ALBERT — All Library Books, journals and Electronic Records Telegrafenberg

1

Electronic Resource

Pharmacokinetic studies in man with sparteine (1970)

Dengler, H. J. ; Eichelbaum, M. ; Hengstmann, J. ; [et al.]

Springer

European journal of clinical pharmacology 2 (1970), S. 189-195

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ISSN: 1432-1041

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary Plasma levels of sparteine were determined in two groups of 8 patients each of whom received 200 mg of sparteine sulphate (Depasan®) intravenously and orally. A method was developed for the determination of sparteine in biological fluids, relying on solvent extraction and gas chromatography. After oral administration, 69.4% of the sparteine was absorbed and peak plasma levels were reached after 46.5 min. After intravenous injection the plasma levels declined with a half life of 117 min. When sparteine is given intravenously, 34.2% of the dose administered is excreted in the urine in the next 24 h as unchanged sparteine. Two metabolites were found in the urine but have not yet been identified. They contribute only a few percent to the total urinary excretion of sparteine. Approximately 50% of sparteine is bound to plasma proteins. — The pharmacokinetics of sparteine after intravenous administration can be described in terms of a one-compartment model. —The tissue distribution of sparteine was studied in preliminary experiments in rats. The drug was accumulated in several tissues, with the greatest concentration in the lungs. The hypothesis is advanced that drugs, which are organic bases with high pKa-values and high lipid solubility, are concentrated mainly in the lungs, followed by the adrenals, spleen, and the heart.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00404298

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2

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Brevity is the soul of wit ... (1983)

Dengler, H. J. ; Gross, F.

Springer

European journal of clinical pharmacology 24 (1983), S. 571-571

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ISSN: 1432-1041

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00542202

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3

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Simultaneous determination of the intravenous and oral pharmacokinetic parameters of D,L-verapamil using stable isotope-labelled verapamil (1981)

Eichelbaum, M. ; Somogyi, A. ; Unruh, G. E. ; [et al.]

Springer

European journal of clinical pharmacology 19 (1981), S. 133-137

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ISSN: 1432-1041

Keywords: verapamil ; pharmacokinetics ; bioavailability ; hepatic first-pass metabolism ; stable isotopes

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary Following i. v. administration, the plasma concentration-time curve of verapamil could best be described by either a mono- or biexponential equation. Total plasma clearance (1.26 l/min) approached liver blood flow (1.5 l/min), so it can be concluded that its clearance is liver blood flow-dependent. Although absorption was almost complete after oral administration, absolute bioavailability (20%) was low, due to extensive hepatic first-pass metabolism. The approach using stable isotope-labelled and unlabelled drug permits simultaneous administration by the intravascular and extravascular routes, thus allowing determination of absolute bioavailability in a single experiment.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00568400

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4

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Superiority of stable isotope techniques in the assessment of the bioavailability of drugs undergoing extensive first pass elimination (1981)

Eichelbaum, M. ; Dengler, H. J. ; Somogyi, A ; [et al.]

Springer

European journal of clinical pharmacology 19 (1981), S. 127-131

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ISSN: 1432-1041

Keywords: verapamil ; tablets ; relative bioavailability ; intraindividual changes ; first-pass metabolism ; stable isotope technique

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary Although the absorption of verapamil is almost complete after oral administration, its bioavailability is low due to extensive hepatic first-pass metabolism. Besides large interindividual differences in first-pass metabolism, pronounced day-to-day intraindividual variations in first-pass metabolism are observed, leading to erroneous results in relative bioavailability studies. Stable isotope techniques, which permit simultaneous administration of a solution and a tablet, can successfully be used to overcome these difficulties. The method has the advantage that two experiments can be carried out in a single test. Furthermore, the number of subjects required in bioavailability studies can be greatly reduced. Using this technique the bioavailability of verapamil tablets (Isoptin® 80) relative to a stable labelled solution of verapamil was found to be 108.1%, with a 95% confidence interval between 89.1 and 127.1%.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00568399

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5

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Defective N-oxidation of sparteine in man: A new pharmacogenetic defect (1979)

Eichelbaum, M. ; Spannbrucker, N. ; Steincke, Barbara ; [et al.]

Springer

European journal of clinical pharmacology 16 (1979), S. 183-187

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ISSN: 1432-1041

Keywords: sparteine ; pharmacogenetic defect ; sparteine-N-oxidation ; defective metabolism ; autosomal recessive trait

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary Sparteine, an antiarrhythmic and oxytocic drug, is metabolised by N1-oxidation. The sparteine-N1-oxide rearranges with loss of water to 2- and 5-dehydrosparteine. 18 (i. e., 5%) out of 360 subjects were unable to metabolise the drug. These persons, who were designated as nonmetabolisers, excreted almost 100% of the administered dose in urine as unchanged drug. The defective metabolism of sparteine was found to have a genetic basis. Sparteine-N1-oxidation appears to be determined by two allelic genes at a single locus where nonmetabolisers are homozygous for an autosomal recessive gene.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00562059

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6

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Book reviews (1970)

Gross, F. ; Dengler, H. J.

Springer

European journal of clinical pharmacology 2 (1970), S. 249-250

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ISSN: 1432-1041

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00404309

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7

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In vitro — In vivo correlation of dissolution, a time scaling problem? Transformation of in vitro results to the in vivo situation, using theophylline as a practical example (1985)

Brockmeier, D. ; Dengler, H. J. ; Voegele, D.

Springer

European journal of clinical pharmacology 28 (1985), S. 291-300

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ISSN: 1432-1041

Keywords: drug dissolution ; theophylline ; in vitro/in vivo correlation ; convolution ; deconvolution ; in vitro/in vivo dissolution ; slow-release formulation

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary Two principal approaches to demonstrating the continuous in vivo relevance of an in vitro dissolution test are outlined. The first uses the convolution technique to predict the concentration-time course in vivo; the second uses deconvolution as a mathematical tool to estimate the in vivo dissolution profile. The weighting function must be known to utilise either technique. Defined by the aim of the analysis the dose-normalized response to the oral solution is regarded as the weighting function (Impulse Response). In both cases the essential step is continuous comparison of the predicted time dependent data with actual readings of the same class. To permit the prediction of concentration-time data from in vitro dissolution data the basic equations for the transformation of the time base from in vitro to in vivo conditions are developed. The transformation is essential, since one cannot assume that the time scales for the in vitro and the in vivo experiment are definitely the same. The estimated in vivo dissolution profile using the deconvolution technique gives a hypothetical image of the true in vivo dissolution curve. Comparison with in vitro dissolution test results, using one of the equivalence testing procedures, reveals how closely and for how long the in vitro dissolution test simulates the in vivo dissolution process. For the formulation of theophylline studied, equivalence of the in vitro and the estimated in vivo dissolution profiles was not confirmed for the entire period of observation, but it was demonstrated for approximately the first 5 h. The later inequivalence is not due to possible non-linear or time-dependent kinetics of theophylline. There is a discussion of whether a change in pH, agitation of the formulation, diffusion conditions or the absorption rate constant along the gastrointestinal tract might explain the biphasic linear correlation of the in vitro and in vivo data observed.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00543326

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8

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Dihydroergotamine increases the bioavailability of orally administered etilefrine (1982)

Hengstmann, J. H. ; Hengstmann, R. ; Schwonzen, S. ; [et al.]

Springer

European journal of clinical pharmacology 22 (1982), S. 463-467

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ISSN: 1432-1041

Keywords: orthostatic hypotension ; etilefrine ; dihydroergotamine ; bioavailability ; combination therapy

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary Etilefrine undergoes considerable first-pass metabolism through conjugation in the gut wall. In six volunteers bioavailability was reduced to 35% for a fast release tablet and to 17% for a sustained release preparation. The addition fo dihydroergotamine (DHE) to the sustained release preparation surprisingly increased bioavailability to 61%. The plasma levels of the main metabolite formed during the passage through the gut wall indicated an increase in the rate of enteric absorption and therefore also in bioavailability by DHE. This might be due to the influence of DHE upon the vascular resistance of the vessels in the gut wall or a change in gastro-intestinal motility with a prolongation of drug contact time within the absorbing gut segment.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00542554

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9

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Pharmacogenetic covariation of defective N-oxidation of sparteine and 4-hydroxylation of debrisoquine (1980)

Bertilsson, L. ; Dengler, H. J. ; Eichelbaum, M. ; [et al.]

Springer

European journal of clinical pharmacology 17 (1980), S. 153-155

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ISSN: 1432-1041

Keywords: sparteine N-oxidation ; debrisoquine 4-hydroxylation ; pharmacogenetics ; debrisoquine metabolism

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary Two subjects from each of the three groups of homozygous rapid, heterozygous, and homozygous non-metabolizers (N-oxidation) of sparteine received a single oral dose of debrisoquine. The urinary ratio of debrisoquine/4-hydroxy-debrisoquine, reflecting the individual's capacity to C-hydroxylate debrisoquine, was closely related to his phenotype for sparteine metabolism. This indicates that the two metabolic reactions are controlled by similar if not identical genetic factors.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00562624

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10

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Influence of the defective metabolism of sparteine on its pharmacokinetics (1979)

Eichelbaum, M. ; Spannbrucker, N. ; Dengler, H. J.

Springer

European journal of clinical pharmacology 16 (1979), S. 189-194

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ISSN: 1432-1041

Keywords: sparteine ; pharmacogenetic defect ; defective metabolism ; pharmacokinetics ; renal excretion

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary Sparteine is metabolized by N1-oxidation, which in some subjects is defective. The defect has a pronounced effect on the kinetics of the drug. In non-metabolisers elimination of sparteine proceeds entirely via renal excretion by a capacity-limited process, 99,9% of the dose being excreted as unchanged drug. In metabolisers the drug is mainly eliminated by metabolic degradation. Pronounced differences in β-phase half-life and total plasma clearance were observed between metabolisers (156 min; 535 ml · min−1) and nonmetabolisers (409 min; 180 ml · min−1).

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00562060

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