ZIB

Hits per page

hits 1 - 7 | 7 hits

Sorting

Electronic Resource

Radioimmunoassay of plasma lisuride in man following intravenous and oral administration of lisuride hydrogen maleate; effect on plasma prolactin level (1981)

Hümpel, M. ; Nieuweboer, B. ; Hasan, S. H. ; [et al.]

Springer

European journal of clinical pharmacology 20 (1981), S. 47-51

add to mindlist on the mindlist

Details

ISSN: 1432-1041

Keywords: lisuride ; prolactin ; plasma levels ; halflife ; pharmacokinetics ; dopamine agonist

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary The development of a sensitive radioimmunoassay for the determination of lisuride in plasma is described. The antiserum against lisuride-4-hemisuccinate-BSA was raised in rabbits. Using this method the plasma levels of lisuride were monitored following one intravenous (25 µg) and two oral (100 µg and 300 µg) doses of lisuride hydrogen maleate in three female and three male volunteers (intraindividual comparison). The plasma prolactin was also determined by radioimmunoassay. Following i. v. injection, the concentration of lisuride declined in three phases, with half-lives of 5 min, 25 min and 2 h. The total plasma clearance of 800±250 ml × min−1 was in the range of “plasma flow” through the liver. In agreement with the high rate of biotransformation, the bioavailability of lisuride administered orally was 10%±7% of the 100-µg dose, and 22%±7% of the 300-µg dose. The plasma prolactin was lowered to 3%–18% of its pretreatment value depending on the route of administration and the dose. The reduction appeared to be short-lived and to be directly dependent on the plasma concentration of lisuride. Following intravenous injection, the prolactin level declined after a so far unexplained lagtime of 0.5 h.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00554666

Permalink

Library	Location	Call Number	Volume/Issue/Year	Availability

Others were also interested in ...

Paper (German National Licenses)

Fulltext

Electronic Resource

Pharmacokinetics and biotransformation of the new benzodiazepine, lormetazepam, in man (1983)

Hümpel, M. ; Stoppelli, I. ; Milia, S. ; [et al.]

Springer

European journal of clinical pharmacology 24 (1983), S. 139-140

add to mindlist on the mindlist

Details

ISSN: 1432-1041

Keywords: benzodiazepine ; lormetazepam ; lormetazepam glucuronide ; transfer to milk ; pharmacokinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00613941

Permalink

Library	Location	Call Number	Volume/Issue/Year	Availability

Others were also interested in ...

Paper (German National Licenses)

Fulltext

Electronic Resource

Influence of repeated oral doses of ethinyloestradiol on the metabolic disposition of [13C2]-ethinyloestradiol in young women (1996)

Kuhnz, W. ; Hümpel, M. ; Biere, H. ; [et al.]

Springer

European journal of clinical pharmacology 50 (1996), S. 231-235

add to mindlist on the mindlist

Details

ISSN: 1432-1041

Keywords: Key words Ethinyloestradiol; clearance ; stable isotope

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Abstract Objective: To examine the influence of daily oral administration of ethinyloestradiol on the total clearance of 13C-labeled ethinyloestradiol in women. Methods: 19, healthy, young women received a single IV dose of 0.06 mg 13C-ethinyloestradiol. Subsequently, they were treated with daily oral doses of 0.06 mg ethinyloestradiol for 8 days. On the last day of oral treatment, they received a further IV dose of 0.06 mg 13C-ethinyloestradiol. The pharmacokinetic parameters clearance, area under the serum level-time curve, terminal half-life, steady-state volume of distribution and mean residence time of 13C-ethinyloestradiol in each volunteer were evaluated after both IV doses, and the corresponding pairs of parameters were examined statistically for the significance of intraindividual differences. Results: Following the first (second) intravenous administration, the mean area under the curve was 2.54 (2.67) ng⋅h⋅ml−1. The terminal half-life and mean residence time were 9.7 (9.6) h and 10.5 (10.1) h, respectively. The steady-state volume of distribution was 4.3 (3.9) l⋅kg−1 and the clearance was 7.0 (6.6) ml⋅ min−1⋅kg−1. No significant difference was observed in any of these parameters between the first and the second IV doses of 13C-EE2. Conclusions: Since the clearance in particular remained unchanged after repeated oral administration of ethinyloetradiol, the hypothesis that ethinyloestradiol can inhibit its own metabolism in vivo can be rejected.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s002280050098

Permalink

Library	Location	Call Number	Volume/Issue/Year	Availability

Others were also interested in ...

Paper (German National Licenses)

Fulltext

Electronic Resource

Pharmacokinetics and biotransformation of the new benzodiazepine, lormetazepam, in man (1982)

Hümpel, M. ; Stoppelli, I. ; Milia, S. ; [et al.]

Springer

European journal of clinical pharmacology 21 (1982), S. 421-425

add to mindlist on the mindlist

Details

ISSN: 1432-1041

Keywords: benzodiazepine ; lormetazepam ; lormetazepam glucuronide ; transfer to milk ; pharmacokinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary The concentrations of lormetazepam and its glucuronide in plasma and milk were determined during administration of 10 daily doses of lormetazepam 2 mg (2 tablets of NOCTAMID® - 1) to five mothers delivered by Caesarian section. Their babies were breast-fed throughout the study, and the plasma levels of lormetazepam and its glucuronide were determined three times in the babies. At 12 and 24h after administration, the plasma level of lormetazepam was about 3.5 ng/ml and 1.8 ng/ml in mothers, and below 0.09 ng/ml in the children. In milk the lormetazepam concentration was below 0.2 ng/ml. The plasma level of glucuronide varied between 24 ng/ml at 12h and 11 ng/ml 24h after administration. Almost no accumulation of unchanged lormetazepam was observed (factor: 1.3). The ratio of the levels of lormetazepam in milk and plasma was estimated to be below 0.06, and for the glucuronide the ratio was 0.04. The quantity of free and conjugated active ingredient transferred to the children via breast milk was calculated to be at most 100 ng/kg, corresponding to 0.35% of the maternal dose, which is regarded as tolerable.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00542330

Permalink

Library	Location	Call Number	Volume/Issue/Year	Availability

Others were also interested in ...

Paper (German National Licenses)

Fulltext

Electronic Resource

Nucleotidveränderungen von 18 S und 28 S ribosomaler RNS aus Rattenleber bei der chemischen Carcinogenese durch N-Nitrosomorpholin (1975)

Hümpel, M.

Springer

Journal of cancer research and clinical oncology 84 (1975), S. 311-323

add to mindlist on the mindlist

Details

ISSN: 1432-1335

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Description / Table of Contents: Zusammenfassung Nach längerdauernder Verabfolgung von N-Nitrosomorpholin (NNM) an weiblichen Wistar-Ratten fanden sich in der ribosomalen RNS (18 S und 28 S-rRNS) der Leber „anormale“ Dinucleotide, welche sich als resistent erwiesen gegenüber Alkali und Milz-Phosphodiesterase. Diese und weitere Befunde werden im Zusammenhang mit der Hypothese diskutiert, daß es während der durch NNM induzierten Carcinogenese in der Leber über einen NNM-Metaboliten zu Basenvernetzungen (“cross-linking”) kommt. Eine Übertragung der Basenvernetzungshypothese als carcinogenes Wirkungsprinzip des NNM auf die DNS vermag die weiteren gewonnenen Ergebnisse zu erklären. In der Literatur berichtete Beobachtungen zum NNM-Stoffwechsel stehen mit dieser Deutung nicht im Widerspruch.

Notes: Summary After administration of N-nitrosomorpholine (NNM) to female Wistar-rats the ribosomal RNA (18 S and 28 S rRNA) of the livers contained “abnormal” dinucleotides which were resistant against treatment with alkali or with spleen phosphodiesterase. These and further observations are discussed in view of the hypothesis that during the induction of liver tumors a metabolite of NNM causes crosslinks of nucleic acid bases. The application of this hypothesis on the effects of NNM upon DNA permits to explain the additional results that have been obtained. Observations on NNM metabolism as reported in the literature are not inconsistent with this interpretation.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00312252

Permalink

Library	Location	Call Number	Volume/Issue/Year	Availability

Others were also interested in ...

Paper (German National Licenses)

Fulltext

Electronic Resource

ZK 90 695: A new antiarthritic drug with tissue targeting properties (1991)

Hümpel, M. ; Günzel, P. ; Biere, H. ; [et al.]

Springer

Inflammation research 32 (1991), S. 22-23

add to mindlist on the mindlist

Details

ISSN: 1420-908X

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01983302

Permalink

Library	Location	Call Number	Volume/Issue/Year	Availability

Others were also interested in ...

Paper (German National Licenses)

Fulltext

Electronic Resource

A single-dose and 3-month clinical—pharmacokinetic study with a new combination oral contraceptive (1995)

Heuner, A. ; Kuhnz, W. ; Heger-Mahn, D. ; [et al.]

Springer

Advances in contraception 11 (1995), S. 207-225

add to mindlist on the mindlist

Details

ISSN: 1573-7195

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Description / Table of Contents: Resumé Cette étude a été réalisée sur 14 jeunes femmes. Le contraceptif oral combiné contenait 75 μg de gestodène (GSD) et 20 μg d'éthinyl oestradiol (EE2) par dose unitaire. Les volontaires ont reçu une dose unique au vingt et unième jour du cycle préliminaire sans traitement (CPj21) et — après une période de 7 jours de sevrage — elles ont absorbé la préparation selon une posologie de 2lj/7j pendant trois mois. Les profils journaliers du taux sérique du produit ont été établis au jour CPj21 et aux jours 1 et 21 des cycles de traitement 1 et 3. En outre, on a suivi tous les deux jours, durant les cycles 1 et 3 du traitment, les taux sériques inférieurs du produit. On a déterminé, selon des méthodes de RIA spécifiquement mises au point ou commercialement disponibles, les taux sériques de GSD, EE2, CBG, SHBG et testostérone (T). L'évaluation pharmacocinétique a été exécutée à l'aide du TOPFIT et les paramètres ont été évalués en vue de déterminer les différences avec les résultats du test-t. Les principales variables ciblées étaient lesC max,t max et ASC pour l'éthinyl oestradiol, GSD et GSD non lié, au jour 21 du cycle 3 par rapport au CPj21. La pharmacocinétique de l'EE2 correspondait à une dose de 20 μg/unité. LeC max d'une dose unique de 65 pg/ml et l'ASC de 612 pg h ml−1 augmentaient de 40 à 60% durant les cycles de traitement par suite d'accumulation. L'EE2 induisait des taux sériques de SHBG de base (102 nmol/l) et de CBG (42 μg/ml) d'environ 220 nmol/l et 87 μl/ml respectivement à la fin des premier et troisième cycles. Les taux sériques de T tombaient à 50% des niveaux de base durant les cycles de traitement et les concentrations de T libre étaient réduites de 60 à 70%. La pharmacocinétique du GSD à la fin des cycles de traitement 1 et 3 était différente de celle d'une dose unique. LesC max d'une dose unique de 3,5 ng/ml et l'ASC0–24h de 22 ng h ml−1 augmentaient jusqu'à des niveaux stables de δ-8,7 ng/ml et 90–106 ng h ml−1 respectivement. La hausse des taux de GSD durant le traitement résulte de deux processus parallèles: accumulation et élargissement du compartiment spécifiquement liant. Ce fait est démontré par des expériences de liaison des protéines, lesquelles indiquent une liaison spécifique accrue (SHBG), passant de 69 à 80% et une réduction de la fraction libre de GSD de 40% au cours du traitement. Les résultats de la pharmacocinétique du GSD et de l'EE2 obtenus dans la présente étude confirment ceux obtenus précédemment avec le Femodene, lorsque la réduction de 10 μg/j de la dose de EE2 est prise en compte.

Abstract: Resumen Este estudio se realizó con 14 mujeres jóvenes. La combinación de anticonceptivos orales contenía 75 μg de gestodén (GDS) y 20 μg de etinil estradiol (EE2) por unidad de dosificación. Las voluntarias recibieron una sola dosis en el vigésimo primer día de un preciclo sin tratamiento (PCd21) y, después de un período de interrupción de siete días — utilizaron la preparación al séptimo día de un programa de 21 días durante tres meses. Se obtuvieron perfiles diarios del nivel sérico de los fármacos en el PCd21 y en los días 1 y 21 de los ciclos del primer y tercer ciclo de tratamiento. Además, se realizó el seguimiento de los niveles séricos mínimos de los fármacos cada dos días durante el primer y tercer ciclo de tratamiento. Los niveles séricos de GSD, EE2, CBG, SHBG y testosterona (T) se determinaron mediante RIA específicamente desarrollados o comercialmente disponibles. La evaluación farmacocinética se realizó con TOPFIT y se evaluaron las diferencias de los parámetros con el test-t. Las principales variables a determinar fueronC máx,t máx y AUC para EE2, GSD y GSD no ligado al vigésimo primer día del tercer ciclo en comparación con PCd21. La farmacocinética de EE2 guardaba conformidad con una dosis de 20 μg/unidad. LaC máx de dosis única de 65 pg/ml y AUC de 612 pg h ml−1 aumentó en un 40–60% durante los ciclos de tratamiento debido a la acumulación. EE2 indujo niveles séricos de SHBG basal (102 nmol/l) y CBG (42 μg/ml) de aproximadamente 220 nmol/l y 87 μg/ml, respectivamente, al final del primer y tercer ciclo de tratamiento. Los niveles séricos de T se redujeron al 50% de los niveles de línea de referencia durante los ciclos de tratamiento y las concentraciones de T libre se redujeron en un 60–70%. La farmacocinética del GSD al concluir el primer y tercer ciclo de tratamiento fue diferente de la correspondiente a la dosis única. LaC máx de dosis única de 3,5 ng/ml y AUC0–24h de 22 ng h ml−1 aumentó a niveles de estado estable de 8–8,7 ng/ml y 90–106 ng h ml−1, respectivamente. El aumento de los niveles de GSD con el tratamiento se debe a dos procesos paralelos, es decir, acumulación y ampliación del compartimiento específico de ligazón. Esto se demostró mediante experimentos de ligazón de proteínas, que señalaron un aumento de la ligazón específica (SHBG) del 69% al 80% y una reducción de la fracción libre de GSD en un 40% durante el tratamiento. Los resultados de la farmacocinética de GSD y EE2 obtenidos en el presente estudio confirman resultados anteriores con Femodene, al tenerse en cuenta la reducción de la dosis de EE2 en 10 μg/d.

Notes: Abstract The study was performed in 14 young women. The combination oral contraceptive contained 75 μg gestodene (GSD) and 20 μg ethinyl estradiol (EE2) per dosage unit. The volunteers received a single dose on day 21 of a treatment-free precycle (PCd21) and, after a washout period of 7 days, used the preparation in a 21 d/7 d schedule for three months. Daily drug serum level profiles were taken on PCd21 and on days 1 and 21 of treatment cycles 1 and 3. In addition, trough drug serum levels were followed every other day during treatment cycles 1 and 3. Serum levels of GSD, EE2, CBG, SHBG and testosterone (T) were determined by means of specifically developed or commercially available RIAs. Pharmacokinetic evaluation was carried out with TOPFIT and parameters were evaluated for differences with thet-test. Main target variables wereC max,t max and AUC for EE2, GSD and unbound GSD on day 21, cycle 3 vs. PCd21. EE2 pharmacokinetics were in agreement with a dose of 20 μg/unit. Single-doseC max of 65 pg/ml and AUC of 612 pg h ml−1 increased by 40–60% during treatment cycles as a result of accumulation. EE2 induced basal SHBG (102 nmol/L) and CBG (42 μg/ml) serum levels to about 220 nmol/L and 87 μg/ml, respectively, at the end of treatment cycles 1 and 3. Serum T levels dropped to 50% of baseline levels during treatment cycles and free T concentrations were reduced by 60–70%. GSD pharmacokinetics at the end of treatment cycles 1 and 3 were different from single-dose pharmacokinetics. Single-doseC max of 3.5 ng/ml and AUC0–24 h of 22 ng h ml−1 increased to steady-state levels of 8–8.7 ng/ml and 90–106 ng h ml−1, respectively. The increase in GSD levels under treatment is the result of two parallel processes, i.e. accumulation and enlargement of the specific binding compartment. This was shown by protein-binding experiments, demonstrating an increase in specific (SHBG) binding from 69% to 80% and a reduction in the free fraction of GSD by 40% during treatment. The results of GSD and EE2 pharmacokinetics obtained in the present study confirm previous results with Femodene, when the reduction in the EE2 dose by 10 μg/d is taken into account.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01978421

Permalink

Library	Location	Call Number	Volume/Issue/Year	Availability

Others were also interested in ...

Paper (German National Licenses)

Fulltext

hits 1 - 7 | 7 hits