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1

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Acute haemodynamic effects of urapidil in patients with chronic left ventricular failure (1988)

Tebbe, U. ; Wurst, W. ; Neuhaus, K. L.

Springer

European journal of clinical pharmacology 35 (1988), S. 305-308

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ISSN: 1432-1041

Keywords: urapidil ; left ventricular failure ; haemodynamic parameters

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary Urapidil, a new alpha1-adrenoceptor blocking drug, has been shown to be effective in the treatment of hypertension. Ten normotensive patients with severe congestive heart failure were given Urapidil 25 mg i.v. twice in 15 min and the haemodynamic effects were measured. There was a significant fall in systolic blood pressure (−16%), mean blood pressure (−13%), left ventricular end-diastolic pressure (−38%), mean pulmonary artery pressure (−31%) and wedge pressure (−40%). Total peripheral resistance fell by 25%, whereas pulmonary arteriolar resistance did not change significantly. Cardiac output increased by 22%. The increase in cardiac output with decreasing peripheral resistance and LV pressures suggests that urapidil may be useful in the therapy of congestive heart failure.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00558269

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2

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Lack of pharmacodynamic and pharmacokinetic interaction between pantoprazole and phenprocoumon in man (1996)

Ehrlich, A. ; Fuder, H. ; Hartmann, M. ; [et al.]

Springer

European journal of clinical pharmacology 51 (1996), S. 277-281

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ISSN: 1432-1041

Keywords: Key words Pantoprazole; Proton pump inhibitor drug interaction ; oral anticoagulant phenprocoumon ; pharmacodynamics ; pharmacokinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Abstract Objective: Pantoprazole is a selective proton pump inhibitor characterized by a low potential to interact with the cytochrome P450 enzymes in man. Due to the clinical importance of an interaction with anticoagulants, this study was carried out to investigate the possible influence of pantoprazole on the pharmacodynamics and pharmacokinetics of phenprocoumon. Methods: Sixteen healthy male subjects were given individually adjusted doses of phenprocoumon to reduce prothrombin time ratio (Quick method) to about 30–40% of normal within the first 5–9 days and to maintain this level. The individual maintenance doses remained unaltered from day 9 on and were administered until day 15. Additionally, on study days 11–15, pantoprazole 40 mg was given per once daily. As a pharmacodynamic parameter, the prothrombin time ratio was determined on days 9 and 10 (reference value) and on days 14 and 15 (test value), and the ratio test/reference was evaluated according to equivalence criteria. Results: The equivalence ratio (test/reference) for prothrombin time ratio was 1.02 (90% confidence interval 0.95–1.09), thus fulfilling predetermined bioequivalence criteria (0.70–1.43). The pharmacokinetic characteristics AUC0–24h and Cmax of S(−)-and R(+)-phenprocoumon were also investigated using equivalence criteria. Equivalence ratios and confidence limits of AUC0–24h and of Cmax of S(−)-phenprocoumon (0.93, 0.87–1.00 for AUC0–24h; 0.95, 0.88–1.03 for Cmax) and of R(+)-phenprocoumon (0.89, 0.82–0.96; 0.9, 0.83–0.98) were within the accepted range of 0.8–1.25. Conclusion: Pantoprazole does not interact with the anticoagulant phenprocoumon on a pharmacodynamic or pharmacokinetic level. Concomitant treatment was well tolerated.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/s002280050198

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3

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Effect of urapidil on steady-state serum digoxin concentration in healthy subjects (1989)

Solleder, P. ; Haerlin, R. ; Wurst, W. ; [et al.]

Springer

European journal of clinical pharmacology 37 (1989), S. 193-194

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ISSN: 1432-1041

Keywords: urapidil ; digoxin ; blood drug level ; pharmacokinetics ; drug absorption/-interaction

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Medicine

Notes: Summary In an open, randomized, two-period change-over study the effect of urapidil, an antihypertensive agent, on steady-state serum digoxin levels was investgated in 12 healthy male volunteers. The subjects were given digoxin 0.25 mg once daily for 4 days to produce a steady-state digoxin level in serum. At the end of that time the subjects received either digoxin monotherapy or digoxin and concomitant treatment with urapidil 60 mg b.d. for a further 4 days. Subsequently the treatments were changed over. The absorption characteristics Cmax and tmax of digoxin were not altered by concomitant urapidil treatment. The geometric mean and nonparametric 95% confidence limits of digoxin relative bioavailability were 97% (93%–103%). Therefore, concomitant administration of urapidil with digoxin treatments did not appear to alter the rate and extent of absorption of the glycoside.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00558231

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4

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Effect of repeated oral administration of BY 1023/SK&F 96022 – a new substituted benzimidazole derivative – on pentagastrin-stimulated gastric acid secretion and pharmacokinetics in man (1990)

SIMON, B. ; MÜLLER, P. ; MARINIS, E. ; [et al.]

Oxford, UK : Blackwell Publishing Ltd

Alimentary pharmacology & therapeutics 4 (1990), S. 0

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ISSN: 1365-2036

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Medicine

Notes: Pentagastrin stimulated gastric secretion was measured in 12 healthy male subjects after repeated once daily oral administration of 20 and 40 mg BY 1023/SK&F 96022 – a new substituted benzimidazole derivative.Twenty milligrams inhibited acid output compared with placebo by 24% (2.5–3.5 h) and 26% (24.5–25.5 h) after the first oral intake. Inhibition increased to 56% and 50%, respectively, after the seventh oral dose. Forty milligrams inhibited acid output by a mean of 51% (2.5 to 3.5 h) and 52% (24.5–25.5) after the first oral intake. After the seventh dose mean inhibition rose to 85% and 66%, respectively.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.1365-2036.1990.tb00483.x

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5

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PANTOPRAZOLE AND 24-HOUR INTRAGASTRIC ACIDITY (1993)

Hartmann, M. ; Bliesath, H. ; &, R. Lühmann ; [et al.]

Oxford, UK : Blackwell Publishing Ltd

Alimentary pharmacology & therapeutics 7 (1993), S. 0

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ISSN: 1365-2036

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Medicine

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.1365-2036.1993.tb00077.x

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6

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Single intravenous administration of the H+, K+-ATPase inhibitor BY 1023/SK&F 96022—inhibition of pentagastrin-stimulated gastric acid secretion and pharmacokinetics in man (1990)

SIMON, B. ; MÜLLER, P. ; BLIESATH, H. ; [et al.]

Oxford, UK : Blackwell Publishing Ltd

Alimentary pharmacology & therapeutics 4 (1990), S. 0

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ISSN: 1365-2036

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Medicine

Notes: The effects of the H+, K+-ATPase inhibitor BY 1023/SK&F 96022 on pentagastrin-stimulated acid secretion have been studied in healthy male volunteers (n= 12). The gastric acid response to submaximal pentagastrin-stimulation (0.6 μg/h/kg b.w.) was dose-dependently inhibited. A single dose of 5 mg decreased acid output by 22% while after 60 mg and 80 mg secretion was almost completely abolished.A good dose linearity was observed for AUC (0, 〉) and Cmax over the dose range from 5 to 80 mg. Elimination half-life, total clearance and volume of distribution of the parent compound were independent of the dose.The drug was well tolerated up to the highest dose of 80 mg. No clinically relevant influence was found on either laboratory screen or cardiovascular parameters.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.1365-2036.1990.tb00468.x

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7

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Twenty-four-hour intragastric pH profiles and pharmacokinetics following single and repeated oral administration of the proton pump inhibitor pantoprazole in comparison to omeprazole. (1996)

Hartmann, M ; Theiss, U ; Huber, R ; [et al.]

Oxford, UK : Blackwell Science Ltd

Alimentary pharmacology & therapeutics 10 (1996), S. 0

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ISSN: 1365-2036

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Medicine

Notes: BACKGROUND: Pantoprazole is a proton pump inhibitor characterized by a low potential to interact with the cytochrome P450 enzyme system in man. Its effect on intragastric pH following single and repeated oral intake was investigated in comparison to omeprazole by continuous intragastric pH-metry at doses recommended for treatment of peptic ulcer disease. METHODS: Sixteen healthy male subjects underwent two dosing periods. From day 1 to day 7, they were given once daily by mouth 40 mg pantoprazole in one period and 20 mg omeprazole in the other period, according to a double-blind randomized crossover design. Twenty-four-hour intragastric pH was recorded and frequent blood samples for pharmacokinetic analysis were taken on day 1 and day 7. A placebo pH profile was obtained prior to each treatment period. RESULTS: Pantoprazole was significantly more effective than omeprazole with regard to increase in 24-h and daytime pH, following both single (median 24-h pH: 1.45 vs. 1.3, P 〈 0.05; median daytime pH: 1.6 vs. 1.3, P 〈 0.01) and repeated (median 24-h pH: 3.15 vs. 2.05, P 〈 0.01; median daytime pH: 3.8 vs. 2.65, P 〈 0.05) oral intake. As compared to the first dose, repeated administration of both drugs markedly increased the effect on intragastric pH. With pantoprazole, steady- state serum concentrations were obtained after the first dose, but not with omeprazole. Both drugs were well tolerated without relevant changes in vital signs of clinical laboratory parameters. CONCLUSION: Pantoprazole 40 mg is significantly more effective than omeprazole 20 mg in raising intragastric pH.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.0953-0673.1996.00359.x

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8

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Antibacterial active components in human urine after administration of penicillins (1979)

Ullmann, U. ; Wurst, W.

Springer

Infection 7 (1979), S. 187-189

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ISSN: 1439-0973

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Description / Table of Contents: Zusammenfassung Der 4-Stunden-Urin von freiwilligen Versuchspersonen und Patienten, die oral oder intravenös Penicilline erhalten hatten, wurde dünnschichtchromatographisch und mit Hilfe der Bioautographie untersucht. Bei nur zwei von 12 Penicillinen — Amoxicillin und Mezlocillin — waren keine antibakteriell aktiven Metaboliten nachzuweisen. Bei den übrigen Penicillinen besaßen diese unterschiedliche antibakterielle Aktivität, wie bei Verwendung verschiedener Testmikroorganismen gezeigt werden konnte. Nach Gabe von Carbenicillinestern wurden drei anti-bakteriell aktive Flecken getrennt, einer von ihnen entsprach dem Penicillin G; die beiden anderen besaßen Aktivität gegenüberPseudomonas aeruginosa. Das Bioautogramm nach Azlocillin-Therapie zeigte zwei Komponenten mit Aktivität gegenüberBacillus subtilis, Staphylococcus aureus undEscherichia coli; gegenüberP. aeruginosa jedoch war nur der schnell wandernde Fleck aktiv. Über die Bildung und die chemische Beschaffenheit dieser zusätzlichen aktiven Komponenten besteht noch weitgehend Unklarheit. Es ist jedoch durchaus möglich, daß sie die Bioverfügbarkeit eines Antibiotikums beeinträchtigen.

Notes: Summary Four-hourly urine from volunteers and patients who had received penicillins orally or intravenously was investigated by means of thin layer chromatography and bioautography. Antibacterially active metabolites were not detected with only two of 12 penicillins, namely amoxicillin and mezlocillin. In the case of the other penicillins the metabolites possessed variable antibacterial activity as could be demonstrated using different test microorganisms. After administration of carbenicillin esters three antibacterially active spots were detected, one of which corresponded to penicillin G; the other two were active againstPseudomonas aeruginosa. The bioautogram after treatment with azlocillin showed two components which were active againstBacillus subtilis, Staphylococcus aureus andEscherichia coli; only the rapid moving component was active againstP. aeruginosa, however. The formation and chemical nature of these additional active components is still to a large extent not understood. It is quite possible, however, that they affect the bio-availability of an antibiotic.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01640941

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9

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Tolerance, safety, and kinetics of the new antineoplastic compound dexniguldipine-HCl after oral administration: a phase I dose-escalation trial (1995)

Ukena, D. ; Boewer, C. ; Oldenkott, B. ; [et al.]

Springer

Cancer chemotherapy and pharmacology 36 (1995), S. 160-164

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ISSN: 1432-0843

Keywords: Key words Dexniguldipine-HCl ; Phase I trial ; Pharmacokinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Dexniguldipine-HCl is a new dihydropyridine compound that exerts selective antiproliferative activity in a variety of tumor models and, in addition, has a high potency in overcoming multidrug resistance. The purpose of this trial was to determine the toxicity and pharmacokinetics of dexniguldipine and to establish a recommended dose for phase II trials. A total of 37 patients with cancer were treated with oral dexniguldipine in increasing doses for up to 7 days. The main parameters evaluated were subjective tolerance and laboratory and cardiovascular parameters (blood pressure and ECG). Blood samples were drawn for analysis of the drug’s pharmacokinetics. Dizziness and nausea were the major adverse events observed in seven patients, but episodes were generally mild and not clearly dose-related. Vomiting occurred in one patient. Hypotensive effects and orthostatic dysregulation were observed in some patients but were not considered to be dose-limiting. Therefore, no dose-limiting toxicity was found and the maximally tolerable dose could not be determined. Pharmacokinetic data showed wide interindividual variation and a dose-dependent increase in steady-state serum concentrations at doses of up to 1,000 mg daily, with no clear further increase being observed at higher doses. Consistently high concentrations were achieved with the 2,500-mg dose. Despite the lack of dose-limiting toxicity, higher doses of dexniguldipine do not appear to be useful for clinical evaluation because of the pharmacokinetic properties of the compound; therefore, 2,500 mg/day is recommended as the daily dose for phase II trials.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00689202

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Tolerance, safety, and kinetics of the new antineoplastic compound dexniguldipine-HCl after oral administration: a phase I dose-escalation trial (1995)

Ukena, D. ; Boewer, C. ; Oldenkott, B. ; [et al.]

Springer

Cancer chemotherapy and pharmacology 36 (1995), S. 160-164

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ISSN: 1432-0843

Keywords: Dexniguldipine-HCl ; Phase I trial ; Pharmacokinetics

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Dexniguldipine-HCl is a new dihydropyridine compound that exerts selective antiproliferative activity in a variety of tumor models and, in addition, has a high potency in overcoming multidrug resistance. The purpose of this trial was to determine the toxicity and pharmacokinetics of dexniguldipine and to establish a recommended dose for phase II trials. A total of 37 patients with cancer were treated with oral dexniguldipine in increasing doses for up to 7 days. The main parameters evaluated were subjective tolerance and laboratory and cardiovascular parameters (blood pressure and ECG). Blood samples were drawn for analysis of the drug's pharmacokinetics. Dizziness and nausea were the major adverse events observed in seven patients, but episodes were generally mild and not clearly dose-related. Vomiting occurred in one patient. Hypotensive effects and orthostatic dysregulation were observed in some patients but were not considered to be dose-limiting. Therefore, no dose-limiting toxicity was found and the maximally tolerable dose could not be determined. Pharmacokinetic data showed wide interindividual variation and a dose-dependent increase in steady-state serum concentrations at doses of up to 1,000 mg daily, with no clear further increase being observed at higher doses. Consistently high concentrations were achieved with the 2,500-mg dose. Despite the lack of dose-limiting toxicity, higher doses of dexniguldipine do not appear to be useful for clinical evaluation because of the pharmacokinetics properties of the compound; therefore, 2,500 mg/day is recommended as the daily dose for phase II trials.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00689202

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