17 research outputs found

    Coordinate Space HFB Calculations for the Zirconium Isotope Chain up to the Two-Neutron Dripline

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    We solve the Hartree-Fock-Bogoliubov (HFB) equations for deformed, axially symmetric even-even nuclei in coordinate space on a 2-D lattice utilizing the Basis-Spline expansion method. Results are presented for the neutron-rich zirconium isotopes up to the two-neutron dripline. In particular, we calculate binding energies, two-neutron separation energies, normal densities and pairing densities, mean square radii, quadrupole moments, and pairing gaps. Very large prolate quadrupole deformations (beta2=0.42,0.43,0.47) are found for the (102,104,112)Zr isotopes, in agreement with recent experimental data. We compare 2-D Basis-Spline lattice results with the results from a 2-D HFB code which uses a transformed harmonic oscillator basis.Comment: 9 pages, 9 figure

    Signal-to-signal-to-noise ratio of full-field Fourier domain optical coherence tomography: experiment

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    We report a new approach in optical coherence tomography (OCT) termed full-field Fourier-domain OCT (3F-OCT). A three-dimensional image of a sample is obtained by digital reconstruction of a three-dimensional data cube, acquired using a Fourier holography recording system illuminated with a swept-source. This paper presents theoretical and experimental study of the signal-to-noise ratio of the full-field approach versus serial image acquisition approach, represented by 3F-OCT and "flying-spot" OCT systems, respectively

    Dialysis-assisted fiber optic spectroscopy for in situ biomedical sensing

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    A miniature fiber optic spectrometer enclosed within a semipermeable (dialysis) membrane is proposed for in vivo interstitial sensing applications. The semipermeable membrane acts as a molecular filter, allowing only small molecules to pass through to the sampling volume. This filtering, in principle, should enable continuous in vivo drug sensing, removing the necessity for complex microdialysis systems. We use a biological phantom to examine the reliable detection of a fluorescence signal from small dye molecules in the presence of large fluorophores and scatterers. We find that spectral artefacts arising from scatterers and large fluorophores are substantially suppressed, simplifying the spectral analysis. In addition, the measured sampling rate of 157 s is superior to existing in vivo tissue assaying techniques such as microdialysis, which can take tens of minutes. (c) 2006 Society of Photo- Optical Instrumentation Engineers

    Optical scatter imaging using digital Fourier microscopy

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    An approach reported recently by Alexandrov et al (2005 Int. J Imag. Syst. Technol. 14 253-8) on optical scatter imaging, termed digital Fourier microscopy (DFM), represents an adaptation of digital Fourier holography to selective imaging of biological matter. The holographic mode of the recording of the sample optical scatter enables reconstruction of the sample image. The form-factor of the sample constituents provides a basis for discrimination of these constituents implemented via flexible digital Fourier filtering at the post-processing stage. As in dark-field microscopy, the DFM image contrast appears to improve due to the suppressed optical scatter from extended sample structures. In this paper, we present the theoretical and experimental study of DFM using a biological phantom that contains polymorphic scatterers
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