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1

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Plasma levels of oxybutynine chloride in children (1994)

Autret, E. ; Jonville, A. P. ; Dutertre, J. P. ; [et al.]

Springer

European journal of clinical pharmacology 46 (1994), S. 83-85

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ISSN: 1432-1041

Keywords: Enuresis ; Oxybutynine chloride ; children ; pharmacokinetics ; adverse effects ; anticholinergic actions

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Abstract Anticholinergic adverse-effects in children treated with conventional doses of oxybutynine led us to measure plasma oxybutynine levels in children. 18 children, aged 5 to 13 y, who required treatment with oxybutynine chloride for daytime incontinence were studied. Plasma concentrations were measured on the fifth day of a course of treatment in which the dose was adapted to the child's body weight; the dose was given twice daily at 12-hour intervals. In 10 children aged between 5 and 8 y, the mean dose was 0.1 mg · kg−1. In 8 children aged between 10 and 13 years, the mean dose was 0.15 mg · kg−1. The highest concentration was usually found between 1 and 2 h after administration. The subsequent fall in concentration was rapid and after 6 h oxybutynine was no longer measurable in 14 of the children. The concentrations found were not different from those seen in adults given equivalent doses. The results show that plasma concentrations in children were not very different from those observed in adults if the dose were adapted to the body weight of the children. No special differences in paediatric use were revealed that might explain the particular adverse-effects. The results of the study argue against the dosage regimen proposed before these adverse events were detected. They strongly favour a dose adapted to the body weight of the child, with a 12-hour interval between doses.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00195921

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2

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Statistical estimations in pharmacokinetics (1974)

Boxenbaum, Harold G. ; Riegelman, Sidney ; Elashoff, Robert M.

Springer

Journal of pharmacokinetics and pharmacodynamics 2 (1974), S. 123-148

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ISSN: 1573-8744

Keywords: pharmacokinetics ; computer program ; NONLIN ; data weighting ; isoniazid

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract Several important statistical aspects of pharmacokinetic analyses by digital computer are discussed. These include selection of appropriate equations, weighting of data, precision of parameter estimates, comparisons of parameters, analysis of weighted residuals, and criteria useful in the selection of particular models. Data obtained after administration of isoniazid and isonicotinuric acid to man are analyzed to illustrate the usefulness of the discussed methods.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01061504

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3

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Enhancement of Tissue Delivery and Receptor Occupancy of Methylprednisolone in Rats by a Liposomal Formulation (1993)

Mishina, Elena V. ; Straubinger, Robert M. ; Pyszczynski, Nancy A. ; [et al.]

Springer

Pharmaceutical research 10 (1993), S. 1402-1410

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ISSN: 1573-904X

Keywords: liposomes ; methylprednisolone ; pharmacokinetics ; tissue distribution ; pharmacodynamics ; glucocorticoid receptors ; drug delivery

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract A liposomal formulation of methylprednisolone (L-MPL) was developed to improve localization of this immunosuppressant in lymphatic tissues. Liposomes containing MPL were formulated from a mixture of phosphatydylcholine and phosphatydylglycerol (molar ratio, 9:1) and sized by extrusion through a 0.1-µm membrane. Male Sprague–Dawley rats received a bolus dose of 2 mg/kg of L-MPL or free MPL in solution (control). Samples of blood, spleen, liver, thymus, and bone marrow were collected at intervals over a 66-hr period. Concentrations of MPL in plasma and organs and free cytosolic glucocorticoid receptors (GCR) in spleen and liver were determined. The plasma MPL profiles for free and L-MPL were bi- and triexponential. Although the alpha phase kinetics of both dosage forms were similar, L-MPL showed a substantially slower elimination phase than did free drug. Incorporation of MPL into liposomes caused the following increases: terminal half-life, from 0.48 (MPL) to 30.13 hr (L-MPL); MRT, from 0.42 to 11.95 hr, V ss, from 2.10 to 21.87 L/kg; and AUC, from 339 to 1093 ng · hr/mL. Uptake of liposomes enhanced significantly the delivery of drug to lymphatic tissues and liver; AUC tissue:plasma ratios for spleen increased 77-fold; for liver, 9-fold; and for thymus, 27-fold. The duration of GCR occupancy was extended 10-fold in spleen and 13-fold in liver by the liposomal formulation. Lymphatic tissue selectivity and extended receptor binding of liposome-delivered MPL offer promise for enhanced immunosuppression.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1018954704886

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4

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Relationship between in vivo drug exposure of the tumor interstitium and inhibition of tumor cell growth in vitro: a study in breast cancer patients (2000)

Müller, Markus ; Bockenheimer, Julia ; Zellenberg, Ulrike ; [et al.]

Springer

Breast cancer research and treatment 60 (2000), S. 211-217

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ISSN: 1573-7217

Keywords: breast cancer ; 5-fluorouracil ; methotrexate ; pharmacodynamics ; pharmacokinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract A novel approach is described to simulate effect site pharmacodynamics of anticancer drugs. This approach is based on (i) the in vivo measurement of unbound, interstitial drug pharmacokinetics (PK) in solid tumor lesions in patients and (ii) a subsequent pharmacodynamic (PD) simulation of the time versus drug concentration profile in an in vitro setting. For this purpose, breast cancer cells (MCF-7) were exposed in vitro to the time versus interstitial tumor concentration profiles of 5-fluorouracil (5-FU) and methotrexate (MTX) from primary breast cancer lesions in patients. This led to a maximal reduction in the viable cell count of 69 on day 4, and of 71 on day 7 for 5-FU and MTX, respectively. This effect was dependent on the initial cell count and was characterized by a high interindividual variability. For 5-FU there was a significant correlation between the maximum antitumor effect and the intratumoral AUC (r = 0.82, p = 0.0005), whereas no correlation could be shown for MTX (r = 0.05, p = 0.88). We conclude, that the in-vivo-PK / in-vitro-PD model presented in this study may provide a rational approach for describing and predicting pharmacodynamics of cytotoxic drugs at the target site. Data derived from this approach support the concept that tumor penetration of 5-FU may be a response-limiting event, while the response to MTX may be determined by events beyond interstitial fluid kinetics.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1006497202341

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5

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Safety, Toxicokinetics and Tissue Distribution of Long-Term Intravenous Liposomal Amphotericin B (ambisome®): A 91-day Study in Rats (2000)

Bekersky, Ihor ; Boswell, Garry W. ; Hiles, Richard ; [et al.]

Springer

Pharmaceutical research 17 (2000), S. 1494-1502

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ISSN: 1573-904X

Keywords: amphotericin B ; liposomes ; pharmacokinetics ; toxicokinetics ; tissue distribution ; toxicity

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract Purpose. Amphotericin B in small, unilamellar liposomes (AmBisome) is safer and produces higher plasma concentrations than other formulations. Because liposomes may increase and prolong tissue exposures, the potential for drug accumulation or delayed toxicity after chronic AmBisome was investigated. Methods. Rats (174/sex) received intravenous AmBisome (1, 4, or 12 mg/kg), dextrose, or empty liposomes for 91 days with a 30-day recovery. Safety (including clinical and microscopic pathology) and toxicokinetics in plasma and tissues were evaluated. Results. Chemical and histopathologic changes demonstrated that the kidneys and liver were the target organs for chronic AmBisome toxicity. Nephrotoxicity was moderate (urean nitrogen [BUN] ≤51 mg/dl; creatinine unchanged). Liposome-related changes (vacuolated macrophages and hypercholesterolemia) were also observed. Although plasma and tissue accumulation was nonlinear and progressive (clearance and volume decreased, half-life increased with dose and time), most toxic changes occurred early, stabilized by the end of dosing, and reversed during recovery. There were no delayed toxicities. Concentrations in liver and spleen greatly exceeded those in plasma; kidney and lung concentrations were similar to those in plasma. Elimination half-lives were 1-4 weeks in all tissues. Conclusions. Despite nonlinear accumulation, AmBisome revealed predictable hepatic and renal toxicities after 91 days, with no new or delayed effects after prolonged treatment at high doses that resulted in plasma levels 〉200 μg/ml and tissue levels 〉3000 μg/g.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1007605024942

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6

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Safety and Toxicokinetics of Intravenous Liposomal Amphotericin B (AmBisome ®) in Beagle Dogs (1999)

Bekersky, Ihor ; Boswell, Garry W. ; Hiles, Richard ; [et al.]

Springer

Pharmaceutical research 16 (1999), S. 1694-1701

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ISSN: 1573-904X

Keywords: amphotericin B ; liposomes ; pharmacokinetics ; tissue distribution ; toxicity ; toxicokinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract Purpose. Amphotericin B (AmB) in small, unilamellar liposomes (AmBisome ®) has an improved therapeutic index, and altered pharmacokinetics. The repeat-dose safety and toxicokinetic profiles of AmBisome were studied at clinically relevant doses. Methods. Beagle dogs (5/sex/group) received intravenous AmBisome (0.25, 1,4, 8, and 16 mg/kg/day), empty liposomes or vehicle for 30 days. AmB was determined in plasma on days 1, 14, and 30, and in tissues on day 31. Safety parameters included body weight, clinical chemistry, hematology and microscopic pathology. Results. Seventeen of twenty animals receiving 8 and 16 mg/kg were sacrificed early due to weight loss caused by reduced food intake. Dose-dependent renal tubular nephrosis, and other effects characteristic of conventional AmB occurred at 1 mg/kg/day or higher. Although empty liposomes and AmBisome increased plasma cholesterol, no toxicities unique to AmBisome were revealed. Plasma ultrafiltrates contained no AmB. AmBisome achieved plasma levels 100-fold higher than other AmB formulations. AmBisome kinetics were non-linear, with clearance and distribution volumes decreasing with increasing dose. This, and nonlinear tissue uptake, suggest AmBisome disposition was saturable. Conclusions. AmBisome has the same toxic effects as conventional AmB, but they appear at much higher plasma exposures. AmBisome's non-linear pharmacokinetics are not associated with increased risk, as toxicity increases linearly with dosage. Dogs tolerated AmBisome with minimal to moderate changes in renal function at doses (4 mg/kg/day) producing peak plasma concentrations of 18−94 µg/mL.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1018997730462

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7

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Physicochemical, Pharmacokinetic and Pharmacodynamic Evaluation of Liposomal Tacrolimus (FK 506) in Rats (1995)

Lee, Mi-Jeong ; Straubinger, Robert M. ; Jusko, William J.

Springer

Pharmaceutical research 12 (1995), S. 1055-1059

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ISSN: 1573-904X

Keywords: tacrolimus (FK 506) ; immunosuppressant ; HCO-60 (castor oil derivatives) ; liposomes ; formulation ; pharmacokinetics ; targeting ; pharmacodynamics ; splenocyte proliferation

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract Purpose. Tacrolimus (FK 506) is a new potent immunosuppressant. Because of poor water solubility, the conventional intravenous dosage forms of FK 506 (C-FK 506) contain surfactants such as HCO-60 which may cause adverse effects. We sought a liposomal formulation of FK 506 (L-FK 506) containing endogenous phospholipids to target drug to the spleen, a major organ controlling the immune system. Methods. L-FK 506, consisting of 0.1 µm diameter vesicles of phosphatidylcholine and phosphatidylglycerol (molar ratio 9:1) and 7.5 mole% drug, was evaluated for in vitro stability. The intravenous disposition profile, spleen distribution, and immunosuppression of L-FK 506 was compared with that of C-FK 506 in the rat after single doses of 0.3 mg/kg. Results. The L-FK 506 showed good in vitro stability. L-FK 506 exhibited an increased volume of distribution at steady-state (Vss) (from 3.41 to 14.71 L/kg) and increased mean residence time (MRT) (from 2.83 to 16.07 hr). FK 506 concentrations in spleen were increased by 40% at 10 hr after administration of the liposomal formulation. The pharmacodynamics of L-FK 506, evaluated by the extent of inhibition of splenocyte proliferation, was comparable to that of C-FK 506. Conclusions. Liposomal FK 506 may be an improved dosage form for parenteral use.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1016222817860

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8

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A Retrospective Analysis of Fenoldopam Renal Excretion in 65 Subjects: Evidence for Possible Intrarenal Formation of Fenoldopam from Its Metabolites (1989)

Ziemniak, John A. ; Boppana, Venkata K. ; Cyronak, Matthew J. ; [et al.]

Springer

Pharmaceutical research 6 (1989), S. 702-705

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ISSN: 1573-904X

Keywords: fenoldopam ; renal excretion ; reversible metabolism ; pharmacokinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract Clinical studies have suggested that the dopamine DA1 agonist, fenoldopam, may exhibit nonlinear renal excretion in humans. A retrospective population pharmacokinetic analysis of the renal excretion of fenoldopam and one of its major metabolites, fenoldopam-8-sulfate, was conducted in 65 healthy volunteers to examine this phenomenon. Fenoldopam-8-sulfate exhibited a mean (±SE) renal plasma clearance of 129 ± 4 ml/min, which was independent of its AUC. In contrast, fenoldopam renal plasma clearance ranged from 2220 to 150 ml/min and decreased nonlinearily with increasing fenoldopam AUC. Fenoldopam renal clearance was characterized as a function of fenoldopam AUC using a nonlinear saturation model. The analysis predicted an initial maximal renal clearance of 2852 ml/min, which decreased to 78 ml/min at maximal inhibition. The fenoldopam AUC required to half-saturate fenoldopam renal clearance was 5.2 ng × hr/ml. The elevated clearance values for fenoldopam, beyond normal physiologic limits for renal blood flow in man, suggest that intrarenal formation of fenoldopam from one or more of its circulating metabolites may be contributing to the observed nonlinear decreases in fenoldopam renal excretion. Preliminary data from our laboratory suggest that in vivo desulfation of fenoldopam-8-sulfate to fenoldopam does occur in the dog.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1015990506743

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Synthesis of Allylic Isoprenoid Diphosphates by SN2 Displacement of Diethyl Phosphate (2000)

Ravn, Matthew M. ; Jin, Qingwu ; Coates, Robert M.

Weinheim : Wiley-Blackwell

Liebigs Annalen 2000 (2000), S. 1401-1410

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ISSN: 1434-193X

Keywords: Phosphorylations ; Deuterium labeling ; Asymmetric labeling ; Terpenoid biosynthesis ; Enzyme inhibitors ; Chemistry ; General Chemistry

Source: Wiley InterScience Backfile Collection 1832-2000

Topics: Chemistry and Pharmacology

Notes: ---Allylic polyenyl diphosphates such as geranyl and (E,E,E)-geranylgeranyl diphosphates are ubiquitous substrates for monoterpene and diterpene synthases and transferases in isoprenoid biosynthesis. These enzyme substrates were prepared in asymmetrically labeled form by reduction of 1-deuterio aldehyde precursors with (R)- and (S)-Alpine boranes®, conversion into diethyl phosphates, and SN2 displacements with tris(tetrabutylammonium) pyrophosphate which occurred slowly with essentially complete inversion of configuration over 2-5 days. The 8α- and 8β-hydroxy-17-nor analogs (13 and 14) of copalyl diphosphate as well as the (15R)-deuterium-labeled form of 13 were similarly prepared from nor-diols 11, (15S)-[15-2H1]-11, and 12 by means of regioselective phosphorylation of the allylic hydroxy groups and displacements with pyrophosphate anion. The configurations and enantiopurities of the deuterium-labeled geraniols, before and after the SN2 displacements, and the diastereopurity of the bicyclic keto alcohol intermediate (15S)-[15-2H1]-15 were determined by conversion into (1S)-camphanate esters and 1H-NMR analysis. Amino alcohol 18 was similarly converted into amino diphosphate 19, 15-aza-14,15-dihydro GGPP, a potential aza analog inhibitor for diterpene synthases which generate stereoisomeric forms of copalyl diphosphate.

Type of Medium: Electronic Resource

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Neue Ergebnisse der Chemie von Insektenpheromonen (1973)

Macconnell, John G. ; Silverstein, Robert M.

Weinheim : Wiley-Blackwell

Zeitschrift für die chemische Industrie 85 (1973), S. 647-657

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ISSN: 0044-8249

Keywords: Chemistry ; General Chemistry

Source: Wiley InterScience Backfile Collection 1832-2000

Topics: Chemistry and Pharmacology

Notes: Pheromone sind Wirkstoffe, die ein Tier, speziell ein Insekt, nach außen abgibt und die auf andere Individuen der gleichen Art einwirken. Der Name ist vom griechischen „pherein“ (übertragen) und „horman“ (erregen, anregen) abgeleitet. Zu den Pheromonen zählen Sexuallockstoffe, Alarmstoffe, „Versammlungspheromone“ u.a. Viele dieser Stoffe wirken bereits in überaus niedriger Konzentration. Unter den Insektenpheromonen befinden sich auffallend viele Derivate langkettiger, wenig verzweigter Kohlenwasserstoffe.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1002/ange.19730851503

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