, respectively. These increases in glucose and glutamine metabolism (especially glucose metabolism) were due in part to the metabolism of intracellular bacteria and/or to the activation of cellular metabolism. Substrate metabolism (especially glucose metabolism) in C53-infected cells was partially reduced by treatment with ofloxacin. It was concluded that cellular fuel metabolism is stimulated at the earliest stage of infection (3 to 4 h) and that treatment with 5 mM ofloxacin does not completely restore substrate metabolism to the levels observed in uninfected cells, possibly because this treatment does not eradicate intracellular S. typhimurium completely.

Published

1998

278. Determination of 2-n-propylquinoline in mouse plasma and liver by high-performance liquid chromatography.

Author

Iglarz M, Baune B, Gantier JC, Hocquemiller R, and Farinotti R

Subjects

Animals, Female, Mice, Quinolines blood, Reproducibility of Results, Spectrophotometry, Ultraviolet, Chromatography, High Pressure Liquid methods, Liver metabolism, Quinolines pharmacokinetics

Abstract

A high-performance liquid chromatographic method was developed for the specific determination of 2-n-propylquinoline, a new anti-leishmaniasis drug, in plasma and liver homogenates of mice. 2-n-Propylquinoline was extracted with methyl-tert.-butyl ether with quinoline as internal standard. Separation was carried out using a Nucleosil C18 column. The mobile phase consisted of methanol-0.005 M ammonium acetate buffer (60:40) at pH 5.5 and 8 for plasma and liver homogenates, respectively. Detection was monitored at 233 nm. The method was validated and shown to be accurate and precise for plasma and liver homogenates. Extraction yield was 96% in plasma and 81% in liver homogenates. This method was used to determine the pharmacokinetic profile of 2-n-propylquinoline following oral administration to mice.

Published

1998

279. Pharmacokinetics of cefuroxime in healthy volunteers: an update.

Author

Massias L, Muller-Serieys C, Farinotti R, and Bergogne-Bérézin E

Subjects

Adult, Area Under Curve, Cefuroxime blood, Cephalosporins blood, Chromatography, High Pressure Liquid, Cross-Over Studies, Double-Blind Method, Humans, Male, Cefuroxime pharmacokinetics, Cephalosporins pharmacokinetics

Published

1998

280. Determination of the inhibitory effect on Toxoplasma growth in the serum of AIDS patients during acute therapy for toxoplasmic encephalitis.

Author

Derouin F, Gérard L, Farinotti R, Maslo C, and Leport C

Subjects

Acquired Immunodeficiency Syndrome blood, Adult, Animals, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents therapeutic use, Anti-Infective Agents blood, Anti-Infective Agents pharmacology, Drug Therapy, Combination, Encephalitis parasitology, Female, Follow-Up Studies, Humans, Macrolides, Male, Pyrimethamine blood, Pyrimethamine pharmacology, Sulfadiazine pharmacology, Toxoplasma growth & development, Toxoplasmosis, Cerebral parasitology, Acquired Immunodeficiency Syndrome complications, Anti-Infective Agents therapeutic use, Encephalitis drug therapy, Pyrimethamine therapeutic use, Sulfadiazine therapeutic use, Toxoplasma drug effects, Toxoplasmosis, Cerebral drug therapy

Abstract

In 26 AIDS patients treated for toxoplasmic encephalitis, the inhibitory effect on Toxoxplasma growth of sequential sera taken before and after initiation of therapy was determined using a culture-based immunoassay and compared with pyrimethamine blood levels. A marked inhibition of Toxoplasma growth was observed 1 day after initiation of therapy with pyrimethamine plus sulfadiazine and was maintained between 67% and 93% throughout the 15-day follow-up period. The degree of inhibition was not correlated to pyrimethamine blood levels and seemed highly potentiated when sulfadiazine rather than macrolides was given in combination with pyrimethamine.

Published

1998

281. Pharmacokinetic parameters and killing rates in serum of volunteers receiving amoxicillin, cefadroxil or cefixime alone or associated with niflumic acid or paracetamol.

Author

Carsenti-Etesse H, Farinotti R, Durant J, Roger PM, De Salvador F, Bernard E, Rouveix B, and Dellamonica P

Subjects

Acetaminophen blood, Acetaminophen pharmacology, Adolescent, Adult, Amoxicillin blood, Amoxicillin pharmacokinetics, Amoxicillin pharmacology, Analgesics, Non-Narcotic pharmacology, Anti-Bacterial Agents pharmacology, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Area Under Curve, Cefadroxil blood, Cefadroxil pharmacokinetics, Cefadroxil pharmacology, Cefixime, Cefotaxime analogs & derivatives, Cefotaxime blood, Cefotaxime pharmacokinetics, Cefotaxime pharmacology, Chromatography, High Pressure Liquid, Cross-Over Studies, Double-Blind Method, Drug Interactions, Female, Haemophilus influenzae drug effects, Humans, Male, Microbial Sensitivity Tests, Niflumic Acid blood, Niflumic Acid pharmacology, Staphylococcus aureus drug effects, Streptococcus pneumoniae drug effects, Acetaminophen pharmacokinetics, Analgesics, Non-Narcotic pharmacokinetics, Anti-Bacterial Agents pharmacokinetics, Anti-Inflammatory Agents, Non-Steroidal pharmacokinetics, Niflumic Acid pharmacokinetics

Abstract

Pharmacokinetic parameters and killing rates in serum of volunteers receiving amoxicillin, cefadroxil or cefixime alone or associated with niflumic acid or paracetamol were studied. Niflumic acid (250 mg) or analgesic and antipyretic drugs such as paracetamol (500 mg) are often combined with antibiotics to avoid inflammation and pain in acute ear, nose and throat diseases. Pharmacokinetic interactions between these two classes of drugs have been described in experimental models, and exceptionally in humans. The aim of the present investigation was to study the interactions of these two drugs with three antibiotics (amoxicillin 500 mg x 2, cefadroxil 500 mg x 2, cefixime 200 mg and one placebo capsule) on pharmacodynamic parameters and on rate of killing in the serum of six healthy volunteers receiving the antibiotic associated or not with the product in a randomized cross-over double-blind trial. The bacteria most often involved in sinusitis, bronchitis and otitis media (Haemophilus influenzae, Streptococcus pneumoniae, Staphylococcus aureus) three target diseases for oral cephalosporins and amoxicillin, were chosen for bacteriological study. Blood samples were obtained at 0.25, 0.50, 1, 1.5, 2, 4, 6 and 12 h after oral administration of antibiotics alone or associated with the drugs. There was a wash-out period of at least 1 week between the eleven sequences. Antibiotics were measured by two methods: bioassay and high performance liquid chromatography (HPLC). All serum samples obtained at peak level, 4 and 6 h were tested for killing rate. Area under the time kill curve was calculated by the trapezoidal rule method and relative bioactivity in percent was defined as follows: (AUC control - AUC test)/AUC control x 100. No pharmacokinetic interaction was found in the AUC and T1/2 of the plasma concentrations of the antibiotics or associated with the drugs, regardless of dose, as determined by HPLC or microbiological assay. For these beta-lactam antibiotics killing rate was found to be time-dependent. Bactericidal activity was improved on H. influenzae when cefixime was associated with niflumic acid and became concentration-dependent. A significant concentration relation was also found with niflumic acid or paracetamol associated with cefixime on Strep. pneumoniae.

Published

1998

282. Critical importance of in vivo amoxicillin and cefotaxime concentrations for synergy in treatment of experimental Enterococcus faecalis endocarditis.

Author

Join-Lambert O, Mainardi JL, Cuvelier C, Dautrey S, Farinotti R, Fantin B, and Carbon C

Subjects

Amoxicillin pharmacokinetics, Animals, Cefotaxime pharmacokinetics, Drug Synergism, Drug Therapy, Combination pharmacokinetics, Rabbits, Amoxicillin therapeutic use, Cefotaxime therapeutic use, Drug Therapy, Combination therapeutic use, Endocarditis, Bacterial drug therapy, Enterococcus faecalis drug effects, Gram-Positive Bacterial Infections drug therapy

Abstract

The synergy between amoxicillin and cefotaxime against two strains of Enterococcus faecalis (JH2-2 and 6370) in vitro and in rabbit endocarditis was investigated. In vitro synergy was obtained only when amoxicillin concentrations were below the MBC and when cefotaxime concentrations were above 1 microg/ml. No synergy was observed in vivo, because of the short period of time during which these pharmacologic requirements were achieved.

Published

1998

283. Influence of renal failure on ciprofloxacin pharmacokinetics in rats.

Author

Nouaille-Degorce B, Veau C, Dautrey S, Tod M, Laouari D, Carbon C, and Farinotti R

Subjects

Administration, Oral, Animals, Anti-Infective Agents administration & dosage, Anti-Infective Agents adverse effects, Ciprofloxacin administration & dosage, Ciprofloxacin adverse effects, Infusions, Parenteral, Kidney surgery, Male, Metabolic Clearance Rate, Nephrectomy, Rats, Rats, Sprague-Dawley, Anti-Infective Agents pharmacokinetics, Ciprofloxacin pharmacokinetics, Kidney drug effects, Renal Insufficiency metabolism

Abstract

Ciprofloxacin pharmacokinetics have been shown to be modified in patients with renal failure (e.g., the intestinal secretion of ciprofloxacin is increased). This study investigated the influence of renal failure on the pharmacokinetics of ciprofloxacin following oral and parenteral administration to rats of a dose of 50 mg/kg of body weight. After parenteral administration, only renal clearance (CLR) was reduced in nephrectomized rats (5.3+/-1.4 versus 17.8+/-4.7 ml/min/kg, P < 0.01, nephrectomized versus control rats). However, nonrenal clearance was increased in nephrectomized rats (32+/-4 versus 15+/-5 ml/min/kg, P < 0.01, nephrectomized versus control rats), suggesting compensatory mechanisms for reduced renal function. After oral administration, apparent total clearance and CLR were reduced (P < 0.01) in nephrectomized rats (117+/-25 and 6.8+/-4.4 ml/min/kg, respectively) compared with the values for control rats (185+/-9 and 22.6+/-5.3 ml/min/kg, respectively) and the area under the concentration-time curve was higher (P < 0.01) for nephrectomized rats (436.3+/-90.5 mg. min/liter) than for control rats (271.3+/-14.3 mg.min/liter). Terminal elimination half lives in the two groups remained constant after oral and parenteral administration. These results suggest an increased bioavailability of ciprofloxacin in nephrectomized rats, which was confirmed by a nonlinear mixed-effect model.

Published

1998

284. Interests of the 'artificial stomach' techniques to study antacid formulations: comparison with in vivo evaluation.

Author

Vatier J, Célice-Pingaud C, and Farinotti R

Subjects

Antacids metabolism, Chemistry, Pharmaceutical, Gastric Acid metabolism, Gastric Emptying drug effects, Gastric Mucosa drug effects, Gastric Mucosa metabolism, Humans, Hydrogen-Ion Concentration, Models, Biological, Pentagastrin pharmacology, Antacids pharmacology, Artificial Organs, Drug Evaluation, Preclinical methods

Abstract

In this overview, the methods for assessing antacid activity in vitro are surveyed, and the problems of their comparison with in vivo methods of evaluation are discussed. In vitro assessment is based on two types of method: static and dynamic. The static method of titration, with end-of-titration pH values ranging between 3.0 and 1.0, has been used to quantify the number of sites capable of binding H+ ions at each end-of-titration pH, and to identify certain chemical mechanisms involved in this binding; in other words, this approach provides the pharmacological characteristics of the drugs tested. In contrast, it does not take into account physiological factors modulating antacid activity, such as gastroduodenal fluxes (including gastric emptying), drug adherence to the mucosa, and acid secretion. The dynamic method was initially based on an artificial stomach model, which has gradually been upgraded to a computer-controlled artificial stomach-duodenum model. This model overcomes certain weaknesses of the static method by simulating flux and pH conditions in the gastroduodenal tract, by taking into account interactions with the gastric mucosa and thereby reproducing the in vivo medium encountered by antacids. It is therefore capable of reflecting the characteristics of antacids, namely their effect on gastric pH and resistance to acidification, at the same time helping to identify the underlying chemicophysical mechanisms. In vivo, the antacid effect can be assessed qualitatively by means of pH-meter studies in healthy volunteers, both in baseline conditions and during secretory stimulation, and also quantitatively by methods based on intragastric titration in response to a liquid meal (IGT). pH-meter studies in baseline conditions come up against the variability of the basal pH and antacid homogenization with gastric contents, which results in a wide range of individual values. This variability is found in pH-meter studies during pentagastrin infusion and, to a lesser degree, in response to a meal. Close correlations have, however, been established between results obtained with the artificial stomach model and in healthy volunteers submitted to pH-metric or IGT studies, with several antacids. It seems that the artificial stomach method is sufficiently reproducible to make it the method of choice for investigating the antacid activity of all drugs aimed at treating acid hypersecretion disorders. In contrast, in vivo studies may be warranted for precise therapeutic indications, such as treatment of duodenal ulcer or gastro-esophageal reflux, in which the therapeutic effect is judged on the basis of an improvement in symptoms and endoscopic criteria, without the need to demonstrate the antacid effect itself.

Published

1998

285. Stereoselective passage of mefloquine through the blood-brain barrier in the rat.

Author

Baudry S, Pham YT, Baune B, Vidrequin S, Crevoisier C, Gimenez F, and Farinotti R

Subjects

Animals, Antimalarials blood, Antimalarials chemistry, Antimalarials metabolism, Brain Chemistry, Half-Life, Male, Mefloquine blood, Mefloquine chemistry, Mefloquine metabolism, Molecular Structure, Organ Size drug effects, Rats, Rats, Wistar, Stereoisomerism, Tissue Distribution, Antimalarials pharmacokinetics, Blood-Brain Barrier drug effects, Mefloquine pharmacokinetics

Abstract

The pharmacokinetics of the enantiomers of mefloquine were studied in the rat after administration of a racemic mixture and of the separate enantiomers (+)-mefloquine and (-)-mefloquine. When 50 mg kg-1 racemic mixture was administered orally for 22 days, plasma concentrations of the (+) enantiomer were 2-3 times higher than those of the (-) enantiomer whereas the opposite was true in every part of the brain (cerebellum, cortex, hippocampus, hypothalamus and striatum). Different concentrations of mefloquine were found in the different regions of the brain; the lowest concentrations of (+/-)-mefloquine (27.0 nmol g-1) were in the cerebellum and the highest (110.0 nmol g-1) in the hippocampus. The main metabolite, carboxymefloquine, was detected in plasma but not in the brain. The results indicate the mefloquine crosses the blood-brain barrier stereoselectively.

Published

1997

286. Absorption of ofloxacin isomers in the rat small intestine.

Author

Rabbaa L, Dautrey S, Colas-Linhart N, Carbon C, and Farinotti R

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Amino Acids pharmacology, Animals, Area Under Curve, Biological Availability, Dipeptides pharmacology, Intestinal Absorption drug effects, Intestine, Small drug effects, Male, Rats, Rats, Sprague-Dawley, gamma-Aminobutyric Acid pharmacology, Anti-Infective Agents pharmacokinetics, Intestinal Absorption physiology, Intestine, Small metabolism, Ofloxacin pharmacokinetics

Abstract

Ofloxacin, a chiral fluoroquinolone, possesses two optical isomers. The antibacterial activity of S-(-)-ofloxacin is 8 to 128 times higher than that of R-(+)-ofloxacin. In the rat, a saturable absorption process has been described for racemic ofloxacin. In the present study we investigated the mechanism underlying the in vivo intestinal absorption of ofloxacin enantiomers in the rat. Blood samples were collected from the portal vein. Our results show that the intestinal absorption of ofloxacin isomers is pH dependent, both enantiomers being best absorbed at neutral pH. S-(-)-Ofloxacin seems to have a greater affinity for the intestinal transporter (initial concentrations at 5 min [C(init)] are 0.17 +/- 0.04 and 0.12 +/- 0.03 microg/ml for S-(-)- and R-(+)-ofloxacin, respectively). Dipeptides fail to modify ofloxacin absorption, but amino acids reduce both isomers' absorption (C(init) is reduced by 53 and 33% with glycine for S-(-)- and R-(+)-ofloxacin, respectively, and by 59 and 42% with L-leucine). Gamma amino butyric acid interferes with the absorption of ofloxacin isomers, but less seriously than do amino acids. Furthermore, ofloxacin competes with other fluoroquinolones or P-glycoprotein substrates for a common secretory pathway, resulting in an increased rate of absorption for both ofloxacin isomers; this is probably an indirect result of their reduced efflux from the apical side of intestinal cells.

Published

1997

287. Increased intestinal absorption of cefixime by nifedipine in the rat intestinal perfusion model: evidence for a neural regulation.

Author

Harcouët L, Lebrec D, Rozé C, Carbon C, and Farinotti R

Subjects

Animals, Cefixime, Cefotaxime pharmacokinetics, Drug Synergism, Enteric Nervous System metabolism, Intestine, Small innervation, Intestine, Small metabolism, Models, Biological, Peptide YY, Peptides pharmacology, Perfusion, Rats, Rats, Sprague-Dawley, Salicylates pharmacokinetics, Salicylic Acid, Cefotaxime analogs & derivatives, Enteric Nervous System drug effects, Intestinal Absorption drug effects, Intestine, Small drug effects, Nifedipine pharmacology

Abstract

In healthy volunteers, the simultaneous administration of nifedipine and cefixime has been shown to increase the oral absorption of the antibiotic. To investigate the pharmacological basis of this interaction, we used an in situ intestinal perfusion technique in the rat. pH 5.5 yielded optimum cefixime absorption, which was greater in segments from the duodenojejunum than in those from the jejunoileum. Cefixime absorption was similar when perfused at 0.5 and 1.0 mg/ml, suggesting transport saturation at the lower concentration. Cefixime arterial and portal blood concentrations after an intestinal perfusion of 0.5 mg/ml cefixime were significantly increased by a previous 15-min intestinal perfusion of 0.05 mg/ml nifedipine. Nifedipine did not significantly alter intestinal blood flow. At the end of the cefixime perfusion, intestinal blood flow was higher in the nifedipine group than in the control group (0.44 +/- 0.12 vs. 0.26 +/- 0.09 ml.min-1.g of intestine wt-1, respectively), although the difference did not reach statistical significance. The absorption kinetics of salicylic acid, which is strictly absorbed by passive diffusion, were unaffected by nifedipine. After 15 and 50 min of recirculation, residual salicylate levels fell from 85.1 +/- 5.6% to 57.1 +/- 2.8% with nifedipine compared with 87.4 +/- 1.4% to 52.8 +/- 1.6% without nifedipine. Thus, the improvement in cefixime absorption by nifedipine was not secondary to increased local blood flows or to induced passive diffusion mechanisms. Nifedipine did not affect intestinal motility. The action of nifedipine appears to indirect, involving a neural regulation, because any increase in cefixime absorption was prevented by tetrodotoxin and hexamethonium administration.

Published

1997

288. Physiology of chemotherapy-induced emesis and antiemetic therapy. Predictive models for evaluation of new compounds.

Author

Veyrat-Follet C, Farinotti R, and Palmer JL

Subjects

Animals, Antineoplastic Agents adverse effects, Disease Models, Animal, Drug Evaluation, Preclinical methods, Humans, Nausea drug therapy, Predictive Value of Tests, Vomiting drug therapy, Antiemetics pharmacology, Nausea chemically induced, Nausea physiopathology, Vomiting chemically induced, Vomiting physiopathology

Abstract

The physiology of emesis has been studied for several hundred years, focusing on the different centres involved and the mechanics of expulsion. The vomiting centre receives inputs from various emetic detectors such as the gut, the vestibular labyrinths and the chemoreceptor trigger zone. Emesis is a common disabling effect in motion sickness, postoperative conditions and in radio- and chemotherapy. Our current understanding of the mechanisms has been provided mainly by the recent introduction of serotonin 5-HT3 receptor antagonists into therapeutic use. Nevertheless, despite the considerable advances made in the understanding of the different pathways involved in emesis, there are number of areas that still require experimental investigation. Different animal and human models are available to study the physiology of emesis and to evaluate the antiemetic activity of new compounds, but they need to be predictors of clinical situations.

Published

1997

289. Effects of nifedipine and diltiazem on pharmacokinetics of cefpodoxime following its oral administration.

Author

Deslandes A, Camus F, Lacroix C, Carbon C, and Farinotti R

Subjects

Administration, Oral, Adult, Anti-Bacterial Agents blood, Ceftizoxime blood, Ceftizoxime pharmacokinetics, Cross-Over Studies, Drug Interactions, Humans, Male, Splanchnic Circulation drug effects, Cefpodoxime Proxetil, Anti-Bacterial Agents pharmacokinetics, Calcium Channel Blockers pharmacology, Ceftizoxime analogs & derivatives, Diltiazem pharmacology, Nifedipine pharmacology

Abstract

We compared the effects of nifedipine and diltiazem on the uptake of cefpodoxime proxetil (CP). The study was aimed at establishing the impact of increased mesenteric blood flow due to calcium channel blockers on passive transport. Twelve volunteers were given CP (200 mg) orally in a crossover design. The absorption, disposition, and elimination parameters of cefpodoxime were compared among the following three treatment groups: CP alone, CP following oral administration of diltiazem (60 mg), or CP following oral administration of nifedipine (20 mg). No statistically significant difference in pharmacokinetic parameters was observed between the three treatment groups.

Published

1996

290. Altered trimethoprim-sulfamethoxazole ratios for prophylaxis and treatment of Toxoplasma gondii and Pneumocystis carinii dual infections in rat model.

Author

Brun-Pascaud M, Chau F, Garry L, Farinotti R, Derouin F, and Girard PM

Subjects

Animals, Anti-Infective Agents adverse effects, Cells, Cultured parasitology, Dose-Response Relationship, Drug, Fluorescent Antibody Technique, Indirect, HIV Infections drug therapy, Lung microbiology, Male, Pneumocystis growth & development, Rats, Rats, Wistar, Toxoplasma growth & development, Trimethoprim, Sulfamethoxazole Drug Combination adverse effects, Anti-Infective Agents administration & dosage, Anti-Infective Agents therapeutic use, Pneumonia, Pneumocystis drug therapy, Pneumonia, Pneumocystis prevention & control, Toxoplasmosis, Animal drug therapy, Toxoplasmosis, Animal prevention & control, Trimethoprim, Sulfamethoxazole Drug Combination administration & dosage, Trimethoprim, Sulfamethoxazole Drug Combination therapeutic use

Abstract

Trimethoprim-sulfamethoxazole (TMP-SMX) is the first-line drug for prophylaxis and treatment of Pneumocystis carinii pneumonia (PCP) and for prophylaxis of toxoplasmosis in HIV-infected patients. Evidence indicating intolerance related to the dose of SMX led us to examine the efficacy of altered TMP-SMX ratios in a corticosteroid-treated rat model. Infections were assessed by counting P. carinii cysts in lung and by titration of Toxoplasma gondii burdens in tissue culture. For prophylaxis, the reference regimen of 20 mg/kg TMP plus 100 mg/kg SMX was effective. Reduced doses of SMX (5 and 20 mg/kg) effective against PCP were effective against toxoplasmosis, provided the TMP dose was increased to 100 mg/kg. For curative treatment, the reversed ratio of 100 mg/kg TMP plus 20 mg/kg SMX was not effective. These results may provide a basis for altering the TMP-SMX ratios in setting of prophylaxis for both infections, especially in HIV infected patients who often poorly tolerate sulfonamides.

Published

1996

291. Clinical pharmacokinetics and metabolism of chloroquine. Focus on recent advancements.

Author

Ducharme J and Farinotti R

Subjects

Animals, Humans, Malaria drug therapy, Malaria metabolism, Stereoisomerism, Tissue Distribution, Antimalarials metabolism, Antimalarials pharmacokinetics, Chloroquine metabolism, Chloroquine pharmacokinetics

Abstract

This paper presents the current state of knowledge on chloroquine disposition, with special emphasis on stereoselectivity and microsomal metabolism. In addition, the impact of the patient's physiopathological status and ethnic origin on chloroquine pharmacokinetics is discussed. In humans, chloroquine concentrations decline multiexponentially. The drug is extensively distributed, with a volume of distribution of 200 to 800 L/kg when calculated from plasma concentrations and 200 L/kg when estimated from whole blood data (concentrations being 5 to 10 times higher). Chloroquine is 60% bound to plasma proteins and equally cleared by the kidney and liver. Following administration chloroquine is rapidly dealkylated via cytochrome P450 enzymes (CYP) into the pharmacologically active desethylchloroquine and bisdesethylchloroquine. Desethylchloroquine and bisdesethylchloroquine concentrations reach 40 and 10% of chloroquine concentrations, respectively; both chloroquine and desethylchloroquine concentrations decline slowly, with elimination half-lives of 20 to 60 days. Both parent drug and metabolite can be detected in urine months after a single dose. In vitro and in vivo, chloroquine and desethylchloroquine competitively inhibit CYP2D1/6-mediated reactions. Limited in vitro studies and preliminary data from clinical experiments and observations point to CYP3A and CYP2D6 as the 2 major isoforms affected by or involved in chloroquine metabolism. In vitro efficacy studies did not detect any difference in potency between chloroquine enantiomers but, in vivo in rats, S(+)-chloroquine had a lower dose that elicited 50% of the maximal effect (ED950) than that of R(-)-chloroquine. Stereoselectivity in chloroquine body disposition could be responsible for this discrepancy. Chloroquine binding to plasma proteins is stereoselective, favouring S(+)-chloroquine (67% vs 35% for the R-enantiomer). Hence, unbound plasma concentrations are higher for R(-)-chloroquine. Following separate administration of the individual enantiomers, R(-)-chloroquine reached higher and more sustained blood concentrations. The shorter half-life of S(+)-chloroquine appears secondary to its faster clearance. Blood concentrations of the S(+)-forms of desethylchloroquine always exceeded those of the R(-)-forms, pointing to a preferential metabolism of S(+)-chloroquine.

Published

1996

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

Author

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

Subjects

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

Abstract

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

Published

1996

293. Intestinal elimination of ofloxacin enantiomers in the rat: evidence of a carrier-mediated process.

Author

Rabbaa L, Dautrey S, Colas-Linhart N, Carbon C, and Farinotti R

Subjects

Animals, Area Under Curve, Chromatography, High Pressure Liquid, In Vitro Techniques, Male, Perfusion, Rats, Rats, Sprague-Dawley, Stereoisomerism, Anti-Infective Agents pharmacokinetics, Carrier Proteins metabolism, Intestinal Mucosa metabolism, Ofloxacin pharmacokinetics

Abstract

The aim of this work was to examine the mechanism involved in intestinal elimination of the two optical isomers of ofloxacin in the rat. An intestinal segment was isolated in situ and perfused with saline, while drug solution was administered via the carotid artery. Blood samples and intestinal effluents were collected and analyzed by a high-performance liquid chromatography method. We observed saturable and stereoselective intestinal elimination of the ofloxacin enantiomers. The elimination process favored the R-(+) form of the molecule. After a parenteral dose of 20 mg of racemic ofloxacin per kg of body weight, intestinal clearances were 0.23 +/- 0.03 versus 0.30 +/- 0.03 ml/min for S-(-)- and R-(+)-ofloxacin, respectively. Ciprofloxacin and pefloxacin interfered with ofloxacin elimination and significantly reduced the intestinal clearance of S-(-)- and R-(+)-ofloxacin. With concomitant ciprofloxacin, intestinal clearances became 0.13 +/- 0.02 versus 0.17 +/- 0.03 ml/min and 0.14 +/- 0.01 versus 0.19 +/- 0.05 ml/min with pefloxacin for S-(-)- and R-(+)-ofloxacin, respectively. Those findings argue for the presence of a common transport system in the rat intestine with variable affinities for fluoroquinolones. In addition, verapamil and quinidine, two P-glycoprotein blockers, significantly reduced the intestinal elimination of both ofloxacin isomers (with concomitant verapamil, intestinal clearances were 0.12 +/- 0.02 versus 0.18 +/- 0.03 ml/min for S-(-)- and R-(+)-ofloxacin, respectively, while with concomitant quinidine, values were 0.18 +/- 0.01 versus 0.23 +/- 0.01 ml/min without modifying their areas under the concentration-time curve in serum. Similar results were found with another fluoroquinolone, ciprofloxacin, in previous work. P-glycoprotein appears to be involved in the intestinal elimination of fluoroquinolones in rats. The characterization of fluoroquinolone intestinal elimination has significant clinical relevance for the better evaluation of the influence of this secretory pathway on antibiotic efficacy and selection of resistant bacteria within the intestinal flora.

Published

1996

294. Role of prostaglandins and nitric oxide on halothane-induced arteriolar dilatation in rat diaphragm.

Author

de Larminat V, Boczkowski J, Dureuil B, Vicaut E, Farinotti R, Aubier M, and Desmonts JM

Subjects

Animals, Arterioles drug effects, Arterioles physiology, Indomethacin pharmacology, Male, Mefenamic Acid pharmacology, Nitric Oxide physiology, Nitric Oxide Synthase antagonists & inhibitors, Nitroarginine pharmacology, Rats, Rats, Sprague-Dawley, Vasodilation physiology, Anesthetics, Inhalation pharmacology, Diaphragm blood supply, Halothane pharmacology, Prostaglandins physiology, Vasodilation drug effects

Abstract

The effects of anaesthetics on the microcirculation of the diaphragm are incompletely understood. Therefore, we assessed by in vivo intravital microscopy in rats the action of halothane on diaphragmatic arteriolar diameter and the role of nitric oxide and prostaglandins on halothane-induced diaphragmatic arteriolar diameter. We studied 54 rats anaesthetized with thiopentone. Dose-response curves to topically applied Krebs' solution saturated with halothane at increasing concentrations of 0%, 1%, 3% and 5% were carried out in the presence of an inhibitor of nitric oxide synthesis (N omega-nitro-L-arginine (LNA), 300 mumol litre-1) or inhibitors of prostaglandin synthesis (mefenamic acid 20 mumol litre-1 or indomethacin 20 mol litre-1) or in the absence of any inhibitor. We found dose-dependent arteriolar dilatation which was abolished by mefenamic acid and indomethacin. In contrast, the effect of halothane was not modified by LNA. These data demonstrated that halothane-induced arteriolar dilatation in the diaphragm of the rat was mediated by prostaglandins but not by nitric oxide.

Published

1996

295. Uptake of mefloquine enantiomers into uninfected and malaria-infected erythrocytes.

Author

Vidrequin S, Gimenez F, Basco LK, Martin C, LeBras J, and Farinotti R

Subjects

Animals, Antimalarials blood, Erythrocytes parasitology, Hydrogen-Ion Concentration, Mefloquine blood, Molecular Conformation, Plasmodium falciparum, Temperature, Antimalarials pharmacokinetics, Erythrocytes metabolism, Mefloquine pharmacokinetics

Published

1996

296. Therapy of visceral leishmaniasis due to Leishmania infantum: experimental assessment of efficacy of AmBisome.

Author

Gangneux JP, Sulahian A, Garin YJ, Farinotti R, and Derouin F

Subjects

Amphotericin B therapeutic use, Animals, Antimony administration & dosage, Antimony therapeutic use, Antiprotozoal Agents therapeutic use, Drug Carriers, Female, Leishmania infantum isolation & purification, Leishmaniasis, Visceral parasitology, Liposomes, Meglumine administration & dosage, Meglumine therapeutic use, Meglumine Antimoniate, Mice, Mice, Inbred BALB C, Organometallic Compounds administration & dosage, Organometallic Compounds therapeutic use, Amphotericin B administration & dosage, Antiprotozoal Agents administration & dosage, Leishmania infantum drug effects, Leishmaniasis, Visceral drug therapy

Abstract

The tolerance and efficacy of amphotericin B (AmB) deoxycholate (Fungizone) were compared with those of liposomal AmB (AmBisome) in a murine model of visceral leishmaniasis induced by Leishmania infantum. Control groups consisted of untreated mice and mice treated with a pentavalent antimonial (Glucantime). BALB/c mice were infected intravenously on day 0 with 10(7) promastigotes of L. infantum and then treated from day 7 to 17 (early treatment group) or from day 60 to 70 (delayed treatment group). The pentavalent antimonial was administered daily by intraperitoneal injection, whereas AmB formulations were administered intravenously on alternate days. On days 20, 60, and 120 (early treatment group) and on days 72 and 125 (delayed treatment group), parasite burdens in the liver, spleen, and lungs were determined by subculturings using a microtitration method. A dose range study showed that administration of AmBisome at the well-tolerated doses of 5 or 50 mg/kg of body weight completely eradicated the parasites from the tissues. At 0.8 mg/kg, AmBisome proved more efficacious than AmB deoxycholate administered at the same dose. We also compared the levels of AmB deoxycholate and AmBisome in plasma and tissue. Mice treated with AmBisome had levels of AmB in tissue much higher than did AmB deoxycholate-treated mice with persistent detectable levels 14 weeks after treatment. These results seem to account for the remarkable efficacy of the liposomal formulation of AmB in the treatment of visceral leishmaniasis due to L. infantum.

Published

1996

297. Importance of penicillinase production for activity of penicillin alone or in combination with sulbactam in experimental endocarditis due to methicillin-resistant Staphylococcus aureus.

Author

Fantin B, Pierre J, Castéla-Papin N, Saint-Julien L, Drugeon H, Farinotti R, and Carbon C

Subjects

Animals, Drug Synergism, Drug Therapy, Combination pharmacology, Female, Penicillins pharmacology, Penicillins therapeutic use, Rabbits, Staphylococcus aureus drug effects, Staphylococcus aureus genetics, Sulbactam pharmacology, Sulbactam therapeutic use, Drug Therapy, Combination therapeutic use, Endocarditis drug therapy, Methicillin Resistance, Penicillinase biosynthesis, Staphylococcal Infections drug therapy, Staphylococcus aureus enzymology

Abstract

The activity of penicillin, alone and in combination with sulbactam, against a heterogeneously methicillin-resistant, penicillinase-producing clinical isolate of Staphylococcus aureus and its penicillinase-negative derivative was investigated in vitro and in a rabbit experimental endocarditis model. Penicillin was significantly more effective than vancomycin against the penicillinase-negative derivative in vivo (P < 0.001), and it sterilized 25% of the vegetations. The combination of penicillin and sulbactam exhibited an in vivo synergistic effect on the penicillinase-producing strain (P < 0.01) but did not produce any advantage over treatment with vancomycin, even when a high dose of sulbactam was used (100 mg/kg of body weight every 6 h). This combination was significantly less effective against the penicillinase-producing strain than was penicillin alone against the penicillinase-negative derivative (P < 0.03). In addition, the most resistant subpopulation of the surviving bacteria, which grew on agar containing 16 micrograms of methicillin per ml, was detected in 5 of 6 animals treated with penicillin and a high dose of sulbactam against the penicillinase-producing strain compared with only 1 of 12 animals treated with penicillin alone against the penicillinase-negative derivative (P < 0.01). We conclude that penicillin is highly effective against penicillinase-negative methicillin-resistant S. aureus and that penicillinase production, rather than methicillin resistance, appears to be the limiting factor for the activity of the penicillin-sulbactam combination against penicillinase-producing, methicillin-resistant S. aureus.

Published

1996

298. [Antacid activity of citrate-bicarbonate complex of effervescent formulations of ranitidine. In vitro analysis using 'artificial stomach-duodenum' model].

Author

Vatier J, Cai S, Slama A, and Farinotti R

Subjects

Antacids pharmacology, Drug Combinations, Duodenum physiology, In Vitro Techniques, Ranitidine administration & dosage, Ranitidine chemistry, Stomach physiology, Tablets, Antacids administration & dosage, Bicarbonates administration & dosage, Bicarbonates pharmacology, Citrates administration & dosage, Citrates pharmacology, Computer Simulation

Abstract

Antacid activity supported by citrate-bicarbonate complex of four effervescent ranitidine forms has been assessed in vitro using an 'artificial stomach-duodenum' model controlled by microcomputer. This model allows (i) maintenance of constant the rates of the fluxes throughout the experiments or (ii) simulation of gastroduodenal flux regulation, in the normal subject (NS) or in the duodenal ulcer patient (DU) situation. The four forms developed a theoretical maximal antacid capacity between 61 and 81 mmol with a maximum intragastric pH between 3.2 and 4.8. In the gastroduodenal flux regulation simulation, antacid activity duration was rapid and included between 85 and 118 min in NS situation (50 to 56 mmol H+ consumed) and between 75 and 93 min in DU situation (43 to 47 mmol H+ consumed). The reduction of acid load penetrating into the duodenum was contained between 36 and 50 per cent. Effervescent compounds exerted a neutralising activity and a buffering capacity close to pH 6.0 (5 per cent of total antacid capacity), related to antacid potency.

Published

1996

299. In vitro assessment of antacid efficacy using a computer-controlled 'artificial stomach-duodenum' model reproducing gastroduodenal flux regulation.

Author

Vatier J, Cai S, Célice-Pingaud C, Castela-Papin N, Mignon M, and Farinotti R

Subjects

Aluminum pharmacology, Aluminum therapeutic use, Antacids therapeutic use, Calcium pharmacology, Calcium therapeutic use, Drug Combinations, Drug Evaluation, Duodenogastric Reflux drug therapy, In Vitro Techniques, Magnesium pharmacology, Magnesium therapeutic use, Antacids pharmacology, Computer Simulation, Duodenum physiology, Stomach physiology

Abstract

We have developed an artificial stomach-duodenum model made up of three compartments representing the stomach, (including a fragment of hog gastric mucosa), the proximal duodenum, and the distal duodenum. Gastroduodenal flow rates are controlled by a microcomputer capable of (1) adjusting gastric emptying and alkaline secretion in the proximal duodenum according to intragastric pH; (2) adjusting pancreatic alkaline secretion according to proximal duodenum pH; and (3) simulating acid response to food ingestion. Antacid drugs were added 90 min after simulated food ingestion in near-physiological or duodenal ulcer conditions. Aluminum phosphate-containing antacids resulted in a persistent antacid effect, due to their adsorption to the gastric mucosa; this prolonged the buffering capacity at pH 2.4 to 120 min. Aluminum+magnesium hydroxides and calcium+magnesium carbonate combinations mainly exerted neutralizing activity, inducing an increase in the gastric emptying rate. In the duodenal ulcer simulation, the pH of the gastric contents was lower and the antacid effect was shorter than in the 'physiological' simulation.

Published

1996

300. Pharmacokinetics of propofol after a single dose in children aged 1-3 years with minor burns. Comparison of three data analysis approaches.

Author

Murat I, Billard V, Vernois J, Zaouter M, Marsol P, Souron R, and Farinotti R

Subjects

Age Factors, Child, Preschool, Female, Humans, Infant, Male, Anesthetics, Intravenous pharmacokinetics, Burns metabolism, Propofol pharmacokinetics

Abstract

Background: No complete pharmacokinetic profile of propofol is yet available in children younger than 3 yr, whereas clinical studies have demonstrated that both induction and maintenance doses of propofol are increased with respect to body weight in this age group compared to older children and adults. This study was therefore undertaken to determine the pharmacokinetics of propofol after administration of a single dose in aged children 1-3 yr requiring anesthesia for dressing change., Methods: This study was performed in 12 children admitted to the burn unit and in whom burn surface area was less than or equal to 12% of total body surface area. Exclusion criteria were: unstable hemodynamic condition, inappropriate fluid loading, associated pulmonary injury, or burn injury older than 2 days. Propofol (4 mg.kg(-1))plus fentanyl (2.5 microg.kg(-1)) was administered while the children were bathed and the burn area cleaned during which the children breathed spontaneously a mixture of oxygen and nitrous oxide (50:50). Venous blood samples of 300 microl were obtained at 5, 15, 30, 60, 90, and 120 min, and 3, 4, 8, and 12 thereafter injection; an earlier sample was obtained from 8 of 12 children. The blood concentration curves obtained for individual children were analyzed by three different methods: noncompartmental analysis, mixed effects population model, and standard two-stage analysis., Results: Using noncompartmental analysis, total clearance of propofol (+/-SD) was 0.053+/-0.013l.kg(-1).min(-1), volume of distribution at steady state9.5 +/- 3.7l.kg(-1),and residence time 188 +/- 85 min. Propofol pharmacokinetics were best described by a weight-proportional three-compartmental model in both population and two-stage analysis. Estimated and derived pharmacokinetic parameters were similar using these two pharmacokinetic approaches. Results of population versus two-stage analysis are as follow: systemic clearance 0.049 versus 0.048 l.kg(-).min(-1), volume of central compartment 1.03 versus 0.95 l.kg(-1), volume of steady state 8.09 versus 8.17 l.kg(-1)., Conclusions: The volume of the central compartment and the systemic clearance were both greater than all values reported in older children and adults. This is consistent with the increased propofol requirements for both induction and maintenance of anesthesia in children 1-3 yr. (Key words: Anesthesia: pediatric. Pharmacokinetics: propofol.)

Published

1996