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  • 1
    Electronic Resource
    Electronic Resource
    [S.l.] : American Institute of Physics (AIP)
    Review of Scientific Instruments 64 (1993), S. 3598-3601 
    ISSN: 1089-7623
    Source: AIP Digital Archive
    Topics: Physics , Electrical Engineering, Measurement and Control Technology
    Notes: The surface temperature of pulse laser heated tungsten targets was determined by a high-speed micropyrometric method. Using a blue line of the heat radiation, a temporal/spatial resolution of 2 ns/10 μm is achieved. Temperatures were traced in the range from 2800 K to the boiling point of tungsten at about 6000 K. The accuracy is about 5%–10% because of uncertain values of the spectral emissivity. However, the accuracy of radiance temperature is limited only by the photon shot noise. Numerical calculations of the one-dimensional heat equation are in satisfactory agreement with the experimental results. If melting occurs, thermocapillary flow reduces the spatial resolution from the Abbe limit to about 10 μm.
    Type of Medium: Electronic Resource
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  • 2
    Electronic Resource
    Electronic Resource
    [S.l.] : American Institute of Physics (AIP)
    Journal of Applied Physics 75 (1994), S. 8027-8031 
    ISSN: 1089-7550
    Source: AIP Digital Archive
    Topics: Physics
    Notes: A time-resolving thermal-emission electron microscope was developed for tracking transient phenomena on pulse-laser-heated metal surfaces. Short-time exposures with a temporal/spatial resolution of 3 ns/1 μm were achieved by adding a high-gain image intensifier and a fast beam blanking unit to a conventional emission microscope. Fast surface heating was realized using a frequency-doubled neodymium yttrium aluminum garnet pulse laser (12 ns full width at half-maximum). Experiments with tungsten and tantalum are presented, showing the potential of this method for imaging fast changes of local surface parameters, e.g., temperature. The emission microscope is found to be a sensitive probe for incipient laser-induced modifications of the surface, even in the conventional mode. Apart from this some technical problems as well as the physical limitations of time-resolved thermal-emission microscopy are discussed.
    Type of Medium: Electronic Resource
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  • 3
    ISSN: 1572-9508
    Keywords: BATSE Spectroscopy Detector ; Detector Calibration ; Gamma Ray Detector ; Gamma Ray Burst
    Source: Springer Online Journal Archives 1860-2000
    Topics: Physics
    Notes: Abstract We describe the channel-to-energy calibration of the Spectroscopy Detectors of the Burst and Transient Source Experiment (BATSE) on the Compton Gamma Ray Observatory (GRO). These detectors consist of NaI(Tl) crystals viewed by photomultiplier tubes whose output in turn is measured by a pulse height analyzer. The calibration of these detectors has been complicated by frequent gain changes and by nonlinearities specific to the BATSE detectors. Nonlinearities in the light output from the NaI crystal and in the pulse height analyzer are shifted relative to each other by changes in the gain of the photomultiplier tube. We present the analytical model which is the basis of our calibration methodology, and outline how the empirical coefficients in this approach were determined. We also describe the complications peculiar to the Spectroscopy Detectors, and how our understanding of the detectors' operation led us to a solution to these problems.
    Type of Medium: Electronic Resource
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  • 4
    ISSN: 1432-1335
    Keywords: Multidrug resistance ; Reversibility ; Cyclosporin A ; Verapamil ; Dexniguldipine
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Abstract Multidrug-resistant tumor cells can be resensitized by combined application of the selecting cytostatic drug and a chemosensitizer, such as cyclosporin A (CsA) or a calcium channel blocker. Since clinical trials on the circumvention of multidrug resistance (MDR) with chemosensitizers report disparate results, we investigated whether tumor cells of the MDR phenotype can develop additional resistance to the cytostatic chemosensitizer combination. Thus, the Adriamycin(ADR)-selected, P-glycoprotein-positive MDR Friend leukemia cell line F4-6RADR was exposed to stepwise increased concentrations of CsA at a constant level of 0.05 μg/ml ADR. The initial CsA concentration (plus 0.05 μg/ml ADR) to inhibit cell growth of F4-6RADR cells by 50% (IC50) was 0.04 μg/ml. By continuous incubation for more than 6 months, the IC50 for CsA (at constant ADR) was elevated to 3.6 μg/ml (90-fold), thus generating the variant F4-6RADR-CsA. The F4-6RADR-CsA cells were cross-resistant for cyclosporin H (CsH), a non-immunosuppressive derivative of CsA. As shown by immunocytochemistry as well as by the polymerase chain reaction and by Western blotting including densitometry, P-glycoprotein was preserved in the F4-6RADR-CsA variant and was expressed at a 4-fold higher level than in F4-6RADR cells. Sodium dodecyl sulfate/polyacrylamide gel electrophoresis analysis could detect no new proteins in F4-6RADR-CsA as compared to F4-6RADR. Interestingly, resistance of F4-6RADR-CsA cells remained reversible for the calcium antagonists verapamil and dihydropyridine B859-35 (dexniguldipine-HCl), indicating that CsA and these compounds interfere with the P glycoprotein function by different pharmacodynamic mechanisms. Transport studies with [14C]ADR, performed in the presence and absence of chemosensitizers, confirmed the good correlation of P-glycoprotein function with the pattern of resistance found in proliferation assays. Cellular accumulation of [3H]cyclosporin was reduced to 71% of that of the F4-6 controls in F4-6RADR-CsA cells, but remained at the level of controls in F4-6RADR cells. Results indicate that increased amounts of the P-glycoprotein — besides other, perhaps more important mechanisms that are as yet unknown — partially mediate CsA resistance in F4-6RADR-CsA cells. We have designated this new form of resistance “secondary combined resistance” (SCR). The results suggest that at least some clinical cases of insensitivity to chemosensitizers or of relapse after reversing therapy could be explained by SCR, and that resensitizing treatment of tumor patients should be based on the consideration of several chemosensitizers of different pharmacodynamics.
    Type of Medium: Electronic Resource
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