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  • 1985-1989  (4)
  • 1980-1984
  • 1960-1964
  • 1985  (4)
Material
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  • 1985-1989  (4)
  • 1980-1984
  • 1960-1964
Year
  • 1
    Electronic Resource
    Electronic Resource
    College Park, Md. : American Institute of Physics (AIP)
    The Journal of Chemical Physics 82 (1985), S. 2110-2117 
    ISSN: 1089-7690
    Source: AIP Digital Archive
    Topics: Physics , Chemistry and Pharmacology
    Notes: Vibrational energy distributions in CO2 molecules formed in the catalytic oxidation of CO on platinum have been measured by using a variety of filtering techniques to analyze infrared chemiluminescent emission. For surface temperatures in the range of 650–1100 K the product molecules were vibrationally excited substantially beyond thermal equilibrium with the surface. Emission spectra observed in the 4.3 μm region were significantly red shifted from the fundamental of the asymmetric stretch at 2349 cm−1, indicating that much of the emission originated from higher lying bend–stretch combination states. The vibrational energy of the product, particularly in the asymmetric stretching mode, was sensitive to the coverage of oxygen present on the catalyst surface. These results are consistent with a model in which bending and asymmetric stretching motions contribute strongly to the reaction coordinate for CO oxidation.
    Type of Medium: Electronic Resource
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  • 2
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    Washington : Periodicals Archive Online (PAO)
    Middle East Journal. 39:1 (1985:Winter) 136 
    ISSN: 0026-3141
    Topics: Ethnic Sciences , History , Political Science , Sociology , Economics
    Description / Table of Contents: MAGHRIB
    Notes: BOOK REVIEWS
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  • 3
    Electronic Resource
    Electronic Resource
    Springer
    Journal of molecular medicine 63 (1985), S. 1075-1080 
    ISSN: 1432-1440
    Keywords: Ouabain binding ; Intact mononuclear leucocytes
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Summary Specific binding of cardiac glycosides to intact human blood cells may be a suitable model for physiological or disease-induced changes in cardiac glycoside binding to human heart muscle. Since the erythrocyte contains no nucleus and has relatively few binding sites compared with heart muscle, intact mononuclear leucocytes were investigated in the present study. Using leucocyte suspensions from 34 normal subjects, 133 measurements of3H-ouabain binding were obtained.3H-Ouabain bound to one type of binding site with an affinity (KD) of 2.8±1.2 × 10−9 M, similar to that of human heart muscle. Association and dissociation were slow processes (k+1, 3.9×104 M−1 sec−1; k−1, 8.1×10−5 sec−1,n=2). The number of ouabain binding sites/leucocyte varied from 18,000 to 60,000 ( $$\bar x \pm SD$$ , 34,600±9,700), with no correlation with the proportion of monocytes present or with the serum K+-level of the donors. Large inter- and intra-individual differences in binding site number were measured which are probably a result of the heterogeneity of the cell suspension used. Thus, the ouabain binding site on human heart muscle and intact mononuclear leucocytes is probably identical. However, the number of binding sites in mixtures of mononuclear leucocytes shows large and inconsistent intraindividual variations, making these studies unsuitable for quantifying drug- or disease-induced changes in ouabain binding site number.
    Type of Medium: Electronic Resource
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  • 4
    Electronic Resource
    Electronic Resource
    Springer
    Journal of molecular medicine 63 (1985), S. 1117-1123 
    ISSN: 1432-1440
    Keywords: Dopamine ; Levodopa ; Positive inotropic effect ; Human heart
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Summary The direct positive inotropic effects of dopamine and its precursor, levodopa, were measured using isolated, contracting human papillary muscle strips taken from patients during mitral valve replacement. Levodopa did not produce any positive inotropic effect at concentrations up to 3×10−3 M. The positive inotropic effects of dopamine were observed at concentrations above 1×10−5 M with the maximal effect at 3×10−3 M — concentrations higher than those observed in therapy. This inotropic effect was reduced by the β1 antagonist, 1-practolol (1×10−6 M); the β2 antagonist, ICI 118,551 HCl (1×10−6 M); the dopamine antagonist, haloperidol (3×10−6 M); the neuronal uptake inhibitor, cocaine (3×10−5 M), but not by the α1, prazosin (1×10−7 M). This indicates that dopamine exerts its positive inotropic effects on human heart muscle mainly through release of noradrenaline, together with possible interactions at β-and dopamine-receptors. The maximal inotropic effect of dopamine was about 50% that of calcium (15 mM, 6.2±0.7 mN) or ouabain (1×10−7 M, 5.0±0.8 mN) when measured in the same muscle strips, possibly due to the reduced cardiac noradrenaline content together with the reduced β-receptor number in congestive heart failure. This concentration of ouabain (1×10−7 M) gave almost maximal inotropy without marked toxicity; when dopamine was then added, only toxicity developed without any further increases in force of contraction. Any haemodynamic benefits of dopamine therapy in optimally digitalis-treated patients are probably due to other cardiovascular effects such as vasodilatation.
    Type of Medium: Electronic Resource
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