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  • 1
    Electronic Resource
    Electronic Resource
    Springer
    European journal of clinical pharmacology 21 (1982), S. 325-330 
    ISSN: 1432-1041
    Keywords: cimetidine ; renal failure ; cimetidine sulphoxide ; pharmacokinetics ; haemodialysis
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology , Medicine
    Notes: Summary A single intravenous dose of cimetidine 200mg was administered to 6 patients with severe chronic renal failure one hour prior to haemodialysis. The plasma concentrations of cimetidine and its sulphoxide metabolite at the start of haemodialysis were 2.74±0.12 and 0.76±0.08 µg/ml, and after dialysis for 4h 1.08±0.10 and 0.51±0.08 µg/ml, respectively (mean ± SE). The average haemodialysis clearance (ClHDa) of cimetidine during dialysis was 46–92ml/min at a dialysate flow rate of 320ml/min and blood flow rates in the 6 patients between 160–240ml/min. The mean ClHDa of the sulphoxide metabolite was 44% higher than that of cimetidine, and ranged between 49–148ml/min. During haemodialysis the mean plasma elimination half-life (t1/2) of cimetidine was 3.24h (range 2.08–5.08) and of the sulphoxide metabolite 9.49h (range 4.70–14.39). There was a significant relationship between the elimination rate constant (β) and ClHDa of the sulphoxide metabolite (p〈0.01), but no such relationship was found between β and ClHDa of cimetidine. However, there was a tendency to a relationship between β of cimetidine and the capacity to metabolise the drug, expressed as the ratio between the plasma concentrations of the sulphoxide metabolite and cimetidine after dialysis for 4h. These ratios ranged between 0.23–0.76, and the lowest ratio was seen in the patient with the lowest β value of cimetidine. Thus, the large variations in the plained by differences in their capacity to metabolise the drug. The mean total amount of cimetidine eliminated during dialysis was 27.3mg (range 17.9–31.8), which was 9.0–15.9% of the given dose. Between 12.2–21.2mg (mean 15.3) of the sulphoxide metabolite was eliminated in the dialysate. Major adjustment of the dose of cimetidine on days of dialysis is not necessary.
    Type of Medium: Electronic Resource
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  • 2
    ISSN: 1432-1041
    Keywords: prizidilol ; antihypertensive effect ; acute and long-term blood pressure control ; plasma renin activity ; acetylator phenotype ; antinuclear antibodies ; side effects ; kinetics
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology , Medicine
    Notes: Summary After an initial placebo period of four weeks 24 patients with primary hypertension were treated with prizidilol, a hydrazinopyridazine derivative with combined vasodilator and non-selective beta-adrenoceptor blocking actions, for a dose titration period of 14 weeks. Prizidilol 200 to 800 mg was given once daily to achieve a target supine diastolic blood pressure (BP)〈90 mmHg. Supine and standing BP recorded 24–27 h after drug intake decreased from 172±17/106±6 mmHg (mean±SD) and 167±18/111±8 mmHg, respectively, after placebo to 159±16/99±8 and 154±18/101±9 mmHg after active treatment for six weeks (mean dose 447 mg), and to 154±16/97±7 and 148±14/97±7 mmHg after treatment for 14 weeks (mean dose 687 mg/day). A slight reduction in HR was seen after treatment for six weeks and in plasma renin activity and urinary methoxycatecholamine excretion after treatment for 14 weeks. A sustained decrease in BP was observed for 10 h after prizidilol 800 mg (n=9), with a maximum antihypertensive effect (mean reduction in supine BP 33/18 mmHg) 2.5 h after dosing, which coincided with the mean peak plasma concentration. The plasma elimination half-life of the drug was 3.9 h (range 2.0–8.9 h). Changing to a twice daily regimen in 17 patients (mean daily dose 748 mg at six months) did not produce any further reduction in the BP (recorded 12–15 h after dosing) as compared to the once daily regimen at 14 weeks. During treatment for up to 24 months, 16 patients did not achieve satisfactory BP control. Eight of them were withdrawn and eight received additional treatment with bendroflumethiazide (2.5–5 mg/day). In 7 of the latter satisfactory BP control was achieved. Side effects were few. Dizziness and tiredness occurred in four patients 2–5 h after prizidilol 600–800 mg once daily. These symptoms partly subsided when the subjects changed to a twice daily regimen. No ocular side-effects were found. Before treatment 13 out of 24 patients had a low titre of IgM antinuclear antibodies (ANA) and one patient also a low titre of IgG ANA. During treatment the frequency of patients with positive ANA-titres became higher, and after treatment for 12 months (n=17) 15 patients had positive IgM and seven patients positive IgG ANA-titres. However, the titres were low and no patient showed a clinical lupus erythematosus syndrome. There was no relation between acetylator phenotype of the patient and acute or longterm effecton BP, pharmacokinetics of the drug or the development of a raised ANA-titre.
    Type of Medium: Electronic Resource
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  • 3
    Electronic Resource
    Electronic Resource
    Springer
    European journal of clinical pharmacology 26 (1984), S. 87-93 
    ISSN: 1432-1041
    Keywords: enprofylline ; pharmacokinetics ; renal elimination ; renal insufficiency ; healthy subjects ; creatinine clearance ; side effects
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology , Medicine
    Notes: Summary Enprofylline, a new bronchodilating drug, was given i.v. at 1.0 mg/kg to 7 healthy subjects and to 14 patients with differing degrees of chronic renal insufficiency. Plasma and urine concentrations of unchanged drug were followed by HPLC. In the patients the plasma half-life was prolonged and the total and renal clearances were reduced in direct proportion to the degree of renal insufficiency as determined by creatinine clearance. The unbound fraction of enprofylline in plasma increased from 55% in the healthy subjects to 66% in the group of patients with the highest degree of renal impairment. The volume of distribution terms, Vβ and Vss, both tended to decrease with decreasing creatinine clearance. When the volume term calculations were based on the unbound drug level in plasma, this tendency was enhanced. Side-effects were noted in 4 subjects, and to some extent were related to the plasma level of the drug.
    Type of Medium: Electronic Resource
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  • 4
    Electronic Resource
    Electronic Resource
    Oxford, UK : Blackwell Publishing Ltd
    Annals of the New York Academy of Sciences 416 (1983), S. 0 
    ISSN: 1749-6632
    Source: Blackwell Publishing Journal Backfiles 1879-2005
    Topics: Natural Sciences in General
    Type of Medium: Electronic Resource
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  • 5
    ISSN: 1572-8838
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology , Electrical Engineering, Measurement and Control Technology
    Notes: Abstract Electrodes for the electrochemical reduction of oxygen have been studied both galvanostatically and by XPS and IR spectroscopy. The electrodes contain a polymeric phthalocyanine catalyst fixed to an activated carbon carrier by a covalent link of imidazol. Various preparation methods have been tried to make conditions for the coupling of imidazol to the carbon surface as mild as possible. It is concluded from the XPS measurements that about one imidazol molecule is present for every second C6 unit on the carbon surface. The treatment described results in highly reversible electrode systems. The lifetime of the electrode is limited to several hundred hours, the sudden decrease thereafter is probably related to a solvolysis of the carbon-nitrogen bond linking the imidazol to the surface.
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  • 6
    Electronic Resource
    Electronic Resource
    Springer
    Journal of applied electrochemistry 11 (1981), S. 489-492 
    ISSN: 1572-8838
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology , Electrical Engineering, Measurement and Control Technology
    Notes: Abstract Electrodes for the electrochemical reduction of oxygen have been studied galvanostatically. The electrodes were of the activated carbon-polymeric iron phthalocyanine (FePc) type, made hydrophobic with a Teflon treatment. A link between the FePc and the carbon was achieved by covalently binding imidazol to the carbon surface and then letting the FePc co-ordinate to the free nitrogen of the imidazol molecule. In this way an initial improvement of the stability of the electrode potential and the polarization data was achieved. It has furthermore been established that the potential responds more rapidly to changes, i.e. it is more reversible, than an analogous electrode based on carbon that has not been treated with imidazol.
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  • 7
    Electronic Resource
    Electronic Resource
    Weinheim : Wiley-Blackwell
    Zeitschrift für anorganische Chemie 478 (1981), S. 119-138 
    ISSN: 0044-2313
    Keywords: Chemistry ; Inorganic Chemistry
    Source: Wiley InterScience Backfile Collection 1832-2000
    Topics: Chemistry and Pharmacology
    Description / Table of Contents: IR-Untersuchungen an koordinativ ungesättigten Oberflächenverbindungen auf Kieselgel. IV. CO-Komplexe mit Chrom(II) und Chrom(III)Drei verschiedene Chrom(II)-Oberflächenverbindungen konnten anhand der IR-Spektren von adsorbiertem CO ermittelt werden. Besonders wichtig für die Erklärung der Untersuchungen sind die Absorptionsbanden zwischen 2050 und 2035 cm-1 und die relativen Intensitäten der CO-Banden bei 2100 und 2120 cm-1. Die Banden zwischen 2192 und 2179 cm-1 zeigen ebenfalls unterschiedliches Verhalten mit jeder der drei Chrom(II)-Oberflächenverbindungen. Zwei Chrom(III)-Oberflächenverbindungen konnten durch das Auftreten entweder einer CO-Bande bei 2200 cm-1 oder von zwei Banden bei 2206 und 2196 cm-1 nachgewiesen werden. Drei Modelle werden für die im Titel genannten Chrom(II)-Verbindungen vorgeschlagen, die alle auf zweikernigen Oberflächenkomplexen beruhen: Modell eins und zwei enthalten Chrom(II)-Ionen mit trans- und cis-Konfiguration in unterschiedlichen Kombinationen und das dritte Modell enthält ein Brückensauerstoffion von einer Siloxangruppe als störenden Liganden. Die drei Modelle erklären die CO-Banden ausreichend und ein Modellvorschlag stimmt nahezu quantitativ mit früheren volumetrischen Adsorptionsmessungen überein, die den überraschenden Effekt einer mit abnehmender Temperatur ebenfalls abnehmenden CO-Adsorption zeigten. Zwei Modelle mit entweder einer Sauerstoff-Doppelbrücke oder nur einer Sauerstoffbrücke werden für die beiden Chrom(III)-Oberflächenverbindungen vorgeschlagen.
    Notes: Three different chromium(II) surface compounds have been identified by their IR spectra of adsorbed CO. Especially important in the interpretation of the experiments are the bands between 2050 and 2035 cm-1 and the relative intensities of the CO bands at 2100 and 2120 cm-1. The bands between 2192 and 2179 cm-1 show also a different pattern for each of the different chromium(II) surface compounds. Two chromium(III) surface compounds could be identified by the presence of either one CO band near 2200 cm-1 or two bands near 2206 and 2196 cm-1. Three models are proposed for the chromium(II) title compounds, all related to dinuclear chromium(II) surface complexes: Models one and two have chromium(II) ions with trans and cis configuration in different combinations, respectively, and the third model has a bridging oxygen ion from a siloxan group as a distorting ligand. The three models explain the CO absorptions sufficiently and one is nearly quantitatively in agreement with previous volumetric adsorption studies of CO on chromium(II), which showed the surprising effect of decreasing CO adsorption with decreasing temperature. Two models for the chromium(III) surface compounds are proposed with either an oxygen double bridge or only one bridging oxygen.
    Additional Material: 12 Ill.
    Type of Medium: Electronic Resource
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  • 8
    Publication Date: 1984-10-01
    Print ISSN: 0378-7753
    Electronic ISSN: 1873-2755
    Topics: Electrical Engineering, Measurement and Control Technology
    Published by Elsevier
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  • 9
    Publication Date: 1983-08-01
    Print ISSN: 0031-6970
    Electronic ISSN: 1432-1041
    Topics: Chemistry and Pharmacology , Medicine
    Published by Springer
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  • 10
    Publication Date: 1982-01-01
    Print ISSN: 0031-6970
    Electronic ISSN: 1432-1041
    Topics: Chemistry and Pharmacology , Medicine
    Published by Springer
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