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31.
The notion that elementary systems correspond to irreducible representations of the Poincaré group is the starting point for this paper, which then goes on to discuss how a semigroup for the time evolution of unstable states and resonances could emerge from the underlying Poincaré symmetry. Important tools in this analysis are the Clebsch-Gordan coefficients for the Poincaré group.  相似文献   
32.
Photomechanical actuation is demonstrated in two coupled liquid crystal elastomer photomechanical optical devices (PODs) acting in series. The response function of an individual POD is characterized and used to predict the temporal response of the coupled system. The predicted coupled-system response agrees with the experiment for several waveforms and frequencies, suggesting that large-scale integration of photomechanical devices is possible.  相似文献   
33.
34.
The conditions during light emission from the fracture of solids have been difficult to determine because such mechanoluminescence (ML) is usually weak. When ML is produced by acoustic cavitation of a liquid slurry of resorcinol crystals, however, we observe bright light emission, which makes it possible to measure plasma conditions by emission spectra: a bimodal heavy atom emission temperature profile is observed with 405+/-22 K (for 80% of emitting CH) and 4015+/-730 K (for 20%), with an electron density and energy of 1.3+/-0.13x10;{14} cm;{-3} and approximately 3.5 eV (i.e., an effective T_{e} approximately 41 000 K).  相似文献   
35.
Partial volume effects are often experienced in diffusion-weighted MRI of biologic tissue. This is when the signal attenuation reflects a mixture of diffusion processes, originating from different tissue compartments, residing in the same voxel. Decomposing the mixture requires elaborated models that account for multiple compartments, yet the fitting problem for those models is usually ill posed. We suggest a novel approach for stabilizing the fitting problem of the multiple-tensors model by a variational framework that adds biologically oriented assumption of neighborhood alignments. The framework is designed to address fiber ambiguity caused by a number of neuronal fiber compartments residing in the same voxel. The method requires diffusion data acquired by common, clinically feasible MRI sequences, and is able to derive familiar tensor quantities for each compartment. Neighborhood alignment is performed by adding piece-wise smooth regularization constraints to an energy function. Minimization with the gradient descent method produces a set of diffusion-reaction partial differential equations that describe a tensor-preserving flow towards a best approximation of the data while maintaining the constraints. We analyze fiber compartment separation capabilities on a synthetic model of crossing fibers and on brain areas known to have crossing fibers. We compare the results with diffusion tensor imaging analysis and discuss applications for the framework.  相似文献   
36.
37.
The SOLEIL synchrotron radiation source is regularly operated in special filling modes dedicated to pump–probe experiments. Among others, the low‐α mode operation is characterized by shorter pulse duration and represents the natural bridge between 50 ps synchrotron pulses and femtosecond experiments. Here, the capabilities in low‐α mode of the experimental set‐ups developed at the TEMPO beamline to perform pump–probe experiments with soft X‐rays based on photoelectron or photon detection are presented. A 282 kHz repetition‐rate femtosecond laser is synchronized with the synchrotron radiation time structure to induce fast electronic and/or magnetic excitations. Detection is performed using a two‐dimensional space resolution plus time resolution detector based on microchannel plates equipped with a delay line. Results of time‐resolved photoelectron spectroscopy, circular dichroism and magnetic scattering experiments are reported, and their respective advantages and limitations in the framework of high‐time‐resolution pump–probe experiments compared and discussed.  相似文献   
38.
The temperature dependence of the features which arise from the 7F0,15D3 absorption transitions in EuOCl as seen by diffuse-reflectance spectroscopy has been investigated. The transitions shift linearly to higher energy with increasing temperature. The ratio of the intensities of the transitions arising from the 7F0 state to those arising from the 7F1 state also appears to be a linear function of temperature.  相似文献   
39.
Abstract

Salts of the [Eu(2,6-pyridinedicarboxylate)3]3- complex anion and various monovalent inorganic and organic counterions (Li+, Na+, K+, Rb+, Cs+, NH4 +, and pyridinium+) have been synthesized and studied by emission spectroscopy. The Eu3+ ion emission spectra exhibited by these salts have been observed with high resolution (less than 1.0 cm?1) and at low temperature (77 K). The emission spectra of these compounds indicate that changing the attached counterion does not affect the site symmetry observed by the europium ion beyond slight distortions indicated by small shifts in the energies of the Eu3+ electronic levels.  相似文献   
40.
Stromal cell-derived factor 1α (SDF-1α) or CXCL12 is a small pro-inflammatory chemoattractant cytokine and a substrate of dipeptidyl peptidase IV (DPP-IV). Proteolytic cleavage by DPP-IV inactivates SDF-1α and attenuates its interaction with CXCR4, its cell surface receptor. To enable investigation of suppression of such inactivation with pharmacologic inhibition of DPP-IV, we developed quantitative mass spectrometric methods that differentiate intact SDF-1α from its inactive form. Using top-down strategy in quantification, we demonstrated the unique advantage of keeping SDF-1α’s two disulfide bridges intact in the analysis. To achieve the optimal sensitivity required for quantification of intact and truncated SDF-1α at endogenous levels in blood, we coupled nano-flow tandem mass spectrometry with antibody-based affinity enrichment. The assay has a quantitative range of 20 pmol/L to 20 nmol/L in human plasma as well as in rhesus monkey plasma. With only slight modification, the same assay can be used to quantify SDF-1α in mice. Using two in vivo animal studies as examples, we demonstrated that it was critical to differentiate intact SDF-1α from its truncated form in the analysis of biomarkers for pharmacologic inhibition of DPP-IV activity. These novel methods enable translational research on suppression of SDF-1 inactivation with DPP-IV inhibition and can be applied to relevant clinical samples in the future to yield new insights on change of SDF-1α levels in disease settings and in response to therapeutic interventions.
Figure
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