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  • 1
    Electronic Resource
    Electronic Resource
    Springer
    European journal of clinical pharmacology 20 (1981), S. 127-133 
    ISSN: 1432-1041
    Keywords: ketoprofen ; pharmacokinetics ; multipledose ; bioavailability ; assay ; modelling
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology , Medicine
    Notes: Summary A commercial capsule containing 50 mg of ketoprofen (Orudis), a simple capsule containing 50 mg of ketoprofen alone and 50 mg of ketoprofen in an aqueous solution were given as separate doses in a randomized sequence to 12 normal adult males. The areas under the resulting plasma concentration-time curves (AUC) were remarkably consistent for each volunteer. The bioavailability from the commerical capsule relative to that from the solution was 99.7%±10.5% and that from the simple capsule was 102%±10%. After 6 of the volunteers had taken the commercial capsule 6 hourly for thirteen doses, their AUC extrapolated to infinity was significantly higher (by 22%) than that after the single dose indicating, contrary to previous reports, accumulation upon multiple dosing. The interdose AUC after the thirteenth dose was, however, statistically indistinguishable from the AUC-to-infinity after the single dose as might be expected from linear kinetics. The ketoprofen solution generated peak plasma concentrations in only one-third the time (21±7 min) required for the capsules (commercial, 72±45; simple, 61±39 min). Despite plasma concentrations being tracked over a 200-fold range, log linearity was not established within 12 h in any of the 42 profiles obtained. A two-compartment open model was fitted to the solution data giving excellent prediction of the time-to-peak and clearance (Cl/F=5.2±1.1 l/h) as determined by eye and by log-trapezoidal rule, respectively.
    Type of Medium: Electronic Resource
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  • 2
    ISSN: 1573-5052
    Keywords: Cyperus alopecuroides ; Hydrilla verticillata ; Ipomoea aquatica ; Primary production ; Scirpus tuberosus ; Sporobolus helvolus ; Standing crop ; Water level
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology
    Notes: Abstract Paspalum distichum L. has been the dominant species in the monsoonal wetlands of the Keoladeo National Park in northcentral India since 1982 when grazing by water buffalo and domestic cattle was halted. Maximum water levels in these wetlands occur immediately after the end of the summer monsoon in late September of early October and then decline until the next summer monsoon the following June. After the normal 1985 monsoon, maximum water depths were around 140 cm. After the poor 1986 monsoon, maximum water depths were only around 60 cm. Paspalum distichum maximum aboveground biomass at four sites ranged from 850 g m-2 at the shallowest site to 3400 g m−2 at a deep water site. The maximum biomass of other vegetation types, which had dominated this wetland prior to 1982, ranged from 1400 g m-2 at a deep water site (Ipomoea aquatica Forsk.) to only 240 g m-2 to 400 g m-2 at a deep-water submersed site (Hydrilla verticillata (L. f.) Royle/Cyperus alopecuroides Rottb.) and at a shallow emergent site (Scirpus tuberosus Desf./Sporobolus helvolus (Trin.) Dur. et Schinz). For all vegetation types, biomass changed seasonally in response to changing water levels and temperatures. After the 1986 monsoon, above-ground biomass for all vegetation types was much lower than it had been after the 1985 monsoon. Mean below-ground biomass was very low in all vegetation types (1 to 47 g m-2). Paspalum distichum had a higher aboveground biomass at nearly all water depths in all seasons than that of the pre-1982 vegetation types. Paspalum distichum belowground biomass, however, is comparable to, or less than, that of the pre-1982 vegetation types. During years with an average monsoon, the overall primary production of these wetlands is estimated to have increased 2.5 to 3.5-fold since they were overgrown with Paspalum distichum.
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  • 3
    ISSN: 1573-8744
    Keywords: disopyramide ; pharmacokinetics ; pharmacodynamics ; electrophysiology ; protein binding ; modelling
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology
    Notes: Abstract The pharmacokinetics and pharmacodynamics of the antiarrhythmic drug, disopyramide, were investigated in 12 volunteers who took 300 mg doses of 3 different capsule preparations and an aqueous oral solution of the drug at 1-week intervals. Concentrations of drug unbound to plasma proteins were measured by a sensitive immunoenzyme assay after ultrafiltration of plasma samples taken serially after dosing. QT interval was measured on serial ECG recordings with correction for changes in heart rate. Unbound concentrations of disopyramide were modelled by an open one-compartment pharmacokinetic model with a zero-order absorption rate and a lag time. There was no significant difference in parameter estimates between the four preparations, except for the lag time, which was significantly shorter for the solution preparation. The saturable protein binding of disopyramide was described by a hyperbolic model including a specific binding site and additional nonspecific binding. The pharmacodynamic relationship between unbound drug concentration and QT prolongation was fit by a simple linear model. This fit was better using unbound concentration of the drug than using total concentrations.
    Type of Medium: Electronic Resource
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