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1. Pharmacokinetics of isoxicam following intravenous, intramuscular, oral and rectal administration in healthy volunteers.

Author

Kolle, EU and Vollmer, KO

Abstract

1 The pharmacokinetic characteristics and bioavailability of isoxicam were investigated in healthy male volunteers following various routes of administration. Plasma concentrations were determined up to 96 or 120 h following each administration using a selective h.p.l.c. method. 2 Twelve subjects received an i.v. and an i.m. injection of 150 mg and an oral dose of 200 mg (two capsules) in a three-way crossover design. 3 The plasma concentration-time curves after intravenous administration followed two compartmental characteristics with a rapid initial distribution phase and a predominant terminal elimination phase. The area under the distribution phase contributed only 0.4% to the total AUC. Mean disposition parameters were: t1/2, lambda 1 = 3.3 min t1/2, lambda z = 28 h, Vc = 5.61, Vdarea = 12.71, CL = 5.1 ml min-1. 4 Following other routes of administration, the isoxicam plasma profile could be adequately described by a one compartment model. 5 After the i.m. dose, isoxicam was rapidly and completely absorbed: within 15 min 40% of the peak concentrations were attained. Maximum plasma concentrations of 11.7 micrograms ml-1 were reached after an average of 3 h. 6 After oral administration isoxicam was completely bioavailable. Mean peak concentrations of 12.3 micrograms ml-1 were obtained within 10 h. 7 The bioavailability of suppositories containing 200 mg of active substance was investigated in another 10 volunteers relative to capsules (2 × 100 mg). The formulations tested were bioequivalent with respect to the amount absorbed. 8 Comparison of AUCs (normalized for dose and body weight) resulting from all treatments, did not show significant differences among the various formulations.(ABSTRACT TRUNCATED AT 250 WORDS) [ABSTRACT FROM AUTHOR]

Published
1986
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2. Metabolism of thymoxamine. I. Studies with 14C-thymoxamine in rats

Author

Vollmer Ko, Poisson A, Liedtke B, von Hodenberg A, and Steinbrecher W

Subjects
Male, Moxisylyte, Metabolite, Blood Pressure, Biology, Pharmacology, Specimen Handling, chemistry.chemical_compound, Pharmacokinetics, medicine, Animals, Bile, Pharmacology (medical), Tissue Distribution, Enterohepatic circulation, Biotransformation, Reabsorption, Prodrug, Glucuronic acid, Myocardial Contraction, Bioavailability, Body Fluids, Rats, chemistry, Chromatography, Thin Layer, medicine.drug, Muscle Contraction
Abstract

Thymoxamine is rapidly and completely absorbed in rats. It is a prodrug which does not enter the systemic circulation in its unchanged form. After either oral or intravenous administration it undergoes rapid and intense metabolism involving four biotransformation reactions: 1. enzymatic hydrolysis to the corresponding phenol (metabolite I), 2. monodemethylation to metabolite II, 3. sulfate conjugation of I and II (metabolites III and IV) and 4. conjugation of I and II with glucuronic acid (metabolites V and VI). With these 6 metabolites identified approximately 95% of the radioactivity can be accounted for in plasma, urine and bile. Whereas the systemic availability of I and II is low, III and IV show high bioavailability. Metabolites I to IV are pharmacologically active, while III a n d IV are less potent than I and II. The radioactivity distribution in tissues is different after oral and intravenous administration consistent with the higher portion of unconjugated metabolites in the body after administration by parenteral route. Although 60% of the labelled compounds is eliminated via bile, the radioactive compounds are almost completely excreted in the urine after both routes of administration. This demonstrates complete reabsorption of the biliary metabolites. Secondary peaks of radioactivity in plasma and organs at 4 hours are explained by the participation of the metabolites in the enterohepatic circulation.

Published
1985

3. Disposition of gabapentin (neurontin) in mice, rats, dogs, and monkeys.

Author

Radulovic LL, Türck D, von Hodenberg A, Vollmer KO, McNally WP, DeHart PD, Hanson BJ, Bockbrader HN, and Chang T

Subjects
Acetates administration & dosage, Administration, Oral, Animals, Anticonvulsants administration & dosage, Autoradiography, Biological Availability, Biotransformation, Chromatography, High Pressure Liquid, Dogs, Female, Gabapentin, Half-Life, Injections, Intravenous, Macaca fascicularis, Male, Mice, Protein Binding, Rats, Rats, Sprague-Dawley, Species Specificity, Tissue Distribution, Acetates pharmacokinetics, Amines, Anticonvulsants pharmacokinetics, Cyclohexanecarboxylic Acids, gamma-Aminobutyric Acid
Abstract

Gabapentin, an analog of gamma-aminobutyric acid, exhibits anticonvulsant properties in both animal models and humans. Gabapentin pharmacokinetics was studied in laboratory animals using HPLC and radiometry. Oral bioavailability was 40% in monkeys administered 25 mg/kg, 79% in mice and rats receiving 50 mg/kg, and 80% in dogs administered 50 mg/kg. Binding to plasma proteins was < 3%. Maximum blood or plasma concentrations generally occurred within 2 hr of an oral dose. In rats and monkeys, increases in maximum plasma concentrations and/or areas under the curve were less than dose-proportional following oral administration, most likely because of saturable absorption. However, intravenous pharmacokinetics in rats were linear over the dosage range of 4-500 mg/kg. Mean intravenous elimination half-life was 1.7 hr in rats, 2.9 hr (14C only) in dogs, and 3.0 hr in monkeys. In rats and dogs, repeated administration did not alter gabapentin or 14C pharmacokinetics. Additionally, gabapentin did not induce hepatic cytochrome P450 monooxygenases in rats. There were no age- (rats only) or gender-associated changes in pharmacokinetic parameters. [14C]Gabapentin was extensively distributed to tissues. In the dog, gabapentin was metabolized to N-methylgabapentin (approximately 34% of dose); whereas metabolism in mouse, rat, and monkey was minimal (< 5%). The principal route of excretion was via urine. In summary, as an antiepileptic drug, gabapentin exhibited desirable pharmacokinetic properties, such as linear elimination kinetics, not highly bound to plasma proteins, not extensively metabolized, and not an inducer of hepatic cytochrome P450.

Published
1995

4. Temperature dependence of the benzodiazepine-receptor interaction.

Author

Quast U, Mählmann H, and Vollmer KO

Subjects
Animals, Brain metabolism, Diazepam metabolism, Flunitrazepam metabolism, In Vitro Techniques, Kinetics, Membranes metabolism, Rats, Receptors, GABA-A, Temperature, Thermodynamics, Receptors, Drug metabolism
Abstract

The temperature dependence of the interaction of three benzodiazepines with their receptors in rat brain membranes containing about 2 microM (endogenous) gamma-aminobutyric acid was investigated. van't Hoff plots of the equilibrium dissociation constants were linear for [3H]diazepam and its N-desmethyl derivative (N-desmethyldiazepam, NDz), whereas for [3H]flunitrazepam a break between two linear portions occurred at about 10 degrees. Binding of diazepam, NDz, and flunitrazepam (for the latter, at temperature greater than 10 degrees) is enthalpy-driven (delta H approximately -40 to -50 kJ/mole with a negligible contribution from delta S. The latter result indicates that the interaction is not a simple hydrophobic association, but that it may be more complex in nature, possibly involving a conformational transition of the receptor-ligand complex. The activation energy for dissociation of the [3H]flunitrazepam- and [3H]diazepam-receptor complexes is about 100 kJ/mole. Consequently, the complexes dissociate about 100 times faster on changing temperature from 0 degrees to 37 degrees.

Published
1982

5. GLC determination of tilidine, nortilidine, and bisnortilidine in biological fluids with a nitrogen-sensitive detector.

Author

Hengy H, Vollmer KO, and Gladigau V

Subjects
Adult, Chromatography, Gas, Dealkylation, Humans, Male, Methods, Tilidine blood, Tilidine urine, Cyclohexanecarboxylic Acids analysis, Tilidine analysis
Abstract

A sensitive and specific GLC method is described to determine therapeutic levels of tilidine and its two main metabolites, nortilidine and bisnortilidine, in plasma and urine. The method involves the extraction of the compounds and an internal standard with cyclohexane from alkalinized samples, followed by back-extraction into 1 N HCl. The hydrochloric acid solution is evaporated to dryness. After liberation of the free bases with ammonia, the residue is subjected to GLC analysis with a nitrogen-phosphorus detector and a 1.8-m (6-ft) glass column packed with 1% CRS 101 and 1.5% LAC-4-R-886 on Gas Chrom Q. Sensitivity in plasma and urine is approximately 1 ng/ml for a 5-ml sample.

Published
1978
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6. [Metabolism and pharmacokinetics of piprozoline in the rat, dog and man. 1. Studies with the radioactively-labeled substance].

Author

Vollmer KO, Hodenberg AV, Poisson A, Bode R, and Schauerte E

Subjects
Administration, Oral, Adult, Animals, Biotransformation, Carbon Radioisotopes, Cholagogues and Choleretics administration & dosage, Chromatography, Thin Layer, Dogs, Humans, Kinetics, Male, Mass Spectrometry, Piperidines administration & dosage, Piperidines metabolism, Rats, Thiazoles administration & dosage, Cholagogues and Choleretics metabolism, Thiazoles metabolism
Abstract

The new choleretic ethyl (Z-3-ethyl-4-oxo-5-piperidino-thiazolidin-2-ylidene) acetate (piprozoline, Gö 919, Probilin) is absorbed well and rapidly in rats, dogs and humans. Maximum 14C plasma concentrations are found 1-2 h after oral administration of the labelled substance to fasting animals and human volunteers. When administered to test persons after breakfast, the absorption is delayed but the absorbed amount is unaffected. Elimination of the radioactivity from the plasma occurs in two phases; 24 h after administration the radioactivity concentration has dropped to 5-8% of the maximum levels. Piprozoline is almost completely metabolized during absorption. The primary metabolic step is the enzymatic hydrolysis of the ester bond to the corresponding acid (metabolite I). At the time of maximum plasma concentration most of the plasma radioactivity corresponds to metabolite I, which also possesses choleretic activity. Approx. 65% of the radioactive dose is eliminated renally in all three species, approx. 60% being excreted within the first 24 h. Approx. 40-60% of the urinary radioactivity can be ascribed to metabolite I, both in its free form and conjugated with glucuronic acid. No unchanged substance is found in the urine. A comparison of the pharmacokinetic and metabolic behaviour of piprozoline in rats, dogs and humans showed that it was similar in all three species.

Published
1977

7. [Metabolism of ethyl DL-trans-2-dimethylamino-1-phenylcyclohex-3-ene-trans-1-carboxylate hydrochloride. 1. Mass spectroscopic structural elucidation of metabolites I and II and their determination in various biological fluids].

Author

Vollmer KO and Achenbach H

Subjects
Analgesics blood, Analgesics urine, Animals, Bile metabolism, Chromatography, Thin Layer, Cyclohexanecarboxylic Acids blood, Cyclohexanecarboxylic Acids urine, Dimethylamines blood, Dimethylamines metabolism, Dimethylamines urine, Dogs, Glucuronates metabolism, Humans, Male, Mass Spectrometry, Rabbits, Rats, Analgesics metabolism, Cyclohexanecarboxylic Acids metabolism
Published
1974

9. Assay of etozolin and its main metabolite, ozolinone, in plasma by high performance liquid chromatography.

Author

Hengy H, Vollmer KO, Gladigau V, and Kölle EU

Subjects
Chromatography, High Pressure Liquid methods, Diuretics, Humans, Piperidines blood, Time Factors, Benzothiadiazines, Sodium Chloride Symporter Inhibitors blood, Thiazoles blood
Abstract

A sensitive and specific method for the determination of the diuretic Ethyl (Z)-(3-methyl-4-oxo-5-piperidino-thiazolidin-2-ylidene) acetate (etozolin, Elkapin) and its pharmacologically active main metabolite, (Z)-(3-methyl-4-oxo-5-piperidino-thiazolidin-2-ylidene) acetic acid (ozolinone), at therapeutic concentrations in plasma is described. The method is based on high performance liquid chromatography and the use of two structurally similar internal standards. Etozolin and its metabolite are extracted from the plasma into dichloromethane at pH 9 and pH 5, respectively, and the resulting residues are analyzed on a silica gel column. The elution peaks are detected by UV absorption at 281 nm. The sensitivity for both compounds is 20 ng/ml plasma. The precision of the method is about +/- 5%. The applicability to pharmacokinetic studies of etozolin is shown.

Published
1980

10. Pharmacokinetics of tilidine and metabolites in man.

Author

Vollmer KO, Thomann P, and Hengy H

Subjects
Administration, Oral, Adult, Chromatography, Gas, Half-Life, Humans, Injections, Intravenous, Male, Tilidine administration & dosage, Tilidine analogs & derivatives, Tilidine metabolism, Cyclohexanecarboxylic Acids pharmacokinetics, Tilidine pharmacokinetics
Abstract

Tilidine is a prodrug from which the active metabolite nortilidine is formed by demethylation. The pharmacokinetics of tilidine (T), nortilidine (NT) and bisnortilidine (BNT) were studied in nine healthy subjects following single intravenous (10 min infusion) and oral 50 mg T-HCl dose as well as following multiple 50 mg T-HCl oral doses. Systemic availability of the parent substance was 6% and of the active metabolite NT 99%. The terminal half-life of NT was 3.3 h following single oral administration, 4.9 h following intravenous administration and 3.6 h following multiple dosing. Following intravenous infusion, concentrations of unchanged substance were found which were 30 times higher than following oral administration. BNT was eliminated with half-lives of 5 h after oral administration and 6.9 h after intravenous administration. Renal elimination of unchanged substance was 1.6% of the dose following intravenous administration and less than 0.1% of the dose following oral administration. Approximately 3% were recovered in urine as NT and 5% as BNT following both routes of administration.

Published
1989

11. [Pharmacokinetic differentiation of benzodiazepines].

Author

Vollmer KO

Subjects
Benzodiazepines, Biotransformation, Dose-Response Relationship, Drug, Drug Administration Schedule, Half-Life, Humans, Kinetics, Metabolic Clearance Rate, Anti-Anxiety Agents blood
Published
1981

12. Pharmacokinetic model of diltiazem.

Author

Kölle EU, Ochs HR, and Vollmer KO

Subjects
Adult, Biological Availability, Diltiazem administration & dosage, Diltiazem blood, Humans, Intestinal Absorption, Kinetics, Male, Models, Biological, Tablets, Benzazepines metabolism, Diltiazem metabolism
Abstract

The pharmacokinetic profile of D-3-acetoxy-cis-2,3-dihydro-5-(2-dimethylamino-ethyl)-2-(p-methoxy-phenyl)-1, 5-benzothiazepin-4(5H)-one hydrochloride (diltiazem . HCl) following i.v. and p.o. administration has been studied in six healthy subjects using a new sensitive GLC method. The volunteers received an i.v. infusion of 20 mg in 20 min, a peroral solution of 120 mg and two 60-mg tablets (Dilzem) in a randomized sequence. The plasma level time courses of the unchanged compound following infusion and peroral solution were simultaneously evaluated by nonlinear regression analysis. The best model was chosen by means of statistical criteria. In all subjects the experimental data could be adequately described by an open three-compartment model with zero order input following infusion and first order absorption following p.o. solution. Using this procedure the following common disposition parameters were obtained for both routes of administration: t1/2 alpha = 0.1 h, t1/2 beta = 2.1 h, t1/2 gamma = 9.8 h (harmonic means derived from individualized fits), Vc = 0.9 +/- 0.4 l/kg, Vss = 5.2 +/- 2.4 l/kg, Cltot = 11.5 +/- 1.8 ml/min/kg. Compared to the beta-phase the terminal gamma phase represents a smaller contribution to the total AUC. The blood/plasma distribution ratio was found to be 1.00 +/- 0.08 (N = 4), the mean hepatic extraction ratio was 0.54. Peak levels appeared 0.6 +/- 0.3 h after the p.o. solution. The mean absolute bioavailability of diltazem based on the individual AUC infinity 0 of the p.o. solution and the infusion was 0.44 +/- 0.10. Following tablet administration, delayed maximum levels were found after 2.8 +/- 0.9 h. Comparing the AUC infinity 0 of tablets and p.o. solution, there was no significant difference between both dosage forms.

Published
1983

14. [ On the metabolism of ethyl-DL-trans-2-dimethylamino-1-phenyl-cyclohex-3-ene-trans-1-carboxylate-hydrochloride (Tilidine-HCl). 2nd Communication: Studies with 14C-labelled substance on rats and dogs].

Author

Vollmer KO and Poisson A

Subjects
Administration, Oral, Animals, Autoradiography, Bile metabolism, Dogs, Female, Injections, Intravenous, Intestinal Absorption, Kinetics, Male, Maternal-Fetal Exchange, Pregnancy, Protein Binding, Rats, Tilidine administration & dosage, Cyclohexanecarboxylic Acids metabolism, Tilidine metabolism
Abstract

Absorption, distribution, metabolism and excretion of the potent analgesic ethyl-DL-trans-2-timethylamino-1-phenyl-chclohex-3-ene-trans-1-carboxylate-hydrochloride (tilidine-HCl, Gö 1261 C, active ingredient of Vloron) were investigated in rats and dogs, using the radioactively labelled substance. Following oral administration, tilidine-HCl is rapidly and completely absorbed from the duodenum. During absorption, tilidine undergoes a marked first-pass effect. In plasma several metabolites are found, part of them occurring in higher concentrations than the unchanged substance. The metabolites are also formed rapidly after parenteral administration, unchanged tilidine being found in higher concentrations than any of the metabolites at all times measured. Following both routes of administration, the Met. I (nortilidine), also possessing a strong analgesic activity, reaches similar plasma levels. 14C distribution studies in rats showed a relatively high concentration of the radioactivity in the excretory organs, liver and kidneys. In brain, muscle tissue and blood much lower 14C concentrations are found. The concentrations measured in the foetal organs correspond to those in the muscle tissue of the mother animals and are, therefore, much lower than in most maternal organs. The radioactivity is eliminated from the foetal organs at the same rate as from the maternal organs. Tilidine is rapidly and completely eliminated with the excrements, nearly exclusively in the form of metabolic products. Rats eliminate 50% of the given radioactivity via the kidneys. The relatively high fecal elimination is based on the biliary metabolites. Following intraduodenal and intravenous administration to rats with an interrupted enterohepatic circulation, about 80% of the dose is eliminated with bile. The biliary metabolites are partly reabsorbed. In dogs, approx. 80% of the applied radioactivity is eliminated with urine.

Published
1976

15. Metabolism of thymoxamine. II. Studies with 14C-thymoxamine in man.

Author

Vollmer KO and Poisson A

Subjects
Administration, Oral, Adult, Biotransformation, Chemical Phenomena, Chemistry, Physical, Chromatography, Thin Layer, Erythrocytes metabolism, Humans, Injections, Intravenous, Kinetics, Male, Moxisylyte blood, Moxisylyte urine, Plasma analysis, Moxisylyte metabolism
Abstract

Thymoxamine is rapidly and completely absorbed in man. Rapid biotransformation is observed after intravenous and oral administration of 40 mg 14C-thymoxamine HCl. No unchanged compound is found in the body. More than 90% of plasma and urine radioactivity could be ascribed to six metabolites: the desacetyl compound (metabolite I), the monodemethylated metabolite I (metabolite II), the sulfate conjugates of I and II (metabolites III and IV) and the glucuronides of I and II (metabolites V and VI). The unconjugated metabolites are observed in plasma only after intravenous administration. Similar patterns for polar metabolites are found in plasma and urine for both routes of administration. The sulfate fraction amounts to about 50-60% and the glucuronide fraction to about 30-40% of the radioactivity, the conjugates of metabolite I being more abundant than those of metabolite II. The elimination of the metabolites is rapid, the half-life of radioactivity elimination being 1.5 h during the first 12 hours and 12 h thereafter. 80% of the radioactivity dose is recovered in the urine within 4 hours. Recovery after four days amounts to 99.8% (i.v.) and 97.7% (oral). The results are discussed with regard to the application of the drug in man, taking into account that not only the unconjugated metabolites but also the sulfate conjugates are pharmacologically active.

Published
1985
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17. [Metabolism and pharmacokinetics of piprozoline in rat, dog and man. 2nd Communication: Determination of metabolic profiles with the aid of an HPLC-radioactivity detection system following direct injection of urine and bile onto a reversed-phase column (author's transl)].

Author

Hodenberg AV, Klemisch W, and Vollmer KO

Subjects
Adult, Animals, Bile metabolism, Chromatography, High Pressure Liquid methods, Dogs, Glucuronates urine, Humans, Male, Piperidines metabolism, Rats, Cholagogues and Choleretics metabolism, Thiazoles metabolism
Abstract

This paper describes the determination of metabolic profiles of 14C marked ethyl (Z-3-ethyl-4-oxo-5-piperidino-thiazolidin-2-ylidene) acetate (piprozoline, Gö 919, Probilin) in rat, dog and human urine and rat bile with the aid of an HPLC-radioactivity detector system following the direct injection of large quantities onto an analytical C-18 column. Metabolite 1 and two glucuronic acid conjugates of metabolite I were determined quantitatively, isolated and identified. Following HPLC separation, the specific detection of radioactivity permits the determination of metabolic profiles without prior clean-up so that unstable metabolites can also be analyzed.

Published
1977

18. Metabolism of thymoxamine. III. Structure elucidation of the metabolites and interspecies comparison.

Author

Vollmer KO and von Hodenberg A

Subjects
Animals, Biotransformation, Cats, Chromatography, High Pressure Liquid, Chromatography, Thin Layer, Dealkylation, Dogs, Female, Glucuronates metabolism, Male, Rats, Species Specificity, Sulfuric Acids metabolism, Moxisylyte metabolism
Abstract

The structures of six metabolites were elucidated using rat urine after intragastric administration of 14C-thymoxamine by means of enzyme incubations, mass spectrometry and synthesis of metabolites: desacetylthymoxamine, N-demethyl-desacetylthymoxamine, the corresponding sulfates and glucuronides. The nature of the conjugates was confirmed by biosynthesis, i.e., co-administration of unlabelled thymoxamine and 35S-sulfate or 14C-glucose. The system high performance liquid chromatography-radioactivity detection was used for interspecies comparison. All biotransformation pathways are seen in rat and man. In dog and cat demethylation is a very minor reaction. Glucuronidation is not observed in the cat.

Published
1985
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19. [Metabolism of Etozolin in rat, dog and man].

Author

von Hodenberg A, Vollmer KO, Klemisch W, and Liedtke B

Subjects
Acetates administration & dosage, Animals, Biotransformation, Carbon Radioisotopes, Chromatography, High Pressure Liquid, Diuretics administration & dosage, Dogs, Humans, Rats, Acetates metabolism, Diuretics metabolism
Abstract

Investigations on the metabolism of the new diuretic ethyl (Z)-(3-methyl-4-oxo-5-piperidino-thiazolidin-2-ylidene) acetate (Gö 687, etozolin, Elkapin) were carried out with urine of rat, dog and man as well as rat bile after enteral administration of the 14C-labelled substance. Seven metabolites were isolated with either the aid of high-pressure liquid chromatography (HPLC) or extraction and thin-layer chromatography. Mass spectroscopy was applied to determine the structures of the metabolites, partly by use of authentic reference substances. Because of the instability of most of the metabolites, some of them showing strong polarity, the described investigations on the metabolic profiles and the enrichment and purification of some metabolites could only be carried out with the HPLC-radioactivity detector system, which requires no clean-up for the samples. The metabolisation process of etozolin is qualitatively equal in rat, dog and man; it is characterized by 3 steps: 1. enzymatic cleavage of the ester group, which leads to the also diuretically active main metabolite (metabolite I) in the plasma of all 3 species; 2. glucuronidation of the resulting metabolite I, leading to metabolites II and III, which are diastereoisomeric esters of the two enantiomeric forms of metabolite I with beta-D-glucuronic acid. 50--60% of the urinary radioactivity can be described with these two metabolisation steps in all 3 species; 3. Oxidation of the piperidine moiety to metabolites IV--VII.

Published
1977

20. High performance liquid chromatography coupled with radioactivity detection: a powerful tool for determining drug metabolite profiles in biological fluids.

Author

Vollmer KO, Klemisch W, and von Hodenberg A

Subjects
2-Hydroxyphenethylamine analogs & derivatives, 2-Hydroxyphenethylamine metabolism, Animals, Carbon Radioisotopes, Cats, Dogs, Humans, Levobunolol metabolism, Microcomputers, Moxisylyte metabolism, Naloxone metabolism, Radioactive Tracers, Rats, Silicic Acid, Thiazoles metabolism, Tritium, Yttrium, Chromatography, High Pressure Liquid, Octopamine analogs & derivatives, Pharmaceutical Preparations metabolism, Scintillation Counting, Silicates
Abstract

High performance liquid chromatography coupled with continuous radioactivity detection represents an advancement in drug metabolism research. Using radioactive substances labelled in biologically stable positions, all metabolites can be specifically detected by radioactivity measurement. Thus no clean-up of biological fluids is required prior to HPLC. This can prevent artefact formation from unstable metabolites, reduces recovery problems and facilitates quantitation. Separation of highly polar and unpolar metabolites is possible in a single chromatographic run using gradient elution and reversed phase materials. This technique is also well-suited for preparative isolation and purification of metabolites for subsequent structure elucidation. Various metabolite profiles of drugs labelled with carbon-14 or tritium are shown. Metabolites of the following drugs are presented: norfenefrine, etozolin, thymoxamine, naloxone, and levobunolol. We review the general methodology and report our experience with this technique. In principle, this technique may be useful for all biological systems in which tracer techniques are applied.

Published
1986
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21. GLC method for the quantification of metabolites of thymoxamine in human plasma.

Author

Hengy H, Von Hodenberg A, and Vollmer KO

Subjects
Biotransformation, Chromatography, Gas, Glucuronates metabolism, Humans, Hydrolysis, Indicators and Reagents, Sulfates blood, Moxisylyte blood
Abstract

A sensitive gas-chromatographic method for quantification of the pharmacologically active metabolites I-IV of thymoxamine in plasma is described. 4-(Hydroxythymyl)-(2'methylbutylaminoethyl)ether, a compound similar to metabolite I, is used as an internal standard. Metabolites I and II the internal standard are extracted with cyclohexane from alkalinized plasma followed by back-extraction into 0.1 N hydrochloric acid. After evaporating the hydrochloric acid solution, the sample is silylated with BSTFA and analyzed by gas-chromatography on a CRS 101/Carbowax 4000 column using a thermoionic detector. For subsequent determination of metabolites III and IV, the extracted plasma is hydrolyzed under conditions in which the phenol sulfates but not the glucuronide conjugates undergo cleavage. The resulting phenols (metabolite I and II) are analyzed as described above. The sensitivity threshold for all 4 compounds is approximately 5 ng/ml plasma based on a 2 ml plasma sample.

Published
1985
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22. Pharmacokinetics and metabolism of gabapentin in rat, dog and man.

Author

Vollmer KO, von Hodenberg A, and Kölle EU

Subjects
Acetates blood, Adult, Animals, Biotransformation, Chromatography, High Pressure Liquid, Dogs, Erythrocytes metabolism, Feces analysis, Female, Gabapentin, Half-Life, Humans, Kinetics, Male, Protein Binding, Rats, Rats, Inbred Strains, Species Specificity, Tissue Distribution, Acetates metabolism, Amines, Cyclohexanecarboxylic Acids, gamma-Aminobutyric Acid
Abstract

This paper describes the pharmacokinetic studies of 1-(aminomethyl)-cyclohexane acetic acid (gabapentin, Gö 3450, CI-945) conducted with the 14C-labelled substance following intravenous and intragastric administration to rats and dogs and oral administration to humans. Gabapentin is well absorbed in rats, dogs and in humans, with maximum blood levels, reached within 1-3 h after peroral administration. Following i.v. administration to rats, similar blood and brain levels of gabapentin are observed after a short distribution phase, whereby concentrations in cerebrum and cerebellum are comparable. The highest concentrations are found in the pancreas and kidneys and the lowest values in adipose tissue. No binding of gabapentin to human plasma proteins or human serum albumin is observed. The distribution coefficient (octanol/buffer pH 7.4) is 7.5 X 10(-2). In man, no biotransformation of gabapentin is observed. In rats, biotransformation is only minor. In dogs, however, a remarkable formation of N-methyl-gabapentin is found. Elimination half-lives range between 2-3 h in rats, 3-4 h in dogs, and 5-6 h in man. Gabapentin is nearly exclusively eliminated via the kidneys. Renal elimination was up to 99.8% in rats and approx. 80% in man following oral administration. The blood level-time course after i.v. administration to rats can well be described by a three-compartment open model. Experiments in rats and dogs demonstrate that pharmacokinetics are not sex-dependent and are not changed after multiple dosage. Pharmacokinetics are shown to be linear in the range tested of 4 to 500 mg/kg i.v. in rats.

Published
1986

23. [Studies on the influence of piprozoline on the microsomal enzyme system of the rat liver (author's transl)].

Author

Friedrich G and Vollmer KO

Subjects
Animals, Enzyme Induction drug effects, Glucuronates metabolism, Hexobarbital metabolism, Hexobarbital pharmacology, Male, Oxidoreductases metabolism, Piperidines pharmacology, Rats, Sleep drug effects, Time Factors, Cholagogues and Choleretics pharmacology, Microsomes, Liver enzymology, Thiazoles pharmacology
Abstract

Studies of hexobarbital sleeping time in rats showed that only a very high dosage of ethyl(Z)-(3-ethyl-4-oxo-5-piperidino-thiazolidin-2-ylidene)-acetate (piprozoline, Gö 919, Problin) (500 mg/kg) produced a weak interaction with the metabolism of hexobarbital; no signs of any induction of the oxidative enzyme system were observed until 4 days after pre-treatment with 3 X 250 mg/kg. Determinations of the in vitro activity of hepatic microsomal enzymes after several days pre-treatment of male Wistar rats with 2 X 250 mg piprozoline/kg per day showed that piprozoline has only a slight inductive effect on some of the enzymes of the oxidative system. Some of the glucuronidation reactions tested showed marked increases.

Published
1977

24. [Metabolism of DL-trans-2-dimethylamino-1-phenyl-cyclohex-3-ene-trans-1-carboxylic acid ester hydrochloride (Tilidine HC1). 3. Renal elimination of metabolites in the rat, dog and man].

Author

Vollmer KO and Hodenberg AV

Subjects
Animals, Biotransformation drug effects, Chromatography, Thin Layer, Dogs, Humans, Hydrogen-Ion Concentration, Intestinal Absorption drug effects, Kidney metabolism, Rats, Tilidine administration & dosage, Tilidine pharmacology, Cyclohexanecarboxylic Acids metabolism, Kidney drug effects, Tilidine metabolism
Published
1977

25. Gas-chromatographic determination of nanogram amounts of enantiomers of nortilidine, a main metabolite of tilidine, in biological specimens.

Author

Hengy H, Vollmer KO, and Gladigau V

Subjects
Animals, Chromatography, Gas, Dealkylation, Fluoroacetates, Humans, Indicators and Reagents chemical synthesis, Male, Methods, Microchemistry, Rats, Stereoisomerism, Tilidine blood, Tilidine urine, Trifluoroacetic Acid chemical synthesis, Cyclohexanecarboxylic Acids analysis, Tilidine analysis
Abstract

We report a specific and sensitive method for determination of the individual optical isomers of nortilidine, a main metabolite of tilidine, with the aid of a nitrogen-sensitive detector. With N-trifluoroacetyl-L-leucyl chloride as chiral reagent, the diastereomeric derivatives of the nortilidine enantiomers could be separated and quantified in the nanogram range. Under these conditions, the enantiomers of bisnortilidine, another main metabolite of tilidine, were also separated. Investigations in rats with the enantiomers of tilidine and nortilidine indicated that no racemization occurs during N-demethylation in the organism. After oral and intravenous administration of 50 mg of tilidine.HCI to a human volunteer, identical concentrations of nortilidine enantiomers were found in the plasma.

Published
1978

26. Binding of beta-adrenoceptor antagonists to rat and rabbit lung: special reference to levobunolol.

Author

Quast U and Vollmer KO

Subjects
Animals, Binding, Competitive drug effects, Dihydroalprenolol metabolism, Female, Heart drug effects, In Vitro Techniques, Male, Membranes metabolism, Rabbits, Rats, Rats, Inbred Strains, Species Specificity, Stereoisomerism, Temperature, Adrenergic beta-Antagonists metabolism, Levobunolol metabolism, Lung metabolism
Abstract

Binding of 3H-dihydroalprenolol (3H-DHA) to beta-adrenoceptors in homogenates from rat and rabbit lung was homogeneous and of high affinity (KD = 0.6 and 1.1 nmol/l at 20 degrees C; 1.1 and 2.2 nmol/l at 37 degrees C). The beta 1-selective antagonists betaxolol, metoprolol, bevantolol and acebutolol displaced 3H-DHA in a biphasic manner. From these data, the beta-adrenoceptor subtype distribution in rat lung homogenates was estimated to be 80% beta 2 (at 20 and 37 degrees C) as compared to 25% beta 2 in rabbit lung homogenates. In general, binding of beta-adrenoceptor antagonists (selective and nonselective) was slightly (less than 2 X) weaker in rabbit than in rat lung homogenates. In rat lung, binding of cardioselective beta-blockers to beta 1-receptors seemed to be more temperature-sensitive than binding to beta 2-receptors or binding of nonselective beta-blockers. Levobunolol, a potent non-cardioselective beta-blocker in pharmacological experiments, displaced 3H-DHA in a homogeneous manner (indicative of non-selectivity). In rat lung homogenates KD values were 0.8 nmol/l at 20 degrees C and 2.1 nmol/l at 37 degrees C. Similar values were found for the metabolites dihydrolevobunolol and hydroxylevobunolol. Surprisingly, d-bunolol, the dextrarotatory enantiomer of bunolol, showed a biphasic displacement curve, the fraction of high affinity sites being 83% in rat lung homogenates and 23% in rabbit lung. This ratio of sites is expected for a beta 2-adrenoceptor preferring ligand. High affinity binding (i.e. supposedly binding to beta 2-receptors) was about 50 times weaker than binding of levobunolol, in agreement with known stereospecificity of beta-adrenoceptor binding.

Published
1984

28. [Human pharmacokinetics of the new potent analgesic DL-trans-2-di-methylamino-1-phenyl-cyclohex-3-en-trans-1-carboxylic acid ethyl ester hydrochloride. 1. Blood level and excretion with urine and feces after single oral administration of 14C-labeled substance].

Author

Vollmer KO and Poisson A

Subjects
Adult, Carbon Isotopes, Cyclohexanecarboxylic Acids blood, Cyclohexanecarboxylic Acids cerebrospinal fluid, Cyclohexanecarboxylic Acids urine, Feces analysis, Humans, Male, Plasma analysis, Time Factors, Cyclohexanecarboxylic Acids metabolism
Published
1970

29. [Research with experimental animals on the mechanism of action of the new choleretic, 3-ethyl-4-oxo-5-piperidino-delta 2, alpha-thiazolidine-acetic acid ethyl ester (Piprozolin)].

Author

Koss FW, Vollmer KO, and Herrmann M

Subjects
1-Propanol pharmacology, Acetates administration & dosage, Acetates metabolism, Acetates pharmacology, Animals, Bile drug effects, Carbon Isotopes, Catheterization, Cats, Dogs, Ethylamines administration & dosage, Ethylamines pharmacology, Ketones metabolism, Male, Piperidines administration & dosage, Piperidines pharmacology, Rabbits, Rats, Rats, Inbred Strains, Thiazoles administration & dosage, Thiazoles pharmacology, Bile metabolism, Cholagogues and Choleretics administration & dosage, Cholagogues and Choleretics pharmacology, Piperidines metabolism, Thiazoles metabolism
Published
1972

31. [The inhibitory effect of cardiac glycosides on 86 Rb-uptake of erythrocytes. II. Specificity of the inhibitory effect with special attention to cymarin (k-strophantin-a) and its derivatives].

Author

Vollmer KO, Wissler JH, and Belz GG

Subjects
Adenosine Triphosphatases antagonists & inhibitors, Erythrocytes drug effects, Erythrocytes enzymology, Humans, In Vitro Techniques, Potassium, Radioisotopes, Sodium, Structure-Activity Relationship, Erythrocytes metabolism, Rubidium blood, Strophanthins pharmacology
Published
1972
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32. [The inhibitory effect of cardiac glycosides on 86 Rb-uptake of erythrocytes. I. Studies on the determination of cymarin (k-strophantin-a) and digitoxin].

Author

Belz GG, Vollmer KO, and Wissler JH

Subjects
Cardanolides analysis, Cardanolides isolation & purification, Digitoxin analysis, Digitoxin isolation & purification, Erythrocytes drug effects, Glycosides analysis, Glycosides isolation & purification, Humans, In Vitro Techniques, Methods, Radioisotopes, Time Factors, Cardanolides pharmacology, Digitoxin pharmacology, Erythrocytes metabolism, Glycosides pharmacology, Rubidium blood
Published
1972
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34. [The pharmacokinetics and metabolism of a new choleretic, 3-ethyl-4-oxo-5-piperidino- 2, -thiazolidineacetic acid ethyl ester (Piprozolin) after enteral administration in the rat].

Author

Vollmer KO and Koss FW

Subjects
Acetates blood, Acetates metabolism, Acetates urine, Administration, Oral, Animals, Bile metabolism, Carbon Isotopes, Cholagogues and Choleretics blood, Cholagogues and Choleretics urine, Digestive System metabolism, Ethylamines blood, Ethylamines urine, Feces analysis, Ketones, Kinetics, Male, Piperidines blood, Piperidines urine, Rats, Thiazoles blood, Thiazoles urine, Cholagogues and Choleretics metabolism, Piperidines metabolism, Thiazoles metabolism
Published
1972

37. [The inhibitory effects of cardiac glycosides on 86 Rb uptake of erythrocytes. 3. The influence of different substances on the inhibitory effect of cymarin on 86 Rb-uptake of erythrocytes].

Author

Wissler JH, Belz GG, and Vollmer KO

Subjects
Drug Interactions, Erythrocytes drug effects, Humans, In Vitro Techniques, Radioisotopes, Strophanthins administration & dosage, Verapamil administration & dosage, Vitamin E administration & dosage, Vitamin E therapeutic use, Erythrocytes metabolism, Rubidium blood, Strophanthins pharmacology, Verapamil pharmacology, Vitamin E pharmacology
Published
1972
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